Acetylcholine (ACh) is the key neurotransmitter involved in cholinergic neurotransmission, which is vital for various cognitive functions, including memory formation and consolidation (Hasselmo, 2006). During learning, cholinergic neurons release ACh to promote the encoding of new memories (Palacios-Filardo and Mellor, 2019). Increased ACh levels in the hippocampus facilitate the consolidation of information into long-term memory (Haam and Yakel, 2017). Optimal levels of ACh in the prefrontal cortex help modulate attentional processes, allowing individuals to concentrate on relevant stimuli and filter out distractions. ACh modulates synaptic plasticity, the ability of synapses to undergo long-lasting changes in strength, through various mechanisms (Obermayer et al., 2017; Palacios-Filardo and Mellor, 2019; Picciotto et al., 2012). One way ACh influences synaptic plasticity is through modulation of Long-Term Potentiation (LTP) (Fernández De Sevilla et al., 2008; Kassab, 2023). LTP, a strengthening of synaptic connections, is a cellular process associated with learning and memory formation. ACh can enhance the induction and maintenance of LTP in certain brain regions. Activation of muscarinic receptors, specifically the M1 subtype, by ACh facilitates the generation of LTP (Dennis et al., 2016). ACh release during learning promotes synaptic strengthening and consolidation of memories. Another form of plasticity, Long-Term Depression (LTD), is also modulated by Ach (Sumi and Harada, 2023). LTD involves the weakening of synaptic connections. ACh can influence LTD in diverse ways depending on the brain region and receptor subtypes involved (Dickinson et al., 2009; Jo et al., 2010; Scheiderer et al., 2006; Volk et al., 2007). In addition, ACh can directly affect the strength of synaptic transmission through its action on presynaptic and postsynaptic receptors (Exley and Cragg, 2008). Activation of presynaptic nicotinic receptors by ACh can enhance neurotransmitter release (Exley and Cragg, 2008; Zhong et al., 2014), leading to an increase in synaptic strength. Postsynaptic nicotinic and muscarinic receptor activation can modulate the excitability of postsynaptic neurons (Chung et al., 2016) influencing the integration of synaptic inputs and the generation of action potentials (Figure 2; Hedrick and Waters, 2015; Ge and Dani, 2005). ACh also modulates the expression of molecules involved in signal transduction pathways associated with synaptic plasticity (Świt et al., 2023) such as protein kinases and phosphatases (Halder and Lal, 2021; Jouvenceau et al., 2006; Peters et al., 2003). Finally, interactions of ACh with other neurotransmitter systems, such as glutamate and dopamine, also modulate synaptic plasticity (Del Arco and Mora, 2005; Suzuki et al., 2001; Xiao et al., 2020). It can influence the release and effects of these neurotransmitters, further shaping synaptic plasticity processes and behaviors (Donovan et al., 2022; Lester et al., 2010). These interactions contribute to the complex regulation of synaptic strength and plasticity in multiple brain regions. Collectively, the duration and magnitude of ACh transients greatly shape the activity of neural networks. Therefore, cholinergic neurons that are abundant in the basal forebrain and hippocampus are involved in learning, memory, attention, and other cognitive processes. This enables cholinesterases (ChE) to modulate in cognition and memory processes in the brain (Lane et al., 2006). These enzymes, which include acetylcholinesterase (AChE) and butyrylcholinesterase (BuChE), are responsible for breaking down ACh in the synaptic cleft (Kandiah et al., 2017). In AD, there is a progressive loss of cholinergic neurons, leading to a reduction in acetylcholine levels in critical brain regions such as the basal forebrain and nucleus basalis of Meynert (Hampel et al., 2018). The degeneration and loss of cholinergic neurons in the AD brain lead to a substantial reduction in the production and release of ACh. Hence, therapeutic approaches targeting the cholinergic system, such as cholinesterase inhibitors (ChEI) (Rozzini et al., 2007) aim to alleviate the cognitive symptoms in AD by increasing acetylcholine levels and enhancing cholinergic neurotransmission (Anand and Singh, 2013; Hampel et al., 2018). Although these treatments do not halt or reverse the underlying cholinergic neuron degeneration, the augmentation of acetylcholine levels improves cognitive processes such as memory, attention, and learning in individuals with AD (Li et al., 2015).

β-secretase, in particular the β-site amyloid precursor protein cleaving enzyme 1 (BACE-1), contributes to the development of AD (Figure 3; Kandalepas and Vassar, 2012). It is primarily involved in the production of Aβ peptides, which are key components of the amyloid plaques developed in the brains of individuals with AD (Masters et al., 1985; Neumann et al., 2018). BACE-1 is responsible for cleaving the amyloid precursor protein (APP) at the β-site, leading to the generation of soluble fragments called β-CTF (C-terminal fragment) (Hunt and Turner, 2009). Subsequently, γ-secretase cleaves β-CTF to produce Aβ peptides of varying lengths, including the toxic Aβ42 form (Hur, 2022). The accumulation of Aβ42 peptides, also known as Aβ aggregates or amyloid aggregates, is believed to be a critical step in the development of amyloid plaques (clumps or deposits of Aβ peptides), a hallmark pathological feature of AD. Aβ peptides tend to misfold and aggregate, leading to the formation of insoluble protein deposits (Frisoni et al., 2022). The specific Aβ peptide involved in aggregation is Aβ42, which has a greater propensity to form aggregates compared to Aβ40. These aggregates take on different forms, including soluble oligomers, protofibrils, and fibrils (Zhang et al., 2011). The most well-known and visible form of Aβ aggregates in AD is the formation of amyloid plaques (Holsinger et al., 2013). These plaques consist of dense accumulations of Aβ fibrils that are insoluble and resistant to degradation. They are typically found in the spaces between neurons in the brain, disrupting normal neuronal functions (Siwecka et al., 2023). Aβ aggregates can also exist in smaller, soluble oligomeric forms. These oligomers are considered to be highly toxic to neurons and are thought to contribute to synaptic dysfunction and neuronal damage. Hence, Aβ oligomers are believed to have a greater impact on cognitive impairment than the fibrillar plaques themselves. Aβ aggregates can interact with and influence the aggregation of tau protein, another key pathological feature of AD. The tau protein stabilizes microtubules in neurons, and its abnormal aggregation leads to the formation of neurofibrillary tangles (Naseri et al., 2019). Aβ aggregates have been found to promote tau aggregation and contribute to neurodegeneration. Aβ aggregates, including both plaques and oligomers, are therefore associated with neurotoxic effects in AD (Lane et al., 2018). The presence of Aβ aggregates, particularly amyloid plaques, is often used as a biomarker for AD diagnosis. Imaging techniques such as positron emission tomography (PET) can detect the accumulation of Aβ plaques in the brain, helping to differentiate AD from other forms of dementia (Thijssen et al., 2021). Therefore, Aβ aggregate inhibitors aim to prevent the formation, promote the disaggregation, or enhance the clearance of such Aβ aggregates in AD (Weller and Budson, 2018). Monoclonal antibodies that specifically bind to Aβ aggregates have been developed to target and clear Aβ aggregates from the brain (Avgerinos et al., 2021). Examples include aducanumab, which has recently been approved by the U.S. Food and Drug Administration (FDA), and solanezumab and gantenerumab, which are currently being evaluated in clinical trials. These antibodies can potentially facilitate the removal of Aβ aggregates through immune-mediated mechanisms or by enhancing their clearance by microglial cells (Shi et al., 2022). There has also been the implication of metals (copper, zinc, and iron) in promoting Aβ aggregation and neurotoxicity (Das et al., 2021). Metal chelators can bind to these metals and prevent their interaction with Aβ, thereby inhibiting or disrupting the aggregation process (Liu et al., 2019). Some examples of metal chelators include clioquinol and PBT2, which have been investigated in preclinical and clinical studi (Lei et al., 2021) Here in this article, we will focus on small molecule anti-aggregation compounds.

Studies have shown that BACE-1 is elevated in the AD brains (Singh et al., 2022; Zhao et al., 2007) This increased activity leads to higher production of Aβ peptides, particularly Aβ42, which have a greater propensity to aggregate and form plaques (Sadleir et al., 2016) The overproduction and deposition of Aβ peptides contribute to neurotoxicity and the progression of AD pathology. Mutations in the genes involved in APP processing represent a risk factor for early-onset AD (Armstrong, 2019). One important causative factor in this regard is Presenilin-1 (PSEN1), which is part of the γ-secretase pathway (Bagaria et al., 2022). Over 300 PSEN1 mutations have been identified (Yang et al., 2023) and thus their contribution toward pathogenesis in rare cases of familial AD (FAD) and early-onset AD are areas of active investigation (Wijeratne et al., 2023). One prominent mutation associated with FAD is the Swedish mutation (also known as the APP670/671 mutation) (Hellström-Lindahl et al., 2009). This mutation alters the BACE-1 cleavage site in the APP gene, resulting in increased production of Aβ peptides. The Swedish mutation has been extensively studied and has provided valuable insights into the role of BACE-1 in AD pathogenesis. Several other BACE-1 mutations have been identified in FAD cases. These mutations lead to increased BACE-1 activity or alter the enzyme’s processing and trafficking. Each mutation may have a specific effect on BACE-1 function, resulting in varied consequences for Aβ production and AD pathology (Bagaria et al., 2022). Collectively, BACE-1 has emerged as a promising therapeutic target for AD (Figure 3). Inhibiting BACE-1 activity could potentially reduce the production of Aβ peptides and slow down the progression of the disease. Researchers have been actively working on developing BACE-1 inhibitors as a potential treatment strategy. However, clinical trials investigating BACE-1 inhibitors have faced challenges, including safety concerns and limited efficacy, underscoring the complexity of targeting this enzyme in AD (Bazzari and Bazzari, 2022; Munj and Patil, 2022; Vassar et al., 1999). For instance, an aspect of BACE-1 inhibitors is selectivity for BACE-1 over other related enzymes. While BACE-1 is the primary enzyme responsible for β-secretase activity, other enzymes, such as BACE-2, share some similarities in structure and function. The selectivity of BACE-1 inhibitors helps minimize potential off-target effects by specifically targeting BACE-1 without interfering with the physiological functions of other related enzymes. While reducing BACE-1 activity may reduce Aβ production and hence AD pathology, it is important to consider the physiological functions of BACE-1. BACE-1 is involved in the processing of other substrates besides APP, and complete inhibition may have unintended consequences. Balancing the reduction of Aβ production with the preservation of normal BACE-1 functions remains a focus of ongoing research.

Other biochemical assays are employed for more benchmark determining factors related to AD, foremost: BACE-1 activity, the protease which cleaves APP that can form insoluble protein deposits. To detect this activity, an assay was created featuring a genetically modified proenzyme with activity dependence on BACE-1 (Verheijen et al., 2006). Once active, the enzyme can be measured at a sensitive threshold. This assay not only displays utility in detecting elevated BACE-1 activity in brain tissue but may also be useful in screening for potential drug therapies (Verheijen et al., 2006).

Glutamine cyclase, also known as glutaminyl cyclase (QC), is an enzyme involved in the post-translational modification of certain peptides and proteins (Schilling et al., 2007). QC’s primary function is to catalyze the cyclization of N-terminal glutamine residues to form pyroglutamate (pGlu) (Fischer and Spiess, 1987). This enzymatic reaction is known as pyroglutamate formation or N-terminal cyclization. The process of pyroglutamate formation involves the removal of the free N-terminal glutamine or glutamate residue and subsequent cyclization of the resulting N-terminal glutaminyl or glutamyl residue. QC catalyzes the cyclization reaction by breaking the peptide bond between the N-terminal glutamine and the adjacent amino acid and then forming a cyclic amide bond, resulting in the formation of pyroglutamate (Coimbra et al., 2023). Pyroglutamate formation plays a role in protein stability and activity, which affects downstream functions and signalling of these molecules. Pyroglutamate formation is known to occur in a variety of peptide hormones, neuropeptides, and other bioactive peptides. Notably, the formation of pyroglutamate-modified Aβ peptides (Bsamen et al., 2018; Cynis et al., 2008) has been observed in the brains of individuals with AD (Figure 3). Although such pyroglutamate-modified Aβ peptides represent a small fraction of total Aβ, they are nonetheless thought to be highly toxic due to resistance to aminopeptidase degradation and ability to provide a seed for amyloid fibril formation (Hook et al., 2014; Nussbaum et al., 2012). Moreover, there are also reports of enhanced QC activity in the brains of people with AD (Gunn et al., 2021). Thus, these modified peptides have been suggested to contribute to the neurodegenerative processes and cognitive decline observed in the disease (Camargo et al., 2021; Jawhar et al., 2011; Wittnam et al., 2012). Inhibiting glutamine cyclase activity has been explored as a potential therapeutic strategy for certain diseases (Huang et al., 2011). For instance, in the context of Alzheimer’s disease, inhibiting glutamine cyclase could prevent the formation of pyroglutamate-modified Aβ peptides (Bayer, 2022), which are known to be more aggregation-prone and toxic than their unmodified counterparts. Several small molecules have been developed as glutamine cyclase inhibitors, and research in this area is ongoing (Hoang et al., 2017). Overall, glutamine cyclase is an important enzyme involved in the post-translational modification of peptides and proteins through the formation of pyroglutamate. Understanding its role and regulation may have implications for the development of therapies targeting specific diseases, including neurodegenerative disorders.

The upregulation of glutaminyl cyclase (QC) activity is strongly linked to the progression of AD; thus, QC inhibitors are a topic of interest for disease treatment. Several studies show evidence of QC inhibitors being biologically active and able to promote treatment. One, in particular, focused on QC inhibitor 23 in PC12 cells, which exhibited upregulation of heat shock proteins 70 and 90, along with the regulation of many other biochemical components related to AD pathology, such as actin gene expression. These results were analyzed with the use of biological assays such as Western blot and ELISA, along with quantitative real-time PCR (Yu et al., 2019).

Histone deacetylase (HDAC) enzymes are important players in regulating gene expression, most notably in epigenetic regulation, with particular relevance to cognitive processes (Figure 2; Saha and Pahan, 2006; Cho and Cavalli, 2014). HDACs are responsible for removing acetyl groups from histone proteins, leading to chromatin compaction and transcriptional repression (Bhansali et al., 2011; 2014; Seto and Yoshida, 2014). This process, known as histone deacetylation, can impact the expression of genes involved in synaptic plasticity, learning, and memory formation (Latcheva et al., 2019). By altering histone acetylation patterns, HDACs modulate the transcription of genes critical for cognitive function. For instance, HDACs influence synaptic plasticity by regulating the expression of genes involved in synaptic remodeling and strengthening, such as neurotrophins, synaptic proteins, and neurotransmitter receptors (Ahmad Ganai et al., 2016). In particular, HDAC activity has been found to influence synaptic plasticity and memory formation. HDACs also play a role in neurogenesis, the generation of new neurons, in the adult brain (Guan et al., 2009; Nieto-Estevez et al., 2022). It was long believed that neurogenesis only occurred during development and early stages of life, but it has now been established that neurogenesis also takes place in specific regions of the adult brain, including the hippocampus (Cuccioli et al., 2015; Kempermann et al., 2015). Deficits in adult hippocampal neurogenesis have been observed in various neurological and psychiatric disorders, including AD. Inhibiting HDAC activity has been associated with increased neurogenesis which considered to be is a neuroprotective process (Shukla and Tekwani, 2020) suggesting a potential role in cognitive enhancement. By regulating gene expression, HDACs influence the expression of genes involved in neuronal survival, antioxidant defence, stress response, and chronic pain (Descalzi et al., 2015; Falkenberg and Johnstone, 2014). Given the involvement of HDACs in cognitive processes, HDAC inhibitors have emerged as potential therapeutic agents for cognitive disorders (Hamze, 2020; Melesina et al., 2021; Thomas et al., 2008). In preclinical studies, HDAC inhibitors have shown promising effects in enhancing synaptic plasticity, promoting memory formation, and ameliorating cognitive deficits. However, it is important to note that further research is needed to fully understand the specific roles of individual HDAC isoforms and to develop selective inhibitors with minimal side effects (Santana et al., 2023).

Finally, immunoprecipitation assays are also useful in quantifying disease components, such as tau protein aggregates, known to cause neurofibrillary tangles^. which are detrimental to brain function. Here, a natural alkaloid, protopine, found in plants that may exert certain biological activities, was employed for the purpose of reducing tau protein aggregate formation for memory improvement. Immunoprecipitation assays were used to study the effects of the drug’s influence on the ubiquitination of pathological tau. Fluorometric assays were useful in assessing how protopine also appears to promote the acetylation of α-tubulin, suggesting that it serves as an HDAC inhibitor (Sreenivasmurthy et al., 2022). which strongly influences neurogenerative diseases’ pathology (Sanchez and Blower, 1997).

The regulation of BACE-1 activity by the cyclic adenosine monophosphate (cAMP) dependent signalling pathway is an emerging topic of interest in AD research (Thathiah and De Strooper, 2011). The cAMP pathway can influence BACE-1 expression at the transcriptional level (Zhao et al., 2016). Activation of stimulatory G protein-coupled receptors (GPCRs) by their ligands, such as neurotransmitters or hormones, leads to the activation of adenylyl cyclase and subsequent production of neuronal cAMP (Figure 4; Cooper, 2003; Muntean et al., 2018) Increased cAMP levels activate protein kinase A (PKA), which can phosphorylate and activate certain transcription factors, including CREB (cAMP response element-binding protein) (Kandel, 2012). Activated CREB can then bind to specific regions of the BACE-1 gene promoter and enhance its transcription, resulting in increased BACE-1 expression (Sambamurti et al., 2004). In addition to transcriptional regulation, the cAMP pathway can also modulate BACE-1 activity through post-translational mechanisms (Nowak et al., 2006; Tamagno et al., 2012). The cAMP pathway can influence the intracellular trafficking and subcellular localization of BACE-1. PKA-mediated phosphorylation of APP has been shown to affect its cellular distribution and trafficking, potentially altering its enzymatic activity and substrate accessibility (Marambaud et al., 1996). The cAMP pathway facilitates crosstalk with other signalling pathways that regulate BACE-1. For example, the cAMP pathway can interact with the Wnt/β-catenin signalling pathway, which has been implicated in AD pathogenesis. Activation of the Wnt/β-catenin pathway has been shown to regulate BACE-1 expression and Aβ production (Chen et al., 2019; Elliott et al., 2018). Understanding the regulation of BACE-1 by the cAMP pathway is important for elucidating the mechanisms underlying Aβ production in AD and for identifying potential therapeutic targets. Importantly, modulating the cAMP pathway or targeting specific GPCRs involved in its activation could be explored as a strategy to modulate BACE-1 expression and activity, ultimately reducing Aβ production in AD. However, it is worth noting that the cAMP pathway is complex and can have pleiotropic effects in different cell types and brain regions, so careful consideration of specificity and potential side effects is crucial in developing targeted interventions. Further research is needed to fully uncover the intricate regulatory mechanisms and their therapeutic implications in AD. Nonetheless, targeting GPCRs has emerged as a potential therapeutic strategy for AD. The cholinergic system, particularly the muscarinic acetylcholine receptors (mAChRs), has been a focus for GPCR-based therapies in AD (as noted above). The loss of cholinergic neurons and a decrease in acetylcholine levels are prominent features of AD. By targeting mAChRs, it is possible to modulate cholinergic neurotransmission and enhance cognitive function. Selective agonists of the M1 and M2 subtypes of mAChRs have been investigated for their potential in improving cognitive deficits in AD. (Brown et al., 2021; Sanjay et al., 2022) Activation of the M1 receptor subtype has shown cognition-enhancing effects by increasing synaptic plasticity, improving memory formation, and promoting neuroprotective mechanisms. M2 receptor activation can also have beneficial effects by modulating neurotransmitter release and reducing Aβ peptide production. Beyond the cholinergic system, other GPCRs have also been investigated as potential targets for AD therapy. For example, the metabotropic glutamate receptors (mGluRs) (Abd-Elrahman et al., 2021) particularly the mGluR5 subtype, have been targeted to modulate glutaminergic signalling and synaptic function (Kumar et al., 2015). Activation of certain serotonin receptors, such as 5-HT6 receptors, has also shown potential in improving cognitive impairments (Benhamú et al., 2014; Czarnota-Łydka et al., 2022; Mdawar et al., 2020). Given the complex nature of AD pathology, combination therapies targeting multiple GPCRs or GPCRs alongside other therapeutic approaches are being explored. Adenosine receptors, particular the A1 and A2A subtype, have recently emerged as putative neuronal GPCR targets in AD (Trinh et al., 2022). Given the role of the noradrenergic system in cognition (Borodovitsyna et al., 2017) and adjusted norepinephrine levels in AD brains (Mann et al., 1982) adrenergic dysfunction in AD represents additional putative GPCR targets (Gannon et al., 2015). The orphan receptors GPR3 and GPR6, of which the endogenous ligand has not yet been uncovered, are additional GPCRs that have gained traction in AD research. [127]. GPR3 overexpression enhances Aβ production while receptor depletion prevents Aβ (Huang et al., 2015; Ricardo and Lehmann, 2009). On the other hand, GPR6 is thought to facilitate neuroprotective effects in AD through the complement pathway (Huang et al., 2015; Ricardo and Lehmann, 2009). Combining treatments that target distinct aspects of the disease, such as Aβ production, neuroinflammation, and synaptic dysfunction, may offer synergistic effects and better therapeutic outcomes. It is important to note that while targeting GPCRs holds promise for AD treatment, the development of GPCR-based therapies is still in the early stages, and much more research is needed to validate their efficacy, safety, and long-term effects in clinical settings. Additionally, the heterogeneity of AD and the diverse functions of GPCRs require careful consideration of patient selection and personalized treatment approaches.

Monitoring cAMP dynamics offers critical insight toward signal transduction, and therefore information transfer, between neuronal circuits. Utilization of genetically encoded cAMP biosensors is beneficial to understanding signaling logistics in the native neuronal environment, as successfully employed in various models of neuronal pathology (Masuho et al., 2018; Muntean et al., 2019; 2021; Sutton et al., 2019). The approach is empowered by the cAMP Encoded Reporter (CAMPER) mouse model that conditionally expresses the FRET-based TEpacVV cAMP biosensor (Muntean et al., 2018). Microglia are of particular importance in the understanding or AD and therapeutic potential because microglial GPCRs are involved in the degradation of amyloid plaques (Haque et al., 2018). This interplay allows for a range of study approaches, especially in respect to neuromodulatory second messengers like cAMP.

Cholinesterases such as acetylcholinesterase (AChE) and butyrylcholinesterase (BuChE) are established drug targets for treatment of Alzheimer’s disease. Various approved drugs targeting cholinesterases, such as tacrine, rivastigmine, donepezil, and galantamine (Figure 5), are available, but these drugs have certain limitations.

Despite limitations, tacrine is an important scaffold for developing new potent anti-Alzheimer’s agents. Rosini et al. have designed and evaluated a new tacrine and a lipoic acid hybrid called lipocrine. Compound 1 showed good anti-cholinesterase activity. Compound 1 (N-(3-((6-chloro-1,2,3,4-tetrahydroacridin-9-yl)amino)propyl)-5-(1,2-dithiolan-3-yl) pentanamide), a chlorine-substituted tacrine, has three carbon containing chain between lipoic acid. It exhibited low nanomolar inhibitory activity against AChE (IC₅₀ = 0.253 ± 0.016 nM) and BuChE (10.8 ± 2.5 nM) in the Ellman’s assay. Lipocrine is one of the first compounds that inhibit AChE and AChE-induced Aβ aggregation and protects against oxidative radical species (Rosini et al., 2005).

Fang et al. synthesized and evaluated 14 NO-donor-tacrine hybrids having anti-Alzheimer’sAlz ‘s’activity. All of them exhibited promising cholinesterase inhibitory activity in-vitro. While compound 2 (2,2-dimethyl-3-oxo-3-((4-((1,2,3,4-tetrahydroacridin-9-yl)amino)butyl)amino) propyl nitrate) depicted high selectivity towards butyrylcholinesterase (IC₅₀ = 7.3 ± 2.0 nM) than acetylcholinesterase (IC₅₀ = 226.0 ± 91 nM) with a 31-fold selective ratio. Compound 2 binds more efficiently to BuChE than AChE due to the steric hindrance of the bulky alkylenediamine spacer. Hepatotoxicity associated with tacrine is the main concern of its prolonged use. In that regard, compound 3 (3-((4-((1,2,3,4-tetrahydroacridin-9-yl)amino)butyl)amino)propyl nitrate) exhibited good AChE inhibitory activity (IC₅₀ = 5.6 ± 0.7 nM) and was less hepatotoxic than tacrine (Fang et al., 2008).

Camps et al. designed, synthesized, and evaluated a series of dual-binding site AChE inhibitors. N-(8-((6-chloro-1,2,3,4-tetrahydroacridin-9-yl)amino)octyl)-3-(5-phenyl-3,4-dihydro-2H-pyrano [3,2-c]quinolin-9-yl)propenamide (4) demonstrates potent activity towards inhibition of AChE (IC₅₀ = 14 ± 1.2 nM). The newly discovered compounds comprise chlorotacrine connected to a pyrano [3,2-c]-quinoline structure through an oligomethylene linker and an amido group. They exhibited a dual binding effect, binding to the active site through tacrine and to a peripheral site through the pyrano [3,2-c]-quinoline moiety. Compound 4 crosses the blood-brain barrier and shows in-vitro inhibition of Aβ aggregation (Camps et al., 2009).

Oset-Gasque et al. developed a non-competitive inhibitor chromenotacrines 5 (11-amino-12-(3,4,5-trimethoxyphenyl)-7,9,10,12-tetrahydro-8H-chromeno [2,3-b]quinolin-3-ol), which is less toxic to human liver cells than tacrine. Compound 5 was identified as a potential AChE inhibitor (IC 50 = 0.041 ± 0.001 µM) binding to the peripheral anionic site. Compound 5 exhibited selective inhibition towards AChE, and kinetic studies revealed moderate brain permeability (Oset-Gasque et al., 2014).

Najafi et al. designed and evaluated new tacrine hybrids introducing triazine substitution at the amine group of tacrine. Compounds 6 (7-chloro-N-((1-(4-methoxybenzyl)-1H-1,2,3-triazol-4-yl)methyl)-1,2,3,4-tetrahydroacridin-9-amine) and 7 (N-((1-(4-methoxybenzyl)-1H-1,2,3-triazol-4-yl)methyl)-1,2,3,4-tetrahydroacridin-9-amine) illustrated anti-cholinesterase activity. Although both compounds 6 and 7 have 4-methoxyphenyl connected to a 1,2,3-triazole moiety, compound 6 with chlorine substitution at 7-position of acridine ring displayed the best AChE inhibitory activity (IC₅₀ = 0.521 ± 0.025 µM), and compound 7 indicated activity against BuChE (IC₅₀ = 0.055 ± 0.012 µM). This reveals that these small structural changes lead to changes in the preferential binding pattern of the enzyme. The compounds were evaluated for neuroprotection and radical scavenging ability. Compound 6 showed moderate neuroprotective activity at 10 mM (cell viability = 65.40% and P < 0.05 vs. H₂O₂ treatment alone), and both compounds 6 and 7 indicated no notable antioxidant activities. Tacrine-1,2,3-triazole hybrids are considered potential agents with anti-cholinesterase activity (Najafi et al., 2017).

Spilovska et al. developed 7-methoxy derivatives, 9-amino-7-methoxy-1,2,3,4-tetrahydro acridine (7-MEOTA) linked with urea and thiourea and amantadine, found less hepatotoxic compared to tacrine. 1-(Adamantan-1-yl)-3-(2-((7-methoxy-1,2,3,4-tetrahydroacridin-9-yl) amino)pentyl)thiourea (8) linked with thiourea from this series showed potent hAChE (IC₅₀ = 0.47 ± 0.09 µM) and BuChE (IC₅₀ = 0.11 ± 0.02 µM) inhibitory activity (Spilovska et al., 2015).

Chand et al. designed tacrine conjugates with hydroxyl benzyl-pyridone (TAC-HBP), showing dual binding at both the catalytic active site (CAS) and peripheral anionic site (PAS) of cholinesterase. 5-(2,4-Dihydroxybenzoyl)-1-(4-((1,2,3,4-tetrahydroacridin-9-yl)amino)butyl) pyridin-2(1H)-one (9) showed promising inhibitory activity against AChE (IC₅₀ = 0.521 ± 0.025 µM). Also, this compound had radical scavenging activity comparable with tacrine (Chand et al., 2016).

Hepnarova et al. designed novel tacrine-benzyl quinolone carboxylic acid (tacrine-BQCA) hybrids with the rationale that tacrine moiety would be responsible for AChE inhibition and BQCA have M1 receptor antagonist properties. N-(3-((6-chloro-1,2,3,4-tetrahydroacridin-9-yl)amino)propyl)-1-(4-methoxybenzyl)-4-oxo-1,4-dihydroquinoline-3-carboxamide 10 indicated a non-selective cholinesterase inhibition profile (IC₅₀ = 0.0745 ± 0.0031 μM) with an affinity towards the M1 receptor and moderate brain permeability (Hepnarova et al., 2018).

Ebrahimi et al. designed a new series of hetero-annulated chromene-fused coumarins against cholinesterase. 7-(3-Hydroxyphenyl)-10,10-dimethyl-7,9,10,11-tetrahydro-6H,8H-chromeno [4,3-b]chromene-6,8-dione (11) having 3-hydroxyphenyl moiety showed the highest inhibitory activity against AChE (IC₅₀ = 3.28 µM) and BuChE (IC₅₀ = 2.19 µM).

Researchers modulated selectivity for AChE and BuChE by introducing substitution at the 3-hydroxyphenyl group. The docking studies with AChE enzyme complexed with donepezil revealed that the coumarin ring was involved in π-π stacking with Trp279 and hydrogen bond with the hydroxyl group, that enabled tight binding with a receptor (Ebrahimi et al., 2016).

Suwanhom et al. similarly studied carboxamide derivatives and designed chromon-2-carboxamido alkylamines. 7-Methoxy-4-oxo-N-(3-(piperidin-1-yl)propyl)-4H-chromene-2-carboxamide (12) displayed a potent AChE inhibitory activity (IC₅₀ = 0.09 ± 0.02 μM) than tacrine (IC₅₀ = 0.13 ± 0.02 μM). The enzyme kinetics revealed that compound 12 is an uncompetitive inhibitor, and the docking study speculated the compound as a dual-binding inhibitor. Also, the cytotoxic effect was less, and the neuroprotective effect was more (Suwanhom et al., 2020).

Singh et al. designed a novel class of 2-phenyl-4H-chromene-4-one derivatives as AChE inhibitors. 2-(4-Fluorophenyl)-7-hydroxy-4H-chromen-4-one (13) showed higher inhibitory activity (IC₅₀ = 8.0 ± 0.37 µM) than donepezil (IC₅₀ = 12.7 nM). The derivatives also exhibited the ability to inhibit advanced glycation end products with additional radical scavenging activity. Docking of compound 13 revealed good binding affinity at CAS and PAS of the enzyme active site (Singh M. et al., 2018).

Macha et al. designed and synthesized tetrahydro-9H-benzo [5,6]chromeno [2,6-b]quinoline-13(14H)-one derivative against AChE and BuChE. The most potent inhibitory activity was shown by 15-(3,4-dihydroxyphenyl)-10,11,12,13,13a,15-hexahydrobenzo [5,6]chromeno [2,3-b]cyclohepta [e]pyridin-14(9H)-one (14) bearing 3,4-dihydroxy phenyl group at 15th position of hexahydrobenzo [5,6]chromeno [2,3-b]cyclohepta [e]pyridine-14(15H)-one scaffold against AChE (IC₅₀ = 0.65 ± 0.06 μM) and BuChE (IC₅₀ = 1.32 ± 0.06 μM). Compound 14 was safe with no hepatotoxicity and was equally active in behavioral studies Y maze, rectangle maze, and jumping box test compared to tacrine. A docking study revealed that the designed compounds bind well within the enzyme’s active site (Machaa et al., 2021).

Zhang et al. developed a series of novel cholinesterase inhibitors by hybridizing coumarin and piperazine pharmacophores. 3-(4-(naphthalen-1-ylmethyl)piperazine-1-carbonyl)-2H-chromen-2-one (15) was identified as a potent inhibitor against hAChE (IC₅₀ = 8.78 ± 0.22 μM), docking study revealed that hybrids target both CAS and PAS of hAChE, also showed no cytotoxicity against neuroblastoma cells (Zhang and Jiang, 2018).

Hu et al. designed 3–(4-aminophenyl)-coumarins for AD treatment, 27 compounds were evaluated for anti-Alzheimer’s activity, and a behavioral inhibition study was performed on a model of zebrafish juveniles. 4-(Chloromethyl)-N-(4-(8-methoxy-2-oxo-2H-chromen-3-yl)phenyl)benzamide (16) exhibited the highest activity against AChE (IC₅₀ = 0.091 ± 0.011 μM) but was slightly weaker than donepezil (IC₅₀ = 0.012 ± 0.001 μM), and BuChE inhibitory activity (IC₅₀ = 0.559 ± 0.017 μM) was more significant than donepezil (IC₅₀ = 2.665 ± 0.015 μM) (Hu et al., 2019).

Tehrani et al. developed coumarin-3-carboxamide-N-morpholine hybrids as cholinesterase inhibitors. Among these compounds, propyl morpholine derivative N-(3-morpholinopropyl)-2-oxo-2H-chromene-3-carboxamide (17) with unsubstituted coumarin moiety depicted the highest AChE inhibitory activity (IC₅₀ = 6.21 ± 0.03 μM). Docking and kinetic studies revealed the dual binding ability of compound 17 (Tehrani et al., 2019).

Kara et al. reported coumarin-based compounds as novel inhibitors of cholinesterase, and 2-(2-oxo-2H-chromen-4-yl) acetamide were identified as potent AChE inhibitors. Among the compounds in the series, N-(2-(4-benzylpiperazin-1-yl)ethyl)-2-(7-hydroxy-8-methyl-2-oxo-2H-chromen-4-yl)acetamide (18) depicted a good pharmacokinetic profile and high activity against both huAChE (IC₅₀ = 0.04 ± 0.01 μM) and BuChE (IC₅₀ = 0.68 ± 0.07 μM) than donepezil huAChE (IC₅₀ = 0.004 ± 0.0001 μM) and BuChE (IC₅₀ = 1.90 ± 0.02 μM). The docking study showed good interaction with the enzyme’s active site, and no hepatotoxicity was observed (Kara et al., 2019).

In another captivating research, Mollazadeh et al. synthesized 2,4-dioxochroman-N-phenyl pyridinium acetamide and evaluated for its AChE and BuChE inhibitory activities. (Z)-1-(2-((3,4-dichlorophenyl)amino)-2-oxoethyl)-3-((((2,4-dioxochroman-3-ylidene)methyl)amino) methyl)pyridin-1-ium chloride (19) was identified as a potent inhibitor for BuChE (IC₅₀ = 3.66 ± 0.11 μM) and also showed good inhibition against AChE (IC₅₀ = 10.30 ± 1.05 μM) compared with the standard drug donepezil. Docking and molecular dynamic studies confirmed that compound 19 interacted with the critical residues of the enzyme’s active site. Also, the in-vitro and in silico toxicity assays demonstrated the active compound to be non-toxic (Mollazadeh et al., 2020).

Lee et al. synthesized alkyl-substituted aurone derivative (Z)-2-(3,4-dimethoxybenzylidene)-6-(2-(piperidin-1-yl)ethoxy)benzofuran-3(2H)-one (20) using sulfuretin as a hit molecule. Researchers compared its potency with sulfuretin and galantamine, which have AChE inhibitory activity. Compound 20 displayed good inhibitory activity against AChE (IC₅₀ = 0.40 ± 0.03 µM), was ca. 1700-fold higher than sulfuretin (IC₅₀ = 698.9 μM) and ca. 6-fold higher than galantamine (IC₅₀ = 2.50 μM) (Lee et al., 2015).

Shaikh et al. synthesized seventeen flavones-8-acrylamides and evaluated them for anti-Alzheimer activity. (E)-2-Cyano-N-cyclohexyl-3-(7-methoxy-4-oxo-2-phenyl-4H-chromen-8-yl)acrylamide (21) demonstrated higher selectivity (IC₅₀ = 0.064 ± 0.004 µM) and inhibition than the approved cholinesterase inhibitors; galantamine and tacrine. Further, kinetic and molecular docking studies indicated that these molecules exhibit mixed inhibition. Compound 21 significantly reduces Aβ-induced toxicity. It contains the N-cyclohexyl group at the amido functional group, offering a neuroprotective effect and less toxicity to human neuroblastoma cells in all concentrations. This series of compounds also displayed anti-oxidant activity (Shaik et al., 2019).

Ghobadian et al. reported N-benzyl-3-carbazolylpyridines as BuChE inhibitors. Compound 22 (3-((9H-carbazol-9-yl)methyl)-1-(4-chlorobenzyl)pyridin-1-ium chloride) (IC₅₀ = 0.073 ± 0.003 µM) was identified as a potent and selective inhibitor of BuChE. A molecular docking study revealed a strong interaction of this compound with CAS and PAS of the enzyme with favorable physicochemical properties as a CNS drug. In addition, compound 22 demonstrated inhibition of self-induced Aβ peptide aggregation and neuroprotective activity (Ghobadian et al., 2018).

In another project by Zang et al., co-workers developed a series of Claulansine F-donepezil hybrids as multitarget drugs. Among 26 compounds studied, six compounds showed excellent AChE inhibitory activity. (E)-3-(8-(t-butyl)-3,3-dimethyl-3,11-dihydropyrano [3,2-a]carbazol-5-yl)-N-((1-(2-chlorobenzyl)piperidin-4-yl)methyl)acrylamide (23) was the most potent (IC₅₀ = 4.34 ± 0.46 μM) and displayed the strongest in-vitro neuroprotective activity. Most importantly, 23 was able to cross BBB and also demonstrated radical scavenging activity in-vitro, proving to be a potential candidate for the treatment of AD (Zang et al., 2021).

Sadeghiana et al. reported a novel series of anti-Alzheimer’s agents. In this study, they designed, synthesized, and evaluated a carbazole-benzyl piperidine hybrid for cholinesterase inhibition. N-(5-(9H-carbazol-9-yl)pentyl)-1-benzylpiperidin-4-amine (24) and N-(6-(9H-carbazol-9-yl)hexyl)-1-benzylpiperidin-4-amine (25) from this series indicated potent anticholinesterase activity. Compound 24 showed IC₅₀ of 16.5 μM for AChE and IC₅₀ of 0.59 μM for BuChE) and 25 showed IC₅₀ of 26.5 μM for AChE and IC₅₀ of 0.18 μM for BuChE. These two compounds also displayed β-secretase inhibition. Here, benzyl piperidine is linked with carbazole via a carbon chain linker. This linker with five (24) and six (25) carbon atoms exhibited good activity (Sadeghian et al., 2020).

Derabli et al. developed new tacrine analogues modified with pyrano-pyrazole. Among the analogues, 4-([1,1′-biphenyl]-4-yl)-3-methyl-2,4,6,7,8,9-hexahydropyrazolo [4′,3':5,6]pyrano [2,3-b]quinolin-5-amine (26) displayed strong AChE inhibition (IC₅₀ = 0.044 ± 0.002 μM) compared to the reference drug galantamine (IC₅₀ = 21.82 ± 4.00 μM) (Derabli et al., 2018).

Kulshreshtha et al. studied novel urea and thiourea derivatives as cholinesterase inhibitors. Among them, N-(5-(2-chlorophenyl)-1,3,4-thiadiazol-2-yl)-4-(2-fluorophenyl)piperazine-1-carboxamide (27) (IC₅₀ = 3.78 ± 0.63 μM) and N-(5-(2-chlorophenyl)-1,3,4-thiadiazol-2-yl)-4-(2-fluorophenyl)piperazine-1-carbothioamide (28) (IC₅₀ = 1.51 ± 0.25 μM) showed promising activity against AChE. In-vivo, behavioral studies on scopolamine-induced animal models indicated that thiourea compound 28 was more potent than urea derivative 27 in alleviating cognition decline (Kulshreshtha and Piplani, 2018).

Pyridine is among the most studied heterocycles in drug design for various diseases, and also it is explored as anti-Alzheimer agent. Badran et al. applied a modern drug design strategy and developed tacrine heterodimer analogues thienopyridines, replacing the benzene ring of tacrine with bio isostere thiophene. 5-(1,2-Dithiolan-3-yl)-N-(3-((5,6,7,8-tetrahydrothieno [2,3-b]quinolin-4-yl)amino)propyl)pentanamide (29) with lipoic acid moiety exhibited higher AChE inhibitory activity (inhibition = 56.73%) than tacrine (inhibition = 54.91%). Lipoic acid moiety possesses antioxidant properties and dual binding affinity to the cholinesterase enzyme (Badran et al., 2013).

In a separate study, Hosseini et al. introduced substitution at the nitrogen atom of the pyridine ring and designed pyridinium derivatives replacing benzyl piperidine moiety of donepezil to obtain the lead compound and further modified to develop 4-oxobenzo [d]1,2,3-triazin benzyl pyridinium derivatives. Among them, 1-(2-nitrobenzyl)-3-((4-oxobenzo [d][1,2,3]triazin-3(4H)-yl)methyl)pyridin-1-ium bromide (30) with 2-nitro substitution in the benzene ring, revealed higher AChE inhibitory activity (IC₅₀ = 0.10 ± 0.01 μM) than donepezil. Docking studies revealed that compound 30 interacted with CAS, PAS, catalytic triad, and oxyanion hole of the AChE enzyme (Hosseini et al., 2020).

Li et al. synthesized novel triazole-based derivatives as cholinesterase inhibitors. 2-Methyl-N-(2-morpholinoethyl)-5-(1-(naphthalen-2-ylmethyl)-1H-1,2,3-triazol-4-yl)benzamide (31), having naphthalene substitution at the triazole ring, exhibited improved anti-cholinesterase activity and selectivity for AChE (IC₅₀ = 7.23 ± 0.16 µM) than BuChE (IC₅₀ = 90.76 ± 0.21 µM). SAR studies demonstrated that the benzene ring with both, electron-withdrawing and donating group substitutions reduced the potency and selectivity of the cholinesterase enzyme. Interestingly, the molecules have physicochemical properties similar to CNS drugs with less cytotoxicity, as observed in human keratinocytes HaCaT and murine fibroblasts NIH-3T3 cell lines. Also, the neuroprotective effect of the molecules was studied in-vitro in SH-SY5Y cells (Li J. C. et al., 2016).

Kamal et al. designed and synthesized a library of (E)-2-aryl-5-styryl-1,3,4-oxadiazole derivatives following a molecular modeling strategy. The library demonstrated good to moderate activity against AChE and docking studies indicated binding of these derivatives was similar to donepezil. (E)-2-(furan-2-yl)-5-(3,4,5-trimethoxystyryl)-1,3,4-oxadiazole (32) exhibited higher activity (IC₅₀ = 13.72 ± 0.01 µM) compared to other heterocyclic derivatives studied (Kamal et al., 2014).

Sukumarapillai et al. developed N-benzyl piperidine-4-one derivatives as anti-Alzheimer’s agents. The compounds synthesized were mono-substituted and di-substituted, showing selective inhibition against BuChE and AChE, respectively. 6-amino-2-benzyl-8-(2-methoxyphenyl)-1,2,3,4-tetrahydroisoquinoline-5,7-dicarbonitrile (33) bearing ortho-methoxy group was potent with mixed-mode inhibitory activity against both AChE (IC₅₀ = 5.61 ± 0.22 µM) and BuChE (IC₅₀ = 0.87 ± 0.03 µM) compared to galantamine (AChE, IC₅₀ = 2.09 ± 0.04 µM and BuChE IC₅₀ = 19.34 ± 0.10 µM). Docking studies revealed that compound 33 displayed hydrophobic interaction at the catalytic triad and choline-binding sites (Sukumarapillai et al., 2016).

Mo et al. designed novel anti-Alzheimer’s agents linking benzyl piperidine with benzimidazolidinone ring, developing benzyl piperidine linked 1,3-dimethylbenz imidazolidinone derivatives. In-vitro cholinesterase inhibition assay demonstrated that the derivatives were good cholinesterase inhibitors. Among the derivatives, N-((1-(3-bromobenzyl)piperidin-4-yl)methyl)-1,3-dimethyl-2-oxo-2,3-dihydro-1H-benzo [d]imidazole -5-sulfonamide (34) was identified as a potent inhibitor of both AChE (IC₅₀ = 0.39 ± 0.15 μM) and BuChE (IC₅₀ = 0.16 ± 0.04 μM) in the sub-micromolar range. Cytotoxicity studies revealed that compound 34 is less hepatotoxic than donepezil. Considerable amelioration of cognitive impairment was observed in scopolamine-treated mice in the Morris maze test, and it also exhibited cytoprotective and antioxidant activity (Mo et al., 2020).

Eghtedari et al. developed tacrine-derived compounds as cholinesterase inhibitors, 5-amino-2-phenyl-4H-pyrano [2,3-b]-quinoline-3-carboxylates. Ethyl 5-amino-4-(3-bromophenyl)-2-phenyl-6,7,8,9-tetrahydro-4H-pyrano [2,3-b]quinoline-3-carboxylate (35) exhibited the most potent activity against AChE (IC₅₀ = 0.069 ± 0.005 µM) and BuChE (IC₅₀ = 1.35 ± 0.07 µM) that was five times more active than tacrine as evaluated by an in-vitro cholinesterase inhibition assay. The SAR by modifying substituents at the fourth position of pyrano moiety with substituted-phenyl ring revealed that electron-withdrawing groups such as chloro and bromo at ortho and meta positions improve the cholinesterase inhibitory potential of the compounds. The toxicity studies on HepG2 cells indicated that these compounds were less cytotoxic than tacrine (Eghtedari et al., 2017).

Pal et al. reported the synthesis and biological evaluation of a novel class of pyridoxine-based triazoles as cholinesterase enzyme inhibitors. Out of seventeen compounds, 5-(((1-(3,5-difluorobenzyl)-1H-1,2,3-triazol-4-yl)methoxy)methyl)-4-(hydroxymethyl)-2-methylpyridin-3-ol (36) showed higher AChE inhibitory activity (IC₅₀ = 1.5609 ± 0.0237 mM). SAR studies revealed that meta and ortho substitutions on the aromatic ring with electron-donating groups were favorable for AChE inhibitory activity. The antioxidant property of compound 36 found with ORAC-FL value was equivalent to trolox, and in silico studies revealed that compound 36 has suitable pharmacokinetic and drug-like properties (Pal et al., 2020).

In a separate research, Loh et al. synthesized novel 3-O-substituted xanthone derivatives possessing more robust anti-cholinesterase activity. Eleven derivatives were identified as potent AChE inhibitors, and 3-(4-phenylbutoxy)-9H-xanthen-9-one (37) was the most potent among them with IC₅₀ of 0.88 ± 0.04 μM. SAR study depicted hydrophobic interactions and hydrogen bonding of the substituents group, particularly saturated linear hydrocarbon chain having four carbons with the addition of phenyl or oxygenated groups are required to elicit activity. Docking studies revealed that the hydrophobic interaction is due to π-π stacking and hydrogen bonding contributed by the xanthone skeleton (Loh et al., 2021).

In another study, Zhang et al. developed novel xanthone-alkyl benzylamine hybrids with an alkyl linker and 1-hydroxy-3-((6-((4-hydroxybenzyl) (methyl)amino)hexyl)oxy)-9H-xanthen-9-one (38) was identified as the most potent AChE inhibitor (IC₅₀ = 0.85 ± 0.043 μM) with balanced dual cholinesterase inhibition. Kinetic analysis and docking studies indicated compound 38 was a mixed type of inhibitor for AChE and BuChE with good blood-brain barrier (BBB) penetrability and antioxidant properties equivalent to trolox. Additionally, memory function improvement was observed in scopolamine-induced amnesia mice (Zhang Z. et al., 2021).

Ozdemir et al. reported the design and synthesis of 6-substituted-3(2H)-pyridazine-2-acetyl-2-(p-substituted benzalhydrazone) derivatives as potent dual cholinesterase inhibitors. (E)-2-(3-(4-(3,4-dichlorophenyl)piperazin-1-yl)-6-oxopyridazin-1(6H)-yl)-N'-(3-methylbenzylidene) acetohydrazide (39) was the most potent compound among the synthesized derivatives for AChE inhibition (IC₅₀ = 75.52 ± 1.76%) and BuChE (IC₅₀ = 62.03 ± 1.82%). Docking studies demonstrated that its binding interactions in AChE active sites were similar to those of the known inhibitors. However, it did not show binding abilities to the active site of BuChE (Özdemir et al., 2017).

Shrivastava et al. designed and synthesized an N-methylene benzenamine nucleus containing 3,5-dimethoxy-N-methylene benzenamine and 4-(methylene amino)benzoic acid derivatives. (E)-N-(3,5-dimethoxyphenyl)-1-(3,4,5-trimethoxyphenyl)methanimine (40) depicted higher AChE inhibition (IC₅₀ = 0.82 ± 0.05 µM) than donepezil evaluated. Ex-vivo studies confirmed the ability of compound 40 to cross the BBB and selective inhibition of AChE. In addition, compound 40 also exhibited good in-vitro radical scavenging ability (Shrivastava et al., 2017).

Tripathi et al. developed 2-amino-6-nitrobenzothiazole-derived hydrazones as AChE inhibitors. (Z)-N'-(5-chloro-2-oxoindolin-3-ylidene)-2-((6-nitrobenzo [d]thiazol-2-yl)amino) acetohydrazide (41) indicated six-fold potency against AChE (IC₅₀ = 0.0035 ± 0.005 µM) than donepezil and tacrine. This compound demonstrated mixed-type reversible enzyme inhibition with a good docking score. Further, the radical scavenging ability of the active molecules was higher as confirmed by α,α-diphenyl-β-picrylhydrazyl (DPPH) radical scavenging assay (Tripathi and Ayyannan, 2018).

In another captivating research, Carrillo et al. synthesized and evaluated aliphatic and aromatic edaravone derivatives as antioxidant and AChE inhibitors by DPPH and in-vitro AChE inhibition assay, respectively. Aliphatic derivatives were not as active as the standard drug galantamine, but aromatic derivatives exhibited better general activity; among them, 3-methyl-1-phenyl-1H-pyrazol-5-yl-4-methylbenzoate (42) showed the highest percent inhibition (inhibition = 41.9 ± 7.3%). Fascinatingly, all synthesized compounds showed drug-like properties capable of crossing BBB, and docking analysis revealed compounds have good interaction at the AChE catalytic gorge site (Barajas-Carrillo et al., 2021).

Davis et al. designed a novel series of isatin-linked 4,4-dimethyl-5-methylene-4,4-dihydro thiazole-2-thiols as AChE inhibitors. 1-(3-((4,4-Dimethyl-5-methylene-4,5-dihydrothiazol-2-yl)thio)propyl)indoline-2,3-dione (43) was the most potent inhibitor (IC₅₀ = 18.2 ± 1.2 μM) and the potency was similar to galantamine. Kinetic studies indicated that compound 43 was a non-competitive reversible inhibitor, whereas molecular modeling indicated interaction with AChE active site. Isatin moiety showed interaction with CAS and 2-thiazoline moiety with PAS of AChE (Davis and Eckroat, 2021).

Xiaokang et al. designed, synthesized, and evaluated non-fused pyrimidinyl thiourea derivatives by screening hit compounds and modifications. These are multifunctional agents. 1-(6-(4-((dipropylamino)methyl)-1H-imidazol-1-yl)pyrimidin-4-yl)-3-ethyl thiourea (44) and 1-ethyl-3-(6-(4-(pyrrolidin-1-ylmethyl)-1H-imidazol-1-yl)pyrimidin-4-yl) thiourea (45) show good inhibition and binding selectivity for AChE. Compound 44 (IC₅₀ = 0.204 μM) and compound 45 (IC₅₀ = 0.067 μM) have been found to exhibit notable AChE inhibition. These compounds demonstrated multiple activities such as specific metal-chelating ability, anti-oxidant effects, and modulation of metal-induced Aβ aggregation (Li X. et al., 2016).

Shidore et al. synthesized novel molecules by fusing cholinesterase inhibitor donepezil and diaryl thiazole. N-((1-(3,5-difluorobenzyl)piperidin-4-yl)methyl)-4,5-di-p-tolylthiazol-2-amine (46) of the series exhibited potent anti-cholinesterase activity with IC₅₀ of 0.30 ± 0.01 µM against AChE, and IC₅₀ = 1.84 ± 0.03 µM against BuChE. In addition, compound 46 also showed in-vitro anti-oxidant and anti-apoptotic properties (Shidore et al., 2016).

Singh et al. synthesized and evaluated pyrazolyl-substituted steroids as neuroprotective agents. Dehydroepiandrosterone is a steroid used to treat neurodegenerative disorders such as Alzheimer’s and Parkinson’s disease, which is substituted at the 16th and 17th positions with the pyrazolinyl group. 10-acetyl-6a,8a-dimethyl-11-(pyridin-4-yl)-1,3,4,5,6,6a,6b,7,8,8a,10,11, 11a,12,12a,12b-hexadecahydronaphtho [2′,1':4,5]indeno [1,2-c]pyrazol-4-yl acetate (47) displays potent neuroprotection with inhibition of AChE with micro moles of AChE/min/mg protein (0.0027 ± 0.0006) (Singh R. et al., 2018).

Tintas et al. synthesized and evaluated 1,4-dihydropyridine derivatives with significant AChE inhibition. 2-((3-Acetyl-1-benzyl-1,4-dihydropyridin-4-yl)methyl)-6,7-dimethoxy-3,4-dihydronaphthalen-1(2H)-one (48) displayed a good AChE inhibitory activity (IC₅₀ = 0.173 µM). These are chiral 1,4-dihydropyridine derivatives that exhibited selectivity for AChE (Ţînţaş et al., 2018).

Parlar et al. designed, synthesized, and evaluated a series of N-benzylpiperidine-3/4-carbohydrazone derivatives for AChE inhibition. These SAR studies showed that the phenyl-substituted compound displayed selectivity for AChE binding. (E)-1-benzyl-N′-(4-nitrobenzylidene)piperidine-3-carbohydrazide (49) and (E)-1-benzyl-N′-(4-(diethylamino) benzylidene)piperidine-3-carbohydrazide (50) demonstrated the most potent activity in the given series of derivatives. Compound 49 indicated better in-vitro AChE inhibition with IC₅₀ = 5.68 μM, and compound 50 diethylamino derivative exhibited AChE inhibition with IC₅₀ = 0.81 μM. It also showed Aβ42 self-aggregation inhibition and anti-oxidant properties (Parlar et al., 2019).

Patel et al. designed, synthesized novel triazinoindole derivatives and evaluated them for anti-cholinesterase activity. N ¹-(5H-[1,2,4]triazino [5,6-b]indol-3-yl)-N ⁶ ,N ⁶-di (pyrrolidin-1-yl)hexane-1,6-diamine (51) exhibited good cholinesterase inhibition from this series of derivatives. Compound 51 indicated IC₅₀ = 0.56 ± 0.02 µM for AChE and IC₅₀ = 1.17 ± 0.09 µM for BuChE. Pyrrolidine moiety in compounds shows better activity than compounds with other amines. These tertiary amines show pie-cation interaction with amino acids present in enzymes. A molecular docking study revealed that amino groups present in molecules interact with various amino acids in enzymes by hydrogen bonding. Compound 51 also exhibited improved anti-oxidant and neuroprotective properties than other molecules in this series (Patel et al., 2019).

The marine ecosystem has a vast amount of different and unique bioactive secondary metabolites. Paudel et al. extracted bromophenols from red algae called Symphyocladia latiuscula Yamada. Further, they evaluated their biological activity against AChE and BuChE. Among all the extracted compounds, 5,5′-(oxybis (methylene))bis (3,4,6-tribromobenzene-1,2-diol) (52) indicated potent inhibition of the cholinesterase enzyme with a K_i value of 0.6 μM for AChE and 0.37 μM for BuChE inhibition. The OH groups in the structure exhibit hydrogen bond interaction with the enzyme revealed by the docking study. It also inhibits Aβ aggregation (Paudel et al., 2019).

Kanhed et al. developed a series of indoloquinoxaline derivatives. These indoloquinoxaline derivatives produced multitargeted activities against Alzheimer’s disease, such as cholinesterase inhibition, self-induced Aβ aggregation inhibition, and antioxidant activity. 6-(6-(Piperidin-1-yl)hexyl)-6H-indolo [2,3-b]quinoxaline (53) exhibits the most potent and selective inhibition of BuChE with IC₅₀ of 0.96 ± 0.31 µM and inhibition of AChE with IC₅₀ of 5.80 ± 0.70 µM, also, 51.24% inhibition of self-induced Aβ aggregation. A docking study revealed that six carbon linkers between amino and indole nitrogen provide better stability to the enzyme ligand complex. At the same time, the pyrrolidine ring presents weak hydrogen bond interaction and the indolo [2,3-b]quinoxaline ring form π-π interaction with the active site of the cholinesterase enzyme (Kanhed et al., 2022).

Donepezil is a primary drug used for the treatment of Alzheimer’s disease. Gupta et al. designed the analogues of donepezil based on the SAR of lead compound indanone moiety. The novel synthesized compounds indicated good in-vivo and in-vitro inhibition of cholinesterase. 3-(4-(4-Fluorobenzoyl)piperidin-1-yl)-1-(4-methoxybenzyl)pyrrolidin-2-one (54) and 1-(3,4-dimethoxybenzyl)-3-((1-(2-(trifluoromethyl)benzyl)piperidin-4-yl)methyl)imidazolidin-2-one (55) exhibited the most potent AChE inhibitory activity from this series with 0.018 ± 0.001 and 0.022 ± 0.002 µMol of AChE/min/mg of protein, respectively (Gupta et al., 2020).

Altamirano-Espino et al. synthesized aminoisophthalic acid derivatives to inhibit acetylcholinesterase with fewer side effects. They have synthesized ten derivatives and evaluated them for AChE inhibition in-vitro and in silico. According to the docking simulation study, electron-poor aminobenzoic acid derivatives show better inhibition than electron-rich ones. However, when a heterocyclic ring is substituted in place of a linear group, it creates a π-π stacking interaction between the aromatic ring and an amino acid in the enzyme, resulting in a lower Ki value. The in-vitro assessment indicates that the derivative with a succinimide substitution compound, 5-(2,5-dioxopyrrolidin-1-yl)isophthalic acid (56), displays the lowest Ki value of 73 µM compared to the other compounds tested (Altamirano-Espino et al., 2020).

Scheide et al. synthesized allylnaphthol and allylphenol derivatives with diselenides via intramolecular electrochemical oxidation and cyclization. Further, they evaluated these compounds for anti-Alzheimer’s activity. From this series of compounds, three compounds revealed good inhibition of AChE. These are 2-(((2-methoxyphenyl)selanyl)methyl)-1,2-dihydronaphtho [2,1-b]furan (57) with IC₅₀ = 10.6 µM, 2-((benzylselanyl)methyl)-1,2-dihydronaphtho [2,1-b]furan (58) with IC₅₀ = 11.6 µM, 2-((thiophen-2-ylselanyl)methyl)-1,2-dihydronaphtho [2,1-b]furan (59) with IC₅₀ = 9.97 µM (Scheide et al., 2020).

Hira et al. studied the potential aldosterone antagonist eplerenone, methyl 4a,6a-dimethyl-2,5′-dioxo-2,4,4a,4′,5a,5′,6,6a,8,9,9a,9b,10,11-tetradecahydro-3H,3′H-spiro [cyclopenta [1,2] phenanthro [4,4a-b]oxirene-7,2′-furan]-10-carboxylate, (60) for the treatment of Alzheimer’s disease. In-vivo and in silico studies showed that eplerenone is an effective drug for reversing STZ (streptozotocin)-induced memory impairment. It may be helpful in the treatment of Alzheimer’s disease and dementia (Hira et al., 2020).

Gok et al. focused on dopamine as a treatment for AD. They have synthesized a series of dopamine analogues by introducing urea and sulfonamide groups into the dopamine moiety, resulting in novel active analogues with potent cholinesterase inhibition and anti-oxidant activity. 2-(2-(3,3-Dimethylureido)ethyl)-4,5-dimethoxy-N,N-dimethylbenzenesulfonamide (61) with N,N-dimethylsulfonamide and N,N-dimethylurea substitution exhibited inhibition of both AChE and BuChE with IC₅₀ values of 298 µM and 321 μM, respectively. Docking studies revealed that this analog had good binding interaction with cholinesterase enzyme. Additionally, its ADME properties were in the acceptable range (Gök et al., 2021).

Taha et al. also synthesized the sulfonamide derivatives based on indole as a basic moiety. From this series, 4-fluoro-N'-(5-hydroxy-1H-indole-2-carbonyl)benzenesulfonohydrazide (62) displayed significant inhibition of AChE with an IC₅₀ value 0.17 ± 0.02 µM. According to the docking study, the sulfonamide group interacts with the active site residues via hydrogen bonding, while the indole aromatic ring forms a π-π interaction. Additionally, the fluorine on the aromatic ring is observed to exhibit an interaction (Taha et al., 2021).

Huperzine A is a natural product having anti-cholinesterase activity, like galantamine. It has been obtained from Huperzia serrata as a sesquiterpene alkaloid. It is used in China as a standard therapy for dementia. Miao et al. modified huperzine and synthesized a new series of N-hetero (aryl) analogues of huperzine A. Further, they evaluated this analog for its anti-Alzheimer’s activity. From this synthesized series, (5R,7S,9S,E)-11-ethylidene-5-((5-methoxy pyridin-2-yl)amino)-7-methyl-5,6,7,8,9,10-hexahydro-5,9-methanocycloocta [b]pyridin-2(1H) -one (63) with 5-methoxy-2-pyridyl substitution displays potent AChE inhibition with IC₅₀ value of 1.5 µM, which is 7.6 times more potent than huperzine A. It also indicated anti-oxidant activity. A molecular docking study speculates that compound 63 has good binding interaction. Aromatic moiety interacts via π-π stacking; methoxy pyridine shows hydrophobic interaction. This analog exhibited neuroprotective properties (Miao et al., 2021).

Murtaza et al. designed, synthesized, and evaluated a set of 2-aminobenzohydrazide and 2,3-dihydroquinazolin-4(1H)-one derivative as anti-cholinesterase agents. (E)-2,5-dichloro-N-(2-(2-(4-hydroxy-3-methoxybenzylidene)hydrazine-1-carbonyl)phenyl)benzene sulfonamide (64) shows dual inhibition of AChE and BuChE with IC₅₀ values of 0.12 ± 0.03 µM and 0.13 ± 1.75 µM, respectively. A molecular docking study revealed that the three aromatic rings in 64 make π-π interaction with amino acids at the active site of cholinesterase. Relative to the preceding compound, heteroatoms exhibit distinct hydrogen bond interactions with amino acids. The molecule’s electronegative density is a crucial determinant of its binding capability. Additionally, this derivative displays a neuroprotective effect (Murtaza et al., 2022). See Supplementary Table 1 for a summary of cholinesterase inhibitors.

The amyloid hypothesis plays a vital role in the pathogenesis of Alzheimer’s disease. Hence the approach of blocking or slowing of Aβ aggregation attracted the attention of medicinal chemists.

Li et al. developed a series of multipotent 2-piperidones against Alzheimer’s disease. 1-(3,4-Dimethoxybenzyl)-4-(3,5-dimethoxyphenyl)-6-(4-hydroxyphenyl)-5-nitro piperidin-2-one (65) exhibited the best concentration-dependant Aβ-self aggregation inhibition (59.11% at 20 µM) evaluated in-vitro by thioflavin T (ThT) fluorescence assay. Further, docking analysis revealed good binding to the active site of myeloid differentiation factor 88 (MyD88), preventing the dimerization of peptides. In addition, the synthesized compounds demonstrated less neurotoxicity and anti-inflammatory properties (Li L. et al., 2016).

In another study, Wang et al. designed and synthesized 8-hydroxyquinolines bearing (benzo[d][1,2]selenazol-3(2H)-one) substitution at second position for the treatment of Alzheimer’s disease. Interestingly, 5-hydroxy-2-(8-hydroxyquinolin-2-yl)benzo [d][1,2] selenazol-3(2H)-one (66) demonstrated inhibition of Cu (II)-induced Aβ aggregation among the derivatives confirmed by ThT fluorescence assay. This compound also showed a good radical scavenging activity (2.6 ± 0.3 µM min^-1) in oxygen radical absorbance capacity (ORAC FL) assay (Wang et al., 2016).

Interestingly, Zang et al. also explored a quinoline scaffold and developed a 4-hydroxy carbazole-8-aminoquinoline dimer, 1-((9H-carbazol-4-yl)oxy)-3-(quinolin-8-ylamino)propan-2-ol (67) as copper-induced Aβ aggregation inhibitor and reported 22.9% inhibition in ThT fluorescence assay. In addition, compound 67 exhibited good copper selective inhibition and neuroprotective effect against Glu-induced cell death in HT22 cells at 10 µM (Zhang et al., 2018).

In a separate study by Kucukkilinc et al., co-workers designed, synthesized, and evaluated 5,6-diaryl-1,2,4-triazine-3-thioacetates against Aβ induced neurotoxicity and H₂O₂ toxicity. The neuroprotective activity of the compounds was evaluated on PC12 and SH-SY5Y cells; surprisingly, ethyl 2-(5-(4-chlorophenyl)-6-(4-methoxyphenyl)-3-thioxo-1,2,4-triazin-2(3H)-yl)acetate (68) was identified as the most potent derivative (EC₅₀ = 14.44 ± 0.85 µM) and was less potent than quercetin (EC₅₀ = 8.18 ± 1.45 µM). Cytometric analysis revealed the possibility of a 40% increase in cell viability in H₂O₂-induced apoptosis. Furthermore, these compounds also improved neuronal cells neurite outgrowth in transferase-mediated dUTP nick end labelling (TUNEL) assay (Tuylu Kucukkilinc et al., 2017).

Plexes are an attractive class of drug discovery. Messori et al. studied ruthenium (III) complexes as an anti-Alzheimer’s agent having potent Aβ blocking properties. Among three metal complexes studied, (69) displayed potent activity against Aβ aggregation in-vitro, and this study confirmed PMRU20 at 20 μM as an effective neuroprotective agent (Messori et al., 2013).

Pagoni et al. synthesized and evaluated 13 novel hybrids of phenols and lipoic acid as Aβ-aggregation inhibitors as well as antioxidant agents. From this series, (E)-5-(1,2-dithiolan-3-yl)-N-(3-(3-(4-hydroxy-3-methoxyphenyl)acrylamido)propyl)pentanamide (70) exhibited in-vitro activity against Aβ-aggregation. Additionally, it also displayed antioxidant properties with cytoprotective and non-cytotoxic action. Ferulic and dihydroxyphenylacetic acid derivatives (structures not shown) as phenolic groups indicate strong free radical scavenging and anti-amyloidogenic properties (Pagoni et al., 2020).

Sirimangkalakitti et al. reported the anti-Alzheimer’s activity of naturally occurring bioflavonoids as β aggregation inhibition. They have studied 27 bioflavonoids with different linkages and methoxy substitution. Among them, flavonoids amentoflavone and its methoxy derivatives show potent inhibition of Aβ aggregation in vitro and bilobetin, 8-(5-(5,7-dihydroxy-4-oxo-4H-chromen-2-yl)-2-methoxyphenyl)-5,7-dihydroxy-2-(4-hydroxyphenyl)-4H-chromen-4-one, (71) displayed an IC₅₀ value of 4.7 µM (Sirimangkalakitti et al., 2019).

Wongrattanakamon et al. studied the anti-Aβ-aggregation activity of guanidinyl tryptophans. In this study, molecular dynamic simulation of Aβ monomer with various derivatives was conducted. Compound 72 indicated potent interference with Aβ monomer movement into the cell. N-(2-(1H-indol-3-yl)ethyl)-2-(2-amino-3-(1H-indol-3-yl)propanamido)-3-hydroxypropanamide (72) exhibited anti-amyloid aggregation with 49.8% ± 1.5% inhibition (Pathomwat et al., 2021).

Utomo et al. developed curcumin-based Aβ aggregation inhibitors. Methyl 2-(4-((1E,6E)-7-(4-hydroxy-3-methoxyphenyl)-3,5-dioxohepta-1,6-dien-1-yl)-2-(trifluoromethyl)phenoxy) acetate (73) (IC₅₀ = 0.007 µM) possessed 100-fold higher activity as Aβ aggregation inhibition than curcumin. Compounds with hydroxyl and methoxycarbonyl groups show more potent inhibition than curcumin. Compound 73 also showed lower cytotoxicity (Yudi Utomo et al., 2021). See Table 1 for a summary of Aβ aggregates inhibitors.

Beta-site amyloid precursor protein cleaving enzyme (BACE-1), also known as β-secretase involved in Alzheimer’s pathogenesis, is a less explored target by the medicinal chemist for treating Alzheimer’s disease.

Liu et al. reported a series of 4-oxo-1,4-dihydro-quinoline-3-carboxamides as BACE-1 enzyme inhibitors. N-(3-bromophenyl)-4-oxo-6-(o-tolyl)-1,4-dihydroquinoline-3-carboxamide (74) was identified as a highly potent analog (IC₅₀ = 1.89 ± 0.09 µM) and showed a high percentage of BACE-1 inhibition (77.6% ± 4.9%) evaluated by fluorescence resonance energy transfer (FRET) assay. Docking studies confirmed affinity to the enzyme’s active site. A good BBB permeability, and lower cellular toxicity were also observed for compound 74 (Liu et al., 2014).

Xu et al. developed a series of 4-aminopyrimidine and 4,6-diaminopyrimidines against Aβ. 2-((4,6-diaminopyrimidin-2-yl)thio)-N-(4-(2-methoxyphenyl)thiazol-2-yl)acetamide (75) (IC₅₀ = 1.4 ± 0.6 μM) was twenty-six-fold more potent than the lead compound as evaluated by FRET assay. Moreover, the parallel artificial membrane permeability assay suggested BBB permeability (Xu X. et al., 2019).

Yazdani et al. designed and synthesized 1,2,4-triazines bearing aryl phenoxy methyl-1,2,3-triazole against the BACE-1 enzyme. Researchers demonstrated that compounds having chloro- and nitro-substitution at the para position of the phenyl ring were potential BACE-1 inhibitors. (E)-3-(2-(4-((1-(4-chlorobenzyl)-1H-1,2,3-triazol-4-yl)methoxy) benzylidene)hydrazinyl)-5,6-diphenyl-1,2,4-triazine (76) with chlorine at the para position of the phenyl ring was a potent inhibitor (IC₅₀ = 8.55 ± 3.37 μM). The neuroprotective activity was assessed on the PC12 neuronal cell line, and moderate neuronal protection was observed for the active analog. Docking studies revealed that these molecules have a high binding affinity to the enzyme’s active site (Yazdani et al., 2018).

Jagtap et al. synthesized 4-substituted 2-amino-3,4-dihydro quinazoline with hairpin turn side chains as novel inhibitors for the BACE-1 enzyme. Among the derivatives, 4-(2-amino-6-benzyl-4-methylquinazolin-3(4H)-yl)-N-cyclohexyl-N-((1-N-methyl-1H-pyrazol-4-yl)methyl)butanamide (77), having 4-methyl substitution bearing N-cyclohexyl-N-(1-methyl-1H-pyrazol-4-ylmethyl)butanamide, exhibited potent BACE-1 enzyme inhibition with an IC₅₀ of 0.38 μM. The docking study showed that the 3,4-dihydro quinazoline scaffold facilitates interaction with the S ₁ , S _2, and S ₁ ' subsites of the BACE-1, and the hairpin turn topology of the side chain provides additional interaction with the S ₂ subsite (Jagtap et al., 2020). See Table 2 for a summary of BACE-1 inhibitors.

Hoang et al. conducted a study on glutaminyl cyclase (QC), a novel target, upon inhibition reduces the production of toxic pyriform of Aβ in the brain of Alzheimer’s patients. The researchers synthesized and evaluated a series of compounds, including N-substituted thiourea, urea, and α-substituted amide derivatives, for their ability to inhibit glutaminyl cyclase in-vitro. The synthesized compounds showed good potency in inhibiting glutaminyl cyclase, with 1-(3,4-dimethoxyphenyl)-3-(3-(5-methyl-1H-imidazol-1-yl)propyl)thiourea (78) exhibiting an IC₅₀ value of 1.3 nM for inhibition of hQC. Structure-activity relationships (SAR) studies revealed that N-substitution increased potency by 20-fold for thiourea, 100-fold for urea, and 8-fold for amide derivatives compared to their unsubstituted counterparts. The in-vivo study conducted using the 5XFAD mouse model demonstrated that these compounds reduced the load of pyriform Aβ and total Aβ in the brain (Hoang et al., 2019).

Hoang et al. developed a library of glutaminyl cyclase inhibitors based on the binding mode of Aβ3E-42 with glutaminyl cyclase. Among these compounds, 1-(4-(4-(2-aminopyridin-4-yl) butoxy)-3-methoxyphenyl)-3-(3-(5-methyl-1H-imidazol-1-yl)propyl)thiourea (79) demonstrated potent inhibitory activity against hQC in-vitro, with an IC₅₀ value of 4.5 nM. In-vivo evaluation demonstrated that this compound effectively achieved the intended therapeutic outcomes. In two different transgenic mouse models of Alzheimer’s disease, APP/PS1 and 5xFAD, compound 79 significantly reduced both total Aβ and pyriform Aβ concentrations in the brain and restored cognitive function. Molecular docking studies revealed that compound 79 exhibited strong interactions with the hQC active site (PDB ID: 3PBB). Additionally, 5-methylimidazole chelated with zinc and formed hydrogen bond interactions (Hoang et al., 2017). See Table 3 for a summary of Glutaminyl Cyclase inhibitors.

Romeiro et al. synthesized HDAC inhibitors derived from cashew nutshell liquid and its derivatives. Methyl 2-(8-(hydroxyamino)-8-oxooctyl)-6-methoxybenzoate (80) exhibited potent inhibition of HDAC1 and HDAC6, with IC₅₀ values of 774.7 ± 14.4 nM and 215.4 ± 28.6 nM, respectively. Compound 80 also efficiently modulated glial cell-induced inflammation and reverted the pro-inflammatory phenotype (Romeiro et al., 2019). See Table 4 for a summary of HDAC inhibitors.

In the past decade, the impact of single-targeted therapies has been modest and transient due to the multifaceted nature of Alzheimer’s disease. Assorted studies have suggested that combination therapy could advance AD treatment despite the lack of evidence that these agents prevent or reverse the disease pathologies. Additionally, these agents prolong the time before the patient requires hospital care.

An effort made by Mao et al. designed and synthesized various compounds, including O-hydroxyl or O-amino benzylamine-tacrine hybrids (structure not shown) by reacting N-(amino-alkyl) tacrine with a salicylaldehyde or derivatives of 2-aminobenzaldehyde. These compounds were tested as multifunctional anti-Alzheimer’s agents against AChE and Aβ aggregates. N ¹,N ¹-dimethyl-N ²-(9-((1,2,3,4-tetrahydroacridin-9-yl)amino)nonyl)benzene-1,2-diamine (81) showed better AChE inhibition (IC₅₀ = 0.55 ± 0.034 nM) and exhibited the potential to inhibit Aβ aggregates (39.4%) with additional antioxidant and metal chelating properties than tacrine. SAR studies revealed AChE inhibitory potency was closely related to the length of the alkylene chain. Hybrids with two, three, and four carbon spacers had weak inhibitory activity. AChE inhibitory activity intensified as the carbon spacer increases; the same trend was observed in both O-hydroxyl or O-amino benzylamine-tacrine hybrids. The most potent hybrid compound, 81 with a 9-carbon spacer, showed the highest inhibitory activity (Mao et al., 2012).

Another study by Roldan-Pena et al. designed tacrine-based homo- and heterodimers with antioxidant tether (selenoureido, dichalcogenide, or selenide) against AChE inhibition. Among these compounds, diselenides and disulfides containing dimers exhibited high activity against the AChE enzyme. N,N'-(disulfanediylbis (pentane-5,1-diyl))bis (1,2,3,4-tetrahydroacridin-9-amine) (82) with disulfide linker was the most potent compound showing strong inhibition against hAChE (IC₅₀ = 1.62 ± 0.10 nM) and good inhibition against Aβ aggregates (61.8% ± 3.4%). Surprisingly, these compounds also displayed promising anti-proliferative activity tested against six human solid tumor cell lines and one non-tumor (BJ-hTert, human fibroblasts) cell line (Roldán-Peña et al., 2017).

Similarly, Jerabek et al. also studied tacrine hybrids and combined structural features of tacrine with resveratrol having antioxidant and anti-neuroinflammatory activity as multi-target-directed ligands (MTDLs) for AD treatment. (E)-5-(4-((6-chloro-1,2,3,4-tetrahydroacridin-9-yl)amino)styryl)benzene-1,3-diol (83) was the most potent hybrid against hAChE (IC₅₀ = 8.8 ± 0.4 µM). Also, it indicated higher inhibition of Aβ self-aggregation (IC₅₀ = 31.2 ± 9.0 µM) than resveratrol. However, among the molecules studied, only compound 83 exhibited low neurotoxicity tested on an AD neuroinflammation cell model (Jeřábek et al., 2017).

In an another interesting study, Cen et al. synthesized a series of tacrine-bifendate conjugates and evaluated their multi-model action as anti-Alzheimer’s agents. These compounds displayed potent cholinesterase and self-induced Aβ aggregation inhibitory activities with methyl 7,7′-dimethoxy-5'-((8-((1,2,3,4-tetrahydroacridin-9-yl)amino)octyl)carbamoyl)-[4,4′-bibenzo[d][1,3]dioxole]-5-carboxylate (84) being the most potent conjugate. Compound 84 displayed IC₅₀ of 27.32 ± 1.61 nM for AChE inhibition and 82.5% ± 10.4% inhibition of Aβ aggregation. Further, a molecular modeling study demonstrated that these compounds target the acetylcholinesterase enzyme’s CAS and PAS sites. Compound 84 also revealed less cytotoxicity on PC12, HepG2, and human liver cell lines (HL-7702) than tacrine (Cen et al., 2017).

In an alternative exciting research, Hiremathad et al. designed a series of tacrine-hydroxy phenyl benzimidazole (TAC-BIM) as multi-targeted drug ligands (MTDL). N-(3-((6-chloro-1,2,3,4-tetrahydroanthracen-9-yl)amino)propyl)-2-(2-hydroxyphenyl)-1H-benzo [d]imidazole -5-carboxamide (85) indicated an improved AChE inhibitory activity (IC₅₀ = 6.3 nM). Also, it exhibited high inhibition of self-induced and Cu-induced Aβ aggregation (inhibition = 39.4%). Additionally, the synthesized compound displayed moderate radical scavenging activity and metal chelating ability. SAR studies demonstrated that chlorine substitution on tacrine is beneficial for enzyme inhibition due to good fitting at the enzyme active site. Further, the analysis speculated that compound 85 had dual binding capacity with CAS and PAS of acetylcholinesterase enzyme due to π-π stacking with three aromatic residues. Neurotoxicity studies revealed that these compounds could inhibit neurotoxicity in neuronal cells (Hiremathad et al., 2018b).

In fascinating research, Jiang et al. reported the first dithiocarbamates with multifunctional activity against AD. Co-workers designed, synthesized, and evaluated novel coumarin-dithiocarbamate hybrids for AD treatment. Biological assay indicated 4-((4-methyl-2-oxo-2H-chromen-7-yl)oxy)butyl piperidine-1-carbodithioate (86) as potent, selective hAChE inhibitory activity (IC₅₀ = 0.027 ± 0.002 μM) and moderate Aβ aggregation inhibition (40.19% ± 2.39%). Kinetic and molecular modeling analysis revealed that compound 86 displayed mixed-type inhibition and interacted well with CAS and PAS of hAChE. In addition, it also enjoyed the metal chelating ability and low toxicity in SH-SY5Y neuroblastoma cells (Jiang N. et al., 2018).

Joubert et al. developed a series of 7-substituted coumarins to study cholinesterase and monoamine oxidase-B (MAO-B) inhibitory activity. These derivatives consisted of a coumarin structure resembling MAO-B inhibitor and a piperidine moiety resembling the 4-benzyl piperidine function of donepezil for AChE inhibition connected via alkyl ether linkage at the seventh position of coumarin. The biological activity assessment indicated that all compounds effectively inhibited human MAO-B over MAO-A. 7-(2-(4-Benzylpiperidin-1-yl)ethoxy)-4-methyl-2-oxo-2H-chromene-3-carbonitrile (87) emerged as the most active derivative against AChE (IC₅₀ = 9.10 µM) and MAO-B (IC₅₀ = 0.30 µM). Molecular modeling suggested that compound 87 can bind to CAS, mid-gorge, and PAS sites of the AChE (Joubert et al., 2017).

Yang et al. designed and synthesized 3-aryl coumarins and investigated their cholinesterase and MAO inhibitory activity. MAO are one of the enzymes whose levels are increased in neurodegenerative disorders; consequently, MAO inhibitors are explored as a complementary alternative in search of new anti-Alzheimer’s agents. Most of the derivatives exhibited moderate to excellent activity; 3-(3,4-dihydroxyphenyl)-7,8-dihydroxy-2H-chromen-2-one (88) displayed the highest activity against AChE (IC₅₀ = 3.04 ± 0.32 μM) and MAO-B (IC₅₀ = 27.03 ± 0.50 μM) (Yang et al., 2019).

Yang et al. designed, synthesized, and evaluated a series of coumarin-pargyline hybrids as dual inhibitors against Alzheimer’s disease. In particular, 7-(4-(ethynyl (methyl)amino)butoxy)-2H-chromen-2-one (89) depicted good inhibitory activity against human MAO-A (IC₅₀ = 3.275 ± 0.040 µM), MAO-B (IC₅₀ = 0.027 ± 0.004 µM) and Aβ aggregation (54%). Moreover, compound 89 indicated low in-vitro cytotoxicity (Yang et al., 2017).

In a separate research study, Qiang et al. reported the design and synthesis of genisteins with carbon spacer-linked alkyl benzylamines as a multifunctional agent against AD. Most of the compounds of the series exhibited potent anti-AChE activity and showed high selectivity for AChE over BuChE. 7-(4-(Ethyl(2-methoxybenzyl)amino)butoxy)-3-(4-(4-(ethyl (2-methoxybenzyl)amino)butoxy)phenyl)-5-hydroxy-4H-chromen-4-one (90) displayed sub-micromolar hAChE inhibition potency (IC₅₀ = 0.35 ± 0.03 µM) and moderately inhibited self-induced Aβ aggregation (inhibition = 35.0 ± 1.0%). Also, it expressed high inhibition of Cu-induced Aβ aggregation with less antioxidant effect. A molecular modeling study suggested that compound 90 showed a mixed-type of inhibition binding to both CAS and PAS of AChE. Due to multifunctional properties, compound 90 can be a promising candidate against AD (Qiang et al., 2014).

Faraji et al. designed seventeen amino alkyl-substituted flavonoids were evaluated for anti-AChE and anti-self-induced Aβ aggregation activity. Among them, 2-(4-((5-(pyrrolidin -1-yl)pentyl)oxy)phenyl)-4H-chromen-4-one (91) demonstrated the best anti-AChE activity (IC₅₀ = 0.01 ± 0.001 μM) and also inhibited self-induced Aβ aggregation (49.2% ± 1.3%). In addition, compound 91 also expressed a neuroprotective effect in PC12 neurons against H₂O₂-induced cell death (Faraji et al., 2019).

A similar type of study was performed by Liu et al. who designed chromone-2-carboxamido-alkylbenzylamines as multifunctional agents against AD. Among the derivatives, N-(4-(ethyl (2-methoxybenzyl)amino)butyl)-5-hydroxy-4-oxo-4H-chromene-2-carboxamide (92) displayed excellent inhibitory potency against AChE (IC₅₀ = 0.07 ± 0.01 µM) and a good inhibitory effect towards self-induced Aβ aggregation (59.2% ± 1.6%) with moderate antioxidant and selective metal chelating activity. A molecular modeling study revealed that compound 92 is a mixed-type inhibitor binding to both CAS and PAS of AChE. SAR studies have suggested that substitutions at the 7-position significantly affected AChE inhibitory activities (Liu et al., 2015).

In an another study, Najafi et al. designed a novel series of chromenone hybrids as anti-Alzheimer’s agents. Compound 93 [7-(4-(6-chloro-2,3-dihydro-1H-cyclopenta [b]quinolin-9-ylamino)phenoxy)-4-methyl-2H-chromen-2-one] exhibited the highest AChE inhibitory activity (IC₅₀ = 16.17 ± 0.02 µM) however, had lower AChE inhibitory activity than reference drug rivastigmine (IC₅₀ = 11.07 µM). In addition, compound 93 demonstrated β-secretase (BACE-1) inhibitory activity with IC₅₀ of 7.99 ± 0.916 µM. Kinetic and molecular modeling studies revealed that compound 93 exhibited good interaction with the CAS and PAS of the AChE; further satisfactory neuroprotection was observed (Najafi et al., 2016).

Reis et al. used a chromone scaffold, developed a small library of chromones, and screened against human cholinesterase and MAOs. Among them, compound 94 [2-(dimethylamino)ethyl (E)-3-(4-oxo-2-(p-tolylcarbamoyl)-4H-chromen-6-yl)acrylate] a most promising multi-target inhibitor displaying dual activity against human AChE (IC₅₀ = 3.69 ± 0.24 μM) and MAO-B (IC₅₀ = 0.63 ± 0.01 μM). Overall, compound 94 stands out as a reversible multi-target inhibitor with favourable permeability and toxicological profiles (Reis et al., 2018).

In a separate study, Mahdavi et al. designed and synthesized benzochromenoquinolines and evaluated them for their cholinesterase and BACE-1 inhibitory activities. Among the synthesized compounds, compound 95 (14-amino-13-(3-nitrophenyl)-2,3,4,13-tetrahydro-1H-benzo [6,7]chromeno [2,3-b]quinoline-7,12-dione) exhibited the highest AChE (IC₅₀ = 0.86 ± 0.04 μM) and BuChE (IC₅₀ = 6.03 ± 0.34 μM) inhibitory activity. Also, it depicted potential BACE-1 inhibition (IC₅₀ = 19.60 ± 0.9 μM) evaluated by FRET assay. In addition, compound 95 also displayed metal chelating ability, and docking results suggested good interaction with the active site (Mahdavi et al., 2019).

Knez et al. reported the synthesis and evaluation of nitroxoline-based analogues designed by combining an 8-hydroxyquinoline scaffold with that of known selective BuChE inhibitors, N-((1-(2,3-dihydro-1H-inden-2-yl)piperidin-3-yl)methyl)-8-hydroxy-N-(2-methoxyethyl)-5-nitro quinoline-7-carboxamide (96) showed the best hBuChE inhibition (IC₅₀ = 0.215 µM) and self-induced Aβ aggregation inhibition (20.1% ± 2.0%). The docking study revealed good interaction of this molecule with the active site, suggesting that chelation of 5-nitroquinolin-8-ol fragment positioned in the acyl binding pocket of huBuChE results in additional interaction with active site residues resulting in increased inhibitory activity (Knez et al., 2015).

Zhao et al. developed a new class of MTDLs based on 7-amino-1,4-dihydro-2H-isoquinolin-3-one for AChE and β-secretase inhibition. Molecular modeling suggested three aromatic moieties interact with CAS and PAS of AChE, and the amide bond enables interaction with BACE-1. In-vitro studies revealed that 3-chloro-N-(2-(2-methoxybenzoyl)-3-oxo-1,2,3,4-tetrahydroisoquinolin-7-yl)benzamide (97) exerted excellent AChE (IC₅₀ = 18.93 ± 1.02 pM) and β-secretase (97.68%) inhibition (Zhao et al., 2017).

Cevik et al. designed and synthesized various substituted quinoxaline-hydrazones and their in-vitro activities were investigated, including cholinesterase and MAO inhibitory activity. (E)-N-methyl-N-(2-(piperazin-1-yl)ethyl)-4-((2-(quinoxalin-2-yl)hydrazineylidene) methyl)aniline (98) exhibited nanomolar inhibitory potency for AChE (IC₅₀ = 0.028 ± 0.001 μM) and MAO-B (IC₅₀ = 0.046 ± 0.002 μM) activity. Molecular modeling suggested that compound 98 could bind to the active site of AChE and MAO-B (Çevik et al., 2020).

Li et al. developed a novel series of pterostilbene-O-acetamido alkyl benzylamines against AD. The derivatives were evaluated as dual inhibitors for AChE and BuChE. They also explored the derivatives for antioxidant, self-induced Aβ aggregation, and hAChE-induced Aβ aggregation inhibition activities. (E)-2-(4-(3,5-dimethoxystyryl)phenoxy)-N-(6-(ethyl (2-methoxybenzyl)amino)hexyl)acetamide (99) was identified as the most active derivative and displayed good inhibitory activity against AChE (IC₅₀ = 0.06 ± 0.03 µM) and BuChE (IC₅₀ = 28.04 ± 1.71 µM). Satisfactory activity was observed against self-induced Aβ aggregation (32.4% ± 1.0%), and hAChE inhibited Aβ aggregation. Kinetic analysis and molecular modeling studies revealed that this derivative exhibited mixed-type inhibition with a binding affinity towards both CAS and PAS of the AChE (Li Y. et al., 2016).

Similarly, Sang et al. reported the design and synthesis of acetamido alkylbenzylamines replacing pterostilbene with scutellarein as multifunctional agents for treating AD. N-(4-(ethyl (2-methoxybenzyl)amino)butyl)-2-(4-(5-hydroxy-6,7-dimethoxy-4-oxo-4H-chromen-2-yl)phenoxy)acetamide (100) was identified as a highly active derivative exhibiting hAChE inhibition (IC₅₀ = 0.039 ± 0.002 µM), moderate self-induced Aβ aggregation inhibition (57.1% ± 1.9%), Cu-induced Aβ aggregation inhibition, and hAChE induced Aβ aggregation inhibition. Also, compound 100 acted as a potential biometal chelator and antioxidant. The improved AChE inhibitory activity was found to be due to good interaction of this molecule with CAS and PAS of AChE. The neuroprotective effect was studied on H₂O₂-induced PC12 cell line and low toxicity in SH-SY5Y cells. Moreover, the scopolamine-induced memory deficit was reversed in mice (Sang et al., 2017b).

Further exploring the alkyl benzylamine scaffold, Zhang et al. developed a series of phthalimide-(N-alkylbenzylamine)cysteamide hybrids based on the multitarget directed ligands (MTDL) strategy. In-vitro study showed that 2-(5,6-dimethoxy-1,3-dioxoisoindolin-2-yl)-N-(3-((2-(dimethylamino)benzyl) (ethyl)amino)propyl)-3-mercaptopropanamide (101) displayed high EeAChE (IC₅₀ = 1.55 ± 0.17 μM) and hAChE (IC₅₀ = 2.23 ± 0.04 μM) inhibition potency, good self-induced Aβ aggregation inhibition (36.08%) and moderate antioxidant effect. Molecular docking revealed the binding of the compound 101 to CAS and PAS of AChE. The neuroprotective effect was also observed against the H₂O₂-induced PC12 cell line (Zhang H. et al., 2021).

Another study conducted by Wieckowska et al., based on the MTDL approach, designed and synthesized a novel series of N-benzyl piperidines containing N-benzyl piperidine moiety combined with phthalimide or isoindole moieties. The most promising results were displayed by compound 102 [(2-(8-(1-(3-chlorobenzyl)piperidin-4-ylamino)octyl)isoindoline-1,3-dione)] against BuChE (IC₅₀ = 0.72 ± 0.038 µM) and Aβ aggregation inhibition (72.5%). Also, improved memory was observed in the scopolamine-induced animal model. Kinetic and docking studies revealed a good molecular interaction with the active site of BuChE (Więckowska et al., 2015).

A group of researchers led by Sang et al. also developed a series of phthalimide-alkylamines as multi-functional agents for treating Alzheimer’s disease. Among them, 2-(3-(benzyl (prop-2-yn-1-yl)amino)propyl)isoindoline-1,3-dione (103) was identified as the most active molecule exhibiting potent and balanced inhibitory activity towards human AChE (IC₅₀ = 1.2 ± 0.07 µM) and MAO-B (IC₅₀ = 2.6 ± 0.05 µM). Kinetic analysis of AChE inhibition and molecular modeling revealed that compound 103 binds to the CAS and PAS site of AChE. Furthermore, this molecule was less cytotoxic (Sang et al., 2017d).

Koca et al. designed and evaluated a series of 5,6-dimethoxy-1H-indene-2-carboxamides as multifunctional drug candidates for AD. N-(4-fluorophenyl)-5,6-dimethoxy-1H-indole-2-carboxamide (104) was identified as the most potent derivative with AChE (IC₅₀ = 2.33 ± 0.021 µM), BuChE (IC₅₀ = 1.08 ± 0.011 µM), and Aβ aggregation (50.3% ± 2.4%) inhibition. These results suggested that compound 104 exhibited more inhibitory activity against BuChE than AChE. Kinetic analysis revealed that these compounds act as non-competitive inhibitors, and docking studies demonstrated the presence of many potential hydrogen bonding interactions with the PAS of BuChE (Koca et al., 2016).

Further, Shahrivar-Gargari et al. studied the carbamates and designed novel indanone-carbamate hybrids by pharmacophore hybridization-based design strategy as anti-Alzheimer’s agents. 3-Chlorophenyl (4-((5,6-dimethoxy-1-oxo-2,3-dihydro-1H-inden-2-yl)methyl)phenyl)carbamate (105) showed the highest inhibition of EeAChE (IC₅₀ = 3.04 ± 0.94 μM), and potent Aβ aggregation (77.5%). Kinetic studies indicated a reversible partial non-competitive type of inhibition. The indanone-carbamate scaffold can be structurally modified and optimized to design novel multitargeted agents against AD (Shahrivar-Gargari et al., 2021).

However, Abedinifar et al. developed and synthesized benzofuran-2-carboxamide-N-benzyl pyridinium halides as novel cholinesterase inhibitors. In-vitro studies revealed that these derivatives are potent inhibitors. Among them, 3-((7-methoxybenzofuran-2-carboxamido)methyl)-1-(2-methylbenzyl)pyridin-1-ium bromide (106) was more potent against BuChE (IC₅₀ = 0.45 ± 0.05 µM) than AChE (IC₅₀ = 2.1 ± 0.1 µM). In addition, a good inhibitory effect on self-induced Aβ aggregation (46.4% ± 2.2%) was also observed. Docking studies revealed hydrogen bonding interaction with the oxygen atom of benzofuran, the amide group’s nitrogen atom, and the benzofuran methoxy moiety (Abedinifar et al., 2018).

While Hiremathad et al. synthesized a series of (3-hydroxy-4-pyridine)-benzofuran hybrids targeting AD. The activity of these molecules was compared with donepezil and N-(2-(3-(benzyloxy)-2-methyl-4-oxopyridin-1(4H)-yl)ethyl)-7-methoxybenzofuran-2-carboxamide (107) emerged as the most active hybrid demonstrating action against multiple targets of AD including AChE inhibitory activity (IC₅₀ = 76 µM) and self-induced Aβ aggregation inhibition (36.1%) (Hiremathad et al., 2018a)

Another study performed by Yun et al. designed and synthesized a series of 2-aryl benzofurans as dual cholinesterase and β-secretase inhibitors. 2-Phenylbenzofuran-4,6-diol (108) demonstrated the potent inhibitory activity against AChE (IC₅₀ = 0.086 ± 0.01 µmolL^-1), BuChE (IC₅₀ = 16.450 ± 2.12 µmolL^-1), and β-secretase (IC₅₀ = 0.043 ± 0.01 µmolL^-1) due to the presence of hydroxyl groups. Compound 108 also displayed low neurotoxicity against normal cells (Yun et al., 2021).

Yang et al. designed a series of 3-arylbenzofuranones and evaluated their cholinesterase and MAO inhibitory activity. Among the series of derivatives, 6,7-dihydroxy-3-(3,4,5-trimethoxyphenyl)benzofuran-2(3H)-one (109) exhibited potent inhibitory activity against AChE (IC₅₀ = 0.089 ± 0.01 μM) and moderate inhibitory activity against MAO-B (IC₅₀ = 149.21 ± 3.39 μM) (Yang et al., 2020).

Later, Maqbool et al. developed cyanopyridine-triazine hybrids and screened them as multitargeted anti-Alzheimer agents. Among the hybrids, 2-(4-(4-((3-chloro-4-fluorophenyl)amino)-6-((3-(trifluoromethyl)phenyl)amino)-1,3,5-triazin-2-yl)piperazin-1-yl) nicotinonitrile (110) exhibited high potency for AChE inhibition (IC₅₀ = 0.059 ± 0.003 µM) with more selectivity for AChE over BuChE and self-induced Aβ aggregation inhibition (83.7% ± 1.13%). Molecular modeling studies revealed these compounds’ interaction with CAS and PAS of AChE. Neuroprotection studies revealed reduced neuronal death induced by H₂O₂-mediated oxidative stress, and in silico studies confirmed drug-like properties (Maqbool et al., 2016).

Continuing the MTDL approach, Sang et al. developed a series of ferulic acid-O-alkylamines for AD treatment. In-vitro studies indicated these derivatives exhibited impressive BuChE and Aβ aggregation inhibition. Notably, (E)-1-(4-benzylpiperidin-1-yl)-3-(4-(4-(3,4-dihydroisoquinolin-2(1H)-yl)butoxy)-3-methoxyphenyl)prop-2-en-1-one (111) was the most potent inhibitor against equine serum BuChE (IC₅₀ = 2.13 ± 0.01 µM), rat BuChE (IC₅₀ = 1.8 ± 0.02 µM) and human serum BuChE (IC₅₀ = 3.82 ± 0.05 µM). Also, potent Aβ aggregation inhibition (50.8% ± 0.82%) and antioxidant activity were indicated. The neuroprotective effect of the active compound with low toxicity against H₂O₂-induced PC12 cell injury and the step-down avoidance test of compound 111 marked a significant reversal of scopolamine-induced memory deficit (Sang et al., 2017a).

Exploring the multifunctional agents, Unsal-Tan et al. developed and synthesized 2-aryl benzimidazoles as multitarget agents against AD. In-vitro studies indicated 2-(4-(4-methylpiperidin-1-yl)phenyl)-1H-benzo [d]imidazole (112) with good inhibitory activity for BuChE (IC₅₀ = 39.56 μM) and also displayed good Aβ anti-aggregation (67.78% ± 0.16%). A molecular modeling study revealed that the compound could reach the catalytic site of BuChE but not AChE. In addition, compound 112 displayed a neuroprotective effect against H₂O₂-induced cell death (Unsal-Tan et al., 2017).

Jalili-Baleh et al. worked on tacrine-like compounds bearing fused pyrazolo [1,2-b] phthalazines and screened for AD treatment. Among them, 15-amino-14-(2-methoxyphenyl)-2,3,4,14-tetrahydro-1H-quinolino [2′,3':3,4]pyrazolo [1,2-b]phthalazine-7,12-dione (113) exhibited higher anti-AChE activity (IC₅₀ = 0.049 µM) than tacrine with high selectivity for AChE over BuChE. Also, the anti-aggregation effect against self-induced Aβ aggregation (25.5% ± 2.9%) was evaluated by ThT fluorescence assay. Cell-based screening of compound 113 against hepatocytes (HepG2) and neuronal cell line (PC12) reported lower toxicity as compared tacrine (Jalili-Baleh et al., 2017).

Another research focused on multitarget agents by Wang et al. designed and synthesized a novel series of cinnamide-dibenzyl amine hybrids against AD. (E)-N-(4-((benzyl (methyl)amino)methyl)phenyl)-3-(3,4-dihydroxyphenyl)acryl amide (114) exhibited significant inhibitory activity against EeAChE (IC₅₀ = 4.64 ± 0.23 µM), hAChE (IC₅₀ = 5.42 ± 0.25 µM), and self-induced Aβ aggregation (56.2% ± 1.21%) with antioxidant and neuroprotective activity and reduced cell death due to oxidative stress in PC12 cell lines. A molecular modeling study suggested that compound 114 targeted both CAS and PAS of AChE (Wang et al., 2017).

Ma et al. designed a series of multitarget ligands deoxyvasicinones by introducing diverse amino acetamide groups at position 6 of the deoxyvasicinone group. In-vitro studies identified 2-((3,5-difluorobenzyl)amino)-N-(9-oxo-1,2,3,9-tetrahydropyrrolo [2,1-b]quinazolin-7-yl)acetamide (115) as the most active compound against hAChE (IC₅₀ = 7.61 ± 0.53 µM) and exhibited moderate to high self-induced Aβ aggregation inhibition (63.9% ± 4.9%). The kinetic analysis confirmed that compound 115 displayed mixed-type inhibition with binding affinity to both CAS and PAS of hAChE (Ma and Du, 2017).

Pandolfi et al. designed pyridines with carbamic or amidic function as cholinesterase inhibitors. Among the series, 5-(benzylamino)pentyl (2,6-dichloropyridin-4-yl)carbamate (116) bearing carbamate moiety exhibited the most potent hAChE inhibition (IC₅₀ = 0.153 ± 0.016 µM). A molecular docking study indicated that compound 116 could bind to AChE by interacting with the enzyme’s CAS and PAS with mixed inhibition. Furthermore, the active compound displayed self-induced Aβ aggregation inhibition (26.5% ± 1.2%) with relatively low toxicity against human astrocytoma T67 and HeLa cell lines (Pandolfi et al., 2017).

Similarly, Jameel et al. also studied multitarget ligands and developed a series of triazine-triazolo pyrimidine hybrids for AD treatment. Among seventeen synthesized compounds, di-substituted triazine-triazole pyrimidine hybrids displayed more potency against AChE. 4-Chloro-6-(4-(5-methyl-[1,2,4]triazolo [1,5-a]pyrimidin-7-yl)piperazin-1-yl)-N-(3-(trifluoromethyl)phenyl)-1,3,5-triazin-2-amine (117) showed the highest activity against AChE (IC₅₀ = 0.065 ± 0.002 µM) and also modulated self-induced Aβ aggregation (75.32% ± 0.34%). Kinetic analysis revealed the interaction of this molecule with the peripheral anionic site of AChE, and in silico studies highlighted the drug-like properties of the derivatives (Jameel et al., 2017).

Zheng et al. reported the design and synthesis of pterostilbene β-aminoalcohols for AD treatment. These derivatives exhibited selective AChE inhibition; (E)-1-(diethylamino)-3-(4-(3,5-dimethoxystyryl)phenoxy)propan-2-ol (118) exhibited the higher inhibitory activity against EeAChE (IC₅₀ = 24.04 ± 1.48 μM) than pterostilbene (less than 5.0% at a concentration of 50 μM). Moreover, compound 118 displayed good self-induced Aβ aggregation inhibition (40.23% ± 1.2%) with moderate antioxidant activity and neuroprotective effect (Zheng et al., 2018).

Erdogan et al. demonstrated the design and synthesis of four compounds with benzoxazolone and benzthiazolone cores as multifunctional agents against AD. Among the derivatives, 6-(3-(4-benzylpiperazin-1-yl)propanoyl)-3-methylbenzo [d]thiazol-2(3H)-one (119) bearing ketone group with benzothiazole core was the most potent analog. In-vitro assay indicated high EeAChE inhibition (IC₅₀ = 0.34 ± 0.16 μM) with moderate anti-self-induced Aβ aggregation (57.5% ± 5.3%). SAR study revealed that the benzothiazole ring was most favorable for AChE and BuChE inhibition, and the ketone group is optimistic for AChE inhibition and the amide group for BuChE inhibition (Erdogan et al., 2021).

Manzoor et al. developed a series of phenyl sulfonyl-pyrimidine carboxylates for AD treatment. Ethyl 2-(4-((4-acetamido-3-chlorophenyl)sulfonyl)piperazin-1-yl)-4-(3,4-dimethoxyphenyl)-6-methylpyrimidine-5-carboxylate (120) among the derivatives displayed excellent inhibitory activity against AChE (IC₅₀ = 47.33 ± 0.02 nM) over BuChE (IC₅₀ = 159.43 ± 0.72 nM). Compound 120 also indicated more potent anti-aggregation activity (51.3%). Enzyme kinetics study revealed a non-competitive type of inhibition and good binding interaction with AChE active site than BuChE suggested by docking. Also, BBB permeability assay and in silico studies reported positive results (Manzoor et al., 2021).

He et al. designed 2-(3-hydroxybenzyl)benzo [d]isothiazol-3-(2H)-ones Mannich bases against AD and demonstrated 2-(3-hydroxy-4-(piperidin-1-ylmethyl)benzyl)-5,6-dimethoxybenzo [d]isothiazol-3(2H)-one (121) to possess high EeAChE inhibitory activity (IC₅₀ = 1.09 ± 0.02 μM) with moderate self-induced Aβ aggregation inhibition (25.0%). In addition, it was also depicted to have metal chelating ability, excellent neuroprotective effect in H₂O₂-induced PC12 cell injury, and good BBB permeability. Moreover, the step-down avoidance test demonstrated that compound 121 had improved scopolamine-induced memory deficit in mice (He et al., 2021).

Gabr et al. developed donepezil analogues as MTDLs against Alzheimer’s disease. BACE-1 inhibition by these donepezil analogues was achieved by introducing amide linkers as the backbone capable of hydrogen-binding with the catalytic site of BACE-1. 1-Benzoyl-N-(3,4-dimethoxyphenyl)piperidine-4-carboxamide (122) emerged as the most active analogues with low nanomolar inhibition against both hAChE (IC₅₀ = 4.11 ± 0.12 nM) and β-secretase (IC₅₀ = 18.3 ± 0.17 nM) than donepezil. Moreover, compound 122 demonstrated metal chelating ability and low toxicity on SH-SY5Y neuroblastoma cells (Gabr and Abdel-Raziq, 2018).

Choubey et al. developed novel N-benzyl pyrrolidine and 1,3,4-oxadiazole hybrids and evaluated them against in-vitro and in-vivo biological activities. Among the synthesized molecules, 1-benzyl-N-((5-(4-(trifluoromethyl)phenyl)-1,3,4-oxadiazol-2-yl)methyl) pyrrolidin-3- amine (123) displayed extensive inhibition against hAChE (IC₅₀ = 0.064 ± 0.006 μM), hBuChE (IC₅₀ = 0.074 ± 0.016 μM), and β-secretase (IC₅₀ = 0.143 ± 0.024 μM). Compound 123 has significant PAS site binding capability, BBB permeability, and neuroprotection ability on SHSY-5Y cell lines. The ex-vivo activity was executed on rat brains and demonstrated reduced AChE levels and oxidative stress (Choubey et al., 2021).

In separate work, Sharma et al. developed a series of N-benzylpiperidine analogues as multi-functional and tested them against Alzheimer’s disease biological targets. 1-Benzyl-N-(4-(trifluoromethyl)benzyl)piperidin-4-amine (124) exhibited excellent inhibitory activity towards hAChE (IC₅₀ = 0.11 ± 0.02 μM) and β-secretase (IC₅₀ = 0.22 ± 0.02 μM). Compound 124 displayed good interaction with the PAS site of AChE, and no detectable neurotoxicity was observed in SH-SY5Y neuroblastoma cell lines. Moreover, the active molecule ameliorated the scopolamine-induced cognitive impairment in elevated plus and Y-maze experiments (Sharma et al., 2019).

Similarly, Saeedi et al. explored the N-benzylpiperidine scaffold and designed a series of N-(1-benzylpiperidin-4-yl)-5-arylisoxazole-3-carboxamides and evaluated them as anti-Alzheimer’s agents, and compound 125 was identified as the best candidate with inhibition of AChE (IC₅₀ = 16.07 ± 0.07 μM), BuChE (IC₅₀ = 15.16 ± 0.22 μM) and BACE-1 (24.3%). A kinetic study indicated mixed-type inhibition for both enzymes and docking study revealed that N-(1-benzylpiperidin-4-yl)-5-(3-nitrophenyl)isoxazole-3-carboxamide (125) fitted well in the enzyme’s active site. Also, this active compound exhibited good metal chelating and neuroprotective activity (Saeedi et al., 2021).

Estrada et al. designed a family of MTDL by linking antioxidant cinnamic-related structures with N-benzyl piperidine or N,N-dibenzyl (N-methyl)amine (DBMA) fragments. The resulting hybrids displayed a balanced biological profile. Among them, (E)-N-(2-(1-benzylpiperidin-4-yl)ethyl)-3-(3,4-dihydroxy phenyl)acrylamide (126) exhibited good activity against human AChE (IC₅₀ = 1.75 ± 0.12 µM), BuChE (IC₅₀ = 0.69 ± 0.12 µM), MAO-A (IC₅₀ = 3.5 ± 0.2 µM) and MAO-B (IC₅₀ = 6.0 ± 0.4 µM). SAR studies revealed that the presence of p-hydroxy groups in a cinnamic acid fragment was essential for getting inhibition and introducing the second hydroxyl at ortho- or meta-increased the inhibitory potency towards MAO. Compound 126 displayed a good neuroprotective effect against human neuroblastoma cell lines SH-SY5Y and also, a neurogenic effect by stimulating the differentiation of adult SGZ-derived neuronal stem cells (Estrada et al., 2016).

Sang et al. designed 2-acetyl-5-O-(amino-alkyl)phenols and evaluated them as multi-function inhibitors for treating Alzheimer’s disease. The results revealed that 1-(4-(3-(4-benzylpiperazin-1-yl)propoxy)-2-hydroxyphenyl)ethan-1-one (127) indicated selective eeAChE inhibitory potency (IC₅₀ = 0.96 ± 0.01 µM) and high MAO-B inhibitory potency (IC₅₀ = 6.8 ± 0.31 µM). Moreover, compound 127 acts as an antioxidant, neuroprotectant, and selective metal-chelating agent (Sang et al., 2017c).

Yang et al. developed salicylaldimines as multi-target-directed ligands for treating Alzheimer’s disease. The biological evaluation identified (E)-4-(((4-(benzyloxy)phenyl)imino)methyl)benzene-1,2,3-triol (128) exhibiting excellent potency for inhibition of self-induced Aβ aggregation (91.3%) and human MAO-B (IC₅₀ = 1.73 ± 0.39 µM). Moreover, compound 128 also displayed remarkable antioxidant, neuroprotective, and significant anti-inflammatory activity (Mezeiova et al., 2021).

Mezeiova et al. designed novel 2-propargyl amino-naphthoquinones as an anti-Alzheimer agent. Among them, 2-(methyl (prop-2-yn-1-yl)amino)naphthalene-1,4-dione (129) exhibited good inhibitory activity against human MAO-A (IC₅₀ = 6.64 ± 0.41 μM) and Aβ aggregation (67.4%). Further, compound 129 displayed a low toxicity and an anti-inflammatory profile in the lipopolysaccharide-stimulated cellular model (Mezeiova et al., 2021). See Supplementary Table 2 for a summary of dual-target inhibitors.

Perez-areales et al. designed, synthesized, and evaluated various derivatives from anti-oxidant lead CR-6 for anti-Alzheimer’s treatment. They have combined two structure backbones of 7-methoxy-2,2-dimethylchroman-6-ol (CR-6) with 6-chlorotacrine with a carbon chain linker. This hybrid molecule demonstrated multiple activities. From this, hybrid N-(8-((6-chloro-1,2,3,4-tetrahydroacridin-9-yl)amino)octyl)-2-(6-hydroxy-7-methoxy-2-methylchroman-2-yl) acetamide (130) indicated potent in-vitro and in-vivo biological activity. Such as hAChE inhibition with IC₅₀ of 3.69 nM, hBuChE inhibition with IC₅₀ of 170 nM, inhibition of DPPH with IC₅₀ of 19.1 µM, inhibition of BACE-1with IC₅₀ of 19.0% µM and Aβ42 percent aggregation inhibition <10, percent tau aggregation inhibition = 15 ± 2.1. In-vivo efficacy study in double transgenic APP/PS1 mice illustrated a positive tendency to improve cognition, amyloid pathology, and oxidative stress (Pérez-Areales et al., 2020).

Jiang et al. designed multi-target-directed ligands as anti-Alzheimer’s agents wherein researchers combined GSK-3β-inhibitor and tacrine as AChE inhibitors via carbon linker, exhibiting multi-targeted activity. 2-(2-(Cyclopropanecarboxamido)pyridin-4-yl)-4-methoxy-N-(3-((1,2,3,4-tetrahydroacridin-9-yl)amino)propyl)thiazole-5-carboxamide (131) indicated the most potent activity from the series of synthesized compounds with AChE inhibition (IC₅₀ = 6.5 nM) and hGSK-3β kinase activity (IC₅₀ = 66 nM). In-vivo study revealed that compound 131 displayed less hepatotoxicity than tacrine. It also indicated potent inhibition of Aβ aggregation at 20 µM. Also, inhibition of tau protein hyperphosphorylation was studied by Western blot analysis at 30 µM (Jiang X. Y. et al., 2018).

Li et al. designed and synthesized a series of aurone Mannich derivatives as multi-functional agents against Alzheimer’s disease. In-vitro assay demonstrated that derivatives are selective AChE inhibitors with multifunctional properties. (Z)-2-(3-Hydroxy-4-(piperidin-1-ylmethyl)benzylidene)-5,6-dimethoxybenzofuran-3(2H)-one (132) exhibited excellent activity against human AChE (IC₅₀ = 0.0371 ± 0.004 µM), self-induced β-aggregation (58.1%), and moderate activity against MAO-B (32%). Moreover, compound 132 also displayed neuroprotective activity against H₂O₂-induced PC12 cell injury and high antioxidant properties (Li et al., 2017).

Leng et al. developed a series of α,β-unsaturated carbonyl-based tetralone derivatives against Alzheimer’s disease. In-vitro experiments revealed that (E)-2-(2-bromo-3,4,5-trimethoxybenzylidene)-4-methyl-3,4-dihydronaphthalen-1(2H)-one (133) displayed inhibitory activity against AChE (IC₅₀ = 0.045 ± 0.02 µM), MAO-B (IC₅₀ = 0.88 ± 0.12 µM), and self-induced β-aggregation (78%). Also, compound 133 displayed a neuroprotective effect against neuronal cell death in PC12 cells (Leng et al., 2016).

Wichur et al. designed 1-Benzylpyrrolidine-3-amine-based derivatives as novel multi-functional agents for treating Alzheimer’s disease. In-vitro studies suggested that 1-benzyl-N-(2-(3-benzylpiperidin-1-yl)ethyl)pyrrolidin-3-amine (134) efficiently inhibited eqBuChE (IC₅₀ = 1.94 ± 0.02 μM), β-aggregation (49%), tau protein (54%), and BACE-1 (24%). Compound 134 also displayed radical scavenging activity and antioxidant activity (Wichur et al., 2020).

Kosak et al. developed a series of N-alkyl piperidine carbamates and evaluated them against AChE, BuChE, and MAO-B. Among them, (1-benzylpiperidin-4-yl)methyl phenylcarbamate (135) was the most promising compound demonstrating activity against AChE (IC₅₀ = 7.31 μM), BuChE (IC₅₀ = 0.56 μM), and MAO-B (IC₅₀ = 26.1 μM). Enzyme kinetics experiments suggested compound 135 as a reversible and non-time-dependent inhibitor for AChE and BuChE. Further, compound 135 was not cytotoxic to human neuronal SH-SY5Y and liver HepG2 cells and prevented β-aggregation induced neuronal cell death (Košak et al., 2020).

Zhu et al. designed a novel series of piperazine derivatives based on the MTDL strategy against Alzheimer’s disease. (R)-1-(2-Hydroxy-4-(2-hydroxy-3-(4-isopropylpiperazin-1-yl)propoxy) phenyl)ethan-1-one (136) was identified as an excellent multi-functional agent depicting activity against eeAChE (IC₅₀ = 7.9 ± 0.26 μM), human MAO-B (IC₅₀ = 9.9 ± 0.79 μM), and BACE-1 (IC₅₀ = 8.3 ± 0.71 μM). Kinetics and molecular modeling study demonstrated that compound 136 had a mixed-type AChE inhibition and good interaction with CAS and PAS site of AChE. Also, compound 136 exhibited good antioxidant activity and neuroprotective effects (Zhu et al., 2021).

Sang et al. developed a novel series of dimethylamino chalcone-O-alkylamines derivatives as multifunctional agents for treating Alzheimer’s disease. Among the derivatives, (E)-1-(4-(4-((2-(dimethylamino)benzyl) (ethyl)amino)butoxy)-2-hydroxyphenyl)-3-(4-(dimethyl amino) phenyl)prop-2-en-1-one (137) displayed the greatest inhibitory activity against self-induced β-aggregation (IC₅₀ = 0.88 ± 0.01 μM), EeAChE (IC₅₀ = 0.69 ± 0.13 μM), and MAO-B (IC₅₀ = 1.0 ± 0.02 μM). Molecular docking study and molecular dynamics simulations provided reasonable explanations for high efficiency. Also, compound 137 exhibited good antioxidant activity and neuroprotective effects (Sang et al., 2021).

Wang et al. synthesized and evaluated chalcone derivatives for anti-Alzheimer activity. The introduction of tetramethylpyrazine to the structure of chalcone, a newer ligustrazine-based compound, was synthesized. These compounds exhibited various target inhibitions, revealing potent anti-Alzheimer activities. From this set of compounds, analog (E)-1-(4-((6,7,8-trimethoxyquinazolin-4-yl)amino)phenyl)-3-(3,5,6-trimethylpyrazin-2-yl)prop-2-en-1-one (138) demonstrated the inhibition of AChE with an IC₅₀ value of 0.10 µM and BuChE with an IC₅₀ value of 22.4 µM. However, this also inhibited MAO-A (IC₅₀ = 47.4 µM) and MAO-B (IC₅₀ = 2.6 µM). Similarly, (E)-1-(2,6-dimethoxypyridin-3-yl)-3-(3,5,6-trimethylpyrazin-2-yl)prop-2-en-1-one (139) displayed inhibition of AChE (IC₅₀ = 0.025 µM), BuChE (IC₅₀ = 2.7 µM), MAO-A (IC₅₀ = 11.4 µM) and MAO-B (IC₅₀ = 8.9 µM). In addition, compound 138 showed better neuroprotection as it is substituted with trimethoxyquinazoline amino moiety than pyrazinyl amino substitution. Moreover, the strong anticholinesterase activity of compound 139 was due to pyridin-3-yl-propanone moiety in the chalcone backbone (Wang et al., 2018).

Rook et al. synthesized and evaluated a series of bivalent β-carbolines. These bivalent β-carbolines act on multiple targets such as AChE/BuChE enzyme and NMDA receptors. This affects both cholinergic and glutamate-induced excitotoxicity to improve treatment. In this series of synthesized agents, 9,9'-(nonane-1,9-diyl)bis (2-methyl-9H-pyrido [3,4-b]indol-2-ium) diiodide (140) demonstrated potent inhibition of AChE (IC₅₀ = 0.5 nM) and BuChE (IC₅₀ = 5.7 nM), whereas it inhibited NMDA receptors with IC₅₀ of 1.4 µM. This bivalent compound has 1000-fold more activity than monovalent compounds. Spacer length in compound 140 should help solubility in cell culture, while more than nine carbon spacer molecules did not show activity. Methylation of second nitrogen gives a permanent positive charge to the compound, increasing activity (Rook et al., 2010).

Viayna et al. synthesized multi-targeted disease-modifying anti-Alzheimer’s agents by combining rhein, huprine, and carbon chain spacer to make a hybrid molecule. Rhein and huprine Y are potent tau aggregation inhibitors that act individually. However, the hybrids of these two molecules inhibited cholinesterase and Aβ-42 aggregation. They have synthesized several racemic and enantiopure hybrid compounds of hydroxyanthraquinone drug rhein and connected to huprine Y via 5 to 11 methylene linkers. This exhibited that multi-targeted activity leads to dual binding inhibition of cholinesterase. Further, they inhibited Aβ aggregation and Tau aggregation inhibition. N-(9-((3-chloro-9-methyl-6,7,10,11-tetrahydro-7,11-methano cycloocta [b]quinolin-12-yl)amino)nonyl)-4,5-dihydroxy-9,10-dioxo-9,10-dihydroanthracene-2-carboxamide (141) showed potent AChE (IC₅₀ = 2.39 nM) and BuChE inhibition (IC₅₀ = 513 nM). In contrast, the ex-vivo activity of compound 141 in hippocampal slices of C57b16 mice proved that this hybrid molecule prevents the loss of synaptic proteins. Although an in-vivo study in transgenic APP-PS1 mice displayed that compound 141 can lower the level of hippocampal total soluble Aβ and reduce APP processing with potent BACE-1 inhibitory activity (IC₅₀ = 80 nM) (Viayna et al., 2014).

Espargaro et al. studied flavonoids and phenolic compounds combined in-vitro and in silico activity as anti-Alzheimer’s agents. Self-aggregation of Aβ peptide is a significant cause of Alzheimer’s disease. Researchers have studied various flavonoids for anti-Alzheimer’s activity by docking, molecular simulation, and Aβ aggregation assay. This study revealed that quercetin (2-(3,4-dihydroxyphenyl)-3,5,7-trihydroxy-4H-chromen-4-one, 142) and apigenin (5,7-dihydroxy-2-(4-hydroxyphenyl)-4H-chromen-4-one, 143) exhibited potent anti-aggregation property (Espargaró et al., 2017).

Ning et al. synthesized and studied the structure-activity relationship of triptolide derivatives for their multi-functional anti-Alzheimer activity. 8a-Isopropyl-10b-methyl-3-oxo-1,2,3,5,5b,6,6a,8,8a,9a,9b,10b-dodecahydrotris (oxireno)[2′,3′:4b,5; 2″,3″:6,7; 2‴,3‴:8a,9] phenanthro [1,2-c]furan-8-yl ((1R,3R,5S,7R)-3,5-dimethyladamantan-1-yl)carbamate (144) is a promising neuroprotective and anti Aβ aggregatory at sub-nanomolar concentration SAR studies revealed that the epoxy group is essential for neuroprotective activity (Ning et al., 2018).

Panek et al. designed, synthesized, and evaluated a novel series of anti-Alzheimer agents. These 1-propane-1,3-diamine derivatives demonstrate multi-functional inhibition of various targets involved in Alzheimer’s disease. It showed activity against cholinesterase, β secretase, Aβ, and tau protein aggregation. From this series of compounds, 1-((3-(tert-butyl)benzyl)amino)-3-((3,3-diphenylpropyl)amino)propan-2-ol (145) displayed good activity with BuChE inhibition IC₅₀ = 7.22 µM while inhibition of β-secretase with IC₅₀ of 41.60 µM. Thioflavin-T assay exhibited inhibition of Aβ aggregation with IC₅₀ value of 3.09 µM and tau aggregation inhibition with IC₅₀ value of 44.4 µM (Panek et al., 2018).

Xu et al. synthesized a novel series of propargylamine-modified pyrimidinylthiourea derivatives as multi-targeted anti-Alzheimer agents. 1-Ethyl-3-(6-(5-((prop-2-yn-1-ylamino) methyl)-1H-benzo [d]imidazol-1-yl)pyrimidin-4-yl)thiourea (146) from this series displays potent dual inhibition with AChE inhibition (IC₅₀ = 0.032 µM) and MAO-B inhibition (IC₅₀ = 2.117 µM). Additionally, compound 146 showed BBB permeability, antioxidant, and in-vivo copper chelating properties. An animal study on alleviating scopolamine-induced cognitive impairment in mice confirmed the inhibition of AChE/MAO-B activity. The presence of the benzimidazole ring in these compounds showed more potent inhibitory activity than the benzopyrazole substitution (Xu Y. et al., 2019).

Xia Xu et al. reported the multi-targeted activity of prenylated compounds obtained from the Psoralea fructus plant, namely, bavachin, bavachinin, bavachalcone, and isobavachalcone. Bavachalcone ((E)-1-(2-hydroxy-4-methoxy-5-(3-methylbut-2-en-1-yl)phenyl)-3-(4-hydroxy phenyl)prop-2-en-1-one, 147) displayed the most potent inhibition of Aβ42 aggregation, antioxidant activity, and AChE inhibition in-vivo and in-vitro. A docking study revealed that bavachalcone showed good binding interaction with the Aβ42 monomer (Xu et al., 2018).

Luo et al. synthesized and evaluated novel graveolinine derivatives as anti-Alzheimer’s agents. From this series of derivatives, 2-(benzo[d][1,3]dioxol-5-yl)-4-(pyrrolidin-1-yl)quinoline (148) expressed the most potent activity with AChE inhibition (IC₅₀ = 0.72 µM) and BuChE inhibition (IC₅₀ = 0.16 µM). It also indicated potent self-induced Aβ aggregation inhibition (62.52%) studied on Thioflavin-T assay. A molecular docking study displayed that quinoline moiety establishes cation-pie interaction with amino acids, while nitrogen from pyrrolidine shows hydrogen bond interaction with the carbonyl group of amino acids (Luo et al., 2020).

Simone et al. evaluated first-class GSK-3β/HDAC dual inhibitors as disease-modifying anti-Alzheimer’s agents. Histone deacetylase (HDAC) and glycogen synthase kinase 3β are vital targets in Alzheimer’s disease for drug discovery. These are designed by connecting hydroxamic acid with the phthalimide by carbon linker and thioamide functional group. From this series of dual inhibitors, 6-(3-(1,3-dioxoisoindolin-5-yl)thioureido)-N-hydroxy hexanamide (149) showed potent in-vitro activity with GSK-3β inhibition (IC₅₀ = 2.69 μM) and inhibition of HDAC1 (IC₅₀ = 12.78 μM), and HDAC6 (IC₅₀ = 3.19 μM). According to a docking study, compound 149 indicated good H-bond interaction with active site residues of the enzymes. Moreover, compound 149 induced an increase in histone acetylation and reduced tau phosphorylation in in-vitro enzyme assays (De Simone et al., 2019).

He et al. designed, synthesized, and evaluated hydroxamic acid-based compounds as a dual inhibitor of N-methyl-D-aspartase receptor (NMDAR) and HDAC for Alzheimer’s disease. As NMDA and histone deacetylase play important roles in neurodegenerative disorders, they are targeted for discovering novel anti-Alzheimer’s agents. A novel series of compounds were synthesized by linking aliphatic chains resembling a linker and aromatic chains, utilizing HDAC inhibitor SAHA and NMDAR inhibitor memantine as precursors. In-vitro HDAC inhibition and NMDAR study reveal that 4-((E)-3-(((1S,3S,7S)-3,5-dimethyladamantan-1-yl) amino)-3-oxoprop-1-en-1-yl)-N-hydroxybenzamide (150) exhibited potent inhibition of HDAC6 (IC₅₀ = 0.18 μM) and of NMDAR (K_i = 0.59 μM). Further study confirmed a selective increase of the levels of HDAC6-directed substrate acetyl-tubulin in plasma. In addition to the neuroprotective properties, compound 150 was also less hepatotoxic (He et al., 2020).

Patel et al. synthesized carbazole-stilbene hybrids as multi-targeted anti-Alzheimer agents. The fusion of carbazole with stilbene-designed hybrids showed activity against multiple targets, such as cholinesterase inhibition, Aβ aggregation inhibition, and anti-oxidant and metal chelating properties. From this hybrid, thiourea substituted (E)-1-(4-(2-(9-ethyl-9H-carbazol-3-yl)vinyl)phenyl)-3-(2-(pyrrolidin-1-yl)ethyl)thiourea (151) displayed potent activity with inhibition of AChE (IC₅₀ value of 2.64 μM) and BuChE (IC₅₀ value of 1.29 μM) and Aβ1–42 aggregation (51.29% at 25 μM concentration). It also possessed copper chelation properties. Docking study revealed that compound 151 exhibited strong covalent binding interaction with the active site of AChE, BuChE, and Aβ peptides (Patel et al., 2020).

Titov et al. reported nitrogen-bridged cyclopenta [a]indenes as novel anti-Alzheimer’s agents. Several molecules were designed, synthesized, and evaluated for their biological activity. 1-(3a-Isopropyl-5,6-dimethoxy-10-methyl-1-phenyl-3,3a,8,8a-tetrahydro-3,8-(epiminomethano)cyclopenta [a]inden-2-yl)ethan-1-one (152) expressed potent inhibition of butyrylcholine esterase with IC₅₀ of 0.034 µM and acetylcholine esterase with IC₅₀ = 20.1 µM. It was influential in neuroprotection and also confirmed less cytotoxicity and good brain permeability. The docking study revealed that compound 152 exhibited hydrophobic interaction with BuChE binding site, presumably enhancing the inhibitory potency and selectivity over the AChE active site (Titov et al., 2021).

Pasieka et al. tested the library of 1-benzylamino-2-hydroxyalkyl as a multi-functional anti-Alzheimer’s agent and identified it as a dual aggregation inhibitor. From all the tested derivatives, 1-((3-(t-butyl)benzyl)amino)-3-((2,2-diphenylpropyl)amino)propan-2-ol (153) exhibited potent activity. In-vitro inhibition of hBuChE displayed IC₅₀ of 5.74 μM, inhibition of hBACE1with IC₅₀ of 41.6 μM and Aβ aggregation inhibition with IC₅₀ = 3.09 μM). The docking study indicated hydrophobic interaction with amyloid (Pasieka et al., 2021). See Table 5 for a summary of multi-target inhibitors.