Two literature searches were performed on the role of NE and α-ARs in MDD and schizophrenia. A PubMed search was carried out on December 11, 2015 and a ProQuest search was carried out on December 18, 2015. Both searches were conducted using the following Medical Subject Heading (MeSH) term search string: “norepinephrine” OR “noradrenaline” OR “alpha adrenergic receptor(s)” OR “beta adrenergic receptor(s)” AND “schizophrenia” OR “major depressive disorder” AND “translational medicine” OR “immunity” OR “microglia” OR “astrocyte(s)” OR “inflammation” OR “gene(s)” OR “brain chemistry” OR “biomarker” OR “neuronal plasticity” OR “cognition” OR “arousal” OR “sleep” OR “psychopharmacology” OR “brain development.” The original searches were limited to the period January 2008–December 2015 and publications in the English language.

The searches yielded a total of 2,427 publications (PubMed, n = 669; ProQuest, n = 1,758). After exclusion of duplicates, articles deemed not relevant, case studies, reviews and meta-analyses, preclinical reports, or articles concerning other indications, abstracts, and full-length text were independently screened for eligibility by all the authors. To focus the review on the most recent information, it was decided that only articles published during the period January 2010–December 2015 would be included in full article screening. Psychotropics used in the treatment of MDD and schizophrenia do not generally exert a direct effect on β-ARs, with these receptors only influenced by a change in overall NE transmission. While some adverse events of psychotropics may be mediated by β-ARs, in order to focus the review on the role of NE related to the pathophysiology of psychiatric disorders, the review was limited to articles discussing the actions of NE at α-ARs only and on drugs with at least a moderate affinity for α-ARs (K_i < 100 nM). A total of 16 research reports were identified as meeting these inclusion criteria (Figure 2) including six clinical trial reports, six genetic studies, two biomarker studies, and two receptor studies (Table 1).

Many investigations have been carried out to determine genetic or metabolic signatures associated with MDD and schizophrenia. As well as providing insights into the pathophysiology of these disorders, these reports may assist clinicians with predicting how patients will respond to therapy and providing more personalized care. We identified six reports investigating the genetic variants of noradrenergic receptors or proteins expressed within the noradrenergic synthetic pathway, and their relationship to either symptoms of MDD and schizophrenia or the side effects of treatment with agents that have activity at α-ARs. We also identified two studies investigating NE metabolites as biomarkers of MDD and schizophrenia, and two studies investigating the binding or distribution of NE-associated receptors or transporters.

The RDoC negative valence system domain includes fear and anxiety (13), and can, along with disturbances in cognitive domain, be used to categorize some of the positive symptoms of schizophrenia, such as hallucinations (60). A biomarker study showed that elevated NE may be associated with cognitive disorganization, poor impulse control, suspiciousness, hostility, and hallucinations (61). Our findings also suggest that NE manipulation can potentially affect the positive symptoms associated with schizophrenia (43, 44), with the long-term study of adjunctive mirtazapine in patients with schizophrenia showing it improved PANSS positive scores (43), although, this may also be related to modulation of several 5-HT receptors (62). The effectiveness of mirtazapine in schizophrenia is supported by a preclinical study that showed that mirtazapine enhanced the AP activity of haloperidol in an apomorphine-induced climbing test in mice (63). Mirtazapine acts as an antagonist of α₂-ARs, as well as serotonin 5-HT₂ and 5-HT₃ receptors (30), so that when used in combination with a first generation AP such as the D₂ receptor antagonist haloperidol, the overall pharmacological profile resembles that of clozapine (43), which was reported to be superior to haloperidol for treating positive symptoms of schizophrenia (64). These findings are also supported by the pharmacological properties of brexpiprazole, a partial agonist at serotonin 5-HT_1A and DA D₂ receptors, and a potent antagonist at serotonin 5-HT_2A and NE α_1B/2C receptors, all at similar potencies (36). Studies with brexpiprazole, recently approved for the treatment of schizophrenia, have demonstrated AP activity in rat models of the positive psychotic symptoms of schizophrenia (65), as well as significantly improved PANSS positive scores in patients with schizophrenia (37).

Compromised ability to think or concentrate is one of the diagnostic features of MDD. An imaging study showed that hyperactivity of the frontal and prefrontal cortices, areas of the brain innervated by noradrenergic neurons, is required for depressed patients to complete a working memory task at a level similar to healthy controls (66). Several cognitive processes, including attention and working memory, have been shown to be linked to NE activity (5). Indeed, cognitive defects in chromosome 22q11 deletion syndrome are associated with the abnormal function of several neurotransmitters, including NE (52). Furthermore, clonidine may exert dual activity by engaging inhibitory presynaptic α₂-ARs, and therefore suppressing NE activity, while at the same time directly stimulating prefrontal cortex postsynaptic α₂-ARs (39). Our review identified a study in which clonidine suppressed memory consolidation in patients with MDD and healthy controls (40). This role of α₂-ARs in learning and memory consolidation is supported by preclinical studies in rats (67, 68), although Kuffel et al. (40) found no effect of noradrenergic blockade on working memory in patients with MDD or healthy participants. This is in contrast to an infusion study in which α₂-AR agonists applied directly to the prefrontal cortex of monkeys and rats resulted in improved working memory performance (69). In addition, it is thought that the α_2A-AR subtype may be the most important for cognitive improvement (5), as the α_2A selective agonist guanfacine is more effective at improving working memory without side effects than clonidine, which also acts at α_2B- and α_2C-ARs (70). High concentrations of NE have also been shown to reduce working memory function through actions at α₁-ARs; indeed, stress-induced cognitive deficits have been shown to be blocked by infusion of an α₁-AR antagonist into the prefrontal cortex of rats (71). Therefore, the balance between the activation of α_2A-ARs and reducing the activity of α₁-ARs may be a factor for consideration when designing pharmacological agents for the improvement of cognitive functions in MDD.

Recent studies have indicated a role for α₁- and α₂-ARs in regulation of cognitive processes, where α₂-AR stimulation may ameliorate working memory deficits and α₁-AR agonism may enhance sustained attention (72). Preclinical studies point to a differential role for subtypes of α₁-ARs in cognition. While activation of α_1A-ARs may have a positive impact on cognition and neurogenesis, α_1B-mediated signaling may be detrimental to cognition and promote apoptosis (73, 74). Furthermore, while α_2A-AR activation mediates improvement in working memory following guanfacine treatment (75), activity at α_2C-ARs may also mediate stress-related psychiatric diseases such as MDD and anxiety disorders (76). Furthermore, α_2C-AR antagonism may be associated with a pro-cognitive effect, in addition to ameliorating anxiety and depression (77). Thus, selective modulation of α-AR subtypes may be advantageous in therapy of MDD. This is indirectly supported by the pharmacological profile of brexpiprazole, which has antagonist activity at both α_1B- and α_2C-ARs (36), and has been shown to be an efficacious adjunctive treatment for patients with MDD (38).

In schizophrenia, defects in the early sensory filter mechanisms are thought to result in cognitive fragmentation, and ultimately hallucinations and delusions (78). Reduced filtering of sensory and sensorimotor information, demonstrated by both a reduced P50 suppression or reduced pre-pulse inhibition of the startle reflex, was corrected by activating α₂-ARs with clonidine (39, 42). Other evidence from our search showed that mirtazapine increased mental speed and attention control in schizophrenia (44), which may be related to its activation of α₂-ARs.

Glutamate has been shown to be crucial for cognitive processing, and pharmacological agents that modulate glutamate transmission, such as ketamine, have demonstrated ADT-like properties (14). Our search results suggested that glutamate transporter gene expression was reduced in LC astrocytes in postmortem brain tissue of patients with MDD (3). LC–NE activity is modulated by glutamatergic input, and so changes in glutamate levels could also indirectly impact the NE signaling. Elsewhere, increased glutamate levels have been reported in the occipital cortex, prefrontal cortex, and plasma of patients with MDD (79–81). Therefore, the benefit of glutamate modulators may in part be due to indirect actions on NE activity.

There was little direct evidence from our review to support a role of NE and α-ARs in the positive valence systems, systems for social processes, or arousal/regulation systems associated with MDD and schizophrenia. However, other studies outside the selection criteria for this review provided some data. Negative symptoms of schizophrenia, such as flat affect and poverty of speech, can be categorized into the social process RDoC system (13). Clinical studies have shown that mirtazapine enhanced the effects of haloperidol, risperidone, and clozapine on negative symptoms (82–84), which support the identified study that showed adjunctive mirtazapine improved PANSS negative scores (43).

Disruptions in sleep cycles and circadian rhythms are common in patients with MDD (85). Moreover, genetic studies have suggested that patients with MDD have both a phase shift of rhythms and a disrupted regulation of circadian genes (86). Since NE neurons project to the hypothalamus, which contains the suprachiasmatic nucleus—the master pacemaker, which coordinates rhythms throughout the brain and body (85), it is possible that NE has a role in modulating these effects. As reviewed elsewhere, imaging studies provide evidence of sleep disruption due to excessive arousal in MDD, while biochemical studies point to an association between elevated NE levels and decreased sleep efficiency (87). Thirty-hour sampling of CSF samples from depressed patients has found elevated NE relative to healthy controls around the clock (88).

When considering individual patient needs, biomarkers which aid in the diagnosis of patients or predict responses to treatment are valuable for successful therapeutic intervention. MDD and schizophrenia were originally thought to be diseases located entirely in the CNS, although recent hypotheses and findings suggest that the pathophysiology of these diseases can be shaped by peripheral endocrine, autonomic, immune, and gut-brain events (24, 89, 90). Several metabolic studies have attempted to identify potential biomarkers for MDD and schizophrenia by assessing changes in enzymatic activity in plasma and saliva. Baseline levels of MHPG in saliva were shown to positively correlate with a high Beck Depression Inventory score in men (19), which provides support to the findings that MHPG concentrations in CSF were correlated with a lifetime burden of mood swings (18). In addition, plasma MHPG has been shown to correlate with negative symptoms and cognitive impairment during early-stage schizophrenia (91).

A patient’s NE metabolites or genetic profile may also help to predict how well they will respond to different treatments, not only with regards to improving symptoms, but also the emergence of adverse events. A study found that patients with MDD that responded to mirtazapine or SSRI treatment had higher baseline saliva MHPG concentrations, although this did not reach statistical significance in patients receiving mirtazapine alone, or when it was used as adjunctive therapy with SSRIs (47). Similarly, risperidone, which acts as an antagonist of α₁- and α₂-ARs (as well as other receptors), was shown not to affect NE, vanillylmandelic acid, or MHPG in the plasma or urine of patients with schizophrenia (35).

Genetic studies identified here suggested that differences in the gene which codes for α_1A-AR are associated with weight gain (50) and metabolic abnormalities (49) during AP treatment of schizophrenia. However, there are many factors that affect weight gain in patients with schizophrenia, and attribution of this adverse reaction to a single receptor type is inappropriate. For example, it has been shown that antagonism of the DA D₂ receptor has both an effect on eating, mediated by 5-HT_2C receptors, and disinhibition of prolactin secretion, which has an impact on lipid and glucose metabolism (92).

The atypical AP olanzapine and the SSRI fluoxetine are often used in combination in patients with treatment-resistant MDD. Previously, olanzapine and fluoxetine have been shown to have a synergistic effect on elevation of NE and DA levels in the rat prefrontal cortex (93), which may be responsible for some of the efficacy of this combination therapy. Therefore, genetic variants in the NET identified in patients with MDD who were not initially responsive to fluoxetine alone may be a marker to predict improvements in these patients after switching to olanzapine–fluoxetine combination (45). Quetiapine was also shown to occupy NET in healthy patients at doses that produce antidepressive effects. This may explain the unique broad spectrum efficacy of quetiapine therapy in psychiatric disorders (55).

The higher density of α₂-ARs in both ADT-free and antidepressant-treated patients with depression compared with matched controls suggests that these receptors are resistant to the observed downregulation of β₁-ARs by ADTs (48). In a preclinical study in rats, treatment with the SSRI citalopram did not result in any adaptive changes in LC neurons, but did indirectly enhance the inhibitory effect of NE on neurons in the LC (94). The activation of inhibitory α₂-ARs resulting from elevation of NE concentrations in the synaptic cleft may underlie this effect (94). Although, desensitization of these receptors may also have occurred, as previously observed in animal studies (95, 96). Furthermore, preclinical evidence also suggests that intact α₁-AR-mediated signaling may be necessary for SSRI induced 5-HT elevation (97).

Both MDD and schizophrenia have been associated with immune abnormalities and dysfunctional inflammatory signaling (98, 99). Elevated peripheral inflammation may precipitate aberrant CNS inflammatory signaling with subsequent disruption of monoamine and glutamate transmission, in part by inappropriately activating brain microglia (100). Both α- and β-ARs have a key role in regulating macrophage and microglia activity (101, 102). Thus, compromised NE transmission may promote a pro-inflammatory phenotype consistent with depressive psychopathology. Intriguingly, a recent study reported a preferential response to an SSRI (escitalopram) in patients with lower levels of an inflammatory marker [C-reactive protein (CRP) <1 mg/mL], compared with depressed patients with higher inflammation (CRP > 3 mg/mL) who had a robust response to a predominantly noradrenergic ADT (nortriptyline) (103). Therefore, one may speculate that noradrenergic ADTs exert some of their therapeutic effect by attenuating excessive inflammatory signaling.

The objective of our systematic review was to determine the role of NE and α-ARs in the pathophysiology of MDD and schizophrenia using evidence from clinical reports. In order to achieve this, a number of specific search terms were implemented, including the use of “alpha adrenergic receptor(s)” as a limiter in the MeSH search-term string. Therefore, any reports that did not contain this term were excluded, even though they may indirectly support the role of NE activity at α-ARs in MDD or schizophrenia. It should also be noted that in order to focus this literature review on recent data, the scope was restricted to publications between 2010 and 2015, which will limit our findings. Finally, it is a daunting challenge to attempt to link receptor activity to specific therapeutic effect, especially as many of the drugs discussed in this review have clinically relevant binding affinities for a number of different receptors, and additionally, these diseases are phenotypically, genetically, and biologically heterogeneous. The lack of a common pathophysiology or homogenous symptom presentation between all patients diagnosed with MDD or schizophrenia will impact the summary of effects linked to α-AR modulation. Moreover, it has been reported that females have a larger LC than males, comprising nearly 3,000 more neurons, which could impact their capacity for NE production and release (104). Given these neurobiological differences, we suggest that gender should be considered as a factor in future clinical studies.