Classical CADASIL is caused by mutations in the NOTCH3 gene located on chromosome 19p13, which is involved in the differentiation and maturation of vascular smooth muscle cells, vascular development during embryogenesis, and vascular integrity. The NOTCH3 gene contains 33 exons and encodes a transmembrane receptor consisting of three structural domains, including the NOTCH extracellular domain (NECD), the transmembrane domain, and the NOTCH intracellular domain (NICD) (5). Among these, exons 2–24 encode Notch3^ECD, which includes 34 epidermal growth factor-like repeats (EGFr), each of which typically includes highly conserved six cysteine residues that form three disulfide bonds. Mutations in the NOTCH3 gene in CADASIL always cause an increase or deletion in the number of cysteine residues within 1 of the EGFr, resulting in an odd number of cysteine residues (usually 5 or 7). That unpaired cysteine residue, which is expected to disrupt normal disulfide bond formation, leads to misfolding of EGFr and increased NOTCH3 multimerization, ultimately causing GOM formation (6). GOM formation has been recognized as a typical pathologic features of CADASIL and has been validated in most patients with classical CADASIL.

Heterozygous missense mutations causing altered cysteine numbers have long been recognized as the typical mutational form of CADASIL, and this pathogenic mutation is located on exons 2–24 encoding the 34 EGFR structural domains. In particular, exon 2–6 is considered a mutational hotspot (7).

With advances in gene sequencing and more and more studies, we have found that some patients harboring NOTCH3 missense mutations that preserve cysteine, in particular the p. Arg61Trp, p. Arg75Pro, p. Asp80Gly and p. Arg213Lys mutations, exhibit clinical syndromes consistent with CADASIL, and skin biopsies of these patients have also found GOM deposits in their skin (8). The newly identified p. Gly73Ala, p. Arg75Gln, p. Ser1418Leu and p. Arg1761His mutations are also potentially pathogenic (9). Converging evidence suggests that in the genetic profile of NOTCH3 cysteine-sparing mutations, mutations are more frequently detected in exon 3, with p. Arg75Pro being the most common type.

In addition to this, many other mutations in NOTCH3 have been reported in recent years, causing CADASIL-like clinical phenotypes. The first category is some reports on homozygous mutations. There is a case report of a homozygous missense mutation c. C1759T (p. Arg587Cys) in NOTCH3 gene found in two brothers from China, both patients showed stroke, gait instability, cognitive impairment and psychiatric disorders. Fused white matter hypersignal and multiple lacunar infarcts were demonstrated on MRI, especially by skin biopsy which revealed characteristic GOM deposits in these two patients (10). Consistently, Tuominen et al. also described a patient with a homozygous mutation in NOTCH3 causing a CADASIL-like clinical phenotype, with the mutation located in c. C475T (p. Arg133Cys), and found GOM deposits (11). However, there have also been case reports of earlier onset and more severe disease phenotypes in patients with pure mutations compared with classic CADASIL (12). Overall, the phenotypes of patients with pure synaptic mutations described to date are almost exclusively within the normal CADASIL spectrum, and the reasons for the variation in clinical severity need to be further explored. The second group consists of small NOTCH3 deletions, duplications, splice site mutations and a deletion/insertion leading to a numerical cysteine alteration. These patients exhibit a classic CADASIL-like clinical phenotype and most of them underwent biopsy with clear GOM deposition (13, 14). Consistent with classical NOTCH3 mutations, almost all of these reported mutations involve alterations in the number of cysteine residues in EGFr, and thus they may be lethal. The paucity of reports of such mutations may be due in part to technical limitations of direct sequencing that miss intronic mutations, large deletions, multiplications, or large rearrangements of the NOTCH3 gene. However, a CADASIL phenotype caused by a 12-base pair deletion that does not result in a change in the number of cysteines was reported in one study. This deletion may alter the spacing between the two cysteines in EGFr, resulting in disruption of the normal disulfide bond (15). The last category is NOTCH3 loss-of-function mutations, including nonsense mutations causing premature stop codons and frameshift deletion. Such mutations do not trigger changes in the number of EGFr cysteine residues and GOM deposition, but cause hereditary small vessel disease phenotypes of varying severity or penetrance, similar to CADASIL (16–19). Although some NOTCH3 mutations outside the exons encoding EGFr have also been reported, whether these mutations cause the CADASIL phenotype remains highly controversial, and more patients with such mutations should be found and examined to clarify the conclusions (20–23).

In summary, in the past 30 years since the identification of classical mutations in the CADASIL-causing gene NOTCH3, we have identified an increasing number of novel NOTCH3 variant types that exhibit clinical manifestations similar t1o those of CADASIL, implying a diversification of the NOTCH3 genotypes that cause CADASIL, partly explaining why this disease is much more prevalent than initially assumed, and is even considered to be the most common type of inherited vascular dementia (Table 1). Therefore, we believe that continuous additions to the CADASIL mutational spectrum are essential to clarify the diagnosis of this disease. However, to avoid erroneous mutation interpretations and diagnoses, our analysis of these patients with NOTCH3 mutations should always include comprehensive NOTCH3 molecular screening, as well as comprehensive clinical (re)evaluation, including skin biopsie.

To date, there have been many genotype–phenotype correlations on NOTCH3 mutations caused by typical cysteine alterations. Several studies have been conducted to analyze the genotype–phenotype correlations from several common specific mutant types (Table 2).

Rutten et al. found from a large-scale genetic variation database study that the frequency of EGFr cysteine-altered NOTCH3 mutations in the general population was 3. 4/ 1,000, a frequency 100-fold higher than the currently estimated prevalence of CADASIL. Those individuals, in whom the mutation accumulates predominantly in EGFr 7–34, have an increased lifetime risk of developing stroke and vascular dementia, albeit with a later onset than in classic CADASIL patients. In contrast, in patients with CADASIL, typical cysteine-altering mutations are predominantly located in EGFr 1–6 (6). This led us to realize that the spectrum of diseases with NOTCH3 mutations could be very broad, including CADASIL. subsequently, in a further study, Rutten et al. demonstrated that in patients diagnosed with CADASIL, mutations in EGFr 1–6 predispose to the classical, more severe CADASIL phenotype, whereas pathogenic variants in EGFr 7–34 more frequently lead to a milder phenotype. Specifically, patients with mutations in EGFr 1–6 had an earlier age of stroke onset by 12 years, shorter survival, and increased white matter high-signal volume compared with patients with mutations in EGFr 7–34, which is consistent with a previous study in Japan (33). Hack et al. reported a novel three-tiered risk classification for the NOTCH3 variants that included not only EGFr structural domains 1–6 but also EGFr structural domains 8, 11, and 26 in high risk, as they found that patients with variants in EGFr structural domains 8, 11, and 26 had similar imaging burden and clinical presentation as patients with variants in EGFr structural domains 1–6 (34). A recent large cohort study not only confirmed the finding that pathogenic variants in EGFr 7–34 cause a milder clinical phenotype than pathogenic variants in EGFr 1–6, but further found that the severity of stroke was similar in EGFr 1–9 and 18–34, and that patients with variants in EGFr 10–17 had a lower risk of stroke than those with EGFr 3–4 (35). Similar to classical CADASIL, the location of mutations in the NOTCH3 retention cysteine gene likewise influences the severity of the disease: exons 1–6 mutations present a more severe clinical manifestation compared to retention cysteine mutations in exons 7–34. This further explains the fact that the cysteine-sparing mutations that have been diagnostic of CADASIL to date are more frequently detected in exon 3: since these patients have more severe clinical manifestations and disease progression, they are more likely to be detected and diagnosed (8, 9).

The current study allows us to confirm location-dependent genotype–phenotype correlations in CADASIL, and that the location of NOTCH3 pathogenicity variants is a key determinant of disease severity in CADASIL, above cardiovascular risk factors and gender, which is an important guideline for the development of a predictive model for NOTCH3 to help us to identify these patients at risk for early onset, severe disease. We need to further explore the molecular mechanisms associated with the location of pathogenic variants of NOTCH3.

There are many reports of NOTCH3 cysteine-sparing mutations with CADASIL-like clinical manifestations. Although the clinical presentation and imaging of patients with NOTCH3 cysteine-sparing mutations are similar to those of classical CADASIL, they are not identical. Cysteine-sparing mutations have a later onset of symptoms than cysteine-associated mutations: the mean age of patients with CADASIL presenting with neurological signs or symptoms is 45–51. 3 year, particularly in men at approximately 50 years and in women at approximately 53 years (36), whereas carriers of NOTCH3 cysteine-sparing mutations have a mean age of 53. 64 years. The most common clinical manifestations in patients with NOTCH3 cysteine-sparing mutations are gait disturbance, cognitive impairment and stroke. The most common cerebral radiologic manifestations were lacunar cerebral infarction and cerebral microhemorrhage. Compared with patients with classical CADASIL, patients with NOTCH3-preserved cysteine mutations had a significantly higher frequency of cognitive impairment and cerebral microhemorrhages, whereas anterior temporal pole and external capsule white matter high signal was rarely observed. The relatively milder white matter involvement in two specific locations, the anterior temporal pole and the external capsule, may be an imaging feature of NOTCH3-preserved galactorrhea mutations (9). We speculate that this may be because the unique convoluted structure and vascularization of the temporal pole is particularly susceptible to myelin depletion or edema, which may result from aggregation of NOTCH3^ECD and microvascular changes (37). In patients with preserved cysteine mutations, these mutations are less involved in GOM deposition and have less effect on interstitial fluid drainage and white matter thinning. This may partly explain the different effects observed for different mutation types in the CADASIL phenotype. However, we need to standardize MRI protocols to ensure consistent detection and characterization of white matter lesions and vascular abnormalities across different patient populations. p. Leu1518Met is a variant located outside of the EGFr region that does not involve a change in the number of cysteines, and Park et al. have reported this variant in a GOM-positive patient with CADASIL (38). Schmidt et al. have linked the p. Leu1518Met variant to be associated with severe white matter lesions (39). p. Leu1518Met was detected in a 36-year-old female patient with severe neurological symptoms and a 47-year-old male patient, both of whom showed extensive white matter involvement on neuroimaging, suggesting that the p. Leu1518Met variant is associated with severe white matter lesions (40). In addition to this, patients with a homozygous NOTCH3 mutation also seem to exhibit a clinical phenotype belonging to the classical clinical spectrum of CADASIL, whereas some reports have emphasized an increased disease severity in homozygous carriers, the exact mechanism of which is still unclear (41).

In summary, the location and type of mutation are major determinants of the clinical phenotype, and further studies are needed to clarify the relationship between CADASIL genotype and phenotype and the underlying mechanisms. However, the manifestation and severity of the disease cannot be explained solely by genotype–phenotype, but may also vary among different races and family lines with the same mutation (42), or even among identical twins (43). This may be related to modifier genes, environmental influences, or other concomitant risk factors that together determine the clinical heterogeneity of the disease.

In the past, it was thought that NOTCH3 mutations caused pure cerebral small-vessel disease-classical CADASIL. However, several studies have shown that NOTCH3 mutations may be present in a variety of intracranial large-artery anomalies causing infarcts associated with large-artery disease, with most of the patients having altered cysteine (44). Eun J (45) and Hyun (44) both confirmed in their clinical studies that intracranial large artery stenosis may not be an incidental phenomenon unrelated to mutations in the NOTCH3 gene. In a study from China, 28 of 37 CADASIL patients (75. 7%) had intracranial large artery anomalies. Usually WMH distribution is symmetrical in CADASIL, but this study suggested that intracranial large artery disease in CADASIL patients may cause an asymmetrical WMH pattern, which may be due to large artery anomalies altering hemodynamics and exacerbating the WMH in the corresponding region. Therefore, this characteristic imaging manifestation could be an important marker of intracranial large artery stenosis in patients with NOTCH3 (46). Hyun et al. suggested that intracranial large artery stenosis in patients with CADASIL may preferentially involve relatively small intracranial arteries because in these patients, the arterial stenosis is usually located in the anterior cerebral artery, the anterior inferior cerebellar artery, or the middle cerebral artery distal to the smaller vessels M1 and M2 (44). This clinical evidence suggests that NOTCH3 mutations cause more than cerebral small-vessel disease and have an important association with intracranial large-artery stenosis, although most cases have been described only in East Asia. One autopsy showed GOM deposition in the aorta, carotid and renal arteries of a patient with CADASIL (47). An autopsy of a patient with CADASIL in Japan showed arterial stenosis in the basilar, internal carotid, anterior cerebral, middle cerebral, and posterior cerebral arteries, which exhibited atherosclerotic changes in the absence of any risk factors (48). Therefore, we hypothesized that stenosis of large intracranial arteries may be related to atherosclerosis, and that endothelial cell damage associated with GOM deposition accelerates the progression of atherosclerosis. In addition to stenosis of the great arteries, congenital anomalies of the intracranial great arteries in CADASIL patients have also been reported, including basilar artery fenestration, vertebral artery (VA) hypoplasia or agenesis, anterior cerebral artery (ACA) shares common trunk, and fetal posterior cerebral artery (FPCA). However, whether these congenital abnormalities of the cerebral vasculature share a common pathogenesis with the stenosis that develops later in life is unclear, and whether these changes are part of the NOTCH3 mutant phenotype has not been further investigated (46).

The mechanism by which NOTCH3 mutations cause atherosclerosis in large arteries has been less well studied. Atherosclerosis is a chronic inflammatory disease caused by the interaction of lipids, macrophages/foam cells and arterial wall cells (49). Chronic inflammation is central to the pathology of atherosclerotic vascular disease and metabolic disorders. In particular, macrophages are involved in the expanded cascade of reactions and play a key role in maintaining the inflammatory response in atherosclerotic plaques, promoting their structural instability, and thrombus formation (50). There are multiple NOTCH3 receptors and ligands expressed in macrophages, among which DII4 and NOTCH3 are co-localized in macrophages within atherosclerotic plaques (51). Fung et al. revealed the role of the DII4-NOTCH pathway in the inflammatory response characterized by macrophage activation: stimulation of pro-inflammatory factors such as LPS and IL-1β increased the expression of DII4 in macrophage expression, triggered hydrolysis and activation of NOTCH proteins, and induced pro-inflammatory molecules and pathways, such as inducible nitric oxide synthase (iNOS), pentraxin 3 (PTX3), mitogen-activated protein kinase (MAPK), Akt, and NF-κB. Notably, DII4-triggered NOTCH signaling increased the expression of DII4 itself, which further demonstrates that the DII4-NOTCH signaling pathway mediates the inflammatory response by accelerating is a positive feedback loop of cell activation leading to atherosclerotic plaque loading, progression and thrombus formation (52). Consistently, blockade of Dll4-Notch signaling using a neutralizing anti-Dll4 antibody attenuated the development of atherosclerosis in LDL receptor-deficient mice (53). VSMC influence atherosclerotic plaque formation in several ways and may determine susceptibility to plaque rupture (54, 55). Among these, trans-differentiation of VSMCs, or their transition from a contractile/quiescent state to a secretory/inflammatory/migratory state plays an important role during atherosclerosis (56). Although the relationship between VSMC and NOTCH signaling during atherosclerosis is unclear, it has been found that atherosclerotic plaques in human carotid and femoral arteries usually have a lot of NOTCH3 proteins, and it is possible that Jagged1 stimulates the NOTCH signaling pathway in VSMCs, which causes pathological changes (57). Adenylate cyclase type 8 (AC8) is known to be involved in trans-differentiation of VSMC. A study by Zela et al. indicated that Jagged1-triggered inhibition of the NOTCH3-HRT3 and/or HRT1 pathways in the context of pathological vascular remodeling enhanced IL1β-mediated up-regulation of AC8 in trans-differentiated VSMC and amplified its deleterious effect on trans-differentiated VSMC differentiation (58). A recent study by Dave et al. linked elastin deficiency to NOTCH signaling (59): although elastin deficiency does not directly contribute to atherosclerosis, degradation of elastin may allow lipid infiltration into atherosclerotic plaques; elastin deficiency in VSMC resulted in reduced levels of DNA methyltransferase 1 (DNMT1) and DNA methylation (an epigenetic marker that drives gene silencing), which induces the expression of key NOTCH pathway genes Jagged1, γ-secretase catalytic subunits PSEN1 and PSEN2 and triggers NOTCH3 activation. That is, upregulation of the NOTCH3 pathway causes accumulation of pathological VSMC during elastin deficiency (59). Therefore, we suggest that lesions of large intracranial arteries may be one of the clinical phenotypes of NOTCH3 mutant disease. The study of the molecular biological mechanism of NOTCH3 mutation-induced lesions in large vessels led us to hypothesize that NOTCH3 mutation is a general vascular lesion affecting all types of intracranial vessels but manifesting predominantly in small vessels rather than a lesion unique to small vessels. We need to further investigate the mechanism and validate it pathologically in stenotic vessels.

To the best of our knowledge, although the vascular lesions in classical CADASIL predominantly involve the intracranium, vascular changes in CADASIL occur along the arterial tree, including the heart (47). Embryological effects of the NOTCH3 receptor pathway responsible for the development of the cardiovascular system support this theory (60). Consistent with the findings of CADASIL intracranial vasculature, we confirmed abnormalities of the coronary microvascular system in myocardial histopathologic examination and found typical CADASIL changes such as GOM deposition, cellular degeneration, and basement membrane thickening (61). In recent years an increasing number of patients with CADASIL present with ischemic coronary artery disease (CAD), and there have been many reports of an association between CADASIL and CAD, albeit with limited evidence. Argirò et al. included 17 patients with CADASIL confirming a blunted coronary flow reserve due to dysfunction of the coronary microcirculation with diffuse hypoperfusion areas (62). In a case report of a patient with CADASIL presenting with angina pectoris without obstructive coronary artery disease, coronary CT angiography demonstrated diffuse vascular irregularities, vascular thickening, and mixed noncalcified/calcified coronary lesions with moderate stenosis (63). Consistently, Rubin et al. performed coronary angiography in patients with CADASIL and found diffuse and irregular stenosis of the involved coronary arteries (64). Thus, these clinical findings suggest that NOTCH3 mutations may have caused coronary microvascular dysfunction and diffuse coronary stenosis rather than coronary atherosclerosis. Also, the more aggressive and accelerated CAD in CADASIL patients may be related to microvascular dysfunction, allowing for a younger age of onset and a broader disease burden (65). NOTCH3 mutations impair the damaged heart through coronary microvascular dysfunction, loss of pericytes, and impaired microvascular maturation recovery, and the main causes of coronary microvascular dysfunction are fibrovascular wall thickening, impaired vascular reactivity, and increased myogenic tone (66).

Several studies have been conducted on the molecular mechanisms of how NOTCH3 mutations cause CAD. Mutations in components of the NOTCH pathway lead to structural abnormalities and dysfunction in the heart. In particular, activation of NOTCH exerts a protective effect against myocardial infarction, cardiac hypertrophy, and alcoholic cardiomyopathy. Binding of NOTCH3 receptors on human coronary smooth muscle cells and Jagged1 ligands on human coronary endothelial cells contributes to increased expression of smooth muscle-α-actinin and calmodulin (67). A recent study demonstrated that the NOTCH3-RBPJk signaling pathway maintains the integrity of the coronary vascular system by regulating the vascular endothelial growth factor A (VEGFA)/vascular endothelial growth factor receptor 2 (VEGFR2)/DII4 pathway. Thus, the absence of the NOTCH3-RBPJk signaling pathway in VSMC leads to heart failure during pressure overload, and alterations in the cardiac vasculature are a direct causative factor (68). Oncostatin M (OSM) is known to be an inflammatory cytokine, and inhibition of OSM signaling inhibits cardiomyocyte remodeling, leading to deterioration of cardiac function after myocardial infarction. A study showed that the mechanism of OSM on cardiac ischemia/reperfusion injury is partially mediated by the NOTCH3/Akt pathway. Thus, a novel role of NOTCH3/Akt signaling contributes to OSM-induced protection against cardiac ischemia/reperfusion injury (69).

NOTCH signaling is considered a key player in metabolism (70), and activation of the NOTCH3 gene may lead to hyperlipidemia. Gong et al. reported 1 family with CADASIL with elevated lipoprotein levels that caused a higher risk of disease (71). Apolipoprotein D (APOD) is known to be a secreted glycoprotein that regulates smooth muscle cells (72, 73). It is associated with lipid metabolism, particularly in plasma mainly associated with High-density lipoprotein HDL, and is abundantly present in atherosclerotic lesions (74). Several studies have demonstrated a correlation between APOD expression and healthy lipid profiles (75). It was shown that cell contact-dependent Notch signaling contributes to the regulation of APOD in mural cells (76). Further experiments revealed that NOTCH3 contributes to the down-regulation of APOD, possibly through the activation of the downstream NOTCH signaling pathway by JAGGED-1 ligand on endothelial cells, which increases the regulation of APOD in wall cells by endothelial cells (77). Therefore, we suggest that mutations in the NOTCH3 gene may cause impairment of the corresponding signaling pathway and increased APOD expression, leading to severe dyslipidemia. Wimmer et al. identified the Dll4-NOTCH3 pathway as a key driver of diabetic vasculopathy in the human vasculature. They constructed vascular organoid models and placed them in a high-glucose environment and observed by electron microscopy a marked increase in collagen IV, as well as fibronectin, laminin, perlecan, and the pro-inflammatory cytokines TNFα and IL6. Mainly pericytes, but also endothelial and MSC-like cells, upregulated ECM synthesis. And we also observed substantial thickening and splitting of the basement membrane layer without changes in vessel diameter. Basement membrane thickening was reduced after blocking NOTCH3 protein and its ligand DLL4, suggesting that the DLL4-NOTCH3 pathway plays an important role in diabetic vasculopathy (78). We speculate that NOTCH3 gene mutations may interfere with the Dll4-NOTCH3 pathway thereby causing blood glucose abnormalities, which suggests that we investigate the association between the CADASIL clinical phenotype and diabetes through more clinical series. However, there are limited studies on the relationship between NOTCH3 mutations and metabolisms such as lipids and glucose, and we need further studies on pathogenesis to clarify the relationship.

In addition to this, NOTCH3 has many associations with human diseases through mutations, altered expression, or dysregulation of its activity or turnover. Although the main function of NOTCH3 is to regulate angiogenesis, dysregulation of NOTCH3 activity may play an important role in tumorigenesis and tumor maintenance. The apparent alteration (and in many cases overactivation) of NOTCH3 signaling activity causes a number of changes, including controlling the tumor-initiating cell phenotype, regulating known upstream or downstream tumor-associated signaling factors, facilitating angiogenesis or tumor invasion, regulating the cell cycle, etc. Recent studies have found that NOTCH3 expression is found in most T-cell acute lymphoblastic leukemias, possibly through the activation of Notch3 signaling by the expression of Dll in endothelial cells thereby promoting the proliferation of T-cell acute lymphoblastic leukemia cells (79). Furthermore, it has been demonstrated that aging is associated with a significant progressive decline in NOTCH3 signaling. This age-related lack of NOTCH3 triggers a decline in vascular function, which subsequently affects lymphatic flow and ultimately leads to degenerative changes (80). Thus, the complex and highly variable functions of NOTCH3 factors have led to diverse associations in human development and disease, and the pathogenesis of these NOTCH3-related diseases almost always involves alterations in the NOTCH3 signaling pathway. However, whether these diseases share the same mechanisms as CADASIL has not been systematically elucidated. Perhaps, further studies of the mechanisms and a more complete understanding of NOTCH signaling will help to generalize the clinical heterogeneity of NOTCH mutations. At the same time, this will underpin the development of means to more specifically target its aberrant activity in different disease contexts.

To date, there have been no case reports of CADASIL patients with concomitant intracranial large artery and coronary artery stenosis. However, previous studies have found typical CADASIL pathologic manifestations such as deposition of GOM in both intracranial large arteries and coronary arteries. Meanwhile, activation or inhibition of the NOTCH signaling pathway caused by NOTCH3 mutations also leads to pathological changes such as VSMCs. In conclusion, NOTCH3 mutations may lead to intracranial aortic anomalies, coronary artery disease, and abnormalities in lipid and glucose metabolism through different mechanisms. NOTCH3 mutations may no longer be simply a disease of the small blood vessels of the brain-typical of CADASIL-but a new spectrum of diseases that share the same pathogenesis as NOTCH3 mutations. However, there is evidence that traditional risk factors such as hypertension, diabetes mellitus, or smoking also contribute to the more severe clinical phenotype of CADASIL. It is possible that the observed cases of intracranial large artery stenosis or coronary artery disease reflect traditional vascular risk factors and diseases (e.g., higher prevalence of intracranial atheromatous plaques in Southeast Asia) rather than representing a true characterization of the pathology associated with NOTCH3 mutations. Therefore, more robust clinical studies and mechanistic investigations are needed to demonstrate that clinical polymorphisms do indeed characterize genetically determined diseases.