Abstract
PurposeCADASIL is a small-vessel disease caused by a cysteine-altering pathogenic variant in one of the 34 epidermal growth factor-like repeat (EGFr) domains of the NOTCH3 protein. We recently found that pathogenic variant in EGFr domains 7–34 have an unexpectedly high frequency in the general population (1:300). We hypothesized that EGFr 7–34 pathogenic variant more frequently cause a much milder phenotype, thereby explaining an important part of CADASIL disease variability.MethodsAge at first stroke, survival and white matter hyperintensity volume were compared between 664 CADASIL patients with either a NOTCH3 EGFr 1–6 pathogenic variant or an EGFr 7–34 pathogenic variant. The frequencies of NOTCH3 EGFr 1–6 and EGFr 7–34 pathogenic variant were compared between individuals in the genome Aggregation Database and CADASIL patients.ResultsCADASIL patients with an EGFr 1–6 pathogenic variant have a 12-year earlier onset of stroke than those with an EGFr 7–34 pathogenic variant, lower survival, and higher white matter hyperintensity volumes. Among diagnosed CADASIL patients, 70% have an EGFr 1–6 pathogenic variant, whereas EGFr 7–34 pathogenic variant strongly predominate in the population.ConclusionNOTCH3 pathogenic variant position is the most important determinant of CADASIL disease severity, with EGFr 7–34 pathogenic variant predisposing to a later onset of stroke and longer survival.
Highlights
CADASIL is the most prevalent hereditary cerebral small-vessel disease, caused by highly distinctive cysteine-altering missense pathogenic variant (PV) in the NOTCH3 gene.[1,2] More than 200 of such distinct NOTCH3 PV have been described in CADASIL families worldwide.[3]
NOTCH3 PV in the population are identical to those found in CADASIL patients, we previously found that the PV in the general population are predominantly located in epidermal growth factor-like repeat (EGFr) domains [7–34] of the NOTCH3 protein, whereas PV in CADASIL patients are predominantly located in EGFr domains [1,2,3,4,5,6]
Mutations in NOTCH3 EGFr domains [1,2,3,4,5,6] are associated with an earlier onset of stroke than PV in EGFr domains [7–34] First, we compared the age at onset of stroke in the 153 Dutch CADASIL patients with an EGFr 1–6 PV with the 98 patients with an EGFr 7–34 PV
Summary
CADASIL (cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy) is the most prevalent hereditary cerebral small-vessel disease, caused by highly distinctive cysteine-altering missense pathogenic variant (PV) in the NOTCH3 gene.[1,2] More than 200 of such distinct NOTCH3 PV have been described in CADASIL families worldwide.[3]. NOTCH3 PV in the population are identical to those found in CADASIL patients, we previously found that the PV in the general population are predominantly located in epidermal growth factor-like repeat (EGFr) domains [7–34] of the NOTCH3 protein, whereas PV in CADASIL patients are predominantly located in EGFr domains [1,2,3,4,5,6] This suggests that EGFr domain [1,2,3,4,5,6] PV are associated with a more severe or ‘classical’ CADASIL phenotype, whereas EGFr 7–34 PV are generally milder. In a small CADASIL cohort we previously showed that EGFr domain [1,2,3,4,5,6] PV are associated
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