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Clinical and neuroradiological spectrum of biallelic variants in NOTCH3.

Iruzubieta, P; Alves, CAPF; Al Shamsi, AM; ElGhazali, G; Zaki, MS; Pinelli, L; Lopergolo, D; Cho, BPH; Jolly, AA; Al Futaisi, A; et al. Iruzubieta, P; Alves, CAPF; Al Shamsi, AM; ElGhazali, G; Zaki, MS; Pinelli, L; Lopergolo, D; Cho, BPH; Jolly, AA; Al Futaisi, A; Al-Amrani, F; Galli, J; Fazzi, E; Vulin, K; Barajas-Olmos, F; Hengel, H; Aljamal, BM; Nasr, V; Assarzadegan, F; Ragno, M; Trojano, L; Ojeda, NM; Çakar, A; Bianchi, S; Pescini, F; Poggesi, A; Al Tenalji, A; Aziz, M; Mohammad, R; Chedrawi, A; De Stefano, N; Zifarelli, G; Schöls, L; Haack, TB; Rebelo, A; Zuchner, S; Koc, F; Griffiths, LR; Orozco, L; Helmes, KG; Babaei, M; Bauer, P; Chan Jeong, W; Karimiani, EG; Schmidts, M; Gleeson, JG; Chung, WK; Alkuraya, FS; Shalbafan, B; Markus, HS; Houlden, H; Maroofian, R (2024) Clinical and neuroradiological spectrum of biallelic variants in NOTCH3. EBioMedicine, 107. p. 105297. ISSN 2352-3964 https://doi.org/10.1016/j.ebiom.2024.105297
SGUL Authors: Maroofian, Reza

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Abstract

BACKGROUND: NOTCH3 encodes a transmembrane receptor critical for vascular smooth muscle cell function. NOTCH3 variants are the leading cause of hereditary cerebral small vessel disease (SVD). While monoallelic cysteine-involving missense variants in NOTCH3 are well-studied in cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL), patients with biallelic variants in NOTCH3 are extremely rare and not well characterised. METHODS: In this study, we present clinical and genetic data from 25 patients with biallelic NOTCH3 variants and conduct a literature review of another 25 cases (50 patients in total). Brain magnetic resonance imaging (MRI) were analysed by expert neuroradiologists to better understand the phenotype associated with biallelic NOTCH3 variants. FINDINGS: Our systematic analyses verified distinct genotype-phenotype correlations for the two types of biallelic variants in NOTCH3. Biallelic loss-of-function variants (26 patients) lead to a neurodevelopmental disorder characterised by spasticity, childhood-onset stroke, and periatrial white matter volume loss resembling periventricular leukomalacia. Conversely, patients with biallelic cysteine-involving missense variants (24 patients) fall within CADASIL spectrum phenotype with early adulthood onset stroke, dementia, and deep white matter lesions without significant volume loss. White matter lesion volume is comparable between patients with biallelic cysteine-involving missense variants and individuals with CADASIL. Notably, monoallelic carriers of loss-of-function variants are predominantly asymptomatic, with only a few cases reporting nonspecific headaches. INTERPRETATION: We propose a NOTCH3-SVD classification depending on dosage and variant type. This study not only expands our knowledge of biallelic NOTCH3 variants but also provides valuable insight into the underlying mechanisms of the disease, contributing to a more comprehensive understanding of NOTCH3-related SVD. FUNDING: The Wellcome Trust, the MRC.

Item Type: Article
Additional Information: © 2024 The Author(s). Published by Elsevier B.V. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
Keywords: CADASIL, Leukoencephalopathy, NOTCH3, Neurodevelopmental disorders, Stroke, Receptor, Notch3, Humans, Female, Male, Alleles, Adult, Middle Aged, Genetic Association Studies, Magnetic Resonance Imaging, CADASIL, Phenotype, Aged, Mutation, Missense, Genetic Predisposition to Disease, Young Adult, Brain, Adolescent
SGUL Research Institute / Research Centre: Academic Structure > Cardiovascular & Genomics Research Institute
Academic Structure > Cardiovascular & Genomics Research Institute > Genomics
Journal or Publication Title: EBioMedicine
ISSN: 2352-3964
Language: eng
Media of Output: Print-Electronic
Related URLs:
Publisher License: Creative Commons: Attribution 4.0
Projects:
Project IDFunderFunder ID
716344European Research Councilhttp://dx.doi.org/10.13039/501100000781
P50 HD105351NICHD NIH HHSUNSPECIFIED
HE 8803/1–1Deutsche Forschungsgemeinschafthttps://doi.org/10.13039/501100001659
499552394Deutsche Forschungsgemeinschafthttp://dx.doi.org/10.13039/501100001659
390939984Deutsche Forschungsgemeinschafthttp://dx.doi.org/10.13039/501100001659
KK.01.1.1.01.0008European Regional Development Fundhttps://doi.org/10.13039/501100008530
RG/4/32218British Heart Foundationhttp://dx.doi.org/10.13039/501100000274
BRC-1215-20014NIHR Cambridge Biomedical Research Centrehttps://doi.org/10.13039/501100018956
RE/18/1/34212Cambridge BHF Centre of Research Excellencehttps://doi.org/10.13039/501100024893
URI: https://openaccess.sgul.ac.uk/id/eprint/117592
Publisher's version: https://doi.org/10.1016/j.ebiom.2024.105297

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