| Literature DB >> 24000151 |
Julie W Rutten1, Elles M J Boon, Michael K Liem, Johannes G Dauwerse, Margot J Pont, Ellen Vollebregt, Anneke J Maat-Kievit, Hendrika B Ginjaar, Phillis Lakeman, Sjoerd G van Duinen, Gisela M Terwindt, Saskia A J Lesnik Oberstein.
Abstract
Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL) is caused by stereotyped missense mutations in NOTCH3. Whether these mutations lead to the CADASIL phenotype via a neomorphic effect, or rather by a hypomorphic effect, is subject of debate. Here, we report two novel NOTCH3 mutations, both leading to a premature stop codon with predicted loss of NOTCH3 function. The first mutation, c.307C>T, p.Arg103*, was detected in two brothers aged 50 and 55 years, with a brain MRI and skin biopsy incompatible with CADASIL. The other mutation was found in a 40-year-old CADASIL patient compound heterozygous for a pathogenic NOTCH3 mutation (c.2129A>G, p.Tyr710Cys) and an intragenic frameshift deletion. The deletion was inherited from his father, who did not have the skin biopsy abnormalities seen in CADASIL patients. These individuals with rare NOTCH3 mutations indicate that hypomorphic NOTCH3 alleles do not cause CADASIL.Entities:
Keywords: CADASIL; NOTCH3; deletion; hypomorphic allele; nonsense mutation
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Year: 2013 PMID: 24000151 DOI: 10.1002/humu.22432
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878