Spectrum of NOTCH3 mutations in Korean patients with clinically suspicious cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy.

[cadasil]

Cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL ) is caused by mutations in the NOTCH 3 gene on chromosome 19 . Previous studies showed that NOTCH 3 contains mutational hotspots that can vary among individuals of different ethnic backgrounds . In this study , we investigated the spectrum of NOTCH 3 mutations in Korean patients with CADASIL . We retrospectively analyzed 156 patients who underwent NOTCH 3 gene testing for molecular diagnosis of CADASIL using Sanger sequencing with a tiered approach . First , we screened previously reported mutational hotspots (exons 2 -6 , 8 , 11 , 18 , 19 , and 22 ). If no mutation was detected and samples were available , we extended our analysis to additional exons (7 , 9 , 10 , 14 , 15 , 20 , 21 , 23 , and 25 ). In 45 of 156 patients (28 .8 %), 29 mutations and 16 novel variants of unknown significance (VUS ) were identified . The p .R 544 C mutation in exon 11 of NOTCH 3 was the most frequently observed mutation (n = 8 ), followed by p .R 75 P in exon 3 (n = 7 ), p .R 332 C in exon 6 (n = 3 ), p .R 54 C in exon 2 (n = 2 ), and p .R 90 C in exon 3 (n = 2 ). Among the VUS , p .R 1175 W in exon 22 , p .S 414 C in exon 8 , and p .N 1207 S in exon 22 were found in 5 , 3 , and 2 patients , respectively . Other mutations and VUS were observed in 1 patient each . Although this was not a prospective , nationwide cohort study , the results above suggested that the spectrum of NOTCH 3 mutations might be different in Koreans than in individuals of Caucasian ethnicity . Therefore , further analysis of Koreans with CADASIL might be necessary to implement a Korean -specific mutation screening paradigm .