The mutational spectrum in Waardenburg syndrome

瓦登堡综合征 小眼畸形相关转录因子 乘客3 生物 遗传学 突变 等位基因 无义突变 索克斯10 移码突变 小眼症 基因 胡说 表型 错义突变 神经嵴 转录因子
作者
Mayada Tassabehji,Valerie Newton,X.-Z. Liu,Angela F. Brady,Dian Donnai,Małgorzata Krajewska‐Walasek,Victoria Murday,Andrew Norman,Ewa Obersztyn,William Reardon,J. C. Rice,Richard C. Trembath,Peter Wieacker,M. Whiteford,Robin Winter,Andrew Read
出处
期刊:Human Molecular Genetics [Oxford University Press]
卷期号:4 (11): 2131-2137 被引量:222
标识
DOI:10.1093/hmg/4.11.2131
摘要

One hundred and thirty-four families or individuals with auditory-pigmentary syndromes such as Waardenburg syndrome (WS) or probable neurocristopathies were screened for mutations in the PAX3 and MITF genes. PAX3 mutations were found in 20/25 families with definite Type 1 WS and 1/2 with Type 3 WS, but in none of 23 with definite Type 2 WS or 36 with other neurocristopathies. The PAX3 mutations included substitutions of conserved amino acids in the paired domain or the homeodomain, splice-site mutations, nonsense mutations and frame-shifting insertions or deletions. No phenotype-genotype correlations were noted within WS1 families. With MITF, mutations likely to affect protein function were found in seven families, five of which had definite Type 2 WS. We conclude that Type 1 and Type 3 WS are allelic and are normally caused by loss of function mutations in PAX3; that Type 2 WS is heterogeneous, with about 20% of cases caused by mutations in MITF, and that individuals with auditory, pigmentary or neural crest syndromes which do not fit stringent definitions of Waardenburg syndrome are unlikely to have mutations in either the PAX3 or MITF genes. The molecular pathology of MITF/microphthalmia mutations appears to be different in humans and mice, with gene dosage having more significant effects in humans than in the mouse.
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