Celli J, Duijf P, Hamel B C, Bamshad M, Kramer B, Smits A P, Newbury-Ecob R, Hennekam R C, Van Buggenhout G, van Haeringen A, Woods C G, van Essen A J, de Waal R, Vriend G, Haber D A, Yang A, McKeon F, Brunner H G, van Bokhoven H
Department of Human Genetics 417, University Hospital Nijmegen, The Netherlands.
Cell. 1999 Oct 15;99(2):143-53. doi: 10.1016/s0092-8674(00)81646-3.
EEC syndrome is an autosomal dominant disorder characterized by ectrodactyly, ectodermal dysplasia, and facial clefts. We have mapped the genetic defect in several EEC syndrome families to a region of chromosome 3q27 previously implicated in the EEC-like disorder, limb mammary syndrome (LMS). Analysis of the p63 gene, a homolog of p53 located in the critical LMS/EEC interval, revealed heterozygous mutations in nine unrelated EEC families. Eight mutations result in amino acid substitutions that are predicted to abolish the DNA binding capacity of p63. The ninth is a frameshift mutation that affects the p63alpha, but not p63beta and p63gamma isotypes. Transactivation studies with these mutant p63 isotypes provide a molecular explanation for the dominant character of p63 mutations in EEC syndrome.
EEC综合征是一种常染色体显性疾病,其特征为缺指(趾)畸形、外胚层发育不良和面部裂隙。我们已将几个EEC综合征家族中的基因缺陷定位到3号染色体q27区域,该区域先前与类EEC疾病——肢体乳腺综合征(LMS)有关。对位于关键的LMS/EEC区间的p53同源基因p63进行分析,发现在9个不相关的EEC家族中存在杂合突变。8个突变导致氨基酸替换,预计会消除p63的DNA结合能力。第9个是移码突变,影响p63α,但不影响p63β和p63γ亚型。对这些突变p63亚型进行的反式激活研究为EEC综合征中p63突变的显性特征提供了分子解释。
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