Cytogenetic and molecular analysis of dynamic mutation associated with fragile X syndrome.

Idengaku zasshi Pub Date : 1994-06-01 DOI:10.1266/jjg.69.259
N Seki, S Ishikiriyama, M Yamauchi, T Hori
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引用次数: 1

Abstract

Fragile X syndrome is the most common familial form of mental retardation and known to be associated with the fragile site at Xq27.3 (FRAXA). The syndrome has recently been characterized by a unique genetic mechanism which involves dynamic mutation due to a heritable unstable DNA sequence, p(CCG)n repeat, in the FRAXA locus. We were asked to make a genetic diagnosis on the case of a normal male who has two brothers and a maternal uncle with mental retardation. We performed the pedigree analysis of the fragile X syndrome using both cytogenetic and molecular techniques. The affected two brothers and the uncle showed cytogenetic expression of the fra (X)(q27.3) and carried hypermethylated full mutation in the FRAXA locus. The phenotypically normal mother also exhibited fragile X expression and was found to be a carrier of premutation. Via female transmission, the premutation converted to full mutation and exhibited somatic heterogeneity and hypermethylation. However, both cytogenetic and molecular data did not show any evidence of fragile X mutation in the normal male client and, thus, excluded the possibility of his being a carrier.

脆性X综合征相关动态突变的细胞遗传学和分子分析。
脆性X综合征是最常见的家族性智力低下,已知与脆性位点Xq27.3 (FRAXA)有关。该综合征最近以独特的遗传机制为特征,该机制涉及FRAXA位点中遗传不稳定的DNA序列p(CCG)n重复引起的动态突变。我们被要求对一个有两个兄弟和一个患有智障的舅舅的正常男性进行基因诊断。我们使用细胞遗传学和分子技术对脆性X综合征进行了系谱分析。受影响的两兄弟和叔父显示fra (X)(q27.3)的细胞遗传学表达,并在FRAXA位点携带高甲基化全突变。表型正常的母亲也表现出脆弱的X表达,并被发现是突变前的携带者。通过雌性传播,预突变转化为完全突变,并表现出体细胞异质性和高甲基化。然而,细胞遗传学和分子数据均未显示正常男性患者有脆性X突变的证据,因此排除了其为携带者的可能性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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