Heitz D, Devys D, Imbert G, Kretz C, Mandel J L
LGME/CNRS, INSERM U184, Institut de Chimie Biologique, Strasbourg, France.
J Med Genet. 1992 Nov;29(11):794-801. doi: 10.1136/jmg.29.11.794.
The fragile X mental retardation syndrome is caused by unstable expansion of a CGG repeat. Two main types of mutation have been categorised. Clinical expression is associated with the presence of the full mutation, while subjects who carry only a premutation do not have mental retardation. Premutations have a high risk of transition to full mutation when transmitted by a female. We have used direct detection of the mutations to characterise large families who illustrate the wide variation in penetrance which has been observed in different sibships (a feature often called the Sherman paradox). A family originally found to show tight genetic linkage between the factor 9 gene and the fragile X locus was reanalysed, confirming the original genotype assignments and the observed linkage. The size of premutations was measured by Southern blotting and by using a PCR based test in 102 carrier mothers and this was correlated with the type of mutation found in their offspring. The risk of transition to full mutation was found to be very low for premutations with a size increase (delta) of about 100 bp, increasing up to 100% when the size of premutation was larger than about 200 bp, even after taking into account (at least partially) ascertainment bias. These results confirm and extend those reported by Fu et al (1991) and Yu et al (1992) and explain the Sherman paradox.(ABSTRACT TRUNCATED AT 250 WORDS)
脆性X智力障碍综合征由CGG重复序列的不稳定扩增引起。已将突变分为两种主要类型。临床表型与完全突变的存在相关,而仅携带前突变的个体没有智力障碍。前突变由女性传递时向完全突变转变的风险很高。我们通过直接检测突变来对大家庭进行特征分析,这些大家庭体现了在不同同胞关系中观察到的广泛的外显率差异(这一特征常被称为谢尔曼悖论)。对最初发现因子9基因与脆性X位点之间存在紧密遗传连锁的一个家庭进行了重新分析,证实了最初的基因型判定和观察到的连锁关系。通过Southern印迹法和基于PCR的检测方法测量了102位携带者母亲前突变的大小,并将其与她们后代中发现的突变类型相关联。发现前突变大小增加(Δ)约100 bp时向完全突变转变的风险非常低,而当前突变大小大于约200 bp时,即使考虑到(至少部分)确诊偏倚,转变风险也会增加到100%。这些结果证实并扩展了Fu等人(1991年)和Yu等人(1992年)报道的结果,并解释了谢尔曼悖论。(摘要截短为250字)
