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[脆性X综合征中不稳定的DNA序列与甲基化]

[Unstable DNA sequence and methylation in fragile X syndrome].

作者信息

Fu S D, Shen Y, Fan Y

机构信息

Institute of Basic Medical Sciences, Chinese Academy of Medical Sciences, Beijing.

出版信息

Zhonghua Yi Xue Za Zhi. 1994 Oct;74(10):611-4, 646-7.

PMID:7842338
Abstract

Fragile X syndrome is characterized as an inherited unstable DNA sequence: the increasement of (CGG)n copy number. It suffered from the inactivation of FMR-1 (fragile X mental retardation 1), which is inhibited by amplification of (CGG)n and methylation of CpG island. The (CGG)n repeat variation in normal Chinese population was detected by PCR with sequencing gel analysis. We also analysed the amplification of (CGG)n and methylation of CpG island at Xq27.3 from 15 individuals in 6 families by Southern hybridization. These results indicate that abnormal methylation of CpG island always occurs in Fra (X) patients together with large amplification of (CGG)n. The (CGG)n could be either stable or amplified in springs of carrier females. These suggest that there would be a new genetic mechanism dynamic mutation.

摘要

脆性X综合征的特征是一种遗传性不稳定DNA序列:(CGG)n拷贝数增加。它因FMR-1(脆性X智力低下1)失活而患病,FMR-1受(CGG)n扩增和CpG岛甲基化抑制。通过PCR结合测序凝胶分析检测了正常中国人群中的(CGG)n重复变异。我们还通过Southern杂交分析了6个家庭中15名个体Xq27.3处(CGG)n的扩增和CpG岛的甲基化情况。这些结果表明,Fra(X)患者中总是会出现CpG岛异常甲基化,同时伴有(CGG)n的大量扩增。(CGG)n在携带者女性的子代中可能稳定,也可能扩增。这些表明可能存在一种新的遗传机制——动态突变。

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