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首页> 外文期刊>Expert Review of Molecular Diagnostics >Molecular diagnosis of Fragile X syndrome.
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Molecular diagnosis of Fragile X syndrome.

机译:易碎X综合征的分子诊断。

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摘要

Fragile X syndrome, the most prevalent inherited cause of mental retardation, is related to hyperexpansion of a polymorphic CGG repeat of the FMR1 gene. Expansion of 55-200 repeats are called premutations and characterize carriers who usually have no mental impairment. The disease causing full mutations exceed 200 CGG repeats, are hypermethylated and lead to transcriptional silencing of the gene and absence of the Fragile X mental retardation protein (FMRP). Diagnostic approaches involve molecular and immunocytochemical techniques. Southern blot, which allows mutations to be detected and methylation status to be determined in a single test, remains the procedure of choice for most laboratories. Modifications of PCR methods, including methylation specific PCR, are also proposed but their implementation is still in question because of inherent difficulties to amplify CGG repeats, distinguish between mosaic patterns and interpret results in female individuals. The FMRP antibody test is also suitable for large population screening and elucidation of Fragile X syndrome cases with no CGG expansion, but it is not widely applied. In search for novel diagnostic approaches, use of PCR as a first prescreening test followed by Southern blot is considered the most reliable procedure.
机译:脆性X综合征是智力障碍最普遍的遗传原因,与FMR1基因的多态CGG重复序列的过度扩增有关。扩展55-200个重复序列称为前突变,可表征通常没有智力障碍的携带者。导致完全突变的疾病超过200个CGG重复序列,被高度甲基化并导致该基因的转录沉默以及脆性X智力低下蛋白(FMRP)的缺失。诊断方法涉及分子和免疫细胞化学技术。 Southern印迹技术可在单个测试中检测突变并确定甲基化状态,仍然是大多数实验室选择的程序。还提出了对PCR方法的修改方法,包括甲基化特异性PCR,但由于扩增CGG重复序列,区分镶嵌图样和解释女性个体的内在困难,其实现方法仍存在疑问。 FMRP抗体测试也适用于没有CGG扩展的大量人群筛查和阐明脆性X综合征病例,但并未得到广泛应用。在寻找新颖的诊断方法时,使用PCR作为第一个预筛选测试,然后进行Southern印迹被认为是最可靠的方法。

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