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利用XIST基因中的转录多态性直接检测非随机X染色体失活

Direct detection of non-random X chromosome inactivation by use of a transcribed polymorphism in the XIST gene.

作者信息

Rupert J L, Brown C J, Willard H F

机构信息

Department of Genetics, Case Western Reserve University School of Medicine, Cleveland, OH 44106-4955, USA.

出版信息

Eur J Hum Genet. 1995;3(6):333-43. doi: 10.1159/000472322.

Abstract

As a result of X chromosome inactivation, females are mosaic for cell lineages in which either the paternal or the maternal X chromosome is active, and, if inactivation were random, each lineage should be present at approximately the same frequency. Detection of instances of non-random X inactivation can be important both clinically and for the study of X chromosome inactivation. Identification of a single-base polymorphism in an expressed region of the human XIST gene has permitted the development of a direct PCR-based assay for randomness of X inactivation. Oligonucleotide primers were designed, incorporating the variant base, and conditions established that allowed allele-specific PCR amplification. As the XIST gene is expressed only from the inactive X chromosome, differential amplification of the alleles in cDNA from heterozygotes can be used as an indicator of non-random inactivation. Using this assay, non-random X chromosome inactivation has been demonstrated in chromosomally abnormal cell lines and in lymphocytes from heterozygous, normal females. Virtually complete non-random X inactivation was also shown in a mother and her daughter, suggesting the existence of some familial factor affecting X chromosome inactivation.

摘要

由于X染色体失活,雌性个体在细胞谱系中是嵌合体,其中父本或母本的X染色体是活跃的。如果失活是随机的,那么每个谱系出现的频率应该大致相同。检测非随机X失活的情况在临床和X染色体失活研究中都可能很重要。人类XIST基因表达区域中单碱基多态性的鉴定使得基于PCR的直接检测X失活随机性的方法得以发展。设计了包含变异碱基的寡核苷酸引物,并确定了允许等位基因特异性PCR扩增的条件。由于XIST基因仅从不活跃的X染色体表达,杂合子cDNA中等位基因的差异扩增可作为非随机失活的指标。使用该检测方法,已在染色体异常细胞系和杂合、正常雌性个体的淋巴细胞中证明了非随机X染色体失活。在一位母亲及其女儿中也显示出几乎完全的非随机X失活,这表明存在一些影响X染色体失活的家族因素。

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