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小鼠体外系统中Rps4、Zfx和Ube1基因X染色体失活的维持

Maintenance of X inactivation of the Rps4, Zfx, and Ube1 genes in a mouse in vitro system.

作者信息

Bressler S L, Lee K H, Adler D A, Chapman V M, Disteche C M

机构信息

Department of Pathology, University of Washington, Seattle 98195.

出版信息

Somat Cell Mol Genet. 1993 Jan;19(1):29-37. doi: 10.1007/BF01233952.

Abstract

Several genes, including RPS4X (ribosomal protein subunit 4), ZFX (zinc finger on the X chromosome), and UBE1 (ubiquitin-activating enzyme), have been shown to be expressed from the inactive X chromosome of cultured human cells. By contrast, these genes are subject to X-chromosome inactivation in tissues from adult mice. We have now examined the inactivation status of these genes in cultured mouse cells to determine whether the differences in X-chromosome inactivation between species is due to an intrinsic difference between human and mouse X-chromosome genes or whether it is a function of gene reactivation in cell culture per se. The expression of three mouse X-chromosome genes, Rps4, Zfx, and Ube1 was examined by reverse transcriptase polymerase chain reaction (RT-PCR) in heterozygous cultured cells from a cross of a laboratory mouse by Mus spretus, which were selected to uniformly express the X chromosome from the laboratory mouse parent. No expression of the M. spretus alleles of these genes was observed in the cell line (Hobmski), which is consistent with the patterns of expression previously observed in mouse in vivo and indicates that these genes remain stably inactivated in an immortalized mouse cell line. By cytogenetic and RT-PCR analyses the Hobmski cell line was shown to retain a late-replicating X chromosome from M. spretus, which expressed the M. spretus allele of the X (inactive) specific transcript (Xist). The Hobmski cell line will be a useful resource for studying the features that maintain X-chromosome genes inactive.

摘要

包括核糖体蛋白亚基4(RPS4X)、X染色体上的锌指蛋白(ZFX)和泛素激活酶(UBE1)在内的几个基因,已被证明可从培养的人类细胞的失活X染色体上表达。相比之下,在成年小鼠的组织中,这些基因会发生X染色体失活。我们现在研究了这些基因在培养的小鼠细胞中的失活状态,以确定物种间X染色体失活的差异是由于人类和小鼠X染色体基因之间的内在差异,还是细胞培养本身导致基因重新激活的结果。通过逆转录聚合酶链反应(RT-PCR)检测了实验室小鼠与西班牙小家鼠杂交产生的杂合培养细胞中三个小鼠X染色体基因Rps4、Zfx和Ube1的表达情况,这些细胞被选择统一表达来自实验室小鼠亲本的X染色体。在该细胞系(Hobmski)中未观察到这些基因的西班牙小家鼠等位基因的表达,这与之前在小鼠体内观察到的表达模式一致,表明这些基因在永生化的小鼠细胞系中保持稳定失活。通过细胞遗传学和RT-PCR分析表明,Hobmski细胞系保留了一条来自西班牙小家鼠的复制较晚的X染色体,该染色体表达了X(失活)特异性转录本(Xist)的西班牙小家鼠等位基因。Hobmski细胞系将成为研究维持X染色体基因失活特征的有用资源。

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