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一个450千碱基对的转基因显示出哺乳动物X染色体失活中心的特性。

A 450 kb transgene displays properties of the mammalian X-inactivation center.

作者信息

Lee J T, Strauss W M, Dausman J A, Jaenisch R

机构信息

Whitehead Institute for Biomedical Research, Massachusetts Institute of Technology, Cambridge 02142, USA.

出版信息

Cell. 1996 Jul 12;86(1):83-94. doi: 10.1016/s0092-8674(00)80079-3.

Abstract

X inactivation results in inactivation of one X chromosome to compensate for gene dosage differences between mammalian females and males. It requires the X-inactivation center (Xic) and Xist in cis. We report that introducing 450 kb of murine Xic/Xist sequences onto autosomes activates female dosage compensation in male ES cells. Xist is induced upon differentiation and can be expressed from both endogenous and ectopic loci, suggesting that elements for counting and choosing Xs are present in the transgene. Differentiating transgenic ES cells undergo excessive cell death. Postnatally, Xist is expressed only from the transgene. Ectopic Xist RNA structurally associates with the autosome and may inactivate a marker gene in cis. These results argue that the Xic is contained within 450 kb and that these sequences are sufficient for chromosome counting, choosing, and initiation of X inactivation.

摘要

X染色体失活导致一条X染色体失活,以补偿哺乳动物雌性和雄性之间的基因剂量差异。它在顺式作用中需要X染色体失活中心(Xic)和Xist基因。我们报道,将450 kb的小鼠Xic/Xist序列导入常染色体可激活雄性胚胎干细胞中的雌性剂量补偿。Xist基因在分化时被诱导,并且可以从内源和异位位点表达,这表明转基因中存在计数和选择X染色体的元件。分化的转基因胚胎干细胞会经历过度的细胞死亡。出生后,Xist基因仅从转基因中表达。异位的Xist RNA在结构上与常染色体相关联,并可能在顺式作用中使一个标记基因失活。这些结果表明,Xic包含在450 kb范围内,并且这些序列足以进行染色体计数、选择和启动X染色体失活。

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