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支架附着区域刺激小鼠植入前胚胎中HSP70.1的表达,但在分化组织中则不然。

Scaffold attachment regions stimulate HSP70.1 expression in mouse preimplantation embryos but not in differentiated tissues.

作者信息

Thompson E M, Christians E, Stinnakre M G, Renard J P

机构信息

Unité de Biologie du Développement, Institut National de la Recherche Agronomique, Jouy-en-Josas, France.

出版信息

Mol Cell Biol. 1994 Jul;14(7):4694-703. doi: 10.1128/mcb.14.7.4694-4703.1994.

Abstract

Eukaryotic interphase chromatin is thought to be organized into topologically discrete, independent domains acting as units upon which differential patterns of gene expression are established. Sequences which attach chromatin to in vitro preparations of a nucleoprotein matrix (scaffold attachment regions [SARs]) may act as domain boundaries, but their role remains poorly defined compared with those of other elements such as locus control regions. We have produced mice homozygous for a transgene which is transcribed as early as the activation of the embryonic genome at the two-cell stage and which is expressed ubiquitously in a number of differentiated tissues. Transgenic lines were generated in the presence or absence of flanking SAR sequences, creating an original model which enabled us to examine the effects of these elements at different developmental stages. In the preimplantation mouse embryo, flanking SARs stimulated transgene expression in a copy-dependent manner. In contrast, in the differentiated tissues of newborn and adult mice, no significant SAR-dependent increase in transgene expression was found, correlation with copy number was lost, and position effects were observed. These results suggest a limited capacity of SARs to act as insulating elements but are consistent with a proposed model of SAR-mediated chromatin opening and closing.

摘要

真核生物间期染色质被认为组织成拓扑学上离散的、独立的结构域,这些结构域作为建立基因表达差异模式的单元。将染色质附着于核蛋白基质体外制备物(支架附着区域[SARs])的序列可能充当结构域边界,但与其他元件(如基因座控制区)相比,它们的作用仍不清楚。我们已经培育出了一种转基因纯合小鼠,该转基因早在二细胞期胚胎基因组激活时就开始转录,并且在许多分化组织中普遍表达。在有或没有侧翼SAR序列的情况下产生转基因系,创建了一个原始模型,使我们能够在不同发育阶段研究这些元件的作用。在植入前的小鼠胚胎中,侧翼SARs以拷贝依赖的方式刺激转基因表达。相反,在新生和成年小鼠的分化组织中,未发现转基因表达有明显的SAR依赖性增加,与拷贝数的相关性丧失,并且观察到位置效应。这些结果表明SARs作为绝缘元件的能力有限,但与提出的SAR介导的染色质开放和关闭模型一致。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cbbc/358842/022bd8441661/molcellb00007-0373-a.jpg

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