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一种与尾型相关的同源结构域蛋白调控肠道特异性基因转录。

A homeodomain protein related to caudal regulates intestine-specific gene transcription.

作者信息

Suh E, Chen L, Taylor J, Traber P G

机构信息

Department of Medicine, University of Pennsylvania School of Medicine, Philadelphia 19104.

出版信息

Mol Cell Biol. 1994 Nov;14(11):7340-51. doi: 10.1128/mcb.14.11.7340-7351.1994.

Abstract

The continually renewing epithelium of the intestinal tract arises from the visceral endoderm by a series of complex developmental transitions. The mechanisms that establish and maintain the processes of cellular renewal, cell lineage allocation, and tissue restriction and spatial assignment of gene expression in this epithelium are unknown. An understanding of the regulation of intestine-specific gene regulation may provide information on the molecular mechanisms that direct these processes. In this regard, we show that intestine-specific transcription of sucrase-isomaltase, a gene that is expressed exclusively in differentiated enterocytes, is dependent on binding of a tissue-specific homeodomain protein (mouse Cdx-2) to an evolutionarily conserved promoter element in the sucrase-isomaltase gene. This protein is a member of the caudal family of homeodomain genes which appear to function in early developmental events in Drosophila melanogaster, during gastrulation in many species, and in intestinal endoderm. Unique for this homeodomain gene family, we show that mouse Cdx-2 binds as a dimer to its regulatory element and that dimerization in vitro is dependent on redox potential. These characteristics of the interaction of Cdx-2 with its regulatory element provide for a number of potential mechanisms for transcriptional regulation. Taken together, these findings suggest that members of the Cdx gene family play a fundamental role both in the establishment of the intestinal phenotype during development and in maintenance of this phenotype via transcriptional activation of differentiated intestinal genes.

摘要

肠道不断更新的上皮组织通过一系列复杂的发育转变源自脏内胚层。在这种上皮组织中,建立和维持细胞更新、细胞谱系分配以及基因表达的组织限制和空间分配过程的机制尚不清楚。了解肠道特异性基因调控可能会提供有关指导这些过程的分子机制的信息。在这方面,我们表明蔗糖酶 - 异麦芽糖酶的肠道特异性转录(该基因仅在分化的肠细胞中表达)依赖于一种组织特异性同源结构域蛋白(小鼠Cdx - 2)与蔗糖酶 - 异麦芽糖酶基因中一个进化保守的启动子元件的结合。这种蛋白质是同源结构域基因尾状家族的成员,该家族似乎在黑腹果蝇的早期发育事件、许多物种原肠胚形成期间以及肠内胚层中发挥作用。对于这个同源结构域基因家族而言独特的是,我们表明小鼠Cdx - 2作为二聚体与其调控元件结合,并且体外二聚化依赖于氧化还原电位。Cdx - 2与其调控元件相互作用的这些特性为转录调控提供了许多潜在机制。综上所述,这些发现表明Cdx基因家族成员在发育过程中肠道表型的建立以及通过分化肠道基因的转录激活维持这种表型方面都发挥着重要作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/878b/359269/44f930c0e3f8/molcellb00011-0316-a.jpg

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