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v-erb A致癌基因蛋白功能域的定位:激素结合域的残余部分在蛋白作用中发挥多种重要作用。

Mapping of functional domains within the v-erb A oncogene protein: the remnants of the hormone binding domain play multiple, vital roles in protein action.

作者信息

Boucher P, Privalsky M L

机构信息

Department of Microbiology, University of California, Davis 95616.

出版信息

Oncogene. 1990 Sep;5(9):1303-11.

PMID:2170895
Abstract

The v-erb A oncogene represents a virally-transduced variant of a thyroid hormone receptor. Biochemical characterization of a series of mutant v-erb A proteins demonstrates that nuclear localization and DNA binding are both necessary for v-erb A function in the neoplastic cell and are mediated by multiple, overlapping domains within the v-erb A polypeptide. Domains of the v-erb A protein necessary for sequence-specific and sequence-independent DNA binding are distinguishable from one another, and encompass sequences projecting beyond the zinc-finger motifs themselves. Although unable to bind T3 thyroid hormone, the remnants of the hormone binding domain continue to play unanticipated essential roles in v-erb A protein function.

摘要

v-erbA癌基因代表甲状腺激素受体的一种病毒转导变体。一系列突变型v-erbA蛋白的生化特性表明,核定位和DNA结合对于v-erbA在肿瘤细胞中的功能都是必需的,并且由v-erbA多肽内的多个重叠结构域介导。v-erbA蛋白中序列特异性和序列非依赖性DNA结合所必需的结构域彼此可区分,并且包含延伸到锌指基序本身之外的序列。尽管无法结合T3甲状腺激素,但激素结合结构域的残余部分在v-erbA蛋白功能中继续发挥意想不到的重要作用。

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