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人乳头瘤病毒导致细胞转化的分子机制。

Molecular mechanisms of transformation by the human papillomaviruses.

作者信息

Howley P M, Münger K, Werness B A, Phelps W C, Schlegel R

机构信息

Laboratory of Tumor Virus Biology, National Cancer Institute, Bethesda, Maryland 20892.

出版信息

Princess Takamatsu Symp. 1989;20:199-206.

PMID:2562182
Abstract

A variety of studies have now indicated that the papillomaviruses associated with cervical carcinoma, HPV-16 and HPV-18, contain two genes (E6 and E7) which have transforming properties. These genes are generally expressed in cervical carcinoma cells. The HPV-16 E7 protein has recently been shown to be a multi-functional protein possessing both transcriptional modulatory and cellular transforming properties similar to those described for adenovirus E1A proteins (1). E7 is able to transactivate the adenovirus E2 promoter and can cooperate with an activated ras oncogene to transform primary baby rat kidney cells. The N-terminal 37 amino acids of all of the E7 proteins of the genital associated HPVs contain regions which are highly conserved and which are quite similar to portions of conserved domains 1 and 2 of adenovirus E1A. These domains in E1A are critical for cellular transformation properties and contain the amino acid sequences involved in binding the product of the retinoblastoma tumor suppressor gene (pRB). Results from a collaborative study with Ed Harlow and Nick Dyson (Cold Spring Harbor Laboratory) have shown that the E7 oncoprotein of HPV-16 can associate with the retinoblastoma gene product in vitro (2). The ability of the E7 proteins encoded by various HPVs to bind pRB has been examined using an in vitro complexing assay. E7 is not sufficient for transformation of human keratinocytes. The co-operation of the HPV-16 E6 and E7 genes has been shown to be important for transformation of these cells (3). Potential intracellular protein targets for E6 are being assessed.

摘要

现在多种研究表明,与宫颈癌相关的乳头瘤病毒HPV - 16和HPV - 18含有两个具有转化特性的基因(E6和E7)。这些基因通常在宫颈癌细胞中表达。最近研究显示,HPV - 16 E7蛋白是一种多功能蛋白,具有与腺病毒E1A蛋白类似的转录调节和细胞转化特性(1)。E7能够反式激活腺病毒E2启动子,并能与激活的ras癌基因协同作用,转化原代新生大鼠肾细胞。所有与生殖器相关的HPV的E7蛋白的N端37个氨基酸包含高度保守的区域,这些区域与腺病毒E1A的保守结构域1和2的部分非常相似。E1A中的这些结构域对于细胞转化特性至关重要,并且包含与视网膜母细胞瘤肿瘤抑制基因(pRB)产物结合的氨基酸序列。与埃德·哈洛和尼克·戴森(冷泉港实验室)合作的研究结果表明,HPV - 16的E7癌蛋白在体外可与视网膜母细胞瘤基因产物结合(2)。已使用体外复合测定法检测了各种HPV编码的E7蛋白与pRB结合的能力。E7不足以使人角质形成细胞发生转化。已证明HPV - 16 E6和E7基因的协同作用对于这些细胞的转化很重要(3)。正在评估E6潜在的细胞内蛋白质靶点。

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