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人乳头瘤病毒E7蛋白在大鼠3Y1细胞中的功能

The E7 functions of human papillomaviruses in rat 3Y1 cells.

作者信息

Watanabe S, Sato H, Komiyama N, Kanda T, Yoshiike K

机构信息

Department of Enteroviruses, National Institute of Health, Tokyo, Japan.

出版信息

Virology. 1992 Mar;187(1):107-14. doi: 10.1016/0042-6822(92)90299-5.

Abstract

Among more than 60 human papillomavirus (HPV) genotypes, several HPVs are believed to be high risk because they are found in close association with cervical carcinoma. We compared the E7 genes from HPVs 1, 6b, 16, 18, and 33 for their transactivating, transforming, and mitogenic functions in a single cell line rat 3Y1. Whereas both the low-risk (1 and 6b) and the high-risk (16, 18, and 33) HPVs were transactivating for the adenovirus E2 promoter, only the high-risk HPVs were capable of focal transformation as assayed by an efficient method using the SR alpha-promoter and in conjunction with the HPV 16 E6 gene. The putative oncogenicity of HPVs appears to be reflected in vitro by the focal transformation, but not by the transactivation. Transient expression of the E7 genes controlled by the dexamethasone-responsive MMTV-LTR showed that the HPV 16 mutant E7s only with residual transforming activity were not mitogenic, but that, although the low-risk HPV E7s were less efficient, both the low-risk and high-risk HPV E7s were capable of inducing cellular DNA synthesis. Probably, the capability to induce cell DNA synthesis is necessary but not sufficient for the E7-mediated focal transformation.

摘要

在60多种人乳头瘤病毒(HPV)基因型中,有几种HPV被认为是高危型,因为它们与宫颈癌密切相关。我们比较了HPV 1、6b、16、18和33的E7基因在单细胞系大鼠3Y1中的反式激活、转化和促有丝分裂功能。低危型(1和6b)和高危型(16、18和33)HPV均可反式激活腺病毒E2启动子,但只有高危型HPV能够通过使用SRα启动子并结合HPV 16 E6基因的有效方法检测到的灶性转化。HPV的假定致癌性在体外似乎通过灶性转化反映出来,而不是通过反式激活。由地塞米松应答性MMTV-LTR控制的E7基因的瞬时表达表明,仅具有残余转化活性的HPV 16突变体E7不具有促有丝分裂作用,但是,尽管低危型HPV E7效率较低,但低危型和高危型HPV E7均能够诱导细胞DNA合成。可能,诱导细胞DNA合成的能力对于E7介导的灶性转化是必要的,但不是充分的。

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