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T抗原在多瘤病毒转化中的作用:c-myc而非c-fos或c-jun的表达是中T抗原的作用靶点。

T antigens' role in polyomavirus transformation: c-myc but not c-fos or c-jun expression is a target for middle T.

作者信息

Rameh L E, Armelin M C

机构信息

Universidade de São Paulo, Instituto de Quimica, Brasil.

出版信息

Oncogene. 1991 Jun;6(6):1049-56.

PMID:1648700
Abstract

Polyoma virus (Py) causes neoplastic transformation in vitro and multiple tumors in vivo. The role played by large and middle T antigens (LT, MT) and their mechanisms of action are focused here. Py-transformed Balb-3T3 cells become independent of platelet-derived growth factor (PDGF) for growth. JE, c-fos, c-jun and c-myc are 'immediate early' genes induced in response to PDGF. To test whether these cellular genes play a role in malignant transformation by Py, we generated a number of transfectant cell lines overexpressing LT, MT or both. Characterization of these cell lines revealed that: (a) MT but not LT causes morphological transformation, ability to grow in agarose suspension; (b) cooperation between LT and MT is evident in vitro, however, high and simultaneous LT and MT expression does not warrant tumorigenic potential; (c) MT expression does not correlate with tumorigenic potential but alters the probability of eliciting tumors; (d) JE and c-myc (but not c-fos or c-jun) are constitutively expressed in MT transfectants. MT induction is followed by c-myc induction 1.5 h later. We conclude that some of the 'immediate-early' genes may play pivotal roles in Py transformation.

摘要

多瘤病毒(Py)在体外可引起肿瘤转化,在体内可引发多种肿瘤。本文重点探讨大T抗原和中T抗原(LT、MT)所起的作用及其作用机制。Py转化的Balb-3T3细胞在生长过程中变得不依赖血小板衍生生长因子(PDGF)。JE、c-fos、c-jun和c-myc是响应PDGF诱导的“立即早期”基因。为了测试这些细胞基因是否在Py介导的恶性转化中发挥作用,我们构建了多个过表达LT、MT或两者的转染细胞系。对这些细胞系的特性分析表明:(a)MT而非LT可导致形态转化,具备在琼脂糖悬液中生长的能力;(b)LT和MT之间的协同作用在体外很明显,然而,LT和MT的高表达且同时表达并不保证具有致瘤潜力;(c)MT的表达与致瘤潜力无关,但会改变引发肿瘤的概率;(d)JE和c-myc(而非c-fos或c-jun)在MT转染细胞中组成性表达。MT诱导后1.5小时会出现c-myc诱导。我们得出结论,一些“立即早期”基因可能在Py转化中起关键作用。

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