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内源性小鼠C型病毒致癌性的获得:env和gag基因变异的影响。

Acquisition of oncogenicity by endogenous mouse type C viruses: effects of variations in env and gag genes.

作者信息

Devare S G, Rapp U R, Todaro G J, Stephenson J R

出版信息

J Virol. 1978 Nov;28(2):457-65. doi: 10.1128/JVI.28.2.457-465.1978.

Abstract

Several dual-tropic isolates derived from the thymuses of preleukemic or leukemic AKR mice and a more recrnt group of viruses generated by in vitro or in vivo passage of a poorly infectious endogenous virus of C3H mouse cells have been shown to be highly oncogenic. By analysis of the immunological properties of their gag gene-coded structural proteins, each of the AKR-derived isolates and two dual-tropic C3H-derived isolates were found to closely resemble AKR murine leukemia virus. In contrast, gag gene-coded proteins of two other leukemogenic isolates of C3H origin, including one ecotropic and one dual-tropic virus, were indistinguishable from those of Moloney murine leukemia virus. All of the oncogenic isolates, including those of AKR and C3H origin, were found to possess common envelope glycoprotein determinants of a unique class not shared by the nononcogenic ecotropic viruses from which they were derived. These findings support the possibility that oncogenic variants of endogenous ecotropic mouse type C viruses are derived by genetic recombination. This recombinational event appears to involve the acquisition, by different ecotropic viruses, of a common class of endogenous virus-coded envelope glycoprotein determinants which are presumably required, but not necessarily sufficient, for oncogenicity.

摘要

从白血病前期或白血病AKR小鼠胸腺中获得的几种双嗜性分离株,以及由C3H小鼠细胞的低感染性内源性病毒经体外或体内传代产生的一组更新的病毒,已被证明具有高度致癌性。通过分析其gag基因编码的结构蛋白的免疫特性,发现每一种源自AKR的分离株和两种源自C3H的双嗜性分离株都与AKR小鼠白血病病毒非常相似。相比之下,另外两种源自C3H的致白血病分离株(包括一种嗜亲性病毒和一种双嗜性病毒)的gag基因编码蛋白与莫洛尼小鼠白血病病毒的蛋白无法区分。所有致癌分离株,包括源自AKR和C3H的分离株,都被发现具有一类独特的共同包膜糖蛋白决定簇,而它们所衍生的非致癌嗜亲性病毒并不具有这类决定簇。这些发现支持了内源性嗜亲性小鼠C型病毒的致癌变体是通过基因重组产生的可能性。这种重组事件似乎涉及不同的嗜亲性病毒获得一类共同的内源性病毒编码包膜糖蛋白决定簇,这些决定簇大概是致癌性所必需的,但不一定足够。

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