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MCF鼠白血病病毒是包膜(env)基因重组体的生化证据。

Biochemical evidence that MCF murine leukemia viruses are envelope (env) gene recombinants.

作者信息

Elder J H, Gautsch J W, Jensen F C, Lerner R A, Hartley J W, Rowe W P

出版信息

Proc Natl Acad Sci U S A. 1977 Oct;74(10):4676-80. doi: 10.1073/pnas.74.10.4676.

Abstract

Recently, a novel class of murine type C virus (MCF), some strains of which are highly oncogenic in the AKR acceleration test, has been isolated from premalignant and malignant thymuses of AKR mice. The biology of these viruses suggested that MCFs are the product of recombination between endogenous ecotropic and xenotropic viruses and, further, that the recombination has taken place within the envelope (env) gene which encodes the surface glycoprotein (gp70) of the virion. We have compared by tryptic peptide analysis, the gp70s of four MCF isolates with the gp70s of various possible parental viruses. In addition, we have compared the tryptic peptides of the gag gene products p30 and p15 from several of these viruses. The results allow the following conclusions: (i) the gp70s of the MCF viruses are not identical to one another and are different from the gp70s of the possible parental viruses tested; (ii) the MCF virus gp70s have tryptic peptides in common with xenotropic virus gp70s as well as with ecotropic virus gp70s; and (iii) the gap region protein, p30, of the MCFs tested is identical to p30 of AKR ecotropic virus (Akv-1 or Akv-2) and distinct from p30 of xenotropic viruses, suggesting that the 5' end of the recombinant viruses is of Akv origin. The findings are discussed with respect to the possible role a recombinant virus might play in leukemogenesis in AKR mice.

摘要

最近,从AKR小鼠的癌前和恶性胸腺中分离出了一类新型的鼠C型病毒(MCF),其中一些毒株在AKR加速试验中具有高度致癌性。这些病毒的生物学特性表明,MCF是内源性亲嗜性病毒和异嗜性病毒之间重组的产物,而且这种重组发生在编码病毒粒子表面糖蛋白(gp70)的包膜(env)基因内。我们通过胰蛋白酶肽分析,将四种MCF分离株的gp70与各种可能的亲本病毒的gp70进行了比较。此外,我们还比较了其中几种病毒的gag基因产物p30和p15的胰蛋白酶肽。结果得出以下结论:(i)MCF病毒的gp70彼此不相同,且与所测试的可能亲本病毒的gp70不同;(ii)MCF病毒的gp70具有与异嗜性病毒gp70以及亲嗜性病毒gp70共有的胰蛋白酶肽;(iii)所测试的MCF的间隔区蛋白p30与AKR亲嗜性病毒(Akv-1或Akv-2)的p30相同,与异嗜性病毒的p30不同,这表明重组病毒的5'端起源于Akv。本文就重组病毒在AKR小鼠白血病发生中可能发挥的作用对这些发现进行了讨论。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0c81/432010/20ca54229e0c/pnas00032-0574-a.jpg

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