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阿贝尔逊鼠白血病病毒的定点缺失确定了转化和致死性所必需的3'序列。

Site-directed deletions of Abelson murine leukemia virus define 3' sequences essential for transformation and lethality.

作者信息

Watanabe S M, Witte O N

出版信息

J Virol. 1983 Mar;45(3):1028-36. doi: 10.1128/JVI.45.3.1028-1036.1983.

Abstract

Abelson murine leukemia virus (A-MuLV) encodes a single protein with tyrosine kinase activity that can transform fibroblast cell lines in vitro and lymphoid target cells in vitro and in vivo. Expression of kinase-active A-MuLV protein can result in a deleterious effect on transformed fibroblast populations, leading to cell death or selection for nonlethal mutants of the virus. These mutants retain expression of the kinase activity but have lost large portions of the carboxy terminus of the Abelson protein. To more precisely map the sequences involved in this lethal effect, we have isolated a series of site-directed deletions from a DNA clone of the P160 wild-type strain of A-MuLV. In addition, a number of unexpected, spontaneous deletions occurring during transfection of NIH 3T3 cells were isolated. These deletions result in expression of carboxy-terminal truncated forms of the A-MuLV protein ranging from 130,000 to 84,000 in molecular weight. Analysis of the transforming and lethal activities of each mutant recovered in its RNA viral form shows that the transformation-essential and lethal-essential sequences do not overlap. These data and our previous work suggest that a function carried by the carboxy-terminal region of the A-MuLV protein acts in cis with the kinase-essential region to mediate the lethal effect.

摘要

阿贝尔逊鼠白血病病毒(A-MuLV)编码一种具有酪氨酸激酶活性的单一蛋白质,该蛋白质在体外可转化成纤维细胞系,在体外和体内均可转化淋巴样靶细胞。激酶活性A-MuLV蛋白的表达可对转化的成纤维细胞群体产生有害影响,导致细胞死亡或选择该病毒的非致死性突变体。这些突变体保留了激酶活性的表达,但缺失了阿贝尔逊蛋白羧基末端的大部分区域。为了更精确地定位与这种致死效应相关的序列,我们从A-MuLV P160野生型菌株的DNA克隆中分离出一系列定点缺失。此外,还分离出了在NIH 3T3细胞转染过程中出现的一些意外的自发缺失。这些缺失导致了分子量从130,000到84,000不等的A-MuLV蛋白羧基末端截短形式的表达。对以RNA病毒形式回收的每个突变体的转化和致死活性进行分析表明,转化必需序列和致死必需序列不重叠。这些数据以及我们之前的研究表明,A-MuLV蛋白羧基末端区域所携带的一种功能与激酶必需区域顺式作用,以介导致死效应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/05f4/256510/5535e7d96a1f/jvirol00150-0142-a.jpg

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