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小鼠原癌基因vav家族成员vav2的分离与鉴定。

Isolation and characterization of murine vav2, a member of the vav family of proto-oncogenes.

作者信息

Schuebel K E, Bustelo X R, Nielsen D A, Song B J, Barbacid M, Goldman D, Lee I J

机构信息

Laboratory of Neurogenetics, National Institute on Alcohol Abuse and Alcoholism, National Institutes of Health, Rockville, Maryland 20852, USA.

出版信息

Oncogene. 1996 Jul 18;13(2):363-71.

PMID:8710375
Abstract

We describe the isolation and characterization of a cDNA encoding murine vav2. vav2 shares 63% and 55% identity at the nucleic acid and amino acid levels, respectively, with vav, a proto-oncogene that plays an essential role in embryonic development and hematopoietic signal transduction. The 100 kDa Vav2 protein contains the characteristic array of structural motifs found in Vav. However, unlike vav, vav2 transcripts are widely distributed in both hematopoietic and non-hematopoietic tissues. In the adult, vav2 mRNA is found at high levels in the spleen, liver, testes and placenta. Northern blot analysis reveals two vav2 mRNA species (designated alpha and beta). The alpha species is expressed throughout development while the alpha and beta species are expressed tissue-specifically in adults. Transfection of NIH3T3 cells with expression vectors containing vav2 deletions demonstrate that elimination of 183 amino terminal residues of Vav2 is sufficient to activate its oncogenic potential. Vav2-induced transformation is characterized by the appearance of foci composed of cells in which cytokinesis and karyokinesis are uncoupled. This phenotype is comparable, but not identical, to morphological changes induced by Vav and other members of the DbI family of oncoproteins. Our results suggest that Vav family members mediate functions important in the regulation of cell architecture and proliferation in most, if not all, tissues.

摘要

我们描述了编码小鼠vav2的cDNA的分离与特性。vav2在核酸水平和氨基酸水平上分别与vav有63%和55%的同源性,vav是一种原癌基因,在胚胎发育和造血信号转导中起关键作用。100 kDa的Vav2蛋白含有Vav中发现的特征性结构基序阵列。然而,与vav不同,vav2转录本在造血和非造血组织中广泛分布。在成体中,vav2 mRNA在脾脏、肝脏、睾丸和胎盘中高水平表达。Northern印迹分析揭示了两种vav2 mRNA种类(命名为α和β)。α种类在整个发育过程中都有表达,而α和β种类在成体中组织特异性表达。用含有vav2缺失的表达载体转染NIH3T3细胞表明,去除Vav2的183个氨基末端残基足以激活其致癌潜能。Vav2诱导的转化的特征是出现由胞质分裂和核分裂解偶联的细胞组成的集落。这种表型与Vav和DbI家族癌蛋白其他成员诱导的形态学变化相似,但不完全相同。我们的结果表明,Vav家族成员在大多数(如果不是全部)组织中调节细胞结构和增殖的重要功能中发挥介导作用。

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