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Akt癌基因及其人类同源物AKT1和AKT2的分子克隆:原发性人类胃腺癌中AKT1的扩增

Molecular cloning of the akt oncogene and its human homologues AKT1 and AKT2: amplification of AKT1 in a primary human gastric adenocarcinoma.

作者信息

Staal S P

出版信息

Proc Natl Acad Sci U S A. 1987 Jul;84(14):5034-7. doi: 10.1073/pnas.84.14.5034.

Abstract

A previous report described the isolation of a directly transforming retrovirus, AKT8, from a spontaneous thymoma of an AKR mouse. The AKT8 provirus has now been molecularly cloned from a transformed, nonproducer cell line. The virus genome contains both viral and nonviral, cell-related sequences; the nonviral sequence has been designated v-akt, the presumed viral oncogene of the AKT8 virus. This gene lacks homology to the 16 other oncogenes tested. The cloned provirus has undergone a partial deletion, during cell passage in vitro, that prevents direct demonstration of the transforming ability of this molecular clone. Two human homologues of the v-akt oncogene, AKT1 and AKT2, were cloned. A survey of 225 human tumors for changes involving AKT1 led to the discovery of a 20-fold amplification of this gene in one of the five gastric adenocarcinomas tested. The results demonstrate that AKT8 has the characteristic structure of a directly transforming retrovirus and that it contains a gene derived from highly conserved cellular sequences that may be involved in the pathogenesis of some human malignancies.

摘要

先前的一份报告描述了从一只AKR小鼠的自发性胸腺瘤中分离出一种直接转化逆转录病毒AKT8。现在已从一个转化的非生产性细胞系中对AKT8前病毒进行了分子克隆。病毒基因组包含病毒和非病毒的、与细胞相关的序列;该非病毒序列已被命名为v-akt,即AKT8病毒的假定病毒癌基因。该基因与所检测的其他16种癌基因均无同源性。在体外细胞传代过程中,克隆的前病毒发生了部分缺失,这使得无法直接证明该分子克隆的转化能力。克隆了v-akt癌基因的两个人类同源物AKT1和AKT2。对225例人类肿瘤进行的涉及AKT1变化的调查发现,在所检测的5例胃腺癌中的1例中该基因有20倍的扩增。结果表明,AKT8具有直接转化逆转录病毒的特征结构,并且它包含一个源自高度保守细胞序列的基因,该基因可能参与某些人类恶性肿瘤的发病机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d0ee/305241/3d19f6dd2980/pnas00279-0379-a.jpg

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