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原癌基因dbl中对其转化活性至关重要的一个区域,与酵母细胞周期基因CDC24以及人类断裂簇基因bcr存在序列相似性。

A region of proto-dbl essential for its transforming activity shows sequence similarity to a yeast cell cycle gene, CDC24, and the human breakpoint cluster gene, bcr.

作者信息

Ron D, Zannini M, Lewis M, Wickner R B, Hunt L T, Graziani G, Tronick S R, Aaronson S A, Eva A

机构信息

Laboratory of Cellular and Molecular Biology, National Cancer Institute, Bethesda, MD 20892.

出版信息

New Biol. 1991 Apr;3(4):372-9.

PMID:2065022
Abstract

Proto-dbl is a human proto-oncogene, whose oncogenic activation was initially detected by DNA transfection. We report significant sequence similarity between the predicted proto-dbl product and the products of CDC24, a Saccharomyces cerevisiae cell division cycle gene required for correct budding and establishment of cell polarity, and bcr, a gene implicated in the pathogenesis of chronic myelogenous leukemia (CML). Of 925 residues of the predicted proto-dbl protein, a stretch of 238 residues showed 29% and 22% identity over a region of similar length of the CDC24 and bcr proteins, respectively. When evolutionarily conservative substitutions were taken into account, the similarities were 68.8% and 71.6% for proto-dbl/CDC24 and proto-dbl/bcr gene products, respectively. Moreover, all three sequences were predicted to be markedly hydrophilic over this region. Very small deletions within the conserved region completely abolished transforming activity of dbl, while extensive deletion outside of this region had no effect. Even substitutions over a small stretch of close similarity with the other proteins substantially impaired transforming activity. Cells transformed by the dbl oncogene, like cdc24 mutants arrested at the nonpermissive temperature, form multinucleate cells. Thus, our findings indicate that the conserved region is an essential domain that may reflect important functional similarities among these otherwise highly divergent molecules.

摘要

原癌基因dbl是一种人类原癌基因,其致癌激活最初是通过DNA转染检测到的。我们报告了预测的原癌基因dbl产物与CDC24(酿酒酵母细胞分裂周期基因,对正确出芽和细胞极性的建立是必需的)以及bcr(一种与慢性粒细胞白血病(CML)发病机制有关的基因)的产物之间存在显著的序列相似性。在预测的原癌基因dbl蛋白的925个残基中,一段238个残基的区域在CDC24和bcr蛋白的相似长度区域分别显示出29%和22%的同一性。当考虑进化保守取代时,原癌基因dbl/CDC24和原癌基因dbl/bcr基因产物的相似性分别为68.8%和71.6%。此外,预计所有三个序列在该区域均具有明显的亲水性。保守区域内的非常小的缺失完全消除了dbl的转化活性,而该区域外的广泛缺失则没有影响。即使是与其他蛋白质有一小段紧密相似性的取代也会显著损害转化活性。由dbl癌基因转化的细胞,如在非允许温度下停滞的cdc24突变体,会形成多核细胞。因此,我们的研究结果表明,保守区域是一个必需结构域,可能反映了这些原本高度不同的分子之间重要的功能相似性。

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