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人类kin17蛋白直接与猿猴病毒40大T抗原相互作用并抑制DNA复制。

Human kin17 protein directly interacts with the simian virus 40 large T antigen and inhibits DNA replication.

作者信息

Miccoli Laurent, Biard Denis S F, Créminon Christophe, Angulo Jaime F

机构信息

CEA, Commissariat à l'Energie Atomique, Laboratoire de Génétique de la Radiosensibilité, Direction des Sciences du Vivant, 92265 Fontenay-aux-Roses, France.

出版信息

Cancer Res. 2002 Oct 1;62(19):5425-35.

Abstract

Kin17 is an evolutionarily conserved DNA-binding protein, which forms intranuclear foci in proliferating cells. Recent data have suggested that human kin17 protein is associated with cell proliferation and unrepaired DNA lesions. Herein, we show that human fibroblasts (MRC5-V2 and CHSV4) immortalized with SV40 overexpress endogenous kin17 protein, as compared with normal diploid human fibroblasts. We observed that certain carcinoma cell lines also up-regulated kin17 protein, suggesting that increased kin17 protein levels may be a consequence of the immortalized phenotype. We report here that the endogenous kin17 protein is located in nucleoplasmic foci and colocalizes with SV40 large T antigen. Purification of human kin17 protein allowed analysis of the physical interaction with T antigen by several in vitro and in vivo assays. Large T antigen and human kin17 protein are part of the same high molecular weight multiprotein complex in human cells. Furthermore, human kin17 protein interacts with T antigen bound to the SV40 DNA origin of replication. Strikingly, the overexpression of human kin17 protein in vivo and the introduction of increased amounts of human kin17 protein in an in vitro assay reduced T-antigen-dependent DNA replication, suggesting that kin17 protein may be involved in the DNA replication process in human cells.

摘要

Kin17是一种进化上保守的DNA结合蛋白,在增殖细胞中形成核内病灶。最近的数据表明,人类kin17蛋白与细胞增殖和未修复的DNA损伤有关。在此,我们表明,与正常二倍体人类成纤维细胞相比,用SV40永生化的人类成纤维细胞(MRC5-V2和CHSV4)过表达内源性kin17蛋白。我们观察到某些癌细胞系也上调了kin17蛋白,这表明kin17蛋白水平的增加可能是永生化表型的结果。我们在此报告,内源性kin17蛋白位于核质病灶中,并与SV40大T抗原共定位。通过几种体外和体内试验对人类kin17蛋白的纯化使得能够分析其与T抗原的物理相互作用。大T抗原和人类kin17蛋白是人类细胞中同一高分子量多蛋白复合物的一部分。此外,人类kin17蛋白与结合在SV40 DNA复制起点的T抗原相互作用。令人惊讶的是,体内人类kin17蛋白的过表达以及体外试验中增加人类kin17蛋白的量会降低T抗原依赖性DNA复制,这表明kin17蛋白可能参与人类细胞中的DNA复制过程。

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