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内源性野生型布卢姆综合征DNA解旋酶的细胞周期调控

Cell cycle regulation of the endogenous wild type Bloom's syndrome DNA helicase.

作者信息

Dutertre S, Ababou M, Onclercq R, Delic J, Chatton B, Jaulin C, Amor-Guéret M

机构信息

Centre National de la Recherche Scientifique, Unité Mixte de Recherche 1598, Institut Gustave Roussy, 39 Rue Camille Desmoulins, 94 805 Villejuif Cedex, France.

出版信息

Oncogene. 2000 May 25;19(23):2731-8. doi: 10.1038/sj.onc.1203595.

DOI:10.1038/sj.onc.1203595
PMID:10851073
Abstract

Bloom's syndrome (BS) is a rare human autosomal recessive disorder characterized by an increased risk to develop cancer of all types. BS cells are characterized by a generalized genetic instability including a high level of sister chromatid exchanges. BS arises through mutations in both alleles of the BLM gene which encodes a 3' - 5' DNA helicase identified as a member of the RecQ family. We developed polyclonal antibodies specific for the NH2- and COOH-terminal region of BLM. Using these antibodies, we analysed BLM expression during the cell cycle and showed that the BLM protein accumulates to high levels in S phase, persists in G2/M and sharply declines in G1, strongly suggestive of degradation during mitosis. The BLM protein is subject to post-translational modifications in mitosis, as revealed by slow migrating forms of BLM found in both demecolcine-treated cells and in mitotic cells isolated from non-treated asynchronous populations. Phosphatase treatment indicated that phosphorylation events were solely responsible for the appearance of the retarded moieties, a possible signal for subsequent degradation. Together, these results are consistent with a role of BLM in a replicative (S phase) and/or post-replicative (G2 phase) process. Oncogene (2000).

摘要

布卢姆综合征(BS)是一种罕见的人类常染色体隐性疾病,其特征是患各种类型癌症的风险增加。BS细胞的特征是普遍存在遗传不稳定性,包括高水平的姐妹染色单体交换。BS是由BLM基因的两个等位基因发生突变引起的,该基因编码一种3'-5'DNA解旋酶,被鉴定为RecQ家族的成员。我们开发了针对BLM氨基末端和羧基末端区域的多克隆抗体。使用这些抗体,我们分析了细胞周期中BLM的表达,结果表明BLM蛋白在S期积累到高水平,在G2/M期持续存在,在G1期急剧下降,这强烈表明在有丝分裂期间会发生降解。如在秋水仙碱处理的细胞和从未经处理的异步群体中分离出的有丝分裂细胞中发现的迁移缓慢的BLM形式所揭示的,BLM蛋白在有丝分裂中会发生翻译后修饰。磷酸酶处理表明磷酸化事件是导致迁移受阻部分出现的唯一原因,这可能是随后降解的信号。总之,这些结果与BLM在复制(S期)和/或复制后(G2期)过程中的作用一致。《癌基因》(2000年)

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Cell cycle regulation of the endogenous wild type Bloom's syndrome DNA helicase.内源性野生型布卢姆综合征DNA解旋酶的细胞周期调控
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