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Purification of RIP60 and RIP100 mammalian proteins with origin-specific DNA-binding and ATP-dependent DNA helicase activities.

机译:纯化具有起源特异性DNA结合和ATP依赖性DNA解旋酶活性的哺乳动物蛋白RIP60和RIP100。

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摘要

Replication of the Chinese hamster dihydrofolate reductase gene (dhfr) initiates near a fragment of stably bent DNA that binds multiple cellular factors. Investigation of protein interactions with the dhfr bent DNA sequences revealed a novel nuclear protein that also binds to domain B of the yeast origin of replication, the autonomously replicating sequence ARS1. The origin-specific DNA-binding activity was purified 9,000-fold from HeLa cell nuclear extract in five chromatographic steps. Protein-DNA cross-linking experiments showed that a 60-kDa polypeptide, which we call RIP60, contained the origin-specific DNA-binding activity. Oligonucleotide displacement assays showed that highly purified fractions of RIP60 also contained an ATP-dependent DNA helicase activity. Covalent radiolabeling with ATP indicated that the DNA helicase activity resided in a 100-kDa polypeptide, RIP100. The cofractionation of an ATP-dependent DNA helicase with an origin-specific DNA-binding activity suggests that RIP60 and RIP100 may be involved in initiation of chromosomal DNA synthesis in mammalian cells.
机译:中国仓鼠二氢叶酸还原酶基因(dhfr)的复制在结合多个细胞因子的稳定弯曲的DNA片段附近开始。对与dhfr弯曲的DNA序列相互作用的蛋白质的研究揭示了一种新型核蛋白,该核蛋白也与酵母复制起点的域B(自主复制序列ARS1)结合。在五个色谱步骤中,从HeLa细胞核提取物中纯化了9,000倍的起源特异性DNA结合活性。蛋白质-DNA交联实验表明,一个60kDa的多肽(我们称为RIP60)包含起源特异性DNA结合活性。寡核苷酸置换分析表明,RIP60的高纯度片段还具有ATP依赖的DNA解旋酶活性。用ATP共价放射性标记表明DNA解旋酶活性位于100 kDa多肽RIP100中。具有起源特异性DNA结合活性的ATP依赖型DNA解旋酶的共馏表明,RIP60和RIP100可能参与哺乳动物细胞中染色体DNA合成的启动。

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