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中国仓鼠二氢叶酸还原酶结构域中复制的起始

Initiation of replication in the Chinese hamster dihydrofolate reductase domain.

作者信息

Hamlin J L, Dijkwel P A, Vaughn J P

机构信息

Department of Biochemistry, University of Virginia School of Medicine, Charlottesville 22908.

出版信息

Chromosoma. 1992;102(1 Suppl):S17-23. doi: 10.1007/BF02451781.

Abstract

Two-dimensional (2-D) gel analysis of replication intermediates in the Chinese hamster dihydrofolate reductase domain has suggested that nascent chains can initiate at any of a large number of sites scattered throughout a approximately 50 kb "initiation locus" (although the level of initiation detected at any given site within this region was relatively low). This result contrasts markedly with data from an in vitro strand switching assay suggesting that > 80% of initiations occur within a single 500 bp fragment lying within the initiation locus. In an effort to reconcile these two disparate views of the initiation reaction, we have questioned the validity of our 2-D gel data in several ways. We show here that: 1) the number of replication bubbles detected in the DHFR locus in the early S period is markedly increased when the cells are released from a synchronizing agent that inhibits initiation per se, rather than from aphidicolin, which is a chain elongation inhibitor; 2) initiation in the DHFR domain occurs only during the first 90 min of the S period, as would be expected of an early-firing origin; 3) a pulse of 3H-thymidine moves through the structures observed on 2-D gels with the kinetics expected of bonafide replication intermediates; and 4) preparations of replication intermediates that are subsequently analyzed on 2-D gels appear, by electron microscopy, to represent the typical theta structures and single-forked molecules expected of bidirectional origins of replication; no unusual structures (e.g., microbubbles) were seen.

摘要

对中国仓鼠二氢叶酸还原酶结构域中复制中间体的二维凝胶分析表明,新生链可在散布于约50 kb“起始位点”内的大量位点中的任何一个起始(尽管在该区域内任何给定位点检测到的起始水平相对较低)。这一结果与体外链交换分析的数据形成鲜明对比,后者表明超过80%的起始发生在起始位点内的一个500 bp片段内。为了调和这两种关于起始反应的不同观点,我们从几个方面质疑了二维凝胶数据的有效性。我们在此表明:1)当细胞从抑制起始本身的同步剂而非链延伸抑制剂阿非迪霉素中释放时,在S期早期在二氢叶酸还原酶位点检测到的复制泡数量显著增加;2)二氢叶酸还原酶结构域中的起始仅发生在S期的前90分钟,这符合早期起始位点的预期;3)3H-胸腺嘧啶脉冲以真正复制中间体预期的动力学穿过二维凝胶上观察到的结构;4)随后在二维凝胶上分析的复制中间体制剂,通过电子显微镜观察,似乎代表了双向复制起始位点预期的典型θ结构和单叉分子;未观察到异常结构(如微泡)。

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