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体外DNA复制过程中染色质的逐步组装。

Stepwise assembly of chromatin during DNA replication in vitro.

作者信息

Smith S, Stillman B

机构信息

Cold Spring Harbor Laboratory, NY 11724.

出版信息

EMBO J. 1991 Apr;10(4):971-80. doi: 10.1002/j.1460-2075.1991.tb08031.x.

Abstract

A cell free system that supports replication-dependent chromatin assembly has been used to determine the mechanism of histone deposition during DNA replication. CAF-I, a human cell nuclear factor, promotes chromatin assembly on replicating SV40 DNA in the presence of a crude cytosol replication extract. Biochemical fractionation of the cytosol extract has allowed separation of the chromatin assembly reaction into two steps. During the first step, CAF-I targets the deposition of newly synthesized histones H3 and H4 to the replicating DNA. This reaction is dependent upon and coupled with DNA replication, and utilizes the newly synthesized forms of histones H3 and H4, which unlike bulk histone found in chromatin, do not bind to DNA by themselves. The H3/H4-replicated DNA complex is a stable intermediate which exhibits a micrococcal nuclease resistant structure and can be isolated by sucrose gradient sedimentation. In the second step, this replicated precursor is converted to mature chromatin by the addition of histones H2A and H2B in a reaction that can occur after DNA replication. The requirement for CAF-I in at least the first step of the reaction suggests a level of cellular control for this fundamental process.

摘要

一种支持依赖复制的染色质组装的无细胞体系已被用于确定DNA复制过程中组蛋白沉积的机制。CAF-I是一种人类细胞核因子,在存在粗制胞质溶胶复制提取物的情况下,它能促进在复制的SV40 DNA上进行染色质组装。对胞质溶胶提取物进行生化分级分离,可将染色质组装反应分为两个步骤。在第一步中,CAF-I将新合成的组蛋白H3和H4沉积到正在复制的DNA上。该反应依赖于DNA复制并与之偶联,利用新合成形式的组蛋白H3和H4,它们与染色质中发现的大量组蛋白不同,自身不会与DNA结合。H3/H4-复制的DNA复合物是一种稳定的中间体,具有微球菌核酸酶抗性结构,可通过蔗糖梯度沉降法分离。在第二步中,通过在DNA复制后可发生的反应中添加组蛋白H2A和H2B,将这种复制的前体转化为成熟的染色质。该反应至少在第一步中对CAF-I的需求表明了对这一基本过程的细胞控制水平。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2e08/452741/36d3e77bcfa4/emboj00102-0236-a.jpg

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