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染色质成熟依赖于持续的DNA复制。

Chromatin maturation depends on continued DNA-replication.

作者信息

Schlaeger E J, Pülm W, Knippers R

出版信息

FEBS Lett. 1983 Jun 13;156(2):281-6. doi: 10.1016/0014-5793(83)80513-4.

Abstract

The structure of [3H]thymidine pulse-labeled chromatin in lymphocytes differs from that of non-replicating chromatin by several operational criteria which are related to the higher nuclease sensitivity of replicating chromatin. These structural features of replicating chromatin rapidly disappear when the [3H]thymidine pulse is followed by a chase in the presence of an excess of non-radioactive thymidine. However, when the rate of DNA replication is reduced, as in cycloheximide-treated lymphocytes, chromatin maturation is retarded. No chromatin maturation is observed when nuclei from pulse-labeled lymphocytes are incubated in vitro in the absence of DNA precursors. In contrast, when these nuclei are incubated under conditions known to be optimal for DNA replication, the structure of replicating chromatin is efficiently converted to that of 'mature', non-replicating chromatin. We conclude that the properties of nascent DNA and/or the distance from the replication fork are important factors in chromatin maturation.

摘要

通过几个操作标准可知,淋巴细胞中经[3H]胸苷脉冲标记的染色质结构与非复制染色质不同,这些标准与复制染色质较高的核酸酶敏感性有关。当在过量非放射性胸苷存在的情况下进行追踪,紧跟在[3H]胸苷脉冲之后,复制染色质的这些结构特征会迅速消失。然而,当DNA复制速率降低时,如在环己酰亚胺处理的淋巴细胞中,染色质成熟会延迟。当脉冲标记淋巴细胞的细胞核在无DNA前体的情况下进行体外孵育时,未观察到染色质成熟。相反,当这些细胞核在已知对DNA复制最适的条件下孵育时,复制染色质的结构能有效地转变为“成熟的”非复制染色质的结构。我们得出结论,新生DNA的特性和/或与复制叉的距离是染色质成熟的重要因素。

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