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艾氏腹水癌细胞早期S期复制子的选择性同步激活

Selective and synchronous activation of early-S-phase replicons of Ehrlich ascites cells.

作者信息

Gekeler V, Epple J, Kleymann G, Probst H

机构信息

Physiologisch-chemisches Institut, Universität Tübingen, Germany.

出版信息

Mol Cell Biol. 1993 Aug;13(8):5020-33. doi: 10.1128/mcb.13.8.5020-5033.1993.

Abstract

Twelve-hour exposure of G1 Ehrlich ascites cells to controlled hypoxia (200 ppm of O2 at 1 bar) suppressed replicon initiation. Synchronous cycling, beginning with a normal S phase, was released by reoxygenation immediately. The addition of cycloheximide at reoxygenation largely resuppressed, after a short initial burst, succeeding replicon initiations. Alkaline sedimentation analysis of growing daughter strand DNA, DNA fiber autoradiography, and analysis of the newly formed DNA demonstrated that normal chain growth and DNA maturation (replicon termination) in the initially activated replicons continued in the presence of cycloheximide. After 2 to 3 h, a low level of cycloheximide-insensitive background replication emerged out of the then-ebbing single surge of activity of the initially released replicons.

摘要

将G1期艾氏腹水细胞置于可控性低氧环境(1巴压力下氧气含量为200 ppm)中12小时,可抑制复制子起始。从正常S期开始的同步循环在复氧后立即恢复。复氧时添加环己酰亚胺,在短暂的初始爆发后,随后的复制子起始大多被再次抑制。对正在生长的子链DNA进行碱性沉降分析、DNA纤维放射自显影以及对新形成的DNA进行分析,结果表明,在存在环己酰亚胺的情况下,最初激活的复制子中的正常链生长和DNA成熟(复制子终止)仍在继续。2至3小时后,在最初释放的复制子当时逐渐减弱的单次活性高峰中,出现了低水平的对环己酰亚胺不敏感的背景复制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bb50/360151/1ff0aff35933/molcellb00020-0582-a.jpg

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