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复制依赖性组蛋白生物合成与细胞周期决定相关联。

Replication-dependent histone biosynthesis is coupled to cell-cycle commitment.

机构信息

Department of Biochemistry, University of Colorado, Boulder, CO 80303.

BioFrontiers Institute, University of Colorado, Boulder, CO 80309.

出版信息

Proc Natl Acad Sci U S A. 2021 Aug 3;118(31). doi: 10.1073/pnas.2100178118.

Abstract

The current model of replication-dependent (RD) histone biosynthesis posits that RD histone gene expression is coupled to DNA replication, occurring only in S phase of the cell cycle once DNA synthesis has begun. However, several key factors in the RD histone biosynthesis pathway are up-regulated by E2F or phosphorylated by CDK2, suggesting these processes may instead begin much earlier, at the point of cell-cycle commitment. In this study, we use both fixed- and live-cell imaging of human cells to address this question, revealing a hybrid model in which RD histone biosynthesis is first initiated in G1, followed by a strong increase in histone production in S phase of the cell cycle. This suggests a mechanism by which cells that have committed to the cell cycle build up an initial small pool of RD histones to be available for the start of DNA replication, before producing most of the necessary histones required in S phase. Thus, a clear distinction exists at completion of mitosis between cells that are born with the intention of proceeding through the cell cycle and replicating their DNA and cells that have chosen to exit the cell cycle and have no immediate need for histone synthesis.

摘要

目前的复制依赖性(RD)组蛋白生物合成模型假定,RD 组蛋白基因的表达与 DNA 复制偶联,仅在 DNA 合成开始后细胞周期的 S 期发生。然而,RD 组蛋白生物合成途径中的几个关键因素被 E2F 上调或被 CDK2 磷酸化,这表明这些过程可能更早开始,即在细胞周期启动时。在这项研究中,我们使用人类细胞的固定和活细胞成像来解决这个问题,揭示了一种混合模型,其中 RD 组蛋白生物合成首先在 G1 期开始,然后在细胞周期的 S 期组蛋白的产生急剧增加。这表明了一种机制,即已经决定进入细胞周期的细胞在开始 DNA 复制之前,会积累少量的 RD 组蛋白,然后在 S 期产生大部分所需的组蛋白。因此,在有丝分裂完成时,已经决定通过细胞周期并复制其 DNA 的细胞和选择退出细胞周期且没有立即需要组蛋白合成的细胞之间存在明显的区别。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/60c9/8346857/47b3650fa26d/pnas.2100178118fig01.jpg

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