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小鼠红白血病细胞分化过程中三类不同组蛋白mRNA水平的变化。

Changes in the levels of three different classes of histone mRNA during murine erythroleukemia cell differentiation.

作者信息

Brown D T, Wellman S E, Sittman D B

出版信息

Mol Cell Biol. 1985 Nov;5(11):2879-86. doi: 10.1128/mcb.5.11.2879-2886.1985.

Abstract

We used a gene-specific S1 nuclease assay to study the changes in steady-state mRNA levels of several core histone variants during the differentiation of murine erythroleukemia cells. These studies allowed us to distinguish three distinct expression classes of histone genes. The expression of the major replication-dependent class of histone genes was tightly linked to DNA synthesis. The concentrations of these transcripts decreased rapidly as cell division slowed during the process of differentiation. In contrast, the replication-independent H3.3 transcript levels were constitutively maintained throughout differentiation and were unaffected by inhibitors of DNA or protein synthesis. We also identified among the cloned histone genes used as probes a third expression class, the partially replication-dependent variants. Expression of these transcripts became transiently uncoupled from the reduced rate of DNA synthesis accompanying the early stages of differentiation. We show that their synthesis is sensitive to the DNA synthesis inhibitor hydroxyurea but that selective uncoupling from DNA synthesis of these histone mRNAs occurs at a specific stage of differentiation. We present several hypotheses to explain how this might be accomplished. The expression characteristics of the mRNAs studied coincided with those of the proteins for which they code, indicating that changes in the relative levels of the different variants is mediated at least in part by changes in mRNA levels.

摘要

我们使用基因特异性 S1 核酸酶分析方法,来研究小鼠红白血病细胞分化过程中几种核心组蛋白变体的稳态 mRNA 水平变化。这些研究使我们能够区分出三种不同的组蛋白基因表达类别。主要的依赖复制的组蛋白基因的表达与 DNA 合成紧密相关。随着细胞分化过程中细胞分裂减缓,这些转录本的浓度迅速下降。相比之下,不依赖复制的 H3.3 转录本水平在整个分化过程中持续维持,并且不受 DNA 或蛋白质合成抑制剂的影响。我们还在用作探针的克隆组蛋白基因中鉴定出了第三种表达类别,即部分依赖复制的变体。这些转录本的表达在分化早期伴随着 DNA 合成速率降低而暂时解偶联。我们表明它们的合成对 DNA 合成抑制剂羟基脲敏感,但这些组蛋白 mRNA 与 DNA 合成的选择性解偶联发生在分化的特定阶段。我们提出了几个假说来解释这可能是如何实现的。所研究的 mRNA 的表达特征与它们所编码的蛋白质的表达特征一致,这表明不同变体相对水平的变化至少部分是由 mRNA 水平的变化介导的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4cdd/369098/da24f7c1bf67/molcellb00141-0012-a.jpg

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