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SET 结构域蛋白 Set3p 促进裂殖酵母细胞分裂的可靠执行。

The SET domain protein, Set3p, promotes the reliable execution of cytokinesis in Schizosaccharomyces pombe.

机构信息

Department of Biology, University of Western Ontario, London, Ontario, Canada.

出版信息

PLoS One. 2012;7(2):e31224. doi: 10.1371/journal.pone.0031224. Epub 2012 Feb 8.

Abstract

In response to perturbation of the cell division machinery fission yeast cells activate regulatory networks that ensure the faithful completion of cytokinesis. For instance, when cells are treated with drugs that impede constriction of the actomyosin ring (low doses of Latrunculin A, for example) these networks ensure that cytokinesis is complete before progression into the subsequent mitosis. Here, we identify three previously uncharacterized genes, hif2, set3, and snt1, whose deletion results in hyper-sensitivity to LatA treatment and in increased rates of cytokinesis failure. Interestingly, these genes are orthologous to TBL1X, MLL5, and NCOR2, human genes that encode components of a histone deacetylase complex with a known role in cytokinesis. Through co-immunoprecipitation experiments, localization studies, and phenotypic analysis of gene deletion mutants, we provide evidence for an orthologous complex in fission yeast. Furthermore, in light of the putative role of the complex in chromatin modification, together with our results demonstrating an increase in Set3p levels upon Latrunculin A treatment, global gene expression profiles were generated. While this analysis demonstrated that the expression of cytokinesis genes was not significantly affected in set3Δ backgrounds, it did reveal defects in the ability of the mutant to regulate genes with roles in the cellular response to stress. Taken together, these findings support the existence of a conserved, multi-protein complex with a role in promoting the successful completion of cytokinesis.

摘要

针对细胞分裂机制的干扰,裂殖酵母细胞会激活调控网络,以确保胞质分裂的准确完成。例如,当细胞被药物处理以阻止肌动球蛋白环的收缩(例如,低剂量的拉曲库铵)时,这些网络确保在进入后续有丝分裂之前完成胞质分裂。在这里,我们鉴定了三个以前未被表征的基因,hif2、set3 和 snt1,它们的缺失导致对 LatA 处理的超敏反应和胞质分裂失败率增加。有趣的是,这些基因与 TBL1X、MLL5 和 NCOR2 是同源的,人类基因编码一个组蛋白去乙酰化酶复合物的组成部分,该复合物在胞质分裂中具有已知的作用。通过共免疫沉淀实验、定位研究和基因缺失突变体的表型分析,我们提供了裂殖酵母中同源复合物的证据。此外,鉴于该复合物在染色质修饰中的假定作用,以及我们的结果表明在拉曲库铵处理后 Set3p 水平增加,生成了全局基因表达谱。虽然这项分析表明在 set3Δ 背景下胞质分裂基因的表达没有显著影响,但它确实揭示了突变体调节对压力有反应的基因的能力的缺陷。总之,这些发现支持存在一个保守的、多蛋白复合物,其在促进胞质分裂的成功完成中具有作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8f29/3275627/6938a9b81f58/pone.0031224.g001.jpg

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