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功能基因组学表明,酵母需要高尔基体/内质网运输、染色质重塑和 DNA 修复才能耐受低剂量 DMSO。

Functional genomics indicates yeast requires Golgi/ER transport, chromatin remodeling, and DNA repair for low dose DMSO tolerance.

机构信息

Department of Nutritional Science and Toxicology, University of California Berkeley, CA, USA.

出版信息

Front Genet. 2013 Aug 13;4:154. doi: 10.3389/fgene.2013.00154. eCollection 2013.

Abstract

Dimethyl sulfoxide (DMSO) is frequently utilized as a solvent in toxicological and pharmaceutical investigations. It is therefore important to establish the cellular and molecular targets of DMSO in order to differentiate its intrinsic effects from those elicited by a compound of interest. We performed a genome-wide functional screen in Saccharomyces cerevisiae to identify deletion mutants exhibiting sensitivity to 1% DMSO, a concentration standard to yeast chemical profiling studies. We report that mutants defective in Golgi/ER transport are sensitive to DMSO, including those lacking components of the conserved oligomeric Golgi (COG) complex. Moreover, strains deleted for members of the SWR1 histone exchange complex are hypersensitive to DMSO, with additional chromatin remodeling mutants displaying a range of growth defects. We also identify DNA repair genes important for DMSO tolerance. Finally, we demonstrate that overexpression of histone H2A.Z, which replaces chromatin-associated histone H2A in a SWR1-catalyzed reaction, confers resistance to DMSO. Many yeast genes described in this study have homologs in more complex organisms, and the data provided is applicable to future investigations into the cellular and molecular mechanisms of DMSO toxicity.

摘要

二甲基亚砜(DMSO)经常被用作毒理学和药物研究中的溶剂。因此,确定 DMSO 的细胞和分子靶标对于将其固有效应与感兴趣化合物引起的效应区分开来非常重要。我们在酿酒酵母中进行了全基因组功能筛选,以鉴定对 1% DMSO 敏感的缺失突变体,这是酵母化学特征研究的标准浓度。我们报告说,高尔基体/内质网运输缺陷的突变体对 DMSO 敏感,包括那些缺乏保守寡聚高尔基体(COG)复合物成分的突变体。此外,缺失 SWR1 组蛋白交换复合物成员的菌株对 DMSO 高度敏感,其他染色质重塑突变体显示出一系列生长缺陷。我们还确定了对 DMSO 耐受性很重要的 DNA 修复基因。最后,我们证明了组蛋白 H2A.Z 的过表达赋予了对 DMSO 的抗性,组蛋白 H2A.Z 在 SWR1 催化的反应中取代染色质相关的组蛋白 H2A。本研究中描述的许多酵母基因在更复杂的生物体中都有同源物,提供的数据可适用于未来对 DMSO 毒性的细胞和分子机制的研究。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a9a9/3741465/a1ddb3a0f9b9/fgene-04-00154-g0001.jpg

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