Nab3 nuclear granule accumulation is driven by respiratory capacity.

IF 1.8 4区 生物学 Q3 GENETICS & HEREDITY
Katherine M Hutchinson, Jeremy C Hunn, Daniel Reines
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引用次数: 3

Abstract

Numerous biological processes involve proteins capable of transiently assembling into subcellular compartments necessary for cellular functions. One process is the RNA polymerase II transcription cycle which involves initiation, elongation, co-transcriptional modification of nascent RNA, and termination. The essential yeast transcription termination factor Nab3 is required for termination of small non-coding RNAs and accumulates into a compact nuclear granule upon glucose removal. Nab3 nuclear granule accumulation varies in penetrance across yeast strains and a higher Nab3 granule accumulation phenotype is associated with petite strains, suggesting a possible ATP-dependent mechanism for granule disassembly. Here, we demonstrate the uncoupling of mitochondrial oxidative phosphorylation by drug treatment or deletions of nuclear-encoded ATP synthase subunit genes were sufficient to increase Nab3 granule accumulation and led to an inability to proliferate during prolonged glucose deprivation, which requires respiration. Additionally, by enriching for respiration competent cells from a petite-prone strain, we generated a low granule-accumulating strain from a relatively high one, providing another link between respiratory competency and Nab3 granules. Consistent with the resulting idea that ATP is involved in granule accumulation, the addition of extracellular ATP to semi-permeabilized cells was sufficient to reduce Nab3 granule accumulation. Deleting the SKY1 gene, which encodes a kinase that phosphorylates nuclear SR repeat-containing proteins and is involved in efficient stress granule disassembly, also resulted in increased granule accumulation. This observation implicates Sky1 in Nab3 granule biogenesis. Taken together, these findings suggest there is normally an equilibrium between termination factor granule assembly and disassembly mediated by ATP-requiring nuclear machinery.

Abstract Image

Nab3核颗粒的积累受呼吸能力的驱动。
许多生物过程都涉及到能够瞬间组装成细胞功能所必需的亚细胞区室的蛋白质。一个过程是RNA聚合酶II转录周期,包括起始、延伸、新生RNA的共转录修饰和终止。酵母必需的转录终止因子Nab3是终止小的非编码rna所必需的,并在葡萄糖去除时积聚成致密的核颗粒。在不同酵母菌株中,Nab3核颗粒积累的外显率不同,并且较高的Nab3颗粒积累表型与较小的菌株相关,这表明可能存在atp依赖的颗粒分解机制。在这里,我们证明了通过药物治疗或核编码ATP合成酶亚基基因的缺失,线粒体氧化磷酸化的解偶联足以增加Nab3颗粒的积累,并导致在需要呼吸的长时间葡萄糖剥夺期间无法增殖。此外,通过从一个微小倾向的菌株中富集呼吸能力细胞,我们从一个相对较高的菌株中产生了一个低颗粒积累的菌株,在呼吸能力和Nab3颗粒之间提供了另一个联系。与由此得出的ATP参与颗粒积累的观点一致,向半透性细胞中添加细胞外ATP足以减少Nab3颗粒的积累。SKY1基因编码一种激酶,该激酶磷酸化核SR重复序列蛋白,并参与有效的应激颗粒分解,删除该基因也会导致颗粒积累增加。这一发现暗示了Sky1参与Nab3颗粒的生物发生。综上所述,这些发现表明,在atp需要的核机制介导的终止因子颗粒组装和拆卸之间通常存在平衡。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Current Genetics
Current Genetics 生物-遗传学
CiteScore
6.00
自引率
0.00%
发文量
34
审稿时长
1 months
期刊介绍: Current Genetics publishes genetic, genomic, molecular and systems-level analysis of eukaryotic and prokaryotic microorganisms and cell organelles. All articles are peer-reviewed. The journal welcomes submissions employing any type of research approach, be it analytical (aiming at a better understanding), applied (aiming at practical applications), synthetic or theoretical. Current Genetics no longer accepts manuscripts describing the genome sequence of mitochondria/chloroplast of a small number of species. Manuscripts covering sequence comparisons and analyses that include a large number of species will still be considered.
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