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在酿酒酵母中进行全基因组筛选,鉴定了参与寿命调控的液泡蛋白分选、自噬、生物合成和 tRNA 甲基化基因。

Genome-wide screen in Saccharomyces cerevisiae identifies vacuolar protein sorting, autophagy, biosynthetic, and tRNA methylation genes involved in life span regulation.

机构信息

Andrus Gerontology Center and Department of Biological Sciences, University of Southern California, Los Angeles, California, United States of America.

出版信息

PLoS Genet. 2010 Jul 15;6(7):e1001024. doi: 10.1371/journal.pgen.1001024.

Abstract

The study of the chronological life span of Saccharomyces cerevisiae, which measures the survival of populations of non-dividing yeast, has resulted in the identification of homologous genes and pathways that promote aging in organisms ranging from yeast to mammals. Using a competitive genome-wide approach, we performed a screen of a complete set of approximately 4,800 viable deletion mutants to identify genes that either increase or decrease chronological life span. Half of the putative short-/long-lived mutants retested from the primary screen were confirmed, demonstrating the utility of our approach. Deletion of genes involved in vacuolar protein sorting, autophagy, and mitochondrial function shortened life span, confirming that respiration and degradation processes are essential for long-term survival. Among the genes whose deletion significantly extended life span are ACB1, CKA2, and TRM9, implicated in fatty acid transport and biosynthesis, cell signaling, and tRNA methylation, respectively. Deletion of these genes conferred heat-shock resistance, supporting the link between life span extension and cellular protection observed in several model organisms. The high degree of conservation of these novel yeast longevity determinants in other species raises the possibility that their role in senescence might be conserved.

摘要

对酿酒酵母的时间寿命的研究,即衡量非分裂酵母种群的存活能力的研究,已经确定了促进从酵母到哺乳动物等生物衰老的同源基因和途径。我们使用竞争的全基因组方法,对大约 4800 个可行的缺失突变体的整套进行了筛选,以鉴定那些增加或减少时序寿命的基因。从初次筛选中重新测试的半数假定的短寿命/长寿命突变体得到了确认,证明了我们方法的有效性。液泡蛋白分选、自噬和线粒体功能相关基因的缺失缩短了寿命,这证实了呼吸和降解过程对于长期生存是必不可少的。在删除后显著延长寿命的基因中,有参与脂肪酸转运和生物合成、细胞信号转导和 tRNA 甲基化的 ACB1、CKA2 和 TRM9。这些基因的缺失赋予了耐热性,支持了在几种模式生物中观察到的寿命延长与细胞保护之间的联系。这些新型酵母长寿决定因素在其他物种中的高度保守性,增加了它们在衰老过程中可能具有保守作用的可能性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/47a5/2904796/7ec34dcbbd5c/pgen.1001024.g001.jpg

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