The chronological lifespan of budding yeast is a model of aging and age-related diseases. This paradigm has recently allowed genome-wide screening of genetic factors underlying post-mitotic viability in a simple unicellular system, which underscores its potential to provide a comprehensive view of the aging process. However, results from different large-scale studies show little overlap and typically lack quantitative resolution to derive interactions among different aging factors. We previously introduced a sensitive, parallelizable approach to measure the chronological-lifespan effects of gene deletions based on the competitive aging of fluorescence-labeled strains. Here, we present a thorough description of the method, including an improved multiple-regression model to estimate the association between death rates and fluorescent signals, which accounts for possible differences in growth rate and experimental batch effects. We illustrate the experimental procedure-from data acquisition to calculation of relative survivorship-for ten deletion strains with known lifespan phenotypes, which is achieved with high technical replicability. We apply our method to screen for gene-drug interactions in an array of yeast deletion strains, which reveals a functional link between protein glycosylation and lifespan extension by metformin. Competitive-aging screening coupled to multiple-regression modeling provides a powerful, straight-forward way to identify aging factors in yeast and their interactions with pharmacological interventions.
An Optimized Competitive-Aging Method Reveals Gene-Drug Interactions Underlying the Chronological Lifespan of Saccharomyces cerevisiae.
优化的竞争性衰老方法揭示了酿酒酵母寿命背后的基因-药物相互作用
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作者:Avelar-Rivas J Abraham, MunguÃa-Figueroa Michelle, Juárez-Reyes Alejandro, Garay Erika, Campos Sergio E, Shoresh Noam, DeLuna Alexander
| 期刊: | Frontiers in Genetics | 影响因子: | 2.800 |
| 时间: | 2020 | 起止号: | 2020 May 14; 11:468 |
| doi: | 10.3389/fgene.2020.00468 | 研究方向: | 发育与干细胞 |
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