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Protein aggregation triggers a declining libido in elder yeasts that still have a lust for life

机译:蛋白质聚集会触发仍具有生命欲望的老酵母中性欲下降

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摘要

Many organisms have to face a physiological decline that is associated with age. Humans and even budding yeast accumulate scars and cellular damages. A single yeast cell can only produce a limited number of daughter cells and thus has a finite replicative lifespan. Many studies have now identified molecular ageing factors and defects in organelle functions linked to the ageing process. However, at the cellular level, the most striking phenotype of yeast elders is their loss of mating ability. This sterility in old cells has been linked to a loss of response to mating pheromone, the peptide that haploid yeast cells send to opposite mating type cells in order to signal their presence and readiness to mate. Our results (Schlissel et al., 2017) demonstrate that old cells are unable to respond to mating pheromone due to age-induced aggregation of the protein Whi3. We recently discovered that Whi3 changes conformation and coalesces when cells experience and memorise a deceptive mating attempt. Together, these results prompt the question of how proteins physiologically aggregating behave during ageing, induce age associated phenotypes and influence the ageing process itself.
机译:许多生物必须面对与年龄有关的生理衰退。人类甚至萌芽的酵母都会积累疤痕和细胞损伤。单个酵母细胞只能产生有限数量的子代细胞,因此具有有限的复制寿命。现在,许多研究已经确定了分子衰老因子和与衰老过程相关的细胞器功能缺陷。但是,在细胞水平上,酵母长老最醒目的表型是其交配能力的丧失。老细胞中的这种无菌性与对交配信息素的反应丧失有关,该信息素是单倍体酵母细胞发送给相反的交配类型细胞的信号,以表示它们的存在和准备交配。我们的结果(Schlissel等人,2017)证明,由于年龄引起的Whi3蛋白聚集,旧细胞无法对交配信息素作出反应。我们最近发现,当细胞经历并记忆欺骗性的交配尝试时,Whi3会改变构象并合并。总之,这些结果引发了一个问题,即蛋白质在老化过程中如何在生理上聚集,诱导与年龄相关的表型并影响老化过程本身。

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