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Proteasomal adaptation to environmental stress links resistance to proteotoxicity with longevity in Caenorhabditis elegans

机译:蛋白酶体对环境压力的适应将秀丽隐杆线虫对蛋白毒性的抵抗力与长寿联系起来

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摘要

The burden of protein misfolding is believed to contribute to aging. However, the links between adaptations to conditions associated with protein misfolding and resistance to the time-dependent attrition of cellular function remain poorly understood. We report that worms lacking aip-1, a homologue of mammalian AIRAP (arsenic-inducible proteasomal 19S regulatory particle-associated protein), are not only impaired in their ability to resist exposure to arsenite but also exhibit shortened lifespan and hypersensitivity to misfolding-prone proteins under normal laboratory conditions. Mammals have a second, constitutively expressed AIRAP-like gene (AIRAPL) that also encodes a proteasome-interacting protein, which shares with AIRAP the property of enhancing peptide accessibility to the proteasome's active site. Genetic rescue experiments suggest that features common to the constitutively expressed worm AIP-1 and mammalian AIRAPL (but missing in the smaller, arsenite-inducible AIRAP) are important to lifespan extension. In worms, a single AIRAP-related protein links proteasomal adaptation to environmental stress with resistance to both proteotoxic insults and maintenance of animal life span under normal conditions.
机译:蛋白质错误折叠的负担被认为会导致衰老。然而,对与蛋白质错误折叠相关的条件的适应与对细胞功能的时间依赖性磨损的抵抗之间的联系仍然知之甚少。我们报告说,蠕虫缺乏aip-1,即哺乳动物AIRAP(砷诱导的蛋白酶体19S调控颗粒相关蛋白)的同系物,不仅削弱了它们抵抗暴露于亚砷酸盐的能力,而且还缩短了寿命,并且对易错折的食物过敏正常实验室条件下的蛋白质。哺乳动物具有第二个组成性表达的AIRAP样基因(AIRAPL),该基因还编码与蛋白酶体相互作用的蛋白,该蛋白与AIRAP具有增强肽对蛋白酶体活性位点可及性的特性。基因挽救实验表明,组成性表达蠕虫AIP-1和哺乳动物AIRAPL的共同特征(但在较小的,由亚砷酸盐诱导的AIRAP中缺失)对于延长寿命很重要。在蠕虫中,单个AIRAP相关蛋白将蛋白酶体适应环境压力与对蛋白毒性侵害的抵抗力和正常条件下动物寿命的维持联系起来。

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