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Reduced Insulin/IGF-1 Signaling Restores the Dynamic Properties of Key Stress Granule Proteins during Aging

机译:减少的胰岛素/ IGF-1信号恢复了衰老过程中关键应激颗粒蛋白的动态特性

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Low-complexity ''prion-like'' domains in key RNA-binding proteins (RBPs) mediate the reversible assembly of RNA granules. Individual RBPs harboring these domains have been linked to specific neurodegenerative diseases. Although their aggregation in neurodegeneration has been extensively characterized, it remains unknown how the process of aging disturbs RBP dynamics. We show that a wide variety of RNA granule components, including stress granule proteins, become highly insoluble with age in C. elegans and that reduced insulin/insulin-like growth factor 1 (IGF-1) daf-2 receptor signaling efficiently prevents their aggregation. Importantly, stress-granule-related RBP aggregates are associated with reduced fitness. We show that heat shock transcription factor 1 (HSF-1) is a main regulator of stress-granule-related RBP aggregation in both young and aged animals. During aging, increasing DAF-16 activity restores dynamic stress-granule-related RBPs, partly by decreasing the buildup of other misfolded proteins that seed RBP aggregation. Longevity-associated mechanisms found to maintain dynamic RBPs during aging could be relevant for neurodegenerative diseases.
机译:关键RNA结合蛋白(RBP)中的低复杂度“ pr病毒样”结构域介导RNA颗粒的可逆组装。携带这些结构域的单个RBP已与特定的神经退行性疾病相关。尽管它们在神经退行性病变中的聚集已得到广泛表征,但衰老过程如何干扰RBP动态仍是未知的。我们显示,包括应激颗粒蛋白在内的各种RNA颗粒成分随着年龄的增长在线虫中变得高度不溶,并且降低的胰岛素/胰岛素样生长因子1(IGF-1)daf-2受体信号传导有效地阻止了它们的聚集。重要的是,与应力颗粒有关的RBP聚集体与适应性降低相关。我们显示,热休克转录因子1(HSF-1)是在年轻和成年动物中与应激颗粒相关的RBP聚集的主要调节剂。在衰老过程中,提高DAF-16活性可恢复动态应激颗粒相关的RBP,部分原因是减少了其他导致RBP聚集的错误折叠蛋白的积累。发现在衰老过程中维持动态RBP的长寿相关机制可能与神经退行性疾病有关。

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