Four glial cells regulate ER stress resistance and longevity via neuropeptide signaling in C. elegans

秀丽隐杆线虫中四种神经胶质细胞通过神经肽信号传导调节内质网应激抵抗力和寿命

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Abstract

The ability of the nervous system to sense cellular stress and coordinate protein homeostasis is essential for organismal health. Unfortunately, stress responses that mitigate disturbances in proteostasis, such as the unfolded protein response of the endoplasmic reticulum (UPR(ER)), become defunct with age. In this work, we expressed the constitutively active UPR(ER) transcription factor, XBP-1s, in a subset of astrocyte-like glia, which extended the life span in Caenorhabditis elegans Glial XBP-1s initiated a robust cell nonautonomous activation of the UPR(ER) in distal cells and rendered animals more resistant to protein aggregation and chronic ER stress. Mutants deficient in neuropeptide processing and secretion suppressed glial cell nonautonomous induction of the UPR(ER) and life-span extension. Thus, astrocyte-like glial cells play a role in regulating organismal ER stress resistance and longevity.

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