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Glia of <i>C. elegans</i> coordinate a protective organismal heat shock response independent of the neuronal thermosensory circuit

Holly K. Gildea, Phillip A. Frankino, Sarah U. Tronnes, Corinne L. Pender, Jenni Durieux, Julian G. Dishart, Hyun Ok Choi, Tayla D. Hunter, Shannon S. Cheung, Ashley E. Frakes, Edward Sukarto, Kevin Wickham, Andrew Dillin

2022Science Advances26 citationsDOIOpen Access PDF

Abstract

Aging organisms lose the ability to induce stress responses, becoming vulnerable to protein toxicity and tissue damage. Neurons can signal to peripheral tissues to induce protective organelle-specific stress responses. Recent work shows that glia can independently induce such responses. Here, we show that overexpression of heat shock factor 1 ( hsf-1 ) in the four astrocyte-like cephalic sheath cells of Caenorhabditis elegans induces a non–cell-autonomous cytosolic unfolded protein response, also known as the heat shock response (HSR). These animals have increased lifespan and heat stress resistance and decreased protein aggregation. Glial HSR regulation is independent of canonical thermosensory circuitry and known neurotransmitters but requires the small clear vesicle release protein UNC-13. HSF-1 and the FOXO transcription factor DAF-16 are partially required in peripheral tissues for non–cell-autonomous HSR, longevity, and thermotolerance. Cephalic sheath glial hsf-1 overexpression also leads to pathogen resistance, suggesting a role for this signaling pathway in immune function.

Topics & Concepts

Cell biologyCaenorhabditis elegansBiologyHeat shock proteinHsp70Heat shockAstrocyteTranscription factorHeat shock factorOrganelleNeuroscienceCentral nervous systemGeneGeneticsGenetics, Aging, and Longevity in Model OrganismsHeat shock proteins researchFOXO transcription factor regulation
Glia of <i>C. elegans</i> coordinate a protective organismal heat shock response independent of the neuronal thermosensory circuit | Litcius