An intracellular pathogen response pathway promotes proteostasis inC. elegans

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Abstract

Summary Maintenance of proteostasis is critical for organismal health. Here we describe a novel pathway that promotes proteostasis, identified through the analysis of C. elegans genes upregulated by intracellular infection. We named this distinct transcriptional signature the Intracellular Pathogen Response (IPR), and it includes upregulation of several predicted ubiquitin ligase complex components such as the cullin cul-6 . Through a forward genetic screen we found pals-22 , a gene of previously unknown function, to be a repressor of the cul-6/ Cullin gene and other IPR gene expression. Interestingly, pals-22 mutants have increased thermotolerance and reduced levels of stress-induced polyglutamine aggregates, likely due to upregulated IPR expression. We found the enhanced stress resistance of pals-22 mutants to be dependent on cul-6 , suggesting that pals-22 mutants have increased activity of a CUL-6/Cullin-containing ubiquitin ligase complex . pals-22 mutant phenotypes are distinct from the well-studied heat shock and insulin signaling pathways, indicating that the IPR is a novel pathway that protects animals from proteotoxic stress.

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