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Lysosomal dysfunction by inactivation of V-ATPase drives innate immune response in C. elegans

Xuepiao Pu, Bin Qi

2024Cell Reports21 citationsDOIOpen Access PDF

Abstract

Pathogens target vacuolar ATPase (V-ATPase) to inhibit lysosomal acidification or lysosomal fusion, causing lysosomal dysfunction. However, it remains unknown whether cells can detect dysfunctional lysosomes and initiate an immune response. In this study, we discover that dysfunction of lysosomes caused by inactivation of V-ATPase enhances innate immunity against bacterial infections. We find that lysosomal V-ATPase interacts with DVE-1, whose nuclear localization serves as a proxy for the induction of mitochondrial unfolded protein response (UPR mt ). The inactivation of V-ATPase promotes the nuclear localization of DVE-1, activating UPR mt and inducing downstream immune response genes. Furthermore, pathogen resistance conferred by inactivation of V-ATPase requires dve-1 and its downstream immune effectors. Interestingly, animals grow slower after vha RNAi, suggesting that the vha -RNAi-induced immune response costs the most energy through activation of DVE-1, which trades off with growth. This study reveals how dysfunctional lysosomes can trigger an immune response, emphasizing the importance of conserving energy during immune defense.

Topics & Concepts

Innate immune systemATPaseCell biologyLysosomeV-ATPaseBiologyAAA proteinsImmune systemImmunityATP synthaseBiochemistryEnzymeImmunologyATP Synthase and ATPases ResearchGenetics, Aging, and Longevity in Model OrganismsMitochondrial Function and Pathology
Lysosomal dysfunction by inactivation of V-ATPase drives innate immune response in C. elegans | Litcius