Simple nutrients bypass the requirement for HLH-30 in coupling lysosomal nutrient sensing to survival

Murphy, John T. and Liu, Haiyan and Ma, Xiucui and Shaver, Alex and Egan, Brian M. and Oh, Clara and Boyko, Alexander and Mazer, Travis and Ang, Samuel and Khopkar, Rohan and Javaheri, Ali and Kumar, Sandeep and Jiang, Xuntian and Ory, Daniel and Mani, Kartik and Matkovich, Scot J. and Kornfeld, Kerry and Diwan, Abhinav and Tissenbaum, Heidi A. (2019) Simple nutrients bypass the requirement for HLH-30 in coupling lysosomal nutrient sensing to survival. PLOS Biology, 17 (5). e3000245. ISSN 1545-7885

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Abstract

Lysosomes are ubiquitous acidified organelles that degrade intracellular and extracellular material trafficked via multiple pathways. Lysosomes also sense cellular nutrient levels to regulate target of rapamycin (TOR) kinase, a signaling enzyme that drives growth and suppresses activity of the MiT/TFE family of transcription factors that control biogenesis of lysosomes. In this study, we subjected worms lacking basic helix–loop–helix transcription factor 30 (hlh-30), the Caenorhabditis elegans MiT/TFE ortholog, to starvation followed by refeeding to understand how this pathway regulates survival with variable nutrient supply. Loss of HLH-30 markedly impaired survival in starved larval worms and recovery upon refeeding bacteria. Remarkably, provision of simple nutrients in a completely defined medium (C. elegans maintenance medium [CeMM]), specifically glucose and linoleic acid, restored lysosomal acidification, TOR activation, and survival with refeeding despite the absence of HLH-30. Worms deficient in lysosomal lipase 2 (lipl-2), a lysosomal enzyme that is transcriptionally up-regulated in starvation in an HLH-30–dependent manner, also demonstrated increased mortality with starvation–refeeding that was partially rescued with glucose, suggesting a critical role for LIPL-2 in lipid metabolism under starvation. CeMM induced transcription of vacuolar proton pump subunits in hlh-30 mutant worms, and knockdown of vacuolar H+-ATPase 12 (vha-12) and its upstream regulator, nuclear hormone receptor 31 (nhr-31), abolished the rescue with CeMM. Loss of Ras-related GTP binding protein C homolog 1 RAGC-1, the ortholog for mammalian RagC/D GTPases, conferred starvation–refeeding lethality, and RAGC-1 overexpression was sufficient to rescue starved hlh-30 mutant worms, demonstrating a critical need for TOR activation with refeeding. These results show that HLH-30 activation is critical for sustaining survival during starvation–refeeding stress via regulating TOR. Glucose and linoleic acid bypass the requirement for HLH-30 in coupling lysosome nutrient sensing to survival.

Item Type: Article
Subjects: STM Library Press > Biological Science
Depositing User: Unnamed user with email support@stmlibrarypress.com
Date Deposited: 28 Jan 2023 07:45
Last Modified: 07 May 2024 05:05
URI: http://journal.scienceopenlibraries.com/id/eprint/193

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