Nature Communications (Dec 2023)

Dissecting the genetic landscape of GPCR signaling through phenotypic profiling in C. elegans

  • Longjun Pu,
  • Jing Wang,
  • Qiongxuan Lu,
  • Lars Nilsson,
  • Alison Philbrook,
  • Anjali Pandey,
  • Lina Zhao,
  • Robin van Schendel,
  • Alan Koh,
  • Tanara V. Peres,
  • Weheliye H. Hashi,
  • Si Lhyam Myint,
  • Chloe Williams,
  • Jonathan D. Gilthorpe,
  • Sun Nyunt Wai,
  • Andre Brown,
  • Marcel Tijsterman,
  • Piali Sengupta,
  • Johan Henriksson,
  • Changchun Chen

DOI
https://doi.org/10.1038/s41467-023-44177-z
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 16

Abstract

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Abstract G protein-coupled receptors (GPCRs) mediate responses to various extracellular and intracellular cues. However, the large number of GPCR genes and their substantial functional redundancy make it challenging to systematically dissect GPCR functions in vivo. Here, we employ a CRISPR/Cas9-based approach, disrupting 1654 GPCR-encoding genes in 284 strains and mutating 152 neuropeptide-encoding genes in 38 strains in C. elegans. These two mutant libraries enable effective deorphanization of chemoreceptors, and characterization of receptors for neuropeptides in various cellular processes. Mutating a set of closely related GPCRs in a single strain permits the assignment of functions to GPCRs with functional redundancy. Our analyses identify a neuropeptide that interacts with three receptors in hypoxia-evoked locomotory responses, unveil a collection of regulators in pathogen-induced immune responses, and define receptors for the volatile food-related odorants. These results establish our GPCR and neuropeptide mutant libraries as valuable resources for the C. elegans community to expedite studies of GPCR signaling in multiple contexts.