rab-27 acts in an intestinal pathway to inhibit axon regeneration in C. elegans.

PLoS Genet

Department of Genetics, Yale University School of Medicine, New Haven, Connecticut, United States of America.

Published: November 2021

AI Article Synopsis

  • Injured axons need to regenerate for proper nervous system function, and this process is influenced by external factors from surrounding non-neuronal tissues.
  • Research in C. elegans reveals that the Rab GTPase rab-27, located in the intestine, inhibits regeneration of GABAergic motor neurons, while re-expressing rab-27 in mutants can restore normal regeneration.
  • Other components involved in intestinal neuropeptide secretion, such as NPDC1/cab-1 and SNAP25/aex-4, also play roles in inhibiting axon regeneration, suggesting that these distal tissues significantly impact the regeneration process.

Article Abstract

Injured axons must regenerate to restore nervous system function, and regeneration is regulated in part by external factors from non-neuronal tissues. Many of these extrinsic factors act in the immediate cellular environment of the axon to promote or restrict regeneration, but the existence of long-distance signals regulating axon regeneration has not been clear. Here we show that the Rab GTPase rab-27 inhibits regeneration of GABAergic motor neurons in C. elegans through activity in the intestine. Re-expression of RAB-27, but not the closely related RAB-3, in the intestine of rab-27 mutant animals is sufficient to rescue normal regeneration. Several additional components of an intestinal neuropeptide secretion pathway also inhibit axon regeneration, including NPDC1/cab-1, SNAP25/aex-4, KPC3/aex-5, and the neuropeptide NLP-40, and re-expression of these genes in the intestine of mutant animals is sufficient to restore normal regeneration success. Additionally, NPDC1/cab-1 and SNAP25/aex-4 genetically interact with rab-27 in the context of axon regeneration inhibition. Together these data indicate that RAB-27-dependent neuropeptide secretion from the intestine inhibits axon regeneration, and point to distal tissues as potent extrinsic regulators of regeneration.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8612575PMC
http://dx.doi.org/10.1371/journal.pgen.1009877DOI Listing

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