4.8 Article

The C-elegans TGF-β dauer pathway regulates longevity via insulin signaling

Journal

CURRENT BIOLOGY
Volume 17, Issue 19, Pages 1635-1645

Publisher

CELL PRESS
DOI: 10.1016/j.cub.2007.08.058

Keywords

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Funding

  1. NHGRI NIH HHS [T32 HG003284, T32 HG003284-07] Funding Source: Medline
  2. NIH HHS [DP2 OD004402-01, DP2 OD004402] Funding Source: Medline

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Background: Previous genetic evidence suggested that the C. elegrans TGF-beta Dauer pathway is responsible solely for the regulation of dauer formation, with no role in longevity regulation, whereas the insulin/IGF-1 signaling (IIS) pathway regulates both dauer formation and longevity. Results: We have uncovered a significant longevity-regulating activity by the TGF-beta Dauer pathway that is masked by an egg-laying (Egl) phenotype; mutants in the pathway display up to 2-fold increases in life span. The expression profiles of adult TGF-beta mutants overlap significantly with IIS pathway profiles: Adult TGF-beta mutants regulate the transcription of many DAF-16-regulated genes, including genes that regulate life span, the two pathways share enriched Gene Ontology categories, and a motif previously associated with DAF-16-regulated transcription (the DAE, or DAF-16-associated element) is overrepresented in the promoters of TGF-beta regulated genes. The TGF-beta Dauer pathway's regulation of longevity appears to be mediated at least in part through insulin interactions with the IIS pathway and the regulation of DAF-16 localization. Conclusions: Together, our results suggest there are TGF-beta-specific downstream targets and functions, but that the TGF-beta and IIS pathways might be more tightly linked in the regulation of longevity than has been previously appreciated.

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