Abstract

The nematode C. elegans secretes a pheromone that controls whether the animal molts into the developmentally arrested, extremely long-lived dauer diapause stage, or into a non-arrested normally aging animal. The dauer pheromone signal is detected by sensory neurons which couple by an unknown neurosecretory mechanism to a response pathway in the various target tissues that are remodeled during the dauer stage. The neuronally- regulated developmental and neuroendocrine changes associated with dauer formation are a model for the hypothalmic/pituitary/somatic and autonomic nervous system signaling axes in vertebrates. We have genetically identified a number of genes that regulate the development or function of the dauer sensory to secretory neural pathway. We propose a molecular analysis of three of these genes, daf2, daf-16, and daf-23. Mutations in daf-2 and daf-23 also cause two to three fold increases in longevity of non-dauer animals, and mutations in daf-16 suppress this increase in longevity. Thus daf-2, daf-16 and daf23 not only regulate diapause, they also regulate senescence. We have shown that daf-23 encodes a phosphatidyl inositol-3 kinase, PI-3 kinase, a protein known from vertebrates to associate with receptor and non-receptor tyrosine kinases. We have shown that the mammalian homologue of DAF-23 can fully complement a daf-23 mutant. PI-3 kinase generates a membrane-bound signaling molecule, phosphatidyl inositol-3,4,5-P3, which couples to unknown effector molecules. Thus daf-23 could control dauer formation and senescence by coupling a tyrosine kinase to downstream effectors, either during development of the nervous system or during pheromone signaling. Our genetic analysis suggests that daf-2 and daf-16 encode proteins that transduce the phosphatidyl inositol signal generated by daf-23. We propose to study how the genes in &his pathway couple phosphatidyl inositol biosynthesis to control neuroendocrine function during diapause. Our analysis of the molecular basis of neurosecretory function in C. elegans could reveal the genes that control the development and function of human neurosecretory pathways, with implication for therapies in diabetes, metabolic disorders, and high blood pressure. In addition, since diapause represents a neurosecretory function that is used across invertebrate phylogeny, including in insect pests, new insecticides designed to inhibit P1P3 signaling and thus induce diapause, with its concomitant suspension of feeding and reproduction, would have important implications for agriculture and indirectly, human health and welfare. Our molecular analysis of senescence in C. elegans may also be broadly applicable to human aging. The long lifespan that is caused by a decrease in PI-3 kinase activity suggests that senescence in C. elegans is regulated by the production of phosphatidyl inositol-3,4,5-P3. Drugs which antagonize the production or activity of this lipid might increase longevity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Project (R01)
Project #
5R01AG014161-05
Application #
6169437
Study Section
Neurology C Study Section (NEUC)
Program Officer
Mccormick, Anna M
Project Start
1996-05-01
Project End
2001-09-14
Budget Start
2000-06-15
Budget End
2001-09-14
Support Year
5
Fiscal Year
2000
Total Cost
$305,984
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
City
Boston
State
MA
Country
United States
Zip Code
02199

  Publications

Riedel, Christian G; Dowen, Robert H; Lourenco, Guinevere F et al. (2013) DAF-16 employs the chromatin remodeller SWI/SNF to promote stress resistance and longevity. Nat Cell Biol 15:491-501
Kimura, K D; Riddle, D L; Ruvkun, G (2011) The C. elegans DAF-2 insulin-like receptor is abundantly expressed in the nervous system and regulated by nutritional status. Cold Spring Harb Symp Quant Biol 76:113-20
Li, Weiqing; Kennedy, Scott G; Ruvkun, Gary (2003) daf-28 encodes a C. elegans insulin superfamily member that is regulated by environmental cues and acts in the DAF-2 signaling pathway. Genes Dev 17:844-58
Wolkow, Catherine A; Munoz, Manuel J; Riddle, Donald L et al. (2002) Insulin receptor substrate and p55 orthologous adaptor proteins function in the Caenorhabditis elegans daf-2/insulin-like signaling pathway. J Biol Chem 277:49591-7
Cahill, C M; Tzivion, G; Nasrin, N et al. (2001) Phosphatidylinositol 3-kinase signaling inhibits DAF-16 DNA binding and function via 14-3-3-dependent and 14-3-3-independent pathways. J Biol Chem 276:13402-10
Lee, R Y; Hench, J; Ruvkun, G (2001) Regulation of C. elegans DAF-16 and its human ortholog FKHRL1 by the daf-2 insulin-like signaling pathway. Curr Biol 11:1950-7
Pierce, S B; Costa, M; Wisotzkey, R et al. (2001) Regulation of DAF-2 receptor signaling by human insulin and ins-1, a member of the unusually large and diverse C. elegans insulin gene family. Genes Dev 15:672-86
Tissenbaum, H A; Hawdon, J; Perregaux, M et al. (2000) A common muscarinic pathway for diapause recovery in the distantly related nematode species Caenorhabditis elegans and Ancylostoma caninum. Proc Natl Acad Sci U S A 97:460-5
Wolkow, C A; Kimura, K D; Lee, M S et al. (2000) Regulation of C. elegans life-span by insulinlike signaling in the nervous system. Science 290:147-50
Paradis, S; Ailion, M; Toker, A et al. (1999) A PDK1 homolog is necessary and sufficient to transduce AGE-1 PI3 kinase signals that regulate diapause in Caenorhabditis elegans. Genes Dev 13:1438-52

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