Abstract

Although there has been tremendous progress towards defining signaling pathways that trigger cell death, an understanding of the mechanisms by which growth factor suppress death and promote survival has remained elusive. Our laboratory has defined a pathway by growth factors interact with the cellular death machinery to inhibit its function. We have identified a protein kinase cascade, the BCL-2 family member, BAD. Once phosphorylated BAD is translocated within the cell so that it promotes survival rather than death. We have found that when over-expressed in neurons BAD triggers cell death unless it is phosphorylated at a specific site, Serine-136, by the Serine/Threonine kinase Akt. It is not yet clear how the phosphorylation of BAD promotes cell survival but that when phosphorylated plays an important role in cell survival. We propose a series of experiments that will: 1) determine if endogenous BAD is phosphorylated at Ser-136 and if this phosphorylation event is mediated by the PI3K/Akt signaling pathway and/or other signaling pathways 2) characterize the protein phosphorylation at Ser-136 inhibits BAD's apoptotic function. 3) investigate the mechanism by which the phosphorylation of BAD inactivates BAD's apoptotic function. 3) investigate the mechanism by which the phosphorylation of BAD inactivates BAD's apoptotic function and stimulates it survival function, 4) characterize the biochemical and biological properties of three novel mammalian BAD homologues that we have recently identified. The characterization of the mechanisms by which Akt and BAD family members regulate cell survival and apoptosis may provide insight into how the disruption of normal survival and apoptotic mechanisms leads to cell degeneration or oncogenesis. As these cellular pathways become better defined it may be possible to treat genetically based, or environmentally induced degenerative disorders or cancers, through the development of small molecule therapeutics that selectively potentiate a component(s) of the survival or death promoting signaling pathways

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Program Projects (P01)
Project #
5P01HD024926-13
Application #
6564680
Study Section
Project Start
2001-12-01
Project End
2002-11-30
Budget Start
Budget End
Support Year
13
Fiscal Year
2002
Total Cost
$208,891
Indirect Cost

  Institution

Name
Dana-Farber Cancer Institute
Department
Type
DUNS #
149617367
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Sauvageot, Claire; Dahia, Patricia L; Lipan, Ovidiu et al. (2005) Distinct temporal genetic signatures of neurogenic and gliogenic cues in cortical stem cell cultures. J Neurobiol 62:121-33
Ross, Sarah E; Greenberg, Michael E; Stiles, Charles D (2003) Basic helix-loop-helix factors in cortical development. Neuron 39:13-25
Oh, S Paul; Yeo, Chang-Yeol; Lee, Youngjae et al. (2002) Activin type IIA and IIB receptors mediate Gdf11 signaling in axial vertebral patterning. Genes Dev 16:2749-54
Brunet, Anne; Kanai, Fumihiko; Stehn, Justine et al. (2002) 14-3-3 transits to the nucleus and participates in dynamic nucleocytoplasmic transport. J Cell Biol 156:817-28
Chan, Joanne; Bayliss, Peter E; Wood, Jeanette M et al. (2002) Dissection of angiogenic signaling in zebrafish using a chemical genetic approach. Cancer Cell 1:257-67
Datta, Sandeep Robert; Ranger, Ann M; Lin, Michael Z et al. (2002) Survival factor-mediated BAD phosphorylation raises the mitochondrial threshold for apoptosis. Dev Cell 3:631-43
Tran, Hien; Brunet, Anne; Grenier, Jill M et al. (2002) DNA repair pathway stimulated by the forkhead transcription factor FOXO3a through the Gadd45 protein. Science 296:530-4
Humbert, Sandrine; Bryson, Elzbieta A; Cordelieres, Fabrice P et al. (2002) The IGF-1/Akt pathway is neuroprotective in Huntington's disease and involves Huntingtin phosphorylation by Akt. Dev Cell 2:831-7
Whitman, M; Mercola, M (2001) TGF-beta superfamily signaling and left-right asymmetry. Sci STKE 2001:re1
Chan, J; Mably, J D; Serluca, F C et al. (2001) Morphogenesis of prechordal plate and notochord requires intact Eph/ephrin B signaling. Dev Biol 234:470-82

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