Apoptosis in lymphocytes represents a fundamental regulatory process for the immune system, and an understanding of that process has far-reaching implications for our understanding of normal homeostasis and immunological disease. While considerable progress has been made towards delineating the central mechanisms of apoptosis, little is known about the signal transduction events that trigger this phenomenon. This renewal application seeks to explore a new concept in apoptotic signaling, one that is based on our continuing progress in understanding the phenomenon of activation-induced apoptosis in T cell hybridomas. The investigator proposes to explore signals that are initiated by DNA damage and related stress in T cells, which culminate in the expression of members of the TNF family of ligands, including Fas-ligand (FasL). By analogy with activation-induced apoptosis, where TCR-mediated signals induce expression of FasL and subsequent interaction with Fas to induce cell death in a cell-autonomous fashion, he proposes that stress-induced signals activate FasL expression (and probably that of related apoptosis-inducing ligands) through engaging the Jun-kinase pathway (to activate AP-1) and the activation of NF-kB. His two major aims in this project are 1) to dissect the signaling events that connect stress to FasL expression and subsequent apoptosis in T cells, and 2) to determine which of the TNF-family ligands (in addition to FasL) participate in stress-induced apoptosis in these cells. T lymphocytes utilize autocrine growth factor/receptor expression as a route to entry into the cell cycle following activation, by inducing transcription of DNA synthesis machinery, and the same general principle appears to apply to autocrine death-inducing ligands which interact with their receptors to trigger apoptosis via activation of the caspase proteases. This is a powerful concept, and the investigator will analyze the activation of the FasL promoter under conditions of stress to evaluate the roles of AP-1, NF-kB, c-Myc, and other relevant transcription factors, and he will compare and contrast these with the events associated with activation-induced FasL transcription (which appear to be different). It is anticipated that results generated in T cells may be relevant to some nonlymphoid systems as well. His focus on T lymphocytes is important in the context of understanding how the immune system responds to DNA damage and related stress to remove potentially damaged cells, that could otherwise pose a threat to immune integrity.

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM052735-10
Application #
6181166
Study Section
Allergy and Immunology Study Section (ALY)
Program Officer
Marino, Pamela
Project Start
1994-09-01
Project End
2002-08-31
Budget Start
2000-09-01
Budget End
2001-08-31
Support Year
10
Fiscal Year
2000
Total Cost
$286,318
Indirect Cost
Name
La Jolla Institute
Department
Type
DUNS #
603880287
City
La Jolla
State
CA
Country
United States
Zip Code
92037
Follis, Ariele Viacava; Llambi, Fabien; Kalkavan, Halime et al. (2018) Regulation of apoptosis by an intrinsically disordered region of Bcl-xL. Nat Chem Biol 14:458-465
Follis, Ariele Viacava; Llambi, Fabien; Merritt, Parker et al. (2015) Pin1-Induced Proline Isomerization in Cytosolic p53 Mediates BAX Activation and Apoptosis. Mol Cell 59:677-84
Caro-Maldonado, Alfredo; Wang, Ruoning; Nichols, Amanda G et al. (2014) Metabolic reprogramming is required for antibody production that is suppressed in anergic but exaggerated in chronically BAFF-exposed B cells. J Immunol 192:3626-36
Follis, Ariele Viacava; Llambi, Fabien; Ou, Li et al. (2014) The DNA-binding domain mediates both nuclear and cytosolic functions of p53. Nat Struct Mol Biol 21:535-43
Follis, Ariele Viacava; Chipuk, Jerry E; Fisher, John C et al. (2013) PUMA binding induces partial unfolding within BCL-xL to disrupt p53 binding and promote apoptosis. Nat Chem Biol 9:163-8
Moldoveanu, Tudor; Grace, Christy R; Llambi, Fabien et al. (2013) BID-induced structural changes in BAK promote apoptosis. Nat Struct Mol Biol 20:589-97
Martinez, Jennifer; Verbist, Katherine; Wang, Ruoning et al. (2013) The relationship between metabolism and the autophagy machinery during the innate immune response. Cell Metab 17:895-900
Green, Douglas R; Rathmell, Jeffrey (2013) Sweet nothings: sensing of sugar metabolites controls T cell function. Cell Metab 18:7-8
Dillon, Christopher P; Oberst, Andrew; Weinlich, Ricardo et al. (2012) Survival function of the FADD-CASPASE-8-cFLIP(L) complex. Cell Rep 1:401-7
Wang, Ruoning; Green, Douglas R (2012) Metabolic checkpoints in activated T cells. Nat Immunol 13:907-15

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