The proposed program project is based on our central hypothesis that novel signaling pathways ar involved in cytoskeletal re-organization upon activation of blood cells. Evidence generated by our group and others suggest that the Wiskott-Aldrich syndrome protein (WASp), vav, the Wiskott-Aldrich syndrome interactive protein (WIP), Cdc42, and others functionally interact to link signaling from surface receptors to the cytoskeleton. This proposal consists of three projects and three cores: Project 1. The murine homologue of the WASp gene has been disrupted in murine ES cells. Somatic chimaeras have been obtained in a Rag-2 deficient complementation system; the lymphoid cells (both T and B cells) are available for characterization. We also have a WAS germline """"""""knock- out"""""""" which should facilitate further investigation into the role of WASP in platelet and immunologic function. A human protein homologous to WASp, called N-Wasp has been identified and sequenced and compared to WASp in its structural domains and function. Project 2. A hitherto unknown protein has been identified by a two hybrid system and named WASp interactive protein (WIP). Its structure and function will be studied and its gene will be targeted in ES cells for the Rag-2 complementation system and for germline """"""""knock-outs"""""""". Project 3. Activation defects in Vav- deficient murine lymphocytes are associated with defects in reorganization of the actin cytoskeleton that are similar to those of human WASp- deficient lymphocytes. Rho-family GTPases, such as Cdc42, have been shown to be effectors of both Vav and WASp. The goal of the proposed work is to eludicate intracellular signaling pathways controlled by Vav and its potential downstream effectors in lymphocytes and, in this context, to dissect the contribution of cytoskeletal versus mitogen and stress- activated protein kinase pathways. Core A will administrate the program. Core B will identify human WASp mutants and make cell lines from these mutants available to Projects 1 and 2. Core C will manage confocal, scanning, high resolution rapid/freeze/freeze dry electron microscopy and transmission electron microscopy and FACS analyses for all projects.

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Program Projects (P01)
Project #
5P01HL059561-02
Application #
2771622
Study Section
Heart, Lung, and Blood Initial Review Group (HLBP)
Project Start
1997-09-30
Project End
2002-08-31
Budget Start
1998-09-01
Budget End
1999-08-31
Support Year
2
Fiscal Year
1998
Total Cost
Indirect Cost
Name
Immune Disease Institute, Inc.
Department
Type
DUNS #
115524410
City
Boston
State
MA
Country
United States
Zip Code
02115
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Vardi, Iddo; Barel, Ortal; Sperber, Michal et al. (2018) Genetic and Structural Analysis of a SKIV2L Mutation Causing Tricho-hepato-enteric Syndrome. Dig Dis Sci 63:1192-1199
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Lexmond, Willem S; Goettel, Jeremy A; Lyons, Jonathan J et al. (2016) FOXP3+ Tregs require WASP to restrain Th2-mediated food allergy. J Clin Invest 126:4030-4044
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Volpi, Stefano; Santori, Elettra; Abernethy, Katrina et al. (2016) N-WASP is required for B-cell-mediated autoimmunity in Wiskott-Aldrich syndrome. Blood 127:216-20
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Gerasimcik, Natalija; Dahlberg, Carin I M; Baptista, Marisa A P et al. (2015) The Rho GTPase Cdc42 Is Essential for the Activation and Function of Mature B Cells. J Immunol 194:4750-8
Begonja, Antonija Jurak; Pluthero, Fred G; Suphamungmee, Worawit et al. (2015) FlnA binding to PACSIN2 F-BAR domain regulates membrane tubulation in megakaryocytes and platelets. Blood 126:80-8
Goettel, Jeremy A; Biswas, Subhabrata; Lexmond, Willem S et al. (2015) Fatal autoimmunity in mice reconstituted with human hematopoietic stem cells encoding defective FOXP3. Blood 125:3886-95

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