Abstract

Integrins are dimeric cell surface receptors that play critical roles in cellular adhesion and migration. Signaling events critical for integrin function include second messenger cascades initiated by other cell surface receptors which modulate integrin avidity for their ligands in addition to signaling pathways initiated by engagement of integrins themselves. We and others have found that the formation of multimolecular complexes nucleated by adapater proteins is essential for both signaling to integrins (inside-out signaling) and signaling by integrins (outside-in signaling). Our laboratory has a long standing interest in the SH2 domain containing leukocyte phosphoprotein of 76kDa (SLP-76), a hematopoietic restricted adapater protein that is critical for function of both immunoreceptors and integrins. The experiments described in this proposal will make use of biochemical, imaging, molecular and genetic approaches to investigate the role of SLP-76 and its associated molecules in integrin responses in cells of both the innate and adaptive immune systems. The work will be divided into three specific aims. The first will explore the inducible interactions between SLP-76 and other proteins upon integrin engagement and the subcellular localization of SLP-76 during integrin function in T cells. One central hypothesis that will be tested is that there are two pools of SLP-76 in the cell, one which regulates immunoreceptor signaling and the second which regulates integrin responses. We will further test the notion that integrin pathway requires an interaction between SLP-76 and three adapter proteins, ADAP (Adhesion and Degranulation-promoting Adapter Protein), SKAP55 (SrcKinase- associated phosphoprotein of 55kDa), and RIAM (Rap1-GTP interacting adapter molecule), and that these adapters collectively nucleate a complex which brings activated Rap-1 to the cell surface.
The second aim of this proposal will take the biochemical and imaging studies of Aim 1 in vivo by generating genetically unique murine lines in which mutations of SLP-76 or its associated molecules are expressed that are predicted to selectively impact T cell immunoreceptor or integrin function.
The third aim will extend our work to the innate immune system by studying the biochemistry and molecular events coordinated by these adapter molecules in neutrophils, both ex vivo and in vivo. Experiments described in this project will make extensive use of both scientific cores and will rely extensively on interactions with the Project Leaders of the other projects of this program. We hope that these studies will provide new insights into how multimolecular complexes integrate signaling pathways leading to appropriate immune cell responses.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA093615-08
Application #
7896830
Study Section
Special Emphasis Panel (ZCA1)
Project Start
Project End
Budget Start
2009-09-01
Budget End
2010-08-31
Support Year
8
Fiscal Year
2009
Total Cost
$338,194
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Type
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Silva, Oscar; Crocetti, Jillian; Humphries, Lisa A et al. (2015) Discs Large Homolog 1 Splice Variants Regulate p38-Dependent and -Independent Effector Functions in CD8+ T Cells. PLoS One 10:e0133353
Comrie, William A; Li, Shuixing; Boyle, Sarah et al. (2015) The dendritic cell cytoskeleton promotes T cell adhesion and activation by constraining ICAM-1 mobility. J Cell Biol 208:457-73
Babich, Alexander; Burkhardt, Janis K (2013) Coordinate control of cytoskeletal remodeling and calcium mobilization during T-cell activation. Immunol Rev 256:80-94
Chen, Emily J H; Shaffer, Meredith H; Williamson, Edward K et al. (2013) Ezrin and moesin are required for efficient T cell adhesion and homing to lymphoid organs. PLoS One 8:e52368
Hammer 3rd, John A; Burkhardt, Janis K (2013) Controversy and consensus regarding myosin II function at the immunological synapse. Curr Opin Immunol 25:300-6
Lazar, Mitchell A; Birnbaum, Morris J (2012) Physiology. De-meaning of metabolism. Science 336:1651-2
Humphries, Lisa A; Shaffer, Meredith H; Sacirbegovic, Faruk et al. (2012) Characterization of in vivo Dlg1 deletion on T cell development and function. PLoS One 7:e45276
Babich, Alexander; Li, Shuixing; O'Connor, Roddy S et al. (2012) F-actin polymerization and retrograde flow drive sustained PLC?1 signaling during T cell activation. J Cell Biol 197:775-87
Burns, Jeremy C; Corbo, Evann; Degen, Janine et al. (2011) The SLP-76 Src homology 2 domain is required for T cell development and activation. J Immunol 187:4459-66
Chang, John T; Ciocca, Maria L; Kinjyo, Ichiko et al. (2011) Asymmetric proteasome segregation as a mechanism for unequal partitioning of the transcription factor T-bet during T lymphocyte division. Immunity 34:492-504

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