The actin and microtubule cytoskeletons regulate critical aspects of T cell biology including development, migration and activation through the organization and stabilization of signaling complexes at the immunological synapse (IS). Likewise, proteins that regulate the cytoskeleton play an equally fundamental role in immune regulation. This renewal application focuses on the newly identified Wiskott - Aldrich syndrome protein (WASP) family member, WASH (WASP and SCAR homologue). Our recent Developmental Cell paper shows that WASH localizes to endosomal subdomains in cells, interacts with microtubules and regulates sorting events at endosomes, in particular transport of cargo from endosomes to the Golgi by the retromer (a complex of proteins involved in sorting receptors from the early/late endosome to the trans-Golgi network), in an Arp2/3- and microtubule-dependent manner. Actin regulatory functions of WASP and WAVE proteins are controlled by unique N-terminal regions, which mediate their incorporation into distinct protein complexes linked to diverse biological functions. Thus, understanding the biochemical make-up and mechanisms that regulate assembly, localization and activity of these cytoskeletal regulators is paramount to understanding their cellular functions. Our preliminary data also demonstrate that WASH exists in a multi-protein complex containing 4 previously uncharacterized proteins (FAM21, SWIP, Strumpellin and CCDC53). Accordingly, a central focus of this proposal is the mechanisms of WASH complex assembly and the mechanisms that control its localization, activity and microtubule interaction (Aim 1). An emerging paradigm suggests that the dynamic endosomal tubulovesicular network is not just involved in receptor degradation and recycling, but is also a site at which receptor signaling can be initiated, sustained or terminated. Our published data indicate that WASH localizes to endosomal subdomains where it regulates endosomal sorting. We now provide preliminary data showing that the WASH complex interacts with several signaling proteins following TCR ligation, localizes on endosomal subdomains following TCR ligation with PLC31, and depletion of the WASH complex attenuates TCR- stimulated signaling including PLC31 activation in DP thymocytes. Taken together, our data suggest that WASH regulates endosomal-sorting pathways involved in TCR-mediated activation and selection. These mechanisms will be examined in Aim 2. In two highly focused aims we will address the hypothesis that WASH functions as part of a macromolecular complex to coordinate actin and microtubule-dependent vesicular trafficking/sorting, which quantitatively regulates TCR signaling leading to distinct T cell fates and functions. The strength of the TCR signal is a critical checkpoint in the regulation of thymocyte selection, T cell activation and effector function. Therefore understanding the regulation of TCR signaling by WASH will provide insight into novel mechanisms of immune regulation. Our proposed studies are outlined in the two Specific Aims below. Results from these studies will enhance our understanding of the mechanisms by which TCR signaling is regulated and will provide insight into novel pathways that could potentially be manipulated to ameliorate immunodeficiency diseases and/or autoimmune/inflammatory conditions.

Public Health Relevance

The actin and microtubule cytoskeletons participate in multiple aspects of T cell biology including development, migration, effector functions and the organization and stabilization of signaling complexes at the immunological synapse. Consequently, proteins that regulate cytoskeletal-dependent processes play a fundamental role in immune regulation. The experiments in this proposal are aimed at understanding the role of the novel actin regulatory protein WASH in T cell activation and thymocyte selection.

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI065474-10
Application #
8653518
Study Section
Special Emphasis Panel (ZRG1-IMM-H (03))
Program Officer
Mallia, Conrad M
Project Start
2005-07-08
Project End
2015-04-30
Budget Start
2014-05-01
Budget End
2015-04-30
Support Year
10
Fiscal Year
2014
Total Cost
$351,277
Indirect Cost
$128,527
Name
Mayo Clinic, Rochester
Department
Type
DUNS #
006471700
City
Rochester
State
MN
Country
United States
Zip Code
55905
Alekhina, Olga; Burstein, Ezra; Billadeau, Daniel D (2017) Cellular functions of WASP family proteins at a glance. J Cell Sci 130:2235-2241
McNally, Kerrie E; Faulkner, Rebecca; Steinberg, Florian et al. (2017) Retriever is a multiprotein complex for retromer-independent endosomal cargo recycling. Nat Cell Biol 19:1214-1225
Jia, Da; Zhang, Jin-San; Li, Fang et al. (2016) Structural and mechanistic insights into regulation of the retromer coat by TBC1d5. Nat Commun 7:13305
Bartuzi, Paulina; Billadeau, Daniel D; Favier, Robert et al. (2016) CCC- and WASH-mediated endosomal sorting of LDLR is required for normal clearance of circulating LDL. Nat Commun 7:10961
Osborne, Douglas G; Piotrowski, Joshua T; Dick, Christopher J et al. (2015) SNX17 affects T cell activation by regulating TCR and integrin recycling. J Immunol 194:4555-66
Li, Haiying; Koo, Yeon; Mao, Xicheng et al. (2015) Endosomal sorting of Notch receptors through COMMD9-dependent pathways modulates Notch signaling. J Cell Biol 211:605-17
Deng, Zhi-Hui; Gomez, Timothy S; Osborne, Douglas G et al. (2015) Nuclear FAM21 participates in NF-?B-dependent gene regulation in pancreatic cancer cells. J Cell Sci 128:373-84
Phillips-Krawczak, Christine A; Singla, Amika; Starokadomskyy, Petro et al. (2015) COMMD1 is linked to the WASH complex and regulates endosomal trafficking of the copper transporter ATP7A. Mol Biol Cell 26:91-103
Osborne, Douglas G; Phillips-Krawczak, Christine A; Billadeau, Daniel D (2015) Monitoring receptor trafficking following retromer and WASH deregulation. Methods Cell Biol 130:199-213
Graham, Daniel B; Osborne, Douglas G; Piotrowski, Joshua T et al. (2014) Dendritic cells utilize the evolutionarily conserved WASH and retromer complexes to promote MHCII recycling and helper T cell priming. PLoS One 9:e98606

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