| Literature DB >> 13678593 |
Christine M Labno1, Carol M Lewis, Daoqi You, Daisy W Leung, Ana Takesono, Natalie Kamberos, Abhinav Seth, Lisa D Finkelstein, Michael K Rosen, Pamela L Schwartzberg, Janis K Burkhardt.
Abstract
Actin polymerization at the immune synapse is required for T cell activation and effector function; however, the relevant regulatory pathways remain poorly understood. We showed previously that binding to antigen presenting cells (APCs) induces localized activation of Cdc42 and Wiskott-Aldrich Syndrome protein (WASP) at the immune synapse. Several lines of evidence suggest that Tec kinases could interact with WASP-dependent actin regulatory processes. Since T cells from Rlk-/-, Itk-/-, and Rlk-/- x Itk-/- mice have defects in signaling and development, we asked whether Itk or Rlk function in actin polymerization at the immune synapse. We find that Itk-/- and Rlk-/- x Itk-/- T cells are defective in actin polymerization and conjugate formation in response to antigen-pulsed APCs. Itk functions downstream of the TCR, since similar defects were observed upon TCR engagement alone. Using conformation-specific probes, we show that although the recruitment of WASP and Arp2/3 complex to the immune synapse proceeds normally, the localized activation of Cdc42 and WASP is defective. Finally, we find that the defect in Cdc42 activation likely stems from a requirement for Itk in the recruitment of Vav to the immune synapse. Our results identify Itk as a key element of the pathway leading to localized actin polymerization at the immune synapse.Entities:
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Year: 2003 PMID: 13678593 PMCID: PMC3417328 DOI: 10.1016/j.cub.2003.08.005
Source DB: PubMed Journal: Curr Biol ISSN: 0960-9822 Impact factor: 10.834