The Importance of LAT in the Activation,Homeostasis, and Regulatory Function of T Cells |
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Authors: | Shudan Shen Mariana I. Chuck Minghua Zhu Deirdre M. Fuller Chih-wen Ou Yang Weiguo Zhang |
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Affiliation: | From the Department of Immunology, Duke University Medical Center, Durham, North Carolina 27710 |
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Abstract: | LAT (linker for activation of T cells) is a transmembrane adaptor protein that plays an essential role in TCR-mediated signaling and thymocyte development. Because LAT-deficient mice have an early block in thymocyte development, we utilized an inducible system to delete LAT in primary T cells to study LAT function in T cell activation, homeostasis, and survival. Deletion of LAT caused primary T cells to become unresponsive to stimulation from the TCR and impaired T cell homeostatic proliferation and long term survival. Furthermore, deletion of LAT led to reduced expression of Foxp3, CTLA-4, and CD25 in Treg cells and impaired their function. Consequently, mice with LAT deleted developed a lymphoproliferative syndrome similar to that in LATY136F mice, although less severe. Our data implicate that LAT has positive and negative roles in the regulation of mature T cells. |
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Keywords: | Adaptor Proteins Immunology Signal Transduction T-cell Receptor Tyrosine-protein Kinase (Tyrosine Kinase) |
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