Semantic Scholar Open Access 2006 131 sitasi

LAT-mediated signaling in CD4+CD25+ regulatory T cell development

S. Koonpaew Shudan Shen L. Flowers Weiguo Zhang

Lihat Sumber DOI

Abstrak

Engagement of the T cell receptor for antigen (TCR) induces formation of signaling complexes mediated through the transmembrane adaptor protein, the linker for activation of T cells (LAT). LAT plays an important role in T cell development, activation, and homeostasis. A knock-in mutation at Tyr136, which is the phospholipase C (PLC)-γ1–binding site in LAT, leads to a severe autoimmune disease in mice. In this study, we show that CD4+CD25+ T reg cells that expressed Foxp3 transcription factor were nearly absent in both thymus and peripheral lymphoid organs of LATY136F mice. This defect was not a result of the autoimmune environment as LATY136F T reg cells also failed to develop in healthy LAT−/− mice that received mixed wild-type and LATY136F bone marrow cells. Moreover, adoptive transfer of normal CD4+CD25+ T reg cells protected neonatal LATY136F mice from developing this disease. These T reg cells effectively controlled expansion of CD4+ T cells in LATY136F mice likely via granzymes and/or TGF-β–mediated suppression. Furthermore, ectopic expression of Foxp3 conferred a suppressive function in LATY136F T cells. Our data indicate that the LAT–PLC-γ1 interaction plays a critical role in Foxp3 expression and the development of CD4+CD25+ T reg cells

Topik & Kata Kunci

Biology Medicine

Penulis (4)

S. Koonpaew

Shudan Shen

L. Flowers

Weiguo Zhang

Format Sitasi

APA MLA BibTeX

Koonpaew, S., Shen, S., Flowers, L., Zhang, W. (2006). LAT-mediated signaling in CD4+CD25+ regulatory T cell development. https://doi.org/10.1084/jem.20050903

Akses Cepat

Lihat di Sumber doi.org/10.1084/jem.20050903

Informasi Jurnal

Tahun Terbit: 2006
Bahasa: en
Total Sitasi: 131×
Sumber Database: Semantic Scholar
DOI: 10.1084/jem.20050903
Akses: Open Access ✓