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Literature DB >> 12682251

The FcR gamma subunit and Syk kinase replace the CD3 zeta-chain and ZAP-70 kinase in the TCR signaling complex of human effector CD4 T cells.

Sandeep Krishnan¹, Vishal G Warke, Madhusoodana P Nambiar, George C Tsokos, Donna L Farber.

Abstract

The TCR-mediated signals required to activate resting T cells have been well characterized; however, it is not known how TCR-coupled signals are transduced in differentiated effector T cells that coordinate ongoing immune responses. Here we demonstrate that human effector CD4 T cells up-regulate the expression of the CD3zeta-related FcRgamma signaling subunit that becomes part of an altered TCR/CD3 signaling complex containing CD3epsilon, but not CD3zeta. The TCR/CD3/FcRgamma complex in effector cells recruits and activates the Syk, but not the ZAP-70, tyrosine kinase. This physiologic switch in TCR signaling occurs exclusively in effector, and not naive or memory T cells, suggesting a potential target for manipulation of effector responses in autoimmune, malignant, and infectious diseases.

Entities: Disease Gene Species

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Year: 2003 PMID： 12682251 DOI： 10.4049/jimmunol.170.8.4189

Source DB: PubMed Journal: J Immunol ISSN： 0022-1767 Impact factor: 5.422

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Cited

38 in total

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Review 2. Targeting lymphocyte signaling pathways as a therapeutic approach to systemic lupus erythematosus.

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3. FcγRIIIa Signaling Modulates Endosomal TLR Responses in Human CD4⁺ T Cells.

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4. Transcription factor Ikaros represses protein phosphatase 2A (PP2A) expression through an intronic binding site.

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5. Genome-wide association study of systemic sclerosis identifies CD247 as a new susceptibility locus.

Authors: Timothy R D J Radstake; Olga Gorlova; Blanca Rueda; Jose-Ezequiel Martin; Behrooz Z Alizadeh; Rogelio Palomino-Morales; Marieke J Coenen; Madelon C Vonk; Alexandre E Voskuyl; Annemie J Schuerwegh; Jasper C Broen; Piet L C M van Riel; Ruben van 't Slot; Annet Italiaander; Roel A Ophoff; Gabriela Riemekasten; Nico Hunzelmann; Carmen P Simeon; Norberto Ortego-Centeno; Miguel A González-Gay; María F González-Escribano; Paolo Airo; Jaap van Laar; Ariane Herrick; Jane Worthington; Roger Hesselstrand; Vanessa Smith; Filip de Keyser; Fredric Houssiau; Meng May Chee; Rajan Madhok; Paul Shiels; Rene Westhovens; Alexander Kreuter; Hans Kiener; Elfride de Baere; Torsten Witte; Leonid Padykov; Lars Klareskog; Lorenzo Beretta; Rafaella Scorza; Benedicte A Lie; Anna-Maria Hoffmann-Vold; Patricia Carreira; John Varga; Monique Hinchcliff; Peter K Gregersen; Annette T Lee; Jun Ying; Younghun Han; Shih-Feng Weng; Christopher I Amos; Fredrick M Wigley; Laura Hummers; J Lee Nelson; Sandeep K Agarwal; Shervin Assassi; Pravitt Gourh; Filemon K Tan; Bobby P C Koeleman; Frank C Arnett; Javier Martin; Maureen D Mayes
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6. Human CD4(+) effector T lymphocytes generated upon TCR engagement with self-peptides respond defectively to IL-7 in their transition to memory cells.

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The FcR gamma subunit and Syk kinase replace the CD3 zeta-chain and ZAP-70 kinase in the TCR signaling complex of human effector CD4 T cells.

1. CREMα suppresses spleen tyrosine kinase expression in normal but not systemic lupus erythematosus T cells.

Review 2. Targeting lymphocyte signaling pathways as a therapeutic approach to systemic lupus erythematosus.

3. FcγRIIIa Signaling Modulates Endosomal TLR Responses in Human CD4⁺ T Cells.

4. Transcription factor Ikaros represses protein phosphatase 2A (PP2A) expression through an intronic binding site.

5. Genome-wide association study of systemic sclerosis identifies CD247 as a new susceptibility locus.

6. Human CD4(+) effector T lymphocytes generated upon TCR engagement with self-peptides respond defectively to IL-7 in their transition to memory cells.

7. Zeta chain expression in T and NK cells in peripheral blood of children with nephrotic syndrome.

Review 8. Small molecules in the treatment of systemic lupus erythematosus.

9. FcgammaRIII mediates immunoglobulin G-induced interleukin-10 and is required for chronic Leishmania mexicana lesions.

Review 10. Signal transduction via the T cell antigen receptor in naïve and effector/memory T cells.