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Literature DB >> 15100286

Lymphocyte activation gene-3 (CD223) regulates the size of the expanding T cell population following antigen activation in vivo.

Creg J Workman¹, Linda S Cauley, In-Jeong Kim, Marcia A Blackman, David L Woodland, Dario A A Vignali.

Abstract

Lymphocyte activation gene-3 (LAG-3) is a CD4-related, activation-induced cell surface molecule that binds to MHC class II with high affinity. In this study, we used four experimental systems to reevaluate previous suggestions that LAG-3(-/-) mice had no T cell defect. First, LAG-3(-/-) T cells exhibited a delay in cell cycle arrest following in vivo stimulation with the superantigen staphylococcal enterotoxin B resulting in increased T cell expansion and splenomegaly. Second, increased T cell expansion was also observed in adoptive recipients of LAG-3(-/-) OT-II TCR transgenic T cells following in vivo Ag stimulation. Third, infection of LAG-3(-/-) mice with Sendai virus resulted in increased numbers of memory CD4(+) and CD8(+) T cells. Fourth, CD4(+) T cells exhibited a delayed expansion in LAG-3(-/-) mice infected with murine gammaherpesvirus. In summary, these data suggest that LAG-3 negatively regulates T cell expansion and controls the size of the memory T cell pool.

Entities: Disease Gene Species

Mesh：

Substances：

Year: 2004 PMID： 15100286 DOI： 10.4049/jimmunol.172.9.5450

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

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Cited

126 in total

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Lymphocyte activation gene-3 (CD223) regulates the size of the expanding T cell population following antigen activation in vivo.

Review 1. Integrative Pharmacology: Advancing Development of Effective Immunotherapies.

2. LAG-3, TGF-β, and cell-intrinsic PD-1 inhibitory pathways contribute to CD8 but not CD4 T-cell tolerance induced by allogeneic BMT with anti-CD40L.

Review 3. Making cold malignant pleural effusions hot: driving novel immunotherapies.

Review 4. Mechanisms of Immune Tolerance in Leukemia and Lymphoma.

5. Molecular, clinicopathological, and immune correlates of LAG3 promoter DNA methylation in melanoma.

6. Functional exhaustion of CD4⁺ T cells induced by co-stimulatory signals from myeloid leukaemia cells.

Review 7. Tim-3, Lag-3, and TIGIT.

Review 8. Costimulatory and Coinhibitory Receptor Pathways in Infectious Disease.

Review 9. Lag-3, Tim-3, and TIGIT: Co-inhibitory Receptors with Specialized Functions in Immune Regulation.

10. Coregulation of CD8+ T cell exhaustion by multiple inhibitory receptors during chronic viral infection.

Lymphocyte activation gene-3 (CD223) regulates the size of the expanding T cell population following antigen activation in vivo.

Review 1. Integrative Pharmacology: Advancing Development of Effective Immunotherapies.

2. LAG-3, TGF-β, and cell-intrinsic PD-1 inhibitory pathways contribute to CD8 but not CD4 T-cell tolerance induced by allogeneic BMT with anti-CD40L.

Review 3. Making cold malignant pleural effusions hot: driving novel immunotherapies.

Review 4. Mechanisms of Immune Tolerance in Leukemia and Lymphoma.

5. Molecular, clinicopathological, and immune correlates of LAG3 promoter DNA methylation in melanoma.

6. Functional exhaustion of CD4+ T cells induced by co-stimulatory signals from myeloid leukaemia cells.

Review 7. Tim-3, Lag-3, and TIGIT.

Review 8. Costimulatory and Coinhibitory Receptor Pathways in Infectious Disease.

Review 9. Lag-3, Tim-3, and TIGIT: Co-inhibitory Receptors with Specialized Functions in Immune Regulation.

10. Coregulation of CD8+ T cell exhaustion by multiple inhibitory receptors during chronic viral infection.

6. Functional exhaustion of CD4⁺ T cells induced by co-stimulatory signals from myeloid leukaemia cells.