Your search keyword '"Basso, Alexandre S"' showing total 2 results

1. Metabolic control of type 1 regulatory T cell differentiation by AHR and HIF1-α.

Author

Mascanfroni, Ivan D, Takenaka, Maisa C, Yeste, Ada, Patel, Bonny, Wu, Yan, Kenison, Jessica E, Siddiqui, Shafiuddin, Basso, Alexandre S, Otterbein, Leo E, Pardoll, Drew M, Pan, Fan, Priel, Avner, Clish, Clary B, Robson, Simon C, and Quintana, Francisco J

Subjects

LYMPHOCYTE metabolism, T cell differentiation, METABOLIC regulation, HYPOXIA-inducible factor 1, ARYL hydrocarbon receptors, CD antigens

Abstract

Our understanding of the pathways that regulate lymphocyte metabolism, as well as the effects of metabolism and its products on the immune response, is still limited. We report that a metabolic program controlled by the transcription factors hypoxia inducible factor-1α (HIF1-α) and aryl hydrocarbon receptor (AHR) supports the differentiation of type 1 regulatory T cell (Tr1) cells. HIF1-α controls the early metabolic reprograming of Tr1 cells. At later time points, AHR promotes HIF1-α degradation and takes control of Tr1 cell metabolism. Extracellular ATP (eATP) and hypoxia, linked to inflammation, trigger AHR inactivation by HIF1-α and inhibit Tr1 cell differentiation. Conversely, CD39 promotes Tr1 cell differentiation by depleting eATP. CD39 also contributes to Tr1 suppressive activity by generating adenosine in cooperation with CD73 expressed by responder T cells and antigen-presenting cells. These results suggest that HIF1-α and AHR integrate immunological, metabolic and environmental signals to regulate the immune response. [ABSTRACT FROM AUTHOR]

Published

2015

2. Oral CD3-specific antibody suppresses autoimmune encephalomyelitis by inducing CD4+CD25−LAP+ T cells.

Author

Ochi, Hirofumi, Abraham, Michal, Ishikawa, Hiroki, Frenkel, Dan, Yang, Kaiyong, Basso, Alexandre S., Wu, Henry, Mei-Ling Chen, Gandhi, Roopali, Miller, Ariel, Maron, Ruth, and Weiner, Howard L.

Subjects

CD antigens, AUTOIMMUNE diseases, ENCEPHALOMYELITIS, IMMUNE system, IMMUNOLOGY

Abstract

A major goal of immunotherapy for autoimmune diseases and transplantation is induction of regulatory T cells that mediate immunologic tolerance. The mucosal immune system is unique, as tolerance is preferentially induced after exposure to antigen, and induction of regulatory T cells is a primary mechanism of oral tolerance. Parenteral administration of CD3-specific monoclonal antibody is an approved therapy for transplantation in humans and is effective in autoimmune diabetes. We found that orally administered CD3-specific antibody is biologically active in the gut and suppresses autoimmune encephalomyelitis both before induction of disease and at the height of disease. Orally administered CD3-specific antibody induces CD4+CD25−LAP+ regulatory T cells that contain latency-associated peptide (LAP) on their surface and that function in vitro and in vivo through a TGF-β–dependent mechanism. These findings identify a new immunologic approach that is widely applicable for the treatment of human autoimmune conditions. [ABSTRACT FROM AUTHOR]

Published

2006