| Literature DB >> 16709924 |
Markus Munder1, Henriette Schneider, Claudia Luckner, Thomas Giese, Claus-Dieter Langhans, Jose M Fuentes, Pascale Kropf, Ingrid Mueller, Armin Kolb, Manuel Modolell, Anthony D Ho.
Abstract
Chronic inflammation is accompanied by impaired T-cell immunity. In the mouse, myeloid cell-associated arginase accounts for the suppression of immune reactivity in various models of tumor growth and chronic infections. Here we show that arginase I is liberated from human granulocytes, and very high activities accumulate extracellularly during purulent inflammatory reactions. Human granulocyte arginase induces a profound suppression of T-cell proliferation and cytokine synthesis. This T-cell phenotype is due to arginase-mediated depletion of arginine in the T-cell environment, which leads to CD3zeta chain down-regulation but does not alter T-cell viability. Our study therefore demonstrates that human granulocytes possess a previously unanticipated immunosuppressive effector function. Human granulocyte arginase is a promising pharmacologic target to reverse unwanted immunosuppression.Entities:
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Year: 2006 PMID: 16709924 DOI: 10.1182/blood-2006-11-010389
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113