학술논문
CD39/adenosine pathway is involved in AIDS progression.
Document Type
article
Author
Maria Nikolova; Matthieu Carriere; Mohammad-Ali Jenabian; Sophie Limou; Mehwish Younas; Ayrin Kök; Sophie Huë; Nabila Seddiki; Anne Hulin; Olivier Delaneau; Hanneke Schuitemaker; Joshua T Herbeck; James I Mullins; Maria Muhtarova; Armand Bensussan; Jean-François Zagury; Jean-Daniel Lelievre; Yves Lévy
Source
PLoS Pathogens, Vol 7, Iss 7, p e1002110 (2011)
Subject
Language
English
ISSN
1553-7366
1553-7374
1553-7374
Abstract
HIV-1 infection is characterized by a chronic activation of the immune system and suppressed function of T lymphocytes. Regulatory CD4+ CD25(high) FoxP3+CD127(low) T cells (Treg) play a key role in both conditions. Here, we show that HIV-1 positive patients have a significant increase of Treg-associated expression of CD39/ENTPD1, an ectoenzyme which in concert with CD73 generates adenosine. We show in vitro that the CD39/adenosine axis is involved in Treg suppression in HIV infection. Treg inhibitory effects are relieved by CD39 down modulation and are reproduced by an adenosine-agonist in accordance with a higher expression of the adenosine A2A receptor on patients' T cells. Notably, the expansion of the Treg CD39+ correlates with the level of immune activation and lower CD4+ counts in HIV-1 infected patients. Finally, in a genetic association study performed in three different cohorts, we identified a CD39 gene polymorphism that was associated with down-modulated CD39 expression and a slower progression to AIDS.