Transcription factor FOXO3a controls the persistence of memory [CD4.sup.+} T cells during HIV infection

Transcription factor FOXO3a controls the persistence of memory [CD4.sup.+} T cells during HIV infection

The persistence of central memory [CD4.sup.+} T cells ([T.sub.CM] cells) is a major correlate of immunological protection in HIV/AIDS, as the rate of [T.sub.CM] cell decline predicts HIV disease progression. In this study, we show that [T.sub.CM] cells and effector memory [CD4.sup.+} T cells ([T.sub...

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Veröffentlicht in:Nature medicine 2008-03, Vol.14 (3), p.266
Hauptverfasser: van Grevenynghe, Julien, Procopio, Francesco A, He, Zhong, Chomont, Nicolas, Riou, Catherine, Zhang, Yuwei, Gimmig, Sylvain, Boucher, Genevieve, Wilkinson, Peter, Shi, Yu, Yassine-Diab, Bader, Said, Elias A, Trautmann, Lydie, Far, Mohamed El, Balderas, Robert S, Boulassel, Mohamed-Rachid, Routy, Jean-Pierre, Haddad, Elias K, Sekaly, Rafick-Pierre
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container_issue 3
container_start_page 266
container_title Nature medicine
container_volume 14
creator van Grevenynghe, Julien
Procopio, Francesco A
He, Zhong
Chomont, Nicolas
Riou, Catherine
Zhang, Yuwei
Gimmig, Sylvain
Boucher, Genevieve
Wilkinson, Peter
Shi, Yu
Yassine-Diab, Bader
Said, Elias A
Trautmann, Lydie
Far, Mohamed El
Balderas, Robert S
Boulassel, Mohamed-Rachid
Routy, Jean-Pierre
Haddad, Elias K
Sekaly, Rafick-Pierre
description The persistence of central memory [CD4.sup.+} T cells ([T.sub.CM] cells) is a major correlate of immunological protection in HIV/AIDS, as the rate of [T.sub.CM] cell decline predicts HIV disease progression. In this study, we show that [T.sub.CM] cells and effector memory [CD4.sup.+} T cells ([T.sub.EM] cells) from [HIV.sup.+] elite controller (EC) subjects are less susceptible to Fas-mediated apoptosis and persist longer after multiple rounds of T cell receptor triggering when compared to [T.sub.CM] and [T.sub.EM] cells from aviremic successfully treated (ST) subjects or from [HIV.sup.-] donors. We show that persistence of [T.sub.CM] cells from EC subjects is a direct consequence of inactivation of the FOXO3a pathway. Silencing the transcriptionally active form of FOXO3a by small interfering RNA or by introducing a FOXO3a dominant-negative form (FOXO3a Nt) extended the long-term survival of [T.sub.CM] cells from ST subjects to a length of time similar to that of [T.sub.CM] cells from EC subjects. The crucial role of FOXO3a in the survival of memory cells will help shed light on the underlying immunological mechanisms that control viral replication in EC subjects.
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title Transcription factor FOXO3a controls the persistence of memory [CD4.sup.+} T cells during HIV infection
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