Cumulative mechanisms of lymphoid tissue fibrosis and T cell depletion in HIV-1 and SIV infections
Ming Zeng, … , John V. Carlis, Ashley T. Haase
Ming Zeng, … , John V. Carlis, Ashley T. Haase
Published February 14, 2011
Citation Information: J Clin Invest. 2011;121(3):998-1008. https://doi.org/10.1172/JCI45157.
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Research Article Virology

Cumulative mechanisms of lymphoid tissue fibrosis and T cell depletion in HIV-1 and SIV infections

Abstract

The hallmark of HIV-1 and SIV infections is CD4+ T cell depletion. Both direct cell killing and indirect mechanisms related to immune activation have been suggested to cause the depletion of T cells. We have now identified a mechanism by which immune activation-induced fibrosis of lymphoid tissues leads to depletion of naive T cells in HIV-1 infected patients and SIV-infected rhesus macaques. The T regulatory cell response to immune activation increased procollagen production and subsequent deposition as fibrils via the TGF-β1 signaling pathway and chitinase 3-like-1 activity in fibroblasts in lymphoid tissues from patients infected with HIV-1. Collagen deposition restricted T cell access to the survival factor IL-7 on the fibroblastic reticular cell (FRC) network, resulting in apoptosis and depletion of T cells, which, in turn, removed a major source of lymphotoxin-β, a survival factor for FRCs during SIV infection in rhesus macaques. The resulting loss of FRCs and the loss of IL-7 produced by FRCs may thus perpetuate a vicious cycle of depletion of T cells and the FRC network. Because this process is cumulative, early treatment and antifibrotic therapies may offer approaches to moderate T cell depletion and improve immune reconstitution during HIV-1 infection.

Authors

Ming Zeng, Anthony J. Smith, Stephen W. Wietgrefe, Peter J. Southern, Timothy W. Schacker, Cavan S. Reilly, Jacob D. Estes, Gregory F. Burton, Guido Silvestri, Jeffrey D. Lifson, John V. Carlis, Ashley T. Haase

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Figure 8

TGF-β1 stimulates the production of CHI3L1 by LT fibroblasts.

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TGF-β1 stimulates the production of CHI3L1 by LT fibroblasts. (A) TGF-β1...
(A) TGF-β1–expressing cells were significantly correlated with CHI3L1 expression in the inguinal LN. Each individual colored symbol represents an individual subject. (B) Immunofluorescent images of CHI3L1 (green staining) in primary human fibroblasts, treated with or without TGF-β1 (250 ng/ml) for 48 hours (representative image of 10). Cell nuclei appear blue (DAPI staining). Scale bars: 50 μm. (C) The extracellular CHI3L1 networks of primary human fibroblasts were quantified for each condition and are reported as CHI3L1 mean fluorescence intensity. Data are expressed as mean ± SD, where 3 independent experiments were performed in quadruplicate. The results are shown with significance where applicable (P < 0.05).