Loss of immune homeostasis dictates SHIV rebound after stem-cell transplantation
Christopher W. Peterson, … , Rafick P. Sékaly, Hans-Peter Kiem
Christopher W. Peterson, … , Rafick P. Sékaly, Hans-Peter Kiem
Published February 23, 2017
Citation Information: JCI Insight. 2017;2(4):e91230. https://doi.org/10.1172/jci.insight.91230.
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Research Article AIDS/HIV Transplantation

Loss of immune homeostasis dictates SHIV rebound after stem-cell transplantation

Abstract

The conditioning regimen used as part of the Berlin patient’s hematopoietic cell transplant likely contributed to his eradication of HIV infection. We studied the impact of conditioning in simian-human immunodeficiency virus–infected (SHIV-infected) macaques suppressed by combination antiretroviral therapy (cART). The conditioning regimen resulted in a dramatic, but incomplete depletion of CD4+ and CD8+ T cells and CD20+ B cells, increased T cell activation and exhaustion, and a significant loss of SHIV-specific Abs. The disrupted T cell homeostasis and markers of microbial translocation positively correlated with an increased viral rebound after cART interruption. Quantitative viral outgrowth and Tat/rev–induced limiting dilution assays showed that the size of the latent SHIV reservoir did not correlate with viral rebound. These findings identify perturbations of the immune system as a mechanism for the failure of autologous transplantation to eradicate HIV. Thus, transplantation strategies may be improved by incorporating immune modulators to prevent disrupted homeostasis, and gene therapy to protect transplanted cells.

Authors

Christopher W. Peterson, Clarisse Benne, Patricia Polacino, Jasbir Kaur, Cristina E. McAllister, Abdelali Filali-Mouhim, Willi Obenza, Tiffany A. Pecor, Meei-Li Huang, Audrey Baldessari, Robert D. Murnane, Ann E. Woolfrey, Keith R. Jerome, Shiu-Lok Hu, Nichole R. Klatt, Stephen DeRosa, Rafick P. Sékaly, Hans-Peter Kiem

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Figure 4

Significant increase in CD4+Ki67+ and CD8+Ki67+ subset proportions following autologous transplantation.

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Significant increase in CD4+Ki67+ and CD8+Ki67+ subset proportions follo...
At the indicated time points, flow cytometry was used to analyze batched peripheral blood mononuclear cell (PBMC) samples for expression of the proliferation marker Ki67 in CD4+ (AC) and CD8+ T cells (DF). Naive, central memory (CM), and effector memory (EM) subsets are shown. Values represent mean ± SD. *P < 0.05, **P < 0.01 by 2-tailed Mann-Whitney test. Near-significant P values are also indicated. Time points along the x axes are defined in Supplemental Table 1.