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Attenuation of HIV-associated human B cell exhaustion by siRNA downregulation of inhibitory receptors
Lela Kardava, … , Susan K. Pierce, Anthony S. Fauci
Lela Kardava, … , Susan K. Pierce, Anthony S. Fauci
Published June 1, 2011
Citation Information: J Clin Invest. 2011;121(7):2614-2624. https://doi.org/10.1172/JCI45685.
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Research Article AIDS/HIV

Attenuation of HIV-associated human B cell exhaustion by siRNA downregulation of inhibitory receptors

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Abstract

Chronic immune activation in HIV-infected individuals leads to accumulation of exhausted tissue-like memory B cells. Exhausted lymphocytes display increased expression of multiple inhibitory receptors, which may contribute to the inefficiency of HIV-specific antibody responses. Here, we show that downregulation of B cell inhibitory receptors in primary human B cells led to increased tissue-like memory B cell proliferation and responsiveness against HIV. In human B cells, siRNA knockdown of 9 known and putative B cell inhibitory receptors led to enhanced B cell receptor–mediated (BCR-mediated) proliferation of tissue-like memory but not other B cell subpopulations. The strongest effects were observed with the putative inhibitory receptors Fc receptor–like–4 (FCRL4) and sialic acid–binding Ig-like lectin 6 (Siglec-6). Inhibitory receptor downregulation also led to increased levels of HIV-specific antibody-secreting cells and B cell–associated chemokines and cytokines. The absence of known ligands for FCRL4 and Siglec-6 suggests these receptors may regulate BCR signaling through their own constitutive or tonic signaling. Furthermore, the extent of FCLR4 knockdown effects on BCR-mediated proliferation varied depending on the costimulatory ligand, suggesting that inhibitory receptors may engage specific pathways in inhibiting B cell proliferation. These findings on HIV-associated B cell exhaustion define potential targets for reversing the deleterious effect of inhibitory receptors on immune responses against persistent viral infections.

Authors

Lela Kardava, Susan Moir, Wei Wang, Jason Ho, Clarisa M. Buckner, Jacqueline G. Posada, Marie A. O’Shea, Gregg Roby, Jenny Chen, Hae Won Sohn, Tae-Wook Chun, Susan K. Pierce, Anthony S. Fauci

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Figure 2

Expression of Siglec-6 and CD85d on tissue-like memory B cells in the peripheral blood of HIV-viremic individuals.

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Expression of Siglec-6 and CD85d on tissue-like memory B cells in the pe...
(A) Representative expression of Siglec-6 and CD85d on B cell subpopulations identified by color coding: CD27–CD21lo tissue-like memory (black), CD27+ classical memory (blue), and CD27–CD21hi naive (red) B cells. Expression of (B) Siglec-6 and (C) CD85d on mature B cell subpopulations of 16–22 HIV-viremic individuals. Horizontal bars indicate medians. Numbers in dot plot in A represent percentages. All stains included CD19 to establish the B cell gate and CD10 to exclude immature/transitional B cells.

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