Abstract
BackgroundWe and others have previously reported that cell membrane-bound TGFβ (mTGFβ) on activated T regulatory (Treg) cells mediates suppressor function. Current findings suggest that a novel protein known as Glycoprotein A Repetitions Predominant (GARP) anchors mTGFβ to the Treg cell surface and facilitates suppressor activity. Recently, we have described that GARP+TGFβ+ Treg cells expand during the course of FIV infection. Because Treg cells are anergic and generally exhibit poor proliferative ability, we asked how Treg homeostasis is maintained during the course of feline immunodeficiency virus (FIV) infection.ResultsHere, we report that Treg cells from FIV+ cats express GARP and mTGFβ and convert T helper (Th) cells into phenotypic and functional Treg cells. Th to Treg conversion was abrogated by anti-TGFβ or anti-GARP treatment of Treg cells or by anti-TGFβRII treatment of Th cells, suggesting that Treg cell recruitment from the Th pool is mediated by TGFβ/TGFβRII signaling and that cell-surface GARP plays a major role in this process.ConclusionsThese findings suggest Th to Treg conversion may initiate a cascade of events that contributes to the maintenance of virus reservoirs, progressive Th cell immunosuppression, and the development of immunodeficiency, all of which are central to the pathogenesis of AIDS lentivirus infections.
Highlights
We and others have previously reported that cell membrane-bound TGFβ on activated T regulatory (Treg) cells mediates suppressor function
T helper (Th) cells are increased during chronic feline immunodeficiency virus (FIV)-infection We have reported that Concanavalin A (ConA)/TGFβ-stimulated CD4+C D25- Th cells are converted to immunosuppressive CD25+membrane-bound TGFβ (mTGFβ)+FoxP3+ Treg cells and that this conversion is abrogated by pre-treatment of ConA-stimulated Th target cells with anti-TGFβ receptor II (TGFβRII) suggesting a TGFβTGFβRII mediated process [17]
Th to induced Treg (iTreg) cell conversion that is mediated by activated CD4+CD25+ mTGFβ+FoxP3+ Treg cells may limit expansion and effector function of anti-viral CD4+ T cells by converting them to CD25+mTGFβ+FoxP3+ iTreg cells, contributing to the Treg cell pool during the progression of AIDS lentivirus infections
Summary
We and others have previously reported that cell membrane-bound TGFβ (mTGFβ) on activated T regulatory (Treg) cells mediates suppressor function. Th to Treg conversion was abrogated by anti-TGFβ or anti-GARP treatment of Treg cells or by anti-TGFβRII treatment of Th cells, suggesting that Treg cell recruitment from the Th pool is mediated by TGFβ/TGFβRII signaling and that cell-surface GARP plays a major role in this process. Recent studies indicate that peripheral Treg cells, once activated, express both mTGFβ and GARP on their surface and that both molecules are instrumental in Treg cell suppressor function [11,12] It is not known if this TGFβ/GARP complex plays a role in recruitment of Treg cells from the Th cell pool but evidence suggests that it may be integral to contact-dependent TGFβ signaling through TGFβRII [11,12]
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