Gld mutation of Fas ligand increases the frequency and up-regulates cell survival genes in CD25+CD4+ TR cells

Mohamood, Abdiaziz S.; Trujillo, Crystal J.; Zheng, Dongfeng; Jie, Chunfa; Murillo, Francisco Martinez; Schneck, Jonathan P.; Hamad, Abdel Rahim A.

doi:10.1093/intimm/dxl057

Cited by 24 publications

(65 citation statements)

References 56 publications

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“…We found that Treg cells derived from both young and old lpr/lpr gld/gld mice ably suppress T cell proliferation in vitro. These data are consistent with other studies that have shown that blocking with an anti-FasL antibody has no effect on Treg cell suppression [39,40], and that Treg cells from gld/gld mice can inhibit gld/gld Th cell proliferation [11]. Conversely, we found that Treg cells suppress the proliferation of Th cells derived from either young or old lpr/lpr gld/gld mice.…”

Section: Discussionsupporting

confidence: 93%

“…Likewise, in some murine models of SLE Treg cells are diminished and/or have reduced Foxp3 protein expression [8][9][10]. In contrast, 16-20 week old C3H gld/gld mice have an increased frequency of Foxp3 + T cells with Foxp3 protein expressed at levels similar to normal mice [11]. The functional capacity of Treg cells to block T cell proliferation in vitro also varies according to strain.…”

Section: Introductionmentioning

confidence: 99%

“…The functional capacity of Treg cells to block T cell proliferation in vitro also varies according to strain. In the C3H gld/gld model, Treg cells inhibited Th cell proliferation while in NZM2410 mice the Treg cells were less effective [10,11]. The ability of Treg cells to block lupus in vivo has also depended upon the symptoms examined.…”

Section: Introductionmentioning

confidence: 99%

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Autoantibody production in lpr/lpr gld/gld mice reflects accumulation of CD4+ effector cells that are resistant to regulatory T cell activity

Hondowicz

Fields

Nish

et al. 2008

Journal of Autoimmunity

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In Fas/FasL deficient mice anti-chromatin Ab production is T cell dependent and is not apparent until after 10 weeks of age. Early control of anti-chromatin antibodies may be due to the counterbalancing influence of Treg cells. Here we show that Treg cells block lpr/lpr gld/gld Th cells from providing help to anti-chromatin B cells in an in vivo transfer system. Interestingly, the percentage and absolute numbers of Foxp3 + Treg cells is elevated in BALB/c-lpr/lpr gld/gld mice and increases with age compared to BALB/c mice. The majority of Foxp3 expression is found in the B220 − CD4 + T cell population, and Foxp3-expressing cells are localized in the splenic PALS (periarteriolar lymphocyte sheath). Strikingly, although the lack of functional Fas/FasL does not affect the ability of Treg cells to block Th cell proliferation, Treg cells can block the IFN-γ differentiation of Th cells from BALB/ c or young BALB-lpr/lpr gld/gld mice but not of pre-existing Th1 cells from older BALB/c-lpr/lpr gld/gld mice. Thus, we suggest autoantibody production is not caused by the lack of Treg cells but by a defect in activation-induced cell death that leads to the accumulation of T effector cells that are resistant to regulatory T cell activity.

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Section: Discussionsupporting

confidence: 93%

Section: Introductionmentioning

confidence: 99%

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Autoantibody production in lpr/lpr gld/gld mice reflects accumulation of CD4+ effector cells that are resistant to regulatory T cell activity

Hondowicz

Fields

Nish

et al. 2008

Journal of Autoimmunity

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“…Forty nanograms of cDNA of each sample was used for each real-time PCR reaction using gene-specific primer and probe sets in the Quant Studio 12 K Flex real-time PCR system. Realtime data were normalized with b-actin and analyzed as previously described 31 and fold change in mRNA expression was calculated using the 2-ΔΔCT method.…”

Section: Adoptive Transfer and Assessment Of Kidney Injurymentioning

confidence: 99%

Double-Negative αβ T Cells Are Early Responders to AKI and Are Found in Human Kidney

Martina¹,

Noel²,

Saxena³

et al. 2016

Journal of the American Society of Nephrology

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“…Although gld mice display elevated Treg numbers, the latter was unaltered in lpr mice (12,13). Moreover, several in vivo studies demonstrated that Treg numbers decline during an immune response as a result of CD95 ligation, whereas others claimed that CD95L expression by Tregs induces responder cell death in vitro (14)(15)(16)(17).…”

Section: Foxp3mentioning

confidence: 99%

Foxp3-Mediated Suppression of CD95L Expression Confers Resistance to Activation-Induced Cell Death in Regulatory T Cells

Weiß

Schmidt

Vobis

et al. 2011

The Journal of Immunology

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CD4+CD25++Foxp3+ regulatory T cells (Tregs) control self-reactive cells to maintain peripheral tolerance. Treg homeostasis has to be controlled tightly to ensure balanced Treg-mediated suppression. One mechanism that regulates the CD4+ T cell pool is activation-induced cell death (AICD). This is mimicked in vitro by TCR restimulation-induced expression of the death ligand CD95L (FasL/APO-1L/CD178) in expanded T cells. These cells express the death receptor CD95 (Fas/APO-1), and binding of CD95L to CD95 results in AICD. In contrast, Tregs do not undergo AICD upon TCR (re)stimulation in vitro despite a functional CD95 cell death pathway. In this study, we show that human and murine Tregs express low levels of CD95L upon stimulation. Knockdown of the transcriptional repressor Foxp3 partially rescues CD95L expression and AICD in human Tregs. Moreover, upon stimulation Foxp3-mutant Tregs from Scurfy mice express CD95L similar to conventional T cells. We further addressed whether exogenous CD95 stimulation provides a mechanism of Treg homeostatic control in vivo in mice. Triggering of CD95 reduced Treg numbers systemically as reflected by in vivo imaging and decreased GFP+ Treg numbers ex vivo. Our study reveals that Foxp3 negatively regulates CD95L expression in Tregs and demonstrates that Tregs are susceptible to homeostatic control by CD95 stimulation.

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Gld mutation of Fas ligand increases the frequency and up-regulates cell survival genes in CD25+CD4+ TR cells

Cited by 24 publications

References 56 publications

Autoantibody production in lpr/lpr gld/gld mice reflects accumulation of CD4+ effector cells that are resistant to regulatory T cell activity

Autoantibody production in lpr/lpr gld/gld mice reflects accumulation of CD4+ effector cells that are resistant to regulatory T cell activity

Double-Negative αβ T Cells Are Early Responders to AKI and Are Found in Human Kidney

Foxp3-Mediated Suppression of CD95L Expression Confers Resistance to Activation-Induced Cell Death in Regulatory T Cells

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