Your search keyword '"Haeryfar, S. M. Mansour"' showing total 4 results

1. Preventing and curing citrulline-induced autoimmune arthritis in a humanized mouse model using a Th2-polarizing iNKT cell agonist.

Author

Walker, Kyle M, Rytelewski, Mateusz, Mazzuca, Delfina M, Meilleur, Shannon A, Mannik, Lisa A, Yue, David, Brintnell, William C, Welch, Ian, Cairns, Ewa, and Haeryfar, S M Mansour

Subjects

AUTOIMMUNE diseases, TRANSGENIC mice, CELLULAR immunity, IMMUNE response, LYMPHOCYTES, JOINT diseases

Abstract

Invariant natural killer T (iNKT) cells are innate lymphocytes with unique reactivity to glycolipid antigens bound to non-polymorphic CD1d molecules. They are capable of rapidly releasing pro- and/or anti-inflammatory cytokines and constitute attractive targets for immunotherapy of a wide range of diseases including autoimmune disorders. In this study, we have explored the beneficial effects of OCH, a Th2-polarizing glycolipid agonist of iNKT cells, in a humanized mouse model of rheumatoid arthritis (RA) in which citrullinated human proteins are targeted by autoaggressive immune responses in mice expressing an RA susceptibility human leukocyte antigen (HLA) DR4 molecule. We found for the first time that treatment with OCH both prevents and cures citrulline-induced autoimmune arthritis as evidenced by resolved ankle swelling and reversed histopathological changes associated with arthritis. Also importantly, OCH treatment blocked the arthritogenic capacity of citrullinated antigen-experienced splenocytes without compromising their global responsiveness or altering the proportion of splenic naturally occurring CD4+CD25+FoxP3+ regulatory T cells. Interestingly, administering the Th1-promoting iNKT cell glycolipid ligand α-C-galactosylceramide into HLA-DR4 transgenic mice increased the incidence of arthritis in these animals and exacerbated their clinical symptoms, strongly suggesting a role for Th1 responses in the pathogenesis of citrulline-induced arthritis. Therefore, our findings indicate a role for Th1-mediated immunopathology in citrulline-induced arthritis and provide the first evidence that iNKT cell manipulation by Th2-skewing glycolipids may be of therapeutic value in this clinically relevant model, a finding that is potentially translatable to human RA. [ABSTRACT FROM AUTHOR]

Published

2012

2. Engagement of glycosylphosphatidylinositol-anchored proteins results in enhanced mouse and human invariant natural killer T cell responses.

Author

Mannik, Lisa A., Chin-Yee, Ian, Sharif, Shayan, Van Kaer, Luc, Delovitch, Terry L., and Haeryfar, S. M. Mansour

Subjects

PROTEINS, LABORATORY mice, KILLER cells, T cells, LYMPHOCYTES, GLYCOLIPIDS, ANTIGENS, ANTI-inflammatory agents

Abstract

Invariant natural killer T ( iNKT) cells are a small subset of lymphocytes that recognize glycolipid antigens in the context of CD1d and consequently produce large quantities of pro-inflammatory and/or anti-inflammatory cytokines. Several transmembrane glycoproteins have been implicated in the co-stimulation of iNKT cell responses. However, whether glycosylphosphatidylinositol (GPI)-anchored proteins can function in this capacity is not known. Here, we demonstrate that antibody-mediated cross-linking of the prototype mouse GPI-anchored protein Thy-1 (CD90) on the surface of a double-negative (CD4CD8) iNKT cell line leads to cytokine production at both the mRNA and protein levels. In addition, Thy-1 triggering enhanced cytokine secretion by iNKT cells that were concomitantly stimulated with α-galactosylceramide (αGC), consistent with a co-stimulatory role for Thy-1 in iNKT cell activation. This was also evident when a CD4 mouse iNKT cell line or primary hepatic NKT cells were stimulated with αGC and/or anti-Thy-1 antibody. Cross-linking Ly-6A/E, another GPI-anchored protein, could also boost cytokine secretion by αGC-stimulated iNKT cells, suggesting that the observed effects reflect a general property of GPI-anchored proteins. To extend these results from mouse to human cells, we focused on CD55, a GPI-anchored protein that, unlike Thy-1, is expressed on human iNKT cells. Cross-linking CD55 augmented αGC-induced iNKT cell responses as judged by more vigorous proliferation and higher CD69 expression. Collectively, these findings demonstrate for the first time that GPI-anchored proteins are able to co-stimulate CD1d-restricted, glycolipid-reactive iNKT cells in both mice and humans. [ABSTRACT FROM AUTHOR]

Published

2011

3. CTLA-4Ig blocks the development and progression of citrullinated fibrinogen-induced arthritis in DR4-transgenic mice.

Author

Yue, David, Brintnell, William, Mannik, Lisa A, Christie, Darah A, Haeryfar, S M Mansour, Madrenas, Joaquín, Chakrabarti, Subrata, Bell, David A, and Cairns, Ewa

Abstract

OBJECTIVE: To assess the role of T cells in the mouse model of citrullinated human fibrinogen-induced rheumatoid arthritis (RA) using CTLA-4Ig, an agent that blocks T cell costimulation, which is required for T cell activation. METHODS: Humanized HLA-DR[beta]1*0401-transgenic (DR4-Tg) mice were immunized with Cit-human fibrinogen to induce arthritis. Prior to, and at the onset or peak of, arthritis, the DR4-Tg mice were treated with CTLA-4Ig or control human IgG1 or were left untreated. Arthritis development and progression were monitored by measuring ankle swelling with calipers and by assessing histopathologic changes. The immune responses to the citrullinated antigens and the corresponding unmodified antigens, as well as the arthritogenicity of lymphocytes from these mice, were examined. The latter was performed using lymphocyte transfers from CTLA-4Ig-treated or control mice via intraperitoneal injection into naive DR4-Tg mice. Recipient mice also received an intraarticular injection of Cit-human fibrinogen, unmodified human fibrinogen, or vehicle. RESULTS: CTLA-4Ig-treated, but not human IgG1-treated, arthritic mice had significantly reduced ankle swelling and pathologic joint damage. Treatment with CTLA-4Ig, but not human IgG1, suppressed Cit-human fibrinogen-induced T cell activation, including citrulline-specific T cell activation, when given prior to disease onset. Transfer of splenic lymphocytes from untreated or human IgG1-treated arthritic mice caused arthritis in recipients, and this occurred when Cit-human fibrinogen, but not unmodified fibrinogen, was deposited into the joint. Splenocytes from CTLA-4Ig-treated mice were unable to transfer arthritis. CONCLUSION: Activated citrulline-specific T cells play a direct role in the development and progression of arthritis in this model of Cit-human fibrinogen-induced RA. [ABSTRACT FROM AUTHOR]

Published

2010

4. Antibody blockade of Thy-1 (CD90) impairsmouse cytotoxic T lymphocyte induction by anti-CD3 monoclonal antibody.

Author

Haeryfar, S. M. Mansour, Conrad, David M., Musgrave, Bruce L., and Hoskin, David W.

Subjects

*MONOCLONAL antibodies, *IMMUNOGLOBULINS, *LYMPHOCYTES, *T cells, *PROTEIN kinase C, *MICE, *CELL receptors

Abstract

SummaryThy-1 (CD90)expressed by mouse T cells is known to have signal transducing properties,but the ability of Thy-1 to enhance cytotoxic T lymphocyte (CTL)development is not well understood. Here we show that stimulationof mouse T cells with monoclonal antibodies (mAb) to CD3, CD28 andThy-1 (clone G7), which were coimmobilized on polystyrene microbeads,resulted in a greater proliferative response than stimulation withonly anti-CD3 and anti-CD28 mAb, indicating that Thy-1 cross-linkingenhanced T cell receptor/CD28-driven T cell activation.Consistent with this finding, Thy-1 blockade with a soluble nonactivatinganti-Thy-1 mAb (clone 30-H12) inhibited anti-CD3-induced proliferationof CD4+ and CD8+ T cells,and the induction of cytotoxic effector cells in a dose-dependentfashion. Interleukin-2 synthesis and CD25 expression were also impairedby Thy-1 blockade. The inhibitory effect involved a defect at orbefore the level of protein kinase C activation because the additionof phorbol ester ablated the anti-Thy-1-mediated inhibition of anti-CD3-inducedT cell activation. The CTL that were induced in the presence ofblocking anti-Thy-1 mAb adhered to target cells but showed reducedexpression of granzyme B and perforin. In contrast, Fas ligand expressionand function was not affected by Thy-1 blockade. We conclude thatThy-1 signalling promotes the in vitro generation of CTLthat kill in a granule-dependent fashion. [ABSTRACT FROM AUTHOR]

Published

2005