Interferon γ (IFN-γ) Is Necessary for the Genesis of Acetylcholine Receptor–induced Clinical Experimental Autoimmune <i>Myasthenia gravis</i> in Mice

Balasa, Balaji; Deng, Cheng; Lee, Jae; Bradley, Linda M.; Dalton, Dyana K.; Christadoss, Premkumar; Sarvetnick, Nora

doi:10.1084/jem.186.3.385

Cited by 175 publications

(119 citation statements)

References 44 publications

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“…The suppressive effect of anti-CD40L Ab in suppression of ongoing chronic EAMG in our study was associated with down-regulation of the pathogenic inflammatory cytokine IFN-␥ and of IL-12 ( Fig. 2), both of which have been previously demonstrated to be directly or indirectly involved in induction of EAMG (31)(32)(33)(34)(35). The selective suppressive effect on Th1-type differentiation by anti-CD40L treatment is consistent with models of other autoimmune diseases such as multiple sclerosis, diabetes, and thyroiditis (17,18,36,37), and with graft-vshost disease and graft rejection (38,39).…”

Section: Figure 3 Effect Of Anti-cd40l Treatment On Costimulatory Famentioning

confidence: 77%

Blockade of CD40 Ligand Suppresses Chronic Experimental Myasthenia Gravis by Down-Regulation of Th1 Differentiation and Up-Regulation of CTLA-4

Barchan

Maiti

et al. 2001

The Journal of Immunology

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Myasthenia gravis (MG) and experimental autoimmune MG (EAMG) are T cell-dependent Ab-mediated autoimmune disorders, in which the nicotinic acetylcholine receptor (AChR) is the major autoantigen. Th1-type cells and costimulatory factors such as CD40 ligand (CD40L) contribute to disease pathogenesis by producing proinflammatory cytokines and by activating autoreactive B cells. In this study we demonstrate the capacity of CD40L blockade to modulate EAMG, and analyze the mechanism underlying this disease suppression. Anti-CD40L Abs given to rats at the chronic stage of EAMG suppress the clinical progression of the autoimmune process and lead to a decrease in the AChR-specific humoral response and delayed-type hypersensitivity. The cytokine profile of treated rats suggests that the underlying mechanism involves down-regulation of AChR-specific Th1-regulated responses with no significant effect on Th2- and Th3-regulated AChR-specific responses. EAMG suppression is also accompanied by a significant up-regulation of CTLA-4, whereas a series of costimulatory factors remain unchanged. Adoptive transfer of splenocytes from anti-CD40L-treated rats does not protect recipient rats against subsequently induced EAMG. Thus it seems that the suppressed progression of chronic EAMG by anti-CD40L treatment does not induce a switch from Th1 to Th2/Th3 regulation of the AChR-specific immune response and does not induce generation of regulatory cells. The ability of anti-CD40L treatment to suppress ongoing chronic EAMG suggests that blockade of CD40L may serve as a potential approach for the immunotherapy of MG and other Ab-mediated autoimmune diseases.

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Section: Figure 3 Effect Of Anti-cd40l Treatment On Costimulatory Famentioning

confidence: 77%

Blockade of CD40 Ligand Suppresses Chronic Experimental Myasthenia Gravis by Down-Regulation of Th1 Differentiation and Up-Regulation of CTLA-4

Barchan

Maiti

et al. 2001

The Journal of Immunology

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“…Although earlier work had indicated that ectopic expression of IFN-c at the neuromuscular junction provoked MG-like disease [33], our current understanding of the role of IFN-c in EAMG is far from conclusive. For example, mice deficient of IFN-c [25] or IFN-c receptor [26] are resistant to EAMG, yet some groups have shown that IFN-c deficiency may not significantly alter the course of disease [27,34]. Thus, while Th1 responses may possibly play a role in the disease depending on the experimental system used, the question arises on whether other inflammatory cytokine(s) with potent propathogenic effects, such as IL-17, are required for the expression of EAMG.…”

Section: Discussionmentioning

confidence: 99%

“…We and others [25][26][27] have previously found that the development of EAMG is not dramatically altered by IFN-c deficiency. To investigate whether the effects of IL-17 on EAMG were related to or depended on IFN-c, we treated IFN-c -/-mice with IL-17 during EAMG induction, using the same regimen used for the B6 mice.…”

Section: Il-17 Facilitates Autoantibody Responses and Clinical Eamg Imentioning

confidence: 93%

CCL2 recruitment of IL‐6‐producing CD11b⁺ monocytes to the draining lymph nodes during the initiation of Th17‐dependent B cell‐mediated autoimmunity

et al. 2008

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The development and function of Th17 cells are influenced in part by the cytokines TGF-b, IL-23 and IL-6, but the mechanisms that govern recruitment and activity of Th17 cells during initiation of autoimmunity remain poorly defined. We show here that the development of autoreactive Th17 cells in secondary lymphoid organs in experimental autoimmune myasthenia gravis -an animal model of human myasthenia gravis -is modulated by IL-6-producing CD11b + cells via the CC chemokine ligand 2 (CCL2). Notably, acetylcholine receptor (AChR)-reactive Th17 cells provide help for the B cells to produce anti-AChR antibodies, which are responsible for the impairment of the neuromuscular transmission that contributes to the clinical manifestations of autoimmunity, as indicated by a lack of disease induction in IL-17-deficient mice. Thus, Th17 cells can promote humoral autoimmunity via a novel mechanism that involves CCL2.

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“…However, IFN-g is still a controversial factor in the pathogenesis of EAMG. B6 Mice with IFN-g or IFN-gR deficiency are less susceptible to EAMG [25,30]. On the contrary, IFN-gdeficient B6 mice developed EAMG with a frequency similar to Spleen and lymph node MNC were obtained from rats receiving TGF-b1-DC, naïve DC or PBS on day 39 p.i.…”

Section: Discussionmentioning

confidence: 99%

Dendritic cells exposed in vitro to TGF-beta1 ameliorate experimental autoimmune myasthenia gravis

et al. 2002

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Interferon γ (IFN-γ) Is Necessary for the Genesis of Acetylcholine Receptor–induced Clinical Experimental Autoimmune Myasthenia gravis in Mice

Cited by 175 publications

References 44 publications

Blockade of CD40 Ligand Suppresses Chronic Experimental Myasthenia Gravis by Down-Regulation of Th1 Differentiation and Up-Regulation of CTLA-4

Blockade of CD40 Ligand Suppresses Chronic Experimental Myasthenia Gravis by Down-Regulation of Th1 Differentiation and Up-Regulation of CTLA-4

CCL2 recruitment of IL‐6‐producing CD11b⁺ monocytes to the draining lymph nodes during the initiation of Th17‐dependent B cell‐mediated autoimmunity

Dendritic cells exposed in vitro to TGF-beta1 ameliorate experimental autoimmune myasthenia gravis

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Interferon γ (IFN-γ) Is Necessary for the Genesis of Acetylcholine Receptor–induced Clinical Experimental Autoimmune Myasthenia gravis in Mice

Cited by 175 publications

References 44 publications

Blockade of CD40 Ligand Suppresses Chronic Experimental Myasthenia Gravis by Down-Regulation of Th1 Differentiation and Up-Regulation of CTLA-4

Blockade of CD40 Ligand Suppresses Chronic Experimental Myasthenia Gravis by Down-Regulation of Th1 Differentiation and Up-Regulation of CTLA-4

CCL2 recruitment of IL‐6‐producing CD11b+ monocytes to the draining lymph nodes during the initiation of Th17‐dependent B cell‐mediated autoimmunity

Dendritic cells exposed in vitro to TGF-beta1 ameliorate experimental autoimmune myasthenia gravis

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CCL2 recruitment of IL‐6‐producing CD11b⁺ monocytes to the draining lymph nodes during the initiation of Th17‐dependent B cell‐mediated autoimmunity