Glatiramer acetate treatment does not modify the clinical course of (NZB x BXSB)F1 lupus murine model

doi:10.1093/intimm/dxn086

International Immunology Advance Access originally published online on August 6, 2008
International Immunology 2008 20(10):1313-1319; doi:10.1093/intimm/dxn086

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Glatiramer acetate treatment does not modify the clinical course of (NZB x BXSB)F1 lupus murine model

Paula Borel¹, Mahdia Benkhoucha¹^,2, Martin S. Weber³^,4, Scott S. Zamvil³, Marie-Laure Santiago-Raber¹ and Patrice H. Lalive¹^,2

¹ Department of Pathology and Immunology, Faculty of Medicine, University of Geneva, Michel Servet 1, 1211 Geneva 4, Switzerland
² Department of Neurosciences, Division of Neurology, Neuroimmunology Laboratory, University Hospital of Geneva, Geneva, Switzerland
³ Department of Neurology, University of California, San Francisco, CA, USA
⁴ Department of Neurology, Technische Universität München, Munich, Germany

Correspondence to: P. H. Lalive; E-mail: patrice.lalive{at}hcuge.ch

Glatiramer acetate (GA, copolymer-1, Copaxone®), a therapyapproved for treatment of multiple sclerosis (MS), preventsand reverses experimental autoimmune encephalomyelitis, theanimal model of MS. In central nervous system autoimmune disease,GA is thought to act through modulation of antigen-presentingcells, such as monocytes, mediating an antigen-independent T_h2shift and development of FoxP3+ regulatory T cells. Recent reportsindicate that GA may also be effective in models of other autoimmunediseases such as uveoretinitis, inflammatory bowel disease andgraft rejection. To date, the potential effect of GA in lupusanimal models has not been described. (NZB x BXSB)F1, male micebearing Y-linked autoimmune acceleration , is a lupus-pronemouse model which is associated with a monocytosis acceleratingdisease progression. These mice were treated with GA beforedisease onset until death and both mortality rate and biologicalparameters were assessed to investigate whether GA may be beneficialin this spontaneous model of systemic lupus erythematosus. GAexerted no beneficial effect on the median survival after upto 7 months of treatment. Humoral and cellular parameters usedas markers for lupus progression, such as anti-chromatin, anti-double-strandedDNA and anti-erythrocytes antibodies, hematocrit and monocytosis,were similarly unchanged. Our study demonstrates that GA hasno significant effect on the progression of the (NZB x BXSB)F1lupus-prone animal model. These results reinforce the hypothesisthat GA may exert its beneficial effect in some specific autoimmunediseases only.

Keywords: Copaxone®, experimental autoimmune encephalitis, (NZB x BXSB)F1 lupus-prone animal model, systemic lupus erythematosus, Y-chromosome-associated accelerator

Transmitting editor: I. Pecht

Received 7 February 2008, accepted 9 July 2008.

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