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Publication : Sjögren's syndrome in the NOD mouse model is an interleukin-4 time-dependent, antibody isotype-specific autoimmune disease.

First Author  Gao J Year  2006
Journal  J Autoimmun Volume  26
Issue  2 Pages  90-103
PubMed ID  16413168 Mgi Jnum  J:105803
Mgi Id  MGI:3616528 Doi  10.1016/j.jaut.2005.11.004
Citation  Gao J, et al. (2006) Sjogren's syndrome in the NOD mouse model is an interleukin-4 time-dependent, antibody isotype-specific autoimmune disease. J Autoimmun 26(2):90-103
abstractText  NOD.B10-H2(b) and NOD/LtJ mice manifest many features of primary and secondary Sjogren's syndrome (SjS), respectively, an autoimmune disease affecting primarily the salivary and lacrimal glands leading to xerostomia (dry mouth) and xerophthalmia (dry eyes). A previous study suggested that the T(H2) cytokine, interleukin (IL)-4, plays an integral role in the development and onset of SjS-like disease in the NOD mouse model. To define further the role of IL-4 in onset of murine SjS-like disease, we have examined two IL4 gene knockout (KO) mouse strains, NOD.IL4(-/-) and NOD.B10-H2(b).IL4(-/-). Unlike NOD.IL4(-/-) mice, NOD.B10-H2(b).IL4(-/-) mice are resistant to development of diabetes. The presence of a dysfunctional IL4 gene did not impede leukocyte infiltration of the salivary glands, yet prevented development of secretory dysfunction. Whereas NOD.B10-H2(b).IL4(-/-) mice exhibited many pathophysiological manifestations of SjS-like disease common to the parental strains, these mice failed to produce anti-muscarinic acetylcholine type-3 receptor (M3R) autoantibodies of the IgG1 isotype. Cytokine mRNA expression profiles and adoptive transfers of T lymphocytes from NOD.B10-H2(b).Gfp mice into NOD.B10-H2(b).IL4(-/-) mice at different ages suggest IL-4 is required during the pre-clinical disease stage (around 12weeks of age) to initiate clinical xerostomia. The results of this study indicate that the failure of NOD.IL4(-/-) and NOD.B10-H2(b).IL4(-/-) mice to synthesize anti-M3R autoantibodies of the IgG1 isotype apparently explains why these mice fail to develop exocrine gland dysfunction, despite exhibiting pre-clinical manifestations of SjS-like disease.
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