1. Complement and arthritis: another step in understanding
- Author
-
Michael M. Frank and C. Garren Hester
- Subjects
medicine.medical_specialty ,Mice, Inbred MRL lpr ,Immunology ,Arthritis ,urologic and male genital diseases ,Mice ,Rheumatology ,Species Specificity ,immune system diseases ,Internal medicine ,Histocompatibility Antigens ,Immunology and Allergy ,Medicine ,Animals ,Lupus Erythematosus, Systemic ,skin and connective tissue diseases ,Autoimmune disease ,Mice, Knockout ,business.industry ,Binding protein ,Complement C4 ,medicine.disease ,Complement system ,Histocompatibility ,Mice, Inbred C57BL ,Editorial ,Renal pathology ,Alternative complement pathway ,Kidney Diseases ,business - Abstract
Systemic lupus erythematosus is a complement-mediated autoimmune disease. While genetic deficiencies of classical pathway components lead to an increased risk of developing systemic lupus erythematosus, end organ damage is associated with complement activation and immune complex deposition. The role of classical pathway regulators in systemic lupus erythematosus is unknown. C4 binding protein (C4bp) is a major negative regulator of the classical pathway. In order to study the role of C4bp deficiency in an established murine model of lupus nephritis, mice with a targeted deletion in the gene encoding C4bp were backcrossed into the MRL/lpr genetic background. Compared with control MRL/lpr mice, C4bp knockout MLR/lpr mice had similar mortality and similar degrees of lymphoproliferation. There were no differences in the extent of proteinuria or renal inflammation. Staining for complement proteins and immunoglobulins in the kidneys of diseased mice revealed no significant strain differences. Moreover, there was no difference in autoantibody production or in levels of circulating immune complexes. In comparison with C57BL/6 mice, MRL/lpr mice had depressed C4 levels as early as 3 weeks of age. The absence of C4bp did not impact serum C4 levels or alter classical pathway hemolytic activity. Given that immune complex renal injury in the MRL/lpr mouse is independent of Fc receptors as well as the major negative regulator of the classical pathway, new mechanisms for immune-complex-mediated renal injury need to be considered.
- Published
- 2008