1. Protection against anti-glomerular basement membrane (GBM)-mediated nephritis in C3- and C4-deficient mice.
- Author
-
Sheerin, N. S., Springall, T., Carroll, M. C., Hartley, B., and Sacks, S. H.
- Subjects
KIDNEY diseases ,BIOLOGICAL membranes ,PROTEIN S deficiency ,THROMBOSIS ,BLOOD coagulation ,PROTEINURIA - Abstract
Mice rendered completely deficient of the complement components C3 or C4 were used to determine the influence of complement activation in the heterologous phase of the anti-GBM disease model. In wild-type animals the disease is characterized by a neutrophil infiltrate, capillary thrombosis, proteinuria and C3 and C4 deposited within the glomerulus. The early infiltration of neutrophils into the glomeruli is greater in wild-type mice (2.8 ± 0.3) compared with C3-deficient (1.4 ± 0.2) and C4-deficient (1.2 ± 0.003) mice. Deficiency also protects against the subsequent development of proteinuria (2.99 ± 1.11 mg/24h, 0.059mg/24h and 0.327 ± 0.14mg/24h in wild-type, C3-deficient and C4- deficient mice, respectively) and decreases glomerular capillary thrombosis in both C3- and C4- deficient mice. The degree of protection is greater in the C3-deficient than the C4-deficient animals, suggesting both classical and alternative pathway involvement. These studies support a critical role for complement in the development of anti-GBM disease. However, the protective effect of complement deficiency can be broken if the dose of nephritogenic antibody is increased. [ABSTRACT FROM AUTHOR]
- Published
- 1997
- Full Text
- View/download PDF