Evolution of renal injury in a chronic model of IgA immune-complex-associated nephropathy

IgA nephropathy (IgAN) is characterized by intense and diffuse IgA mesangial deposits, a variety of histopathological changes and unpredictable clinical course. To elucidate the cause of the discrepancy between the unvariable IgA deposition and the histological picture, we examined the short- and lo...

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Published inNephrology, dialysis, transplantation Vol. 10; no. 11; p. 2035
Main Authors Montinaro, V, Aventaggiato, L, Cavallo, T, Rifai, A
Format Journal Article
LanguageEnglish
Published England 01.11.1995
Subjects
Animals
Antigen-Antibody Complex - immunology
Cell Division
Chronic Disease
Disease Models, Animal
Fluorescent Antibody Technique
Glomerulonephritis, IGA - immunology
Glomerulonephritis, IGA - metabolism
Glomerulonephritis, IGA - pathology
Immunoglobulin A - immunology
Mice
Proteinuria - metabolism
Proteinuria - pathology
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Summary:IgA nephropathy (IgAN) is characterized by intense and diffuse IgA mesangial deposits, a variety of histopathological changes and unpredictable clinical course. To elucidate the cause of the discrepancy between the unvariable IgA deposition and the histological picture, we examined the short- and long-term influence of glomerular IgA immune complexes (IgA-IC) on the progression of renal lesions in experimental IgAN. IgA-IC renal deposits were induced by sequential administration of IgA antiphosphorylcholine and pneumococcal C polysaccharide. Mice treated every other day by three injections (groups A) or nine injections (groups B) were sacrificed 24 h and 1, 4, or 8 weeks (groups 1-4) after cessation of treatment. Group A1 showed segmental glomerular necrosis and thrombosis. Lesions then converted to segmental mesangial proliferation (A2), more pronounced in A3 and minimal in A4. Group B1 showed severe proliferative glomerulonephritis and segmental necrosis. The pattern altered to mesangial expansion with glomerular/interstitial infiltration in B2, milder features in B3 and residual mesangial proliferation in B4. Proteinuria increased progressively during treatment reaching its maximum in group B1, but it returned to near normal levels in group B4. The development of proteinuria paralleled glomerular/interstitial T cell infiltration. These findings demonstrate that renal histopathological alterations observed in experimental IgA nephropathy are sustainable only by continuous deposition of nephritogenic IgA-IC.
ISSN:0931-0509
DOI:10.1093/ndt/10.11.2035