Summary
A distinct, hitherto unknown renal histopathological appearance, consisting of diffuse thickening of the glomerular basement membrane (GBM) with fine intramembranous electron-dense deposits, was observed in the renal biopsies from three patients with collagen diseases. In each case, proteinuria was mild with normal urinary sediment. On light microscopy there were no particular abnormalities but a mild thickening of the glomerular capillary wall. Immunofluorescence studies revealed faint linear or extremely fine granular IgG deposition along the capillary wall. On electron microscopy, the GBM was diffusely thickened with fine intramembranous electron-dense deposits without spike formation. No other deposits were seen in the glomerulus. These histological features resembled those of membranous glomerulonephritis (MGN), although the possibility of the early change of MGN is excluded by specific findings in these cases. Other GBM-thickening diseases such as diabetic glomerulosclerosis were ruled out clinically and histologically. Our cases have a singular renal histopathology which differs from any of the previously established classifications of glomerular lesions. It may be a specific change associated with some type of collagen disease.
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References
Churg J, Sobin LH (1982) Renal disease — classification and atlas of glomerular diasases. Igaku Shoin, Tokyo New York, pp 54, 223
Couser WG (1985) Mechanisms of glomerular injury in immunecomplex disease. Kidney Int 28:569–583
Couser WG, Salant DJ (1980) In situ immune complex formation and glomerular injury. Kidney Int 17:1–13
Couser WG, Steinmuller DR, Stilmant MM, Salant DJ, Lowenstein LM (1978) Experimental glomerulonephritis in the isolated perfused rat kidney. J Clin Invest 62:1275–1287
Fukuda K, Seino J, Kinoshita Y, Sudo K, Horigome I, Saito T, Furuyama T, Yoshinaga K (1985a) Circulating immune complex like materials which bind to heat inactivated Clq interfere with the Clq solid phase assay for immune complexes. Tohoku J Exp Med 146:449–456
Fukuda K, Seino J, Kinoshita Y, Sudo K, Horigome I, Furuyama T, Yoshinaga K (1985b) Modified anti-C3 immune complex assay which avoids interference by anti-F(ab′)2 antibodies. Tohoku J Exp Med 146:337–347
Makker SP, Moorthy B (1981) In situ immune complex formation in isolated perfused kidney using homologous antibody. Lab Invest 44:1–12
Mannik M (1980) Physicochemical and functional relationships of immune complexes. J Invest Dermatol 74:333–338
Mannik M (1982) Pathophysiology of circulating immune complexes. Arthritis Rheum 25:783–787
Sasaki T, Ishida S, Onodera S, Saito T, Furuyama T, Yoshinaga K (1978) Passive hemagglutination and hemolysis tests for the detection of anti-DNA antibody. J Immunol Methods 22:327–337
Tan EM, Cohen AS, Fries J, Masi T, McShane D, Rothfield NF, Schaller JG (1982) The 1982 revised criteria for the classification of systemic lupus erythematodes. Arthritis Rheum 25:1271–1277
Van Damme BJC, Fleuren GJ, Bakker WW, Vernier RL, Hoedemaeker PJ (1978) Experimental glomerulonephritis in the rat induced by antibodies directed against tubular antigens. IV. Fixed glomerular antigens in the pathogenesis of heterologous immune complex glomerulonephritis. Lab Invest 38:502–510
Zollinger HU, Mihatsch MJ (1978) Renal pathology in biopsy. Springer, Berlin Heidelberg New York, pp 267–269
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Sato, H., Saito, T. & Yoshinaga, K. Intramembranous fine deposit disease associated with collagen disorders: a new morphological entity?. Vichows Archiv A Pathol Anat 420, 447–451 (1992). https://doi.org/10.1007/BF01600517
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DOI: https://doi.org/10.1007/BF01600517