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Altered steady‐state levels of mrna coding for extracellular matrices in renal tissues of ddy mice, an animal model for iga nephropathy
Author(s) -
Tomino Yasuhiko,
Nakamura Tsukasa,
Ebihara Isao,
Funabiki Kazuhiko,
Yaguchi Yutaka,
Shimizu Masahiko,
Shirato Isao,
Koide Hikaru
Publication year - 1991
Publication title -
journal of clinical laboratory analysis
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.536
H-Index - 50
eISSN - 1098-2825
pISSN - 0887-8013
DOI - 10.1002/jcla.1860050207
Subject(s) - laminin , microbiology and biotechnology , glomerular basement membrane , antiserum , extracellular matrix , basement membrane , complementary dna , type iv collagen , chemistry , renal glomerulus , kidney , messenger rna , extracellular , biology , antibody , endocrinology , proteinuria , glomerulonephritis , immunology , gene , biochemistry
Correlations between the steady‐state mRNA levels of extracellular matrices using specific cDNA probes for the α1 chain of type IV collagen (α1 (IV) chain); laminin A, B1, and B2 chains; and heparan sulfate proteoglycan (HSPG); and glomerular injuries in ddY mice were evaluated. Eight‐, sixteen‐ and forty‐week‐old ddY mice were used in this study. ICR mice of the same age served as control. Extracted total RNA of pooled kidneys was fixed on a filter and then hybridized with the cDNA probes. Renal cryostat sections were incubated with rabbit anti‐mouse type IV collagen, laminin, and HSPG antisera and then stained with FITC‐labeled goat anti‐rabbit IgG antiserum. The sections were also stained with FITC‐labeled goat anti‐mouse IgA, IgM, IgG, and C3 antisera. In light microscopy, the average number of glomerular cells was calculated at each age. Increased expression of extracellular matrices genes for the α1(IV) chain; laminin A, B1, and B2 chains; and HSPG was found in renal tissues of ddY mice. Staining of type IV collagen, laminin, and HSPG was observed in renal tissues of ddY mice at each age. Increased proteinuria in 40‐week‐old ddY mice might be related to the decrease in glomerular basement membrane HSPG which acts as the anionic sites in such areas. Marked proliferation and or expansion of glomerular cells and mesangial matrices were observed in 40 week‐old‐ddY mice. The intensity of IgA and C3 deposits in the glomeruli was parallel to the levels of mRNA for such components. It appears that increased mRNA levels for such matrices coincided with the development of renal injuries in ddY mice. It is concluded that evaluation of steady‐state mRNA levels of the extracellular matrices in renal tissues of ddY mice is useful in determining progressive mechanisms in patients with IgA nephropathy.

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