Modified scanning electron microscopy reveals pathological crosstalk between endothelial cells and podocytes in a murine model of membranoproliferative glomerulonephritis

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Md. Abdul Masum
Osamu Ichii
Yaser Hosny Ali Elewa
Teppei Nakamura
Yuki Otani
Marina Hosotani
Yasuhiro Kon
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[1] Hokkaido University,Laboratory of Anatomy, Department of Basic Veterinary Sciences, Faculty of Veterinary Medicine
[2] Sher-e-Bangla Agricultural University,Department of Anatomy, Histology and Physiology, Faculty of Animal Science and Veterinary Medicine
[3] Zagazig University,Department of Histology, Faculty of Veterinary Medicine
[4] Section of Biological Safety Research,undefined
[5] Chitose Laboratory,undefined
[6] Food Research Laboratories,undefined
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This study evaluated endothelial cells and podocytes, both being primary components of the glomerular filtration barrier, in the progression of membranoproliferative glomerulonephritis (MPGN) using modified scanning electron microscopy (mSEM) analysis. BXSB/MpJ-Yaa model mice exhibited autoimmune-mediated MPGN characterised by elevated serum autoantibody levels, albuminuria, renal dysfunctional parameters, and decreased glomerular endothelial fenestrations (EF) and podocyte foot process (PFP) effacement with immune cell infiltration. Similar to transmission electron microscopy, mSEM revealed a series of pathological changes in basement membrane and densities of EF and PFP in BXSB/MpJ-Yaa compared with control BXSB/MpJ at different stages. Further, immunopositive area of endothelial marker (CD34), podocyte functional molecules (Nephrin, Podocin, Synaptopodin, and Wilms’ tumour 1 (WT1)), and vascular endothelial growth factor A (VEGF A) significantly decreased in the glomerulus of BXSB/MpJ-Yaa compared with BXSB at final stage. The indices of glomerular endothelial injuries (EF density and immunopositive area of CD34 and VEGF A) and podocyte injuries (PEP density and immunopositive area of podocyte functional molecules) were also significantly correlated with each other and with indices of autoimmune disease and renal dysfunction. Thus, our results elucidated the pathological crosstalk between endothelial cells and podocytes in MPGN progression and the usefulness of mSEM for glomerular pathological analysis.
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