%0 Generic %A S.N., Verouti %A E.C., Tsilibary %A E., Fragopoulou %A C., Iatrou %A C.A., Demopoulos %A A.S., Charonis %A S.A., Charonis %A G.I., Drossopoulou %D 2017 %T Supplementary Material for: Vitamin D Receptor Activators Upregulate and Rescue Podocalyxin Expression in High Glucose-Treated Human Podocytes %U https://karger.figshare.com/articles/dataset/Supplementary_Material_for_Vitamin_D_Receptor_Activators_Upregulate_and_Rescue_Podocalyxin_Expression_in_High_Glucose-Treated_Human_Podocytes/5468680 %R 10.6084/m9.figshare.5468680.v1 %2 https://karger.figshare.com/ndownloader/files/9457819 %2 https://karger.figshare.com/ndownloader/files/9457822 %2 https://karger.figshare.com/ndownloader/files/9457825 %K Glomerular epithelial cells %K Vitamin D %K Vitamin D receptor %K High glucose %K Podocalyxin %K Diabetic nephropathy %X

Background: Vitamin D is beneficial in human and experimental chronic kidney disease, the leading cause of which is diabetic nephropathy. Vitamin D through its receptor, VDR, provides renal protection in diabetic nephropathy, but limited data exist about its effect on podocytes. Renal podocytes form the main filtration barrier possessing a unique phenotype maintained by proteins including podocalyxin and nephrin, the expression of which is suppressed in pathological conditions. Methods: We used immortalized human podocytes (human glomerular epithelial cells, HGEC) to assess podocalyxin and nephrin expression after treatment with 1,25-dihydroxyvitamin D3 (calcitriol) and its analogue paricalcitol. The involvement of VDR was investigated by silencing with hVDR-siRNA and ChIP analysis. Results: HGEC exhibit high glucose-mediated downregulation of podocalyxin and nephrin, loss of which has been linked with loss of the permselective renal barrier and proteinuria. Calcitriol and paricalcitol reversed high glucose-induced decrease of nephrin and significantly enhanced podocalyxin expression in podocytes cultured in high glucose. HGEC express VDR and retinoid X receptor (RXR). In the presence of calcitriol and paricalcitol, VDR expression was upregulated and VDR colocalized with RXR in the nucleus. VDR knockdown abolished the protective action of calcitriol and paricalcitol on podocalyxin expression indicating that podocalyxin activation of expression is partly mediated by VDR. Furthermore, VDR specifically regulates podocalyxin expression by bounding to a site upstream of the podocalyxin promoter. Conclusion: Vitamin D analogues maintain and, furthermore, re-activate the expression of specialized components of podocytes including podocalyxin, hence they provide protection against loss of the permselective renal barrier, with molecular mechanisms elucidated herein.

%I Karger Publishers