| Literature DB >> 27650733 |
Anissa Moktefi1, Shao-Yu Zhang1, Pauline Vachin1, Virginie Ory1, Carole Henique1, Vincent Audard2, Catherine Rucker-Martin3, Elodie Gouadon3, Michael Eccles4, Andreas Schedl5, Laurence Heidet6, Mario Ollero1, Djillali Sahali7, Andre Pawlak1.
Abstract
The WT1 (Wilm's tumor suppressor) gene is expressed throughout life in podocytes and is essential for the functional integrity of the glomerular filtration barrier. We have previously shown that CMIP (C-Maf inducing protein) is overproduced in podocyte diseases and alters intracellular signaling. Here we isolated the proximal region of the human CMIP promoter and showed by chromatin immunoprecipitation assays and electrophoretic-mobility shift that Wilm's tumor protein (WT1) bound to 2 WT1 response elements, located at positions -290/-274 and -57/-41 relative to transcription start site. Unlike the human CMIP gene, only one Wt1 response element was identified in the mouse Cmip proximal promoter located at position -217/-206. Luciferase reporter assays indicated that WT1 dose-dependently inhibited the transcriptional induction of the CMIP promoter. Transfection of decoy oligonucleotides mimicking the WT1 response elements prevented the inhibition of WT1 on CMIP promoter activity. Furthermore, WT1 silencing promoted Cmip expression. In line with these findings, the abundance of Cmip was early and significantly increased at the transcript and protein level in podocytes displaying a primary defect in Wt1, including Denys-Drash syndrome and Frasier syndrome. Thus, WT1 is a major repressor of the CMIP gene in physiological situations, while conditional deletion of CMIP in the developing kidney did not affect the development of mature glomeruli.Entities:
Keywords: cell signaling; gene expression; kidney development; nephrotic syndrome; podocyte; transcription regulation
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Year: 2016 PMID: 27650733 DOI: 10.1016/j.kint.2016.07.016
Source DB: PubMed Journal: Kidney Int ISSN: 0085-2538 Impact factor: 10.612