| Literature DB >> 24067439 |
Hassan Izzedine1, Melanie Mangier2, Virginie Ory2, Shao-Yu Zhang2, Kelhia Sendeyo2, Khedidja Bouachi3, Vincent Audard3, Christine Péchoux4, Jean C Soria5, Christophe Massard5, Rastilav Bahleda5, Edward Bourry1, David Khayat6, Alain Baumelou1, Philippe Lang3, Mario Ollero2, Andre Pawlak2, Djillali Sahali3.
Abstract
Renal toxicity constitutes a dose-limiting side effect of anticancer therapies targeting vascular endothelial growth factor (VEGF). In order to study this further, we followed up 29 patients receiving this treatment, who experienced proteinuria, hypertension, and/or renal insufficiency. Eight developed minimal change nephropathy/focal segmental glomerulopathy (MCN/FSG)-like lesions and 13 developed thrombotic microangiopathy (TMA). Patients receiving receptor tyrosine kinase inhibitors (RTKIs) mainly developed MCN/FSG-like lesions, whereas TMA complicated anti-VEGF therapy. There were no mutations in factor H, factor I, or membrane cofactor protein of the complement alternative pathway, while plasma ADAMTS13 activity persisted and anti-ADAMTS13 antibodies were undetectable in patients with TMA. Glomerular VEGF expression was undetectable in TMA and decreased in MCN/FSG. Glomeruli from patients with TMA displayed a high abundance of RelA in endothelial cells and in the podocyte nuclei, but c-mip was not detected. Conversely, MCN/FSG-like lesions exhibited a high abundance of c-mip, whereas RelA was scarcely detected. RelA binds in vivo to the c-mip promoter and prevents its transcriptional activation, whereas RelA knockdown releases c-mip activation. The RTKI sorafenib inhibited RelA activity, which then promoted c-mip expression. Thus, our results suggest that c-mip and RelA define two distinct types of renal damage associated with VEGF-targeted therapies.Entities:
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Year: 2013 PMID: 24067439 DOI: 10.1038/ki.2013.344
Source DB: PubMed Journal: Kidney Int ISSN: 0085-2538 Impact factor: 10.612