| Literature DB >> 29716796 |
Daisuke Mori1, Isao Matsui2, Akihiro Shimomura3, Nobuhiro Hashimoto1, Ayumi Matsumoto1, Karin Shimada1, Satoshi Yamaguchi1, Tatsufumi Oka1, Keiichi Kubota1, Sayoko Yonemoto1, Yusuke Sakaguchi4, Atsushi Takahashi1, Yasunori Shintani5, Seiji Takashima5, Yoshitsugu Takabatake1, Takayuki Hamano4, Yoshitaka Isaka1.
Abstract
Protein carbamylation is a posttranslational modification that can occur non-enzymatically in the presence of high concentrations of urea. Although carbamylation is recognized as a prognostic biomarker, the contribution of protein carbamylation to organ dysfunction remains uncertain. Because vascular calcification is common under carbamylation-prone situations, we investigated the effects of carbamylation on this pathologic condition. Protein carbamylation exacerbated the calcification of human vascular smooth muscle cells (hVSMCs) by suppressing the expression of ectonucleotide pyrophosphate/phosphodiesterase 1 (ENPP1), a key enzyme in the generation of pyrophosphate, which is a potent inhibitor of ectopic calcification. Several mitochondrial proteins were carbamylated, although ENPP1 itself was not identified as a carbamylated protein. Rather, protein carbamylation reduced mitochondrial membrane potential and exaggerated mitochondria-derived oxidative stress, which down-regulated ENPP1. The effects of carbamylation on ectopic calcification were abolished in hVSMCs by ENPP1 knockdown, in mitochondrial-DNA-depleted hVSMCs, and in hVSMCs treated with a mitochondria-targeted superoxide scavenger. We also evaluated the carbamylation effects using ex vivo and in vivo models. The tunica media of a patient with end-stage renal disease was carbamylated. Thus, our findings have uncovered a previously unrecognized aspect of uremia-related vascular pathology.Entities:
Keywords: oxidative stress; urea; vascular calcification
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Year: 2018 PMID: 29716796 DOI: 10.1016/j.kint.2018.01.033
Source DB: PubMed Journal: Kidney Int ISSN: 0085-2538 Impact factor: 10.612