Vascular Calcification Is Accelerated by Hyponatremia and Low Osmolality.

IF 7.4 1区医学 Q1 HEMATOLOGY

Arteriosclerosis, Thrombosis, and Vascular Biology Pub Date : 2024-09-01 Epub Date: 2024-07-11 DOI:10.1161/ATVBAHA.123.320069

Shumei Matsueda, Shunsuke Yamada, Kumiko Torisu, Hiromasa Kitamura, Toshiharu Ninomiya, Toshiaki Nakano, Takanari Kitazono

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Abstract

Background: Hyponatremia, frequently observed in patients with chronic kidney disease, is associated with increased cardiovascular morbidity and mortality. Hyponatremia or low osmolality induces oxidative stress and cell death, both of which accelerate vascular calcification (VC), a critical phenotype in patients with chronic kidney disease. Whether hyponatremia or low osmolality plays a role in the pathogenesis of VC is unknown.

Methods: Human vascular smooth muscle cells (VSMCs) and mouse aortic rings were cultured in various osmotic conditions and calcifying medium supplemented with high calcium and phosphate. The effects of low osmolality on phenotypic change and oxidative stress in the cultured VSMCs were examined. Microarray analysis was conducted to determine the main signaling pathway of osmolality-related VC. The transcellular sodium and calcium ions flux across the VSMCs were visualized by live imaging. Furthermore, the effect of osmolality on calciprotein particles (CPPs) was investigated. Associations between arterial intimal calcification and hyponatremia or low osmolality were examined by a cross-sectional study using human autopsy specimens obtained in the Hisayama Study.

Results: Low osmolality exacerbated calcification of the ECM (extracellular matrix) of cultured VSMCs and mouse aortic rings. Oxidative stress and osteogenic differentiation of VSMCs were identified as the underlying mechanisms responsible for low osmolality-induced VC. Microarray analysis showed that low osmolality activated the Rac1 (Ras-related C3 botulinum toxin substrate 1)-Akt (protein kinase B) pathway and reduced NCX1 (Na-Ca exchanger 1) expression. Live imaging showed synchronic calcium ion efflux and sodium ion influx via NCX1 when extracellular sodium ion concentrations were increased. An NCX1 inhibitor promoted calcifying media-induced VC by reducing calcium ion efflux. Furthermore, low osmolality accelerated the generation and maturation steps of CPPs. The cross-sectional study of human autopsy specimens showed that hyponatremia and low osmolality were associated with a greater area of arterial intimal calcification.

Conclusions: Hyponatremia and low osmolality promote VC through multiple cellular processes, including the Rac1-Akt pathway activation.

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低钠血症和低渗透压会加速血管钙化

背景：慢性肾病患者经常出现低钠血症，这与心血管疾病发病率和死亡率的增加有关。低钠血症或低渗透压会诱导氧化应激和细胞死亡，两者都会加速血管钙化（VC），这是慢性肾病患者的一个重要表型。方法：将人血管平滑肌细胞（VSMC）和小鼠主动脉环在不同的渗透压条件和补充了高钙和磷酸盐的钙化培养基中进行培养。研究了低渗透压对培养 VSMC 表型变化和氧化应激的影响。通过芯片分析确定了渗透压相关 VC 的主要信号通路。通过活体成像观察了VSMC的钠离子和钙离子跨细胞通量。此外，还研究了渗透压对钙蛋白颗粒（CPPs）的影响。一项横断面研究利用久山研究中获得的人体尸检标本检验了动脉内膜钙化与低钠血症或低渗透压之间的关系：结果：低渗透压加剧了培养 VSMC 和小鼠主动脉环的 ECM（细胞外基质）的钙化。氧化应激和 VSMC 的成骨分化被认为是低渗透压诱导 VC 的潜在机制。微阵列分析表明，低渗透压激活了 Rac1（Ras 相关 C3 肉毒毒素底物 1）-Akt 通路，并降低了 NCX1（Na-Ca 交换子 1）的表达。实时成像显示，当细胞外钠离子浓度增加时，钙离子通过 NCX1 同步外流，钠离子同步流入。NCX1抑制剂通过减少钙离子外流促进了钙化介质诱导的VC。此外，低渗透压加速了 CPPs 的生成和成熟步骤。对人体尸检标本的横断面研究表明，低钠血症和低渗透压与动脉内膜钙化面积增大有关：结论：低钠血症和低渗透压通过多种细胞过程（包括 Rac1-Akt 通路激活）促进血管钙化。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Arteriosclerosis, Thrombosis, and Vascular Biology 医学-外周血管病

CiteScore

15.60

自引率

2.30%

发文量

337

审稿时长

2-4 weeks

期刊介绍： The journal "Arteriosclerosis, Thrombosis, and Vascular Biology" (ATVB) is a scientific publication that focuses on the fields of vascular biology, atherosclerosis, and thrombosis. It is a peer-reviewed journal that publishes original research articles, reviews, and other scholarly content related to these areas. The journal is published by the American Heart Association (AHA) and the American Stroke Association (ASA). The journal was published bi-monthly until January 1992, after which it transitioned to a monthly publication schedule. The journal is aimed at a professional audience, including academic cardiologists, vascular biologists, physiologists, pharmacologists and hematologists.

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