[Cardiovascular calcification and accelerated atherosclerosis in chronic kidney disease].

Mario Cozzolino, Alessandra Butti, Giusy Chiarelli, Lisa Rocca-Rey, Gaia Santagostino, Maurizio Gallieni, Diego Brancaccio
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Abstract

Cardiovascular disease is the first cause of morbidity and mortality in dialysis patients. Hyperphosphatemia and elevated serum calcium-phosphate levels have recently been investigated as inducing factors on extraskeletal calcification in this population. In vitro studies demonstrated that human aortic smooth muscle cells calcify when incubated in a high phosphate medium, where calcium and calcitriol are not changed. Furthermore, the lack of inhibitory proteins, such as fetuin and matrix Gla protein, is a possible main determinant of calcium-phosphate deposition in soft tissues. The classical treatment of hyperphosphatemia and secondary hyperparathyroidism in dialysis patients consists of calcium-based phosphate binders and calcitriol administration. Unfortunately, this "first-generation" therapy is not free of dramatic side effects. New free-calcium and -aluminum phosphate binders, new vitamin D metabolites, and calcimimetics are examples of "second-generation" therapies that may prevent vascular calcification and possibly prevent some of the burden of cardiovascular disease in uremia.

[慢性肾病的心血管钙化和动脉粥样硬化加速]。
心血管疾病是透析患者发病和死亡的首要原因。高磷血症和血清磷酸钙水平升高最近被研究为该人群骨骼外钙化的诱导因素。体外研究表明,人主动脉平滑肌细胞在高磷酸盐培养基中培养时钙化,其中钙和骨化三醇没有改变。此外,缺乏抑制蛋白,如胎蛋白和基质Gla蛋白,可能是软组织中磷酸钙沉积的主要决定因素。透析患者高磷血症和继发性甲状旁腺功能亢进的经典治疗包括钙基磷酸盐结合剂和骨化三醇。不幸的是,这种“第一代”疗法并非没有明显的副作用。新的游离钙和磷酸铝结合剂、新的维生素D代谢物和钙化剂是“第二代”疗法的例子,它们可能预防血管钙化,并可能预防尿毒症中心血管疾病的一些负担。
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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