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慢性肾脏病中心肾综合征与维生素 D 受体激活

Cardiorenal syndrome and vitamin D receptor activation in chronic kidney disease.

机构信息

Harold Simmons Center for Kidney Disease Research and Epidemiology, Los Angeles Biomedical Research Institute at Harbor-UCLA Medical Center, Torrance, CA, USA; St. John Cardiovascular Reserach Center, Los Angeles Biomedical Research Institute at Harbor-UCLA Medical Center, Torrance, CA, USA.

Harold Simmons Center for Kidney Disease Research and Epidemiology, Los Angeles Biomedical Research Institute at Harbor-UCLA Medical Center, Torrance, CA, USA.

出版信息

Kidney Res Clin Pract. 2012 Mar;31(1):12-25. doi: 10.1016/j.krcp.2011.12.006. Epub 2012 Jan 18.

Abstract

Cardiorenal syndrome (CRS) refers to a constellation of conditions whereby heart and kidney diseases are pathophysiologically connected. For clinical purposes, it would be more appropriate to emphasize the pathophysiological pathways to classify CRS into: (1) hemodynamic, (2) atherosclerotic, (3) uremic, (4) neurohumoral, (5) anemic-hematologic, (6) inflammatory-oxidative, (7) vitamin D receptor (VDR) and/or FGF23-, and (8) multifactorial CRS. In recent years, there have been a preponderance data indicating that vitamin D and VDR play an important role in the combination of renal and cardiac diseases. This review focuses on some important findings about VDR activation and its role in CRS, which exists frequently in chronic kidney disease patients and is a main cause of morbidity and mortality. Pathophysiological pathways related to suboptimal or defective VDR activation may play a role in causing or aggravating CRS. VDR activation using newer agents including vitamin D mimetics (such as paricalcitol and maxacalcitol) are promising agents, which may be related to their selectivity in activating VDR by means of attracting different post-D-complex cofactors. Some, but not all, studies have confirmed the survival advantages of D-mimetics as compared to non-selective VDR activators. Higher doses of D-mimetic per unit of parathyroid hormone (paricalcitol to parathyroid hormone ratio) is associated with greater survival, and the survival advantages of African American dialysis patients could be explained by higher doses of paricalcitol (>10 μg/week). More studies are needed to verify these data and to explore additional avenues for CRS management via modulating VDR pathway.

摘要

心脏肾脏综合征(CRS)是指心脏和肾脏疾病在病理生理学上相互关联的一系列病症。出于临床目的,更适合强调病理生理学途径将 CRS 分类为:(1)血流动力学,(2)动脉粥样硬化,(3)尿毒症,(4)神经激素,(5)贫血血液学,(6)炎症-氧化,(7)维生素 D 受体(VDR)和/或 FGF23-,和(8)多因素 CRS。近年来,有大量数据表明维生素 D 和 VDR 在肾脏和心脏疾病的结合中发挥重要作用。本综述重点介绍了一些关于 VDR 激活及其在 CRS 中的作用的重要发现,CRS 常见于慢性肾脏病患者,是发病率和死亡率的主要原因。与 VDR 激活不足或缺陷相关的病理生理学途径可能在引起或加重 CRS 中发挥作用。使用包括维生素 D 类似物(如帕立骨化醇和麦考钙醇)在内的新型药物激活 VDR 是一种很有前途的方法,这可能与其通过吸引不同的后-D 复合物辅助因子来选择性激活 VDR 有关。一些(但不是全部)研究证实了 D 类似物作为非选择性 VDR 激活剂的生存优势。每单位甲状旁腺激素(帕立骨化醇与甲状旁腺激素的比值)使用更高剂量的 D 类似物与更大的生存相关,并且非洲裔美国透析患者的生存优势可以用更高剂量的帕立骨化醇(>10μg/周)来解释。需要更多的研究来验证这些数据,并通过调节 VDR 途径探索治疗 CRS 的其他途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3052/4715094/6edfd24fe01a/gr1.jpg

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