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双膦酸盐在血管钙化和骨代谢中的作用:临床概述

Role of Bisphosphonates in Vascular calcification and Bone Metabolism: A Clinical Summary.

作者信息

Dayanand Pradeep, Sandhyavenu Harigopal, Dayanand Sandeep, Martinez Jasmin, Rangaswami Janani

机构信息

Department of Internal Medicine, University of Miami/JFK Medical Center, Atlantis, FL, United States.

Cardiovascular Division, Mayo clinic, Rochester, MN, United States.

出版信息

Curr Cardiol Rev. 2018;14(3):192-199. doi: 10.2174/1573403X14666180619103258.

Abstract

BACKGROUND

Vascular calcification is known to be a strong risk factor for cardiovascular adverse events and mortality. Atherosclerosis, diabetes, aging, abnormal bone mineral homeostasis and high uremic milieu such as chronic kidney disease are major factors that contribute to the progression of vascular calcification. Several mechanisms such as the osteoblastic transition of vascular smooth muscle cells in response to oxidative stress have shed light on the active nature of vascular calcification, which was once thought to be a passive process. The fine interplay of regulatory factors such as PTH, vitamin D3, FGF 23 and klotho reflect the delicate balance between vascular calcification and bone mineralization. Any disturbance affecting this equilibrium of the bonemineral- vascular axis results in accelerated vascular calcification. Bisphosphonates share similar mechanism of action as statins, and hence several studies were undertaken in humans to verify if the benefits proven to be obtained in animal models extended to human models too. This yielded conflicting outcomes which are outlined in this review. This was attributed mainly to inadequate sample size and flaws in the study design. Therefore, this benefit can only be ascertained if studies addressing this are undertaken.

CONCLUSION

This review seeks to highlight the pathophysiologic phenomena implicated in vascular and valvular calcification and summarize the literature available regarding the use of bisphosphonates in animal and human models. We also discuss novel treatment approaches for vascular calcification, with emphasis on chronic kidney disease and calciphylaxis.

摘要

背景

血管钙化是心血管不良事件和死亡的一个重要危险因素。动脉粥样硬化、糖尿病、衰老、骨矿物质稳态异常以及诸如慢性肾脏病等高尿毒症环境是导致血管钙化进展的主要因素。一些机制,如血管平滑肌细胞响应氧化应激而发生成骨细胞转变,揭示了血管钙化的活性本质,血管钙化曾被认为是一个被动过程。甲状旁腺激素(PTH)、维生素D3、成纤维细胞生长因子23(FGF 23)和klotho等调节因子之间的精细相互作用反映了血管钙化与骨矿化之间的微妙平衡。任何影响骨矿物质 - 血管轴这种平衡的干扰都会导致血管钙化加速。双膦酸盐与他汀类药物有相似的作用机制,因此在人体中进行了多项研究,以验证在动物模型中已证实的益处是否也适用于人体模型。这产生了相互矛盾的结果,本综述对此进行了概述。这主要归因于样本量不足和研究设计存在缺陷。因此,只有进行针对此问题的研究才能确定这种益处。

结论

本综述旨在强调血管和瓣膜钙化所涉及的病理生理现象,并总结关于双膦酸盐在动物和人体模型中应用的现有文献。我们还讨论了血管钙化的新型治疗方法,重点是慢性肾脏病和钙化防御。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f044/6131409/f5b8e827f758/CCR-14-192_F1.jpg

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