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血液透析血管通路功能障碍:细胞与分子视角

Hemodialysis vascular access dysfunction: a cellular and molecular viewpoint.

作者信息

Roy-Chaudhury Prabir, Sukhatme Vikas P, Cheung Alfred K

机构信息

Division of Nephrology, MSB G-251, University of Cincinnati, 231 Albert Sabin Way, Cincinnati, OH 45267-0585.

出版信息

J Am Soc Nephrol. 2006 Apr;17(4):1112-27. doi: 10.1681/ASN.2005050615.

Abstract

Hemodialysis vascular access dysfunction is a major cause of morbidity and hospitalization in the hemodialysis population. The major cause of hemodialysis vascular access dysfunction is venous stenosis as a result of neointimal hyperplasia. Despite the magnitude of the clinical problem, however, there has been a paucity of novel therapeutic interventions in this field. This is in marked contrast to a recent plethora of targeted interventions for the treatment of arterial neointimal hyperplasia after coronary angioplasty. The reasons for this are two-fold. First there has been a relative lack of cellular and molecular research that focuses on venous neointimal hyperplasia in the specific setting of hemodialysis vascular access. Second, there have been inadequate efforts by the nephrology community to translate the recent advances in molecular and interventional cardiology into therapies for hemodialysis vascular access. This review therefore (1) briefly examines the different forms of hemodialysis vascular access that are available, (2) describes the pathology and pathogenesis of hemodialysis vascular access dysfunction in both polytetrafluoroethylene grafts and native arteriovenous fistulae, (3) reviews recent concepts about the pathogenesis of vascular stenosis that could potentially be applied in the setting of hemodialysis vascular access dysfunction, (4) summarizes novel experimental and clinical therapies that could potentially be used in the setting of hemodialysis vascular access dysfunction, and, finally, (5) offers some broad guidelines for future innovative translational and clinical research in this area that hopefully will reduce the huge clinical morbidity and economic costs that are associated with this condition.

摘要

血液透析血管通路功能障碍是血液透析人群发病和住院的主要原因。血液透析血管通路功能障碍的主要原因是内膜增生导致的静脉狭窄。然而,尽管这一临床问题严重,但该领域新的治疗干预措施却很少。这与最近针对冠状动脉血管成形术后动脉内膜增生的大量靶向干预措施形成了鲜明对比。原因有两方面。首先,相对缺乏针对血液透析血管通路特定环境下静脉内膜增生的细胞和分子研究。其次,肾脏病学界在将分子和介入心脏病学的最新进展转化为血液透析血管通路治疗方法方面的努力不足。因此,本综述(1)简要探讨现有的不同形式的血液透析血管通路,(2)描述聚四氟乙烯移植物和天然动静脉内瘘中血液透析血管通路功能障碍的病理和发病机制,(3)回顾可能适用于血液透析血管通路功能障碍的血管狭窄发病机制的最新概念,(4)总结可能用于血液透析血管通路功能障碍的新的实验和临床治疗方法,最后,(5)为该领域未来的创新转化和临床研究提供一些广泛的指导方针,有望减少与这种疾病相关的巨大临床发病率和经济成本。

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