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首页> 外文期刊>Journal of bone and mineral research: the official journal of the American Society for Bone and Mineral Research >Poor Vitamin K Status Is Associated With Low Bone Mineral Density and Increased Fracture Risk in End-Stage Renal Disease
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Poor Vitamin K Status Is Associated With Low Bone Mineral Density and Increased Fracture Risk in End-Stage Renal Disease

机译:较差的维生素K状态与低骨矿物密度有关,末期肾病患者的骨折风险增加

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摘要

Chronic kidney disease and osteoporosis are major public health problems associated with an aging population. Vitamin K insufficiency is prevalent among patients with end-stage renal disease (ESRD). Preliminary data indicate that poor vitamin K status may compromise bone health and that increased inflammation may be in the causal pathway. We performed an ancillary analysis of data collected in the frame of prospective observational cohort studies exploring various aspects of bone health in de novo renal transplant recipients to investigate the association between vitamin K status, inflammation, bone mineral density, and incident clinical fractures. Parameters of mineral metabolism (including biointact PTH and FGF23, sclerostin, calcidiol, calcitriol) and inflammation (CRP and IL-6), osteoprotegerin, bone turnover markers (P1NP, BsAP, and TRAP5B), and dephosphorylated-uncarboxylated Matrix Gla Protein (dp-ucMGP) were assessed on blood samples collected immediately prior to kidney transplantation in 468 patients. Areal bone mineral density (aBMD) was measured at the lumbar spine and femoral neck by dual-energy X-ray absorptiometry within 14 days posttransplant. Poor vitamin K status, defined by dp-ucMGP 500 nmol/L, was highly prevalent (90%). High dp-ucMGP levels independently associated with elevated inflammatory markers and low aBMD. No associations were observed between vitamin K status and bone turnover markers. During a median follow-up of 5.1 years, 33 patients sustained a fragility fracture. In Cox-proportional hazards analysis, a dp-ucMGP above median associated with incident fractures, independent of classical determinants, including age, gender, history of fracture, and aBMD (HR 2.21; 95% CI, 1.00 to 4.91; p 0.05). In conclusion, poor vitamin K status associates with inflammation and low aBMD in patients with ESRD and confers an increased risk of incident fractures in de novo renal transplant recipients. (c) 2018 American Society for Bone and Mineral Research.
机译:慢性肾病和骨质疏松症是与老龄化人口相关的主要公共卫生问题。患有终末期肾病(ESRD)的患者中的维生素K不足普遍存在。初步数据表明,较差的维生素K状态可能会损害骨骼健康,并且增加的炎症可能处于因果途径。我们对探讨了预期观察队框架框架中收集的数据进行了辅助分析,探讨了Novo肾移植受者的各个方面,探讨了维生素K状态,炎症,骨密度和事件临床骨折之间的关联。矿物代谢参数(包括生物膜PTH和FGF23,硬化素,钙质,钙质)和炎症(CRP和IL-6),骨盆素,骨周转标记物(P1NP,BSAP和TRAP5B),以及去磷酸化 - 无羧化基质GLA蛋白(DP在468例患者在肾移植之前立即收集的血液样品评估-C -UCMGP。通过在后翻盖14天内通过双能X射线吸收测量在腰椎和股骨颈上测量区域骨矿物密度(ABMD)。由DP-UCMGP&GT定义的维生素K状态较差,500 nmol / L所定义,高度普遍(90%)。高DP-UCMGP水平与炎症标记升高和低ABMD独立相关。在维生素K状态和骨质周转标记之间没有观察到任何关联。在5.1岁的中位随访期间,33名患者持续脆弱骨折。在Cox比例危害分析中,与入射骨折相关的中位数的DP-UCMGP,独立于经典决定因素,包括年龄,性别,骨折病史和ABMD(HR 2.21; 95%CI,1.00至4.91; P <0.05 )。总之,维生素K状况差与ESRD患者的炎症和低ABMD,并赋予De Novo肾移植受者的发生骨折的风险增加。 (c)2018年美国骨骼和矿物学学会。

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