慢性肾脏病 5 期患者 2 年皮质骨和小梁骨丢失:生化和临床预测因素。
Two-year cortical and trabecular bone loss in CKD-5D: biochemical and clinical predictors.
机构信息
Division of Nephrology Bone and Mineral Metabolism, University of Kentucky, 800 Rose Street, Room MN 564, Lexington, KY, 40503, USA.
Department of Radiology, University of Kentucky, Lexington, KY, USA.
出版信息
Osteoporos Int. 2018 Jan;29(1):125-134. doi: 10.1007/s00198-017-4228-4. Epub 2017 Oct 9.
UNLABELLED
This prospective two-year study of patients on chronic dialysis measured changes in bone mineral density (BMD). Patients with higher baseline BMD and shorter dialysis vintage lost more bone. Treatment with anti-hypertensives acting on the central nervous system was protective against bone loss. Baseline serum levels of sclerostin and bone-specific alkaline phosphatase predicted bone loss.
INTRODUCTION
This prospective 2-year study of chronic kidney disease on dialysis (CKD-5D) patients assessed trabecular and cortical bone loss at the hip and spine and examined potential demographic, clinical, and serum biochemical predictors of bone loss.
METHODS
Eighty-nine CKD-5D patients had baseline, year 1, and year 2 bone mineral density (BMD) measurements using dual X-ray absorptiometry (DXA) and quantitative computed tomography (QCT); concurrent blood samples were drawn and clinical variables recorded. No study treatments occurred.
RESULTS
The 2-year total hip BMD change was - 5.9% by QCT and - 3.1% by DXA (p < 0.001). Spinal BMD was unchanged. QCT total hip cortical mass and volume decreased (- 7.3 and - 10.0%); trabecular volume increased by 5.9% (ps < 0.001). BMD changes did not vary with age, BMI, race, diabetes, smoking, or exercise. Patients with higher baseline BMD and shorter dialysis vintage lost more bone (p < 0.05). Vitamin D analogs and phosphate binders were not protective against bone loss; cinacalcet was protective by univariate but not by multivariable analysis. CNS-affecting antihypertensives were protective against loss of BMD, cortical mass, cortical volume (ps < 0.05) and trabecular mass (p = 0.007). These effects remained after adjustment. BSAP correlated with changes in BMD, cortical mass, and volume (p < 0.01) as did sclerostin (inversely).
CONCLUSIONS
There was severe cortical bone loss at the hip best recognized by QCT. Patients with shorter dialysis vintage and less pre-existing bone loss lost more bone, while treatment with CNS-acting antihypertensives was protective. BSAP and sclerostin were useful markers of bone loss.
目的
本前瞻性研究对慢性透析患者进行了为期两年的研究,以测量骨矿物质密度(BMD)的变化。基线 BMD 较高和透析时间较短的患者骨丢失更多。作用于中枢神经系统的抗高血压药物治疗对骨丢失具有保护作用。基线血清骨硬化蛋白和骨特异性碱性磷酸酶水平预测骨丢失。
简介
本前瞻性研究对慢性肾脏病 5 期透析(CKD-5D)患者进行了研究,评估了髋部和脊柱的小梁和皮质骨丢失,并检查了潜在的人口统计学、临床和血清生化预测骨丢失的因素。
方法
89 例 CKD-5D 患者使用双能 X 线吸收仪(DXA)和定量计算机断层扫描(QCT)进行了基线、第 1 年和第 2 年的骨矿物质密度(BMD)测量;同时采集血样并记录临床变量。未进行研究治疗。
结果
2 年时,QCT 全髋关节 BMD 变化为-5.9%,DXA 为-3.1%(p<0.001)。脊柱 BMD 无变化。QCT 全髋关节皮质骨质量和体积减少(-7.3%和-10.0%);小梁体积增加 5.9%(p<0.001)。BMD 变化与年龄、BMI、种族、糖尿病、吸烟或运动无关。基线 BMD 较高和透析时间较短的患者骨丢失更多(p<0.05)。维生素 D 类似物和磷酸盐结合剂不能预防骨丢失;西那卡塞通过单变量分析有保护作用,但多变量分析没有。作用于中枢神经系统的降压药对 BMD、皮质骨质量、皮质骨体积(p<0.05)和小梁骨质量(p=0.007)的丢失具有保护作用。这些作用在调整后仍然存在。BSAP 与 BMD、皮质骨质量和体积的变化相关(p<0.01),而骨硬化蛋白则相反。
结论
髋部有严重的皮质骨丢失,最好通过 QCT 来识别。透析时间较短、基础骨丢失较少的患者骨丢失更多,而使用作用于中枢神经系统的降压药治疗具有保护作用。BSAP 和骨硬化蛋白是骨丢失的有用标志物。
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