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降低晚期慢性肾脏病患者接受地舒单抗治疗后发生低钙血症的风险:一项质量改进计划。

Reducing the risk of denosumab-induced hypocalcemia in patients with advanced chronic kidney disease: a quality improvement initiative.

机构信息

Schulich School of Medicine and Dentistry, Western University, London, ON, Canada.

Division of Endocrinology and Metabolism, Western University, London, ON, Canada.

出版信息

Arch Osteoporos. 2023 Nov 21;18(1):138. doi: 10.1007/s11657-023-01341-8.

Abstract

UNLABELLED

Denosumab can improve bone health in advanced kidney disease (CKD) but is associated with hypocalcemia. We created a clinical care pathway focused on the safe provision of denosumab in advanced CKD that reduced the risk of hypocalcemia by 37% at our hospital. Similar pathways could be adopted and tested in other centers.

PURPOSE

There is an increased risk of hypocalcemia with denosumab in advanced chronic kidney disease (CKD). We aimed to reduce the proportion of patients with advanced CKD who experienced denosumab-induced hypocalcemia at our center.

METHODS

We conducted a quality improvement (QI) project of patients with CKD stage 3b or less (i.e., estimated glomerular filtration rate <45 mL/min/1.73m including dialysis) who were part of the Osteoporosis and Bone Disease Program at St. Joseph's Health Care London (Canada) between December 2020 and January 2023. Our intervention was a clinical care pathway which optimized CKD mineral and bone disorder (CKD-MBD) and 25-hydroxyvitamin levels; provided calcium and vitamin D prophylaxis; promoted multidisciplinary communication between bone and kidney specialists; and carefully monitored calcium post-denosumab injection. Our primary outcome measure was the proportion of patients with hypocalcemia (defined by albumin-corrected serum calcium <1.9mmol/L) at 60 days. Process measures included the appropriate provision of calcium and vitamin D prophylaxis. Balance measures included the development of hypercalcemia and hyperphosphatemia following prophylaxis. We used plan-do-see-act cycles to study four tests of change and presented results using descriptive statistics and run charts.

RESULTS

There were 6 patients with advanced CKD treated with denosumab prior to the implementation of our care pathway (March 2015-October 2020; 83% receiving dialysis). At the time of their denosumab injection, 83% were using 500-1000 mg of calcium, and 83% used 1000-2000 IU of vitamin D. Fifty percent developed denosumab-induced hypocalcemia. Following the implementation of our care pathway, 15 patients (40% receiving dialysis) were treated with denosumab. Ninety-three percent received calcium at a daily dose of 350 to 2250 mg and 87% received 1000-2000 IU of vitamin D. Thirteen percent developed denosumab-induced hypocalcemia. There was no hypercalcemia or hyperphosphatemia.

CONCLUSIONS

A clinical care pathway focused on the safe provision of denosumab in advanced CKD reduced the risk of hypocalcemia in patients treated in our hospital. Similar pathways could be adopted and tested in other centers.

摘要

目的

在晚期慢性肾脏病(CKD)中,使用地舒单抗会增加低钙血症的风险。我们旨在降低我院接受地舒单抗治疗的 CKD 晚期患者发生地舒单抗诱导性低钙血症的比例。

方法

我们开展了一项针对加拿大圣约瑟夫医疗保健伦敦(St. Joseph's Health Care London)骨质疏松症和骨病项目中 CKD3b 期或更早期(即估算肾小球滤过率<45ml/min/1.73m,包括透析)患者的质量改进(QI)项目。我们的干预措施是一种临床护理路径,其优化了 CKD 矿物质和骨代谢紊乱(CKD-MBD)及 25-羟维生素 D 水平;提供了钙和维生素 D 预防措施;促进了骨科和肾科专家之间的多学科沟通;并在地舒单抗注射后仔细监测血钙。我们的主要结局指标是 60 天时发生低钙血症(白蛋白校正血清钙<1.9mmol/L)的患者比例。过程指标包括钙和维生素 D 预防措施的合理提供。平衡指标包括预防后发生高钙血症和高磷血症的情况。我们使用计划-执行-检查-行动(PDCA)循环研究了四项变更测试,并使用描述性统计和运行图表展示了结果。

结果

在我们的护理路径实施之前(2015 年 3 月至 2020 年 10 月;83%的患者接受透析),有 6 例晚期 CKD 患者接受了地舒单抗治疗。在接受地舒单抗注射时,83%的患者使用了 500-1000mg 的钙,83%的患者使用了 1000-2000IU 的维生素 D。50%的患者发生了地舒单抗诱导性低钙血症。在实施我们的护理路径后,有 15 例(40%的患者接受透析)患者接受了地舒单抗治疗。93%的患者每日接受 350-2250mg 的钙,87%的患者接受 1000-2000IU 的维生素 D。13%的患者发生了地舒单抗诱导性低钙血症。未发生高钙血症或高磷血症。

结论

一项专注于在晚期 CKD 中安全提供地舒单抗的临床护理路径降低了我院接受治疗的患者发生低钙血症的风险。其他中心可以采用并测试类似的路径。

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