Chronic Disease Research Group, Minneapolis Medical Research Foundation, Minneapolis, MN.
Center for Observational Research, Amgen Inc, Thousand Oaks, CA.
Am J Kidney Dis. 2016 Aug;68(2):266-276. doi: 10.1053/j.ajkd.2016.02.038. Epub 2016 Mar 12.
Little is known about epoetin alfa (EPO) dosing at dialysis centers after implementation of the US Medicare prospective payment system and revision of the EPO label in 2011.
Retrospective cohort study.
SETTING & PARTICIPANTS: Approximately 412,000 adult hemodialysis patients with Medicare Parts A and B as primary payer in 2009 to 2012 to describe EPO dosing and hemoglobin patterns; of these, about 70,000 patients clustered in about 1,300 dialysis facilities to evaluate facility-level EPO titration practices and patient-level outcomes in 2012.
Facility EPO titration practices when hemoglobin levels were <10 and >11g/dL (grouped treatment variable) determined from monthly EPO dosing and hemoglobin level patterns.
Patient mean hemoglobin levels, red blood cell transfusion rates, and all-cause and cause-specific hospitalization rates using a facility-based analysis.
Monthly EPO dose and hemoglobin level, red blood cell transfusion rates, and all-cause and cause-specific hospitalization rates.
Monthly EPO doses declined across all hemoglobin levels, with the greatest decline in patients with hemoglobin levels < 10g/dL (July-October 2011). In 2012, nine distinct facility titration practices were identified. Across groups, mean hemoglobin levels differed slightly (10.5-10.8g/dL) but within-patient hemoglobin standard deviations were similar (∼0.68g/dL). Patients at facilities implementing greater dose reductions and smaller dose escalations had lower hemoglobin levels and higher transfusion rates. In contrast, patients at facilities that implemented greater dose escalations (and large or small dose reductions) had higher hemoglobin levels and lower transfusion rates. There were no clinically meaningful differences in all-cause or cause-specific hospitalization events across groups.
Possibly incomplete claims data; excluded small facilities and those without consistent titration patterns; hemoglobin levels reported monthly; inferred facility practice from observed dosing.
Following prospective payment system implementation and labeling revisions, EPO doses declined significantly. Under the new label, facility EPO titration practices were associated with mean hemoglobin levels (but not standard deviations) and transfusion use, but not hospitalization rates.
在美国医疗保险按预定支付制度实施以及 2011 年修订红细胞生成素(EPO)标签后,对于透析中心的 EPO 给药剂量知之甚少。
回顾性队列研究。
2009 年至 2012 年间,约有 412000 名主要由医疗保险 A 部分和 B 部分支付的成年血液透析患者,描述 EPO 剂量和血红蛋白模式;其中,约有 70000 名患者聚集在大约 1300 家透析中心,以评估 2012 年的设施水平 EPO 滴定实践和患者水平的结果。
根据每月 EPO 剂量和血红蛋白水平模式,当血红蛋白水平<10 和>11g/dL 时(分组治疗变量)确定设施 EPO 滴定实践。
使用基于设施的分析,患者平均血红蛋白水平、红细胞输血率以及全因和特定原因的住院率。
每月 EPO 剂量和血红蛋白水平、红细胞输血率以及全因和特定原因的住院率。
所有血红蛋白水平的 EPO 剂量逐月下降,血红蛋白水平<10g/dL 的患者下降最大(2011 年 7 月至 10 月)。2012 年,确定了九种不同的设施滴定实践。在各组之间,平均血红蛋白水平略有不同(10.5-10.8g/dL),但患者内血红蛋白标准差相似(~0.68g/dL)。在实施更大剂量减少和较小剂量增加的设施中,患者的血红蛋白水平较低,输血率较高。相比之下,在实施更大剂量增加(以及较大或较小剂量减少)的设施中,患者的血红蛋白水平较高,输血率较低。各组之间的全因或特定原因的住院事件没有临床意义上的差异。
可能不完整的索赔数据;排除了小设施和没有一致滴定模式的设施;血红蛋白水平按月报告;从观察到的剂量推断设施实践。
在实施按预定支付制度和修订标签后,EPO 剂量显著下降。根据新标签,设施的 EPO 滴定实践与平均血红蛋白水平(但不是标准差)和输血使用相关,但与住院率无关。
