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降低接受大剂量甲氨蝶呤治疗患者尿液碱化阈值的相关结局。

Outcomes Associated with Reducing the Urine Alkalinization Threshold in Patients Receiving High-Dose Methotrexate.

作者信息

Drost Sarah A, Wentzell Jason R, Giguère Pierre, McLurg Darcy L, Sabloff Mitchell, Kanji Salmaan, Nguyen Tiffany T

机构信息

Pharmacy Department, The Ottawa Hospital, Ottawa, Ontario, Canada.

The Ottawa Hospital Research Institute, Ottawa, Ontario, Canada.

出版信息

Pharmacotherapy. 2017 Jun;37(6):684-691. doi: 10.1002/phar.1935. Epub 2017 May 12.

Abstract

STUDY OBJECTIVES

Urine alkalinization increases methotrexate (MTX) solubility and reduces the risk of nephrotoxicity. The objectives of this study were to determine whether a reduction in the urine pH threshold from 8 to 7 in patients receiving high-dose methotrexate (HDMTX) results in a shorter length of hospital stay, delayed MTX clearance, or higher rates of nephrotoxicity; and to determine whether specific factors were associated with prolonged MTX clearance.

DESIGN

Retrospective cohort study.

SETTING

Hematology service of a large university-affiliated teaching hospital in Ottawa, Canada.

PATIENTS

Sixty-five adults with 150 HDMTX exposures who had elective admissions for HDMTX between September 1, 2014, and December 18, 2015, were included. Thirty-four patients (with 79 HDMTX exposures) had their urine alkalinized to a pH of 8 or higher, and 31 patients (with 71 HDMTX exposures) had their urine alkalinized to a pH of 7 or higher, after an institutional change in the urine pH threshold from 8 to 7 was implemented on May 1, 2015.

MEASUREMENTS AND MAIN RESULTS

Data related to patient demographics, urine alkalinization, MTX serum concentration monitoring, hospital length of stay, and renal function were collected retrospectively from patients' electronic health records. Lowering the urine pH threshold from 8 to 7 did not significantly affect hospital length of stay (absolute difference 3.5 hrs, 95% confidence interval -4.0 to 10.9) or clearance of MTX (elimination rate constant 0.058 in the pH of 7 or higher group vs 0.064 in the pH of 8 or higher group, p=0.233). Nephrotoxicity rates were similar between groups (15.5% in the pH of 7 or higher group vs 10.1% in the pH of 8 or higher group, p=0.34). Higher MTX dose and interacting medications (e.g., proton pump inhibitors and sulfonamide antibiotics) were significantly associated with delayed MTX elimination.

CONCLUSION

No significant differences in HDMTX-associated hospital length of stay, MTX clearance, or rates of nephrotoxicity were noted between patients in the urine pH of 7 or higher and 8 or higher groups. Interacting medications and higher MTX dose were associated with delayed MTX elimination, suggesting that a closer review of interacting medications before HDMTX administration may be warranted.

摘要

研究目的

尿液碱化可增加甲氨蝶呤(MTX)的溶解度并降低肾毒性风险。本研究的目的是确定在接受大剂量甲氨蝶呤(HDMTX)治疗的患者中,将尿液pH阈值从8降至7是否会导致住院时间缩短、MTX清除延迟或肾毒性发生率升高;并确定是否有特定因素与MTX清除时间延长相关。

设计

回顾性队列研究。

地点

加拿大渥太华一家大型大学附属医院的血液科。

患者

纳入了65名成年人,他们在2014年9月1日至2015年12月18日期间因HDMTX进行了择期入院治疗,共经历了150次HDMTX暴露。在2015年5月1日机构将尿液pH阈值从8降至7后,34名患者(79次HDMTX暴露)的尿液被碱化至pH值为8或更高,31名患者(71次HDMTX暴露)的尿液被碱化至pH值为7或更高。

测量指标及主要结果

从患者的电子健康记录中回顾性收集了与患者人口统计学、尿液碱化、MTX血清浓度监测、住院时间和肾功能相关的数据。将尿液pH阈值从8降至7对住院时间(绝对差异3.5小时,95%置信区间-4.0至10.9)或MTX清除率(pH值为7或更高组的消除速率常数为0.058,pH值为8或更高组为0.064,p = 0.233)没有显著影响。两组的肾毒性发生率相似(pH值为7或更高组为15.5%,pH值为8或更高组为10.1%,p = 0.34)。较高的MTX剂量和相互作用的药物(如质子泵抑制剂和磺胺类抗生素)与MTX清除延迟显著相关。

结论

尿液pH值为7或更高组与8或更高组的患者在HDMTX相关的住院时间、MTX清除率或肾毒性发生率方面没有显著差异。相互作用的药物和较高的MTX剂量与MTX清除延迟相关,这表明在给予HDMTX之前对相互作用的药物进行更密切的审查可能是必要的。

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