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评估与静脉单剂量碳酸氢钠相比,在接受大剂量甲氨蝶呤治疗的成年人中,添加乙酰唑胺至口服或静脉碳酸氢钠与静脉碳酸氢钠单药治疗相比作为尿液碱化的影响。

Assessing the impact of adding acetazolamide to oral or intravenous sodium bicarbonate as compared with intravenous bicarbonate monotherapy as urinary alkalinization in adults receiving high-dose methotrexate.

机构信息

University of Georgia College of Pharmacy, Augusta, GA, USA.

Department of Pharmacy, Augusta University Medical Center, 1120 15th Street, HM 104, Augusta, GA, 30912, USA.

出版信息

Support Care Cancer. 2021 Mar;29(3):1527-1534. doi: 10.1007/s00520-020-05646-z. Epub 2020 Jul 28.

Abstract

PURPOSE

High-dose methotrexate (HD-MTX) requires urine alkalinization to pH ≥ 7 for adequate excretion to prevent toxicity. Due to shortages of IV sodium bicarbonate (IV-NaHCO3), few reports have demonstrated utility of oral bicarbonate (PO-NaHCO3); however, the addition of acetazolamide (Acet) has not been well described. Our study compares outcomes between alkalinization methods of IV-NaHCO3 monotherapy versus IV-NaHCO2 + Acet and PO-NaHCO3 + Acet.

METHODS

A single-center, IRB exempt, retrospective review was conducted from Jan 2016 to Sept 2019 of adults receiving HD-MTX ≥ 500 mg/m. The primary outcome was time from start of alkalinization to pH ≥ 7. Secondary outcomes included time from start of alkalinization to initiation of HD-MTX, time to MTX clearance, length of stay (LOS), percentage of urine pH assessments < 7, and incidence of MTX toxicity. Statistical analysis was performed using SAS9.4 with alpha 0.05.

RESULTS

Overall demographics (n = 196 HD-MTX cycles for 55 patients) include a mean age 55 years, HD-MTX dose ~ 5400 mg/m, and 69% with a diagnosis of lymphoma. Adjusting for baseline demographic differences among groups, median time from first dose alkalinization to pH ≥ 7 and to start of HD-MTX was longer for those receiving IV-NaHCO3 (n = 41) vs either IV-NaHCO3 + Acet (n = 70) or PO-NaHCO3 + Acet (n = 76) (p = 0.0001). HD-MTX clearance to a level < 0.1 μmol/L was not improved with the addition of Acet. No difference existed among groups for pH results < 7, LOS, or incidence of MTX toxicity (p > 0.05).

CONCLUSIONS

Addition of Acet to NaHCO3 reduces time to pH ≥ 7 and initiation of HD-MTX but does not appear to improve LOS, MTX toxicities, or time to MTX clearance.

摘要

目的

大剂量甲氨蝶呤(HD-MTX)需要尿液碱化至 pH 值≥7 以充分排泄,以防止毒性。由于静脉注射碳酸氢钠(IV-NaHCO3)短缺,很少有报告表明口服碳酸氢钠(PO-NaHCO3)的效用;然而,乙酰唑胺(Acet)的添加并未得到很好的描述。我们的研究比较了 IV-NaHCO3 单药治疗与 IV-NaHCO2+Acet 和 PO-NaHCO3+Acet 碱化方法的结果。

方法

对 2016 年 1 月至 2019 年 9 月期间接受≥500mg/m 的 HD-MTX 的成年人进行了单中心、IRB 豁免、回顾性研究。主要结局是从碱化开始到 pH 值≥7 的时间。次要结局包括从碱化开始到开始 HD-MTX 的时间、MTX 清除时间、住院时间(LOS)、尿液 pH 值评估<7 的百分比以及 MTX 毒性的发生率。使用 SAS9.4 进行统计分析,α 值为 0.05。

结果

总体人口统计学(n=55 例患者的 196 个 HD-MTX 周期)包括平均年龄 55 岁,HD-MTX 剂量约为 5400mg/m,69%的患者诊断为淋巴瘤。调整组间基线人口统计学差异后,接受 IV-NaHCO3(n=41)的患者从首次碱化到 pH 值≥7 和开始 HD-MTX 的时间中位数长于接受 IV-NaHCO3+Acet(n=70)或 PO-NaHCO3+Acet(n=76)(p=0.0001)。添加 Acet 并未改善 MTX 清除至<0.1μmol/L 的水平。各组之间 pH 值<7、LOS 或 MTX 毒性的发生率无差异(p>0.05)。

结论

在 NaHCO3 中添加 Acet 可缩短 pH 值≥7 和开始 HD-MTX 的时间,但似乎不会改善 LOS、MTX 毒性或 MTX 清除时间。

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