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地塞米松与地塞米松加氢化可的松预防紫杉醇治疗妇科癌症引起的过敏反应的随机对照试验

Randomized, Controlled Trial of Dexamethasone Versus Dexamethasone Plus Hydrocortisone as Prophylaxis for Hypersensitivity Reactions Due to Paclitaxel Treatment for Gynecologic Cancer.

作者信息

Jeerakornpassawat Dhammapoj, Suprasert Prapaporn

机构信息

Division of Gynecologic Oncology, Department of Obstetrics and Gynecology, Faculty of Medicine, Chiang Mai University, Chiang Mai, Thailand.

出版信息

Int J Gynecol Cancer. 2017 Oct;27(8):1794-1801. doi: 10.1097/IGC.0000000000001069.

Abstract

OBJECTIVE

The aim of this study was to assess intravenous hydrocortisone (HCT) added to standard dexamethasone (DXM) prophylaxis for paclitaxel-associated hypersensitivity reactions (HSRs).

METHODS

Paclitaxel naives scheduled for 6 cycles of paclitaxel (plus platinum) were randomized to DXM alone (20 mg intravenously [IV]) versus DXM plus HCT (100 mg IV) as premedication including chlorpheniramine (10 mg IV), diphenhydramine (25 mg orally), and ranitidine (50 mg IV) 30 minutes before infusion. Clinic nurses observed for HSRs. Groups were well balanced for cancer type, stage, drug allergy, chemotherapy naivete, mean age, body mass index, and paclitaxel dose.

RESULTS

The 44 DXM controls underwent 213 cycles and the 42 investigational DXM plus HCT group 192 per protocol cycles. Hypersensitivity reactions were observed among 9 (4.2%) DXM only cycles compared with 1 (0.5%) among DXM plus HCT cycles (P = 0.022). Hypersensitivity reactions occurred in 8 (18%) DXM only patients and in 1 (2.4%) among those correctly receiving DXM plus HCT (P = 0.030). All HSRs occurred in cycles 1 to 3, within 10 to 40 minutes after infusion initiation, and peaked in cycle 2 (5/39) for DXM recipients and in cycle 3 (1/30) for DXM plus HCT. Hypersensitivity reaction severity was grade 1 in 3 DXM only recipients and grade 2 in 6 DXM and 1 DXM plus HCT. A sole grade 3 HSR was in an intention-to-treat DXM-HCT patient, who erroneously received no HCT. Hypersensitivity reaction symptoms were facial flushing (8 episodes), dyspnea (7), palmar rash (1), and transient hypotension (1). Paclitaxel infusion was suspended for treatment of HSRs; in all cases, symptoms mitigated and infusion successfully restarted for the remaining dose.

CONCLUSIONS

Adding HCT to routine DXM prophylaxis significantly decreased paclitaxel HSR frequency.

摘要

目的

本研究旨在评估在标准地塞米松(DXM)预防紫杉醇相关过敏反应(HSR)的基础上添加静脉注射氢化可的松(HCT)的效果。

方法

计划接受6个周期紫杉醇(加铂类)治疗的初治患者被随机分为两组,一组仅接受DXM(静脉注射20 mg),另一组接受DXM加HCT(静脉注射100 mg)作为预处理,同时在输注前30分钟给予氯苯那敏(静脉注射10 mg)、苯海拉明(口服25 mg)和雷尼替丁(静脉注射50 mg)。临床护士观察HSR情况。两组在癌症类型、分期、药物过敏史、化疗初治情况、平均年龄、体重指数和紫杉醇剂量方面均衡良好。

结果

44例DXM对照组患者共接受213个周期治疗,42例接受DXM加HCT的研究组患者按方案共接受192个周期治疗。仅接受DXM的周期中有9例(4.2%)出现过敏反应,而DXM加HCT的周期中仅有1例(0.5%)出现过敏反应(P = 0.022)。仅接受DXM的患者中有8例(18%)出现过敏反应,而正确接受DXM加HCT的患者中仅有1例(2.4%)出现过敏反应(P = 0.030)。所有HSR均发生在第1至3周期,在输注开始后10至40分钟内出现,仅接受DXM的患者在第2周期过敏反应发生率最高(5/39),接受DXM加HCT的患者在第3周期过敏反应发生率最高(1/30)。仅接受DXM的患者中有3例过敏反应严重程度为1级,6例仅接受DXM和1例接受DXM加HCT的患者过敏反应严重程度为2级。唯一1例3级HSR发生在意向性治疗的DXM - HCT组患者中,该患者错误地未接受HCT。过敏反应症状包括面部潮红(8次发作)、呼吸困难(7次)、手掌皮疹(1次)和短暂性低血压(1次)。因HSR暂停紫杉醇输注进行治疗;所有病例中,症状均缓解,剩余剂量的输注成功重启。

结论

在常规DXM预防基础上添加HCT可显著降低紫杉醇HSR的发生率。

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