Tan Marianne, Xu Richard, Seth Rahul
Department of Pharmacy, Stony Brook University Hospital, Stony Brook, NY 11794-7310, USA.
Curr Med Res Opin. 2004 Jun;20(6):879-82. doi: 10.1185/030079904125003728.
Comparative studies examining the use of oral serotonin type 3 (5-HT(3)) receptor antagonists for the management of acute chemotherapy-induced nausea and vomiting (CINV) are limited. Therefore, we performed an experiential open-label pilot study at Stony Brook Hospital to allow clinicians to make informed formulary decisions at our institution and to stimulate further study. Specifically, the objective of this study was to compare the effectiveness of oral granisetron versus oral dolasetron for prophylaxis of acute CINV.
The study was conducted during the period of 1 February 2001 to 31 March 2001. Patients (n = 26) with lymphoma or malignancies of the lungs, larynx, or uterus undergoing moderately high and highly emetogenic chemotherapy were studied. Patients admitted during February (n = 13) were administered a single oral dose of 100 mg of dolasetron; those admitted in March (n = 13) received a single oral dose of 2mg of granisetron. All patients were administered intravenous dexamethasone 20 mg before the initiation of chemotherapy.
Patients were monitored for at least 24 h by clinicians. The data recorded for each patient included age, sex, the number of episodes of nausea and emesis, the intensity of nausea (when applicable), and the number of doses of rescue antiemetic medication administered (when applicable).
Overall, granisetron provided significantly greater control of acute CINV than dolasetron. More patients treated with granisetron experienced total control of nausea and vomiting (69.2 vs 23.1%, p < 0.05). Fewer granisetron-treated patients experienced emesis (7.7 vs 53.8%, p < 0.05) and nausea (30.8 vs 76.9%, p < 0.05). Of those patients who experienced nausea, intensity was significantly less with granisetron than with dolasetron (p < 0.05). Consequently, a significantly greater proportion of patients treated with dolasetron required a rescue antiemetic and significantly more doses of rescue antiemetics (both p < 0.01).
These data suggest that oral granisetron may demonstrate improved CINV outcomes compared with oral dolasetron in patients undergoing moderately high and highly emetogenic chemotherapy.
关于口服5-羟色胺3(5-HT(3))受体拮抗剂用于治疗急性化疗引起的恶心和呕吐(CINV)的比较研究有限。因此,我们在石溪大学医院进行了一项经验性开放标签试验研究,以便临床医生在我们机构做出明智的处方决定,并促进进一步研究。具体而言,本研究的目的是比较口服格拉司琼与口服多潘立酮预防急性CINV的有效性。
该研究在2001年2月1日至2001年3月31日期间进行。对患有淋巴瘤或肺、喉或子宫恶性肿瘤且正在接受中度高致吐性和高度致吐性化疗的患者(n = 26)进行了研究。2月份入院的患者(n = 13)口服单剂量100mg多潘立酮;3月份入院的患者(n = 13)口服单剂量2mg格拉司琼。所有患者在化疗开始前静脉注射20mg地塞米松。
临床医生对患者进行至少24小时的监测。记录的每位患者的数据包括年龄、性别、恶心和呕吐发作次数、恶心强度(如适用)以及使用的解救止吐药物剂量(如适用)。
总体而言,格拉司琼对急性CINV的控制效果明显优于多潘立酮。接受格拉司琼治疗的患者中,更多患者的恶心和呕吐得到了完全控制(69.2%对23.1%,p < 0.05)。接受格拉司琼治疗的患者呕吐(7.7%对53.8%,p < 0.05)和恶心(30.8%对76.9%,p < 0.05)的发生率更低。在那些经历恶心的患者中,格拉司琼组的恶心强度明显低于多潘立酮组(p < 0.05)。因此,接受多潘立酮治疗的患者中,需要使用解救止吐药的比例明显更高,且使用的解救止吐药剂量也明显更多(均p < 0.01)。
这些数据表明,在接受中度高致吐性和高度致吐性化疗的患者中,口服格拉司琼与口服多潘立酮相比,可能在CINV治疗效果上更优。
Zotero 插件