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The impact of 5-hydroxytryptamine-receptor antagonists on chemotherapy treatment adherence, treatment delay, and nausea and vomiting

机译:5-羟色胺受体拮抗剂对化疗依从性,治疗延迟,恶心和呕吐的影响

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Purpose: To determine the incidence of chemotherapy-induced nausea/vomiting (CINV) and chemotherapy treatment delay and adherence among patients receiving palonosetron versus other 5-hydroxytryptamine receptor antagonist (5-HT3 RA) antiemetics. Materials and methods: This retrospective claims analysis included adults with primary malignancies who initiated treatment consisting of single-day intravenous highly emetogenic chemotherapy (HEC) or moderately EC (MEC) regimens. Treatment delay was defined as a gap in treatment at least twice the National Comprehensive Cancer Network-specified cycle length, specific to each chemotherapy regimen. Treatment adherence was determined by the percentage of patients who received the regimen-specific recommended number of chemotherapy cycles within the recommended time frame. Results: We identified 1,832 palonosetron and 2,387 other 5-HT3 RA (“other”) patients who initiated HEC therapy, and 1,350 palonosetron users and 1,379 patients on other antiemetics who initiated MEC therapy. Fewer patients receiving palonosetron experienced CINV versus other (HEC, 27.5% versus 32.2%, P=0.0011; MEC, 36.1% versus 41.7%, P=0.0026), and fewer treatment delays occurred among patients receiving palonosetron versus other (HEC, 3.2% versus 6.0%, P<0.0001; MEC, 17.0% versus 26.8%, P<0.0001). Compared with the other cohort, patients receiving palonosetron were significantly more adherent to the index chemotherapy regimen with respect to the recommended time frame (HEC, 74.7% versus 69.7%, P=0.0004; MEC, 43.1% versus 37.3%, P=0.0019) and dosage (HEC, 27.3% versus 25.8%, P=0.0004; MEC, 15.0% versus 12.6%, P=0.0019). Conclusion: Palonosetron more effectively reduced occurrence of CINV in patients receiving HEC or MEC compared with other agents in this real-world setting. Additionally, patients receiving palonosetron had better adherence and fewer treatment delays than patients receiving other 5-HT3 RAs.
机译:目的:确定接受帕洛诺司琼与其他5-羟色胺受体拮抗剂(5-HT3 RA)止吐药的患者发生化学诱导的恶心/呕吐(CINV)的发生率以及化学治疗的延迟和依从性。资料和方法:这项回顾性索赔分析包括患有原发性恶性肿瘤的成年人,这些成年人开始接受由单日静脉内高度致癌化疗(HEC)或中度EC(MEC)方案组成的治疗。治疗延迟的定义是针对每种化疗方案,治疗间隔至少是国家综合癌症网络规定的周期长度的两倍。治疗依从性由在建议的时间范围内接受方案特定的建议化疗周期数的患者百分比确定。结果:我们确定了1,832例帕洛诺司琼和2387例开始进行HEC治疗的5-HT3 RA(“其他”)患者,以及1,350例帕洛诺司琼使用者和1,379例开始使用MEC治疗的其他止吐药。接受帕洛诺司琼的患者接受CINV相对于其他患者(HEC,27.5%对32.2%,P = 0.0011; MEC,36.1%对41.7%,P = 0.0026),并且接受帕洛诺司琼与其他药物相比(HEC,3.2%)对比6.0%,P <0.0001; MEC对比17.0%,对比26.8%,P <0.0001)。与其他队列相比,接受帕洛诺司琼的患者在推荐的时间范围内对索引化疗方案的依从性更高(HEC,74.7%对69.7%,P = 0.0004; MEC,43.1%对37.3%,P = 0.0019)和剂量(HEC,27.3%对25.8%,P = 0.0004; MEC,15.0%对12.6%,P = 0.0019)。结论:在这种实际情况下,与其他药物相比,帕洛诺司琼可以更有效地减少接受HEC或MEC的患者中CINV的发生。此外,接受帕洛诺司琼的患者比接受其他5-HT3 RA的患者具有更好的依从性和更少的治疗延迟。

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