Early switch from intravenous to oral antibiotic therapy in patients with cancer who have low-risk neutropenic sepsis: the EASI-SWITCH RCT.

IF 3.5 2区医学 Q1 HEALTH CARE SCIENCES & SERVICES

Health technology assessment Pub Date : 2024-03-01 DOI:10.3310/RGTP7112

Vicky Coyle, Caroline Forde, Richard Adams, Ashley Agus, Rosemary Barnes, Ian Chau, Mike Clarke, Annmarie Doran, Margaret Grayson, Danny McAuley, Cliona McDowell, Glenn Phair, Ruth Plummer, Dawn Storey, Anne Thomas, Richard Wilson, Ronan McMullan

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There is variation in practice in timing of switch to oral antibiotics after commencement of empirical intravenous antibiotic therapy.Objectives: To establish the clinical and cost effectiveness of early switch to oral antibiotics in patients with neutropenic sepsis at low risk of infective complications.Design: A randomised, multicentre, open-label, allocation concealed, non-inferiority trial to establish the clinical and cost effectiveness of early oral switch in comparison to standard care.Setting: Nineteen UK oncology centres.Participants: Patients aged 16 years and over receiving systemic anticancer therapy with fever (≥ 38°C), or symptoms and signs of sepsis, and neutropenia (≤ 1.0 × 109/l) within 24 hours of randomisation, with a Multinational Association for Supportive Care in Cancer score of ≥ 21 and receiving intravenous piperacillin/tazobactam or meropenem for < 24 hours were eligible. Patients with acute leukaemia or stem cell transplant were excluded.Intervention: Early switch to oral ciprofloxacin (750 mg twice daily) and co-amoxiclav (625 mg three times daily) within 12-24 hours of starting intravenous antibiotics to complete 5 days treatment in total. Control was standard care, that is, continuation of intravenous antibiotics for at least 48 hours with ongoing treatment at physician discretion.Main outcome measures: Treatment failure, a composite measure assessed at day 14 based on the following criteria: fever persistence or recurrence within 72 hours of starting intravenous antibiotics; escalation from protocolised antibiotics; critical care support or death.Results: The study was closed early due to under-recruitment with 129 patients recruited; hence, a definitive conclusion regarding non-inferiority cannot be made. 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引用次数: 0

Abstract

Background: Neutropenic sepsis is a common complication of systemic anticancer treatment. There is variation in practice in timing of switch to oral antibiotics after commencement of empirical intravenous antibiotic therapy.

Objectives: To establish the clinical and cost effectiveness of early switch to oral antibiotics in patients with neutropenic sepsis at low risk of infective complications.

Design: A randomised, multicentre, open-label, allocation concealed, non-inferiority trial to establish the clinical and cost effectiveness of early oral switch in comparison to standard care.

Setting: Nineteen UK oncology centres.

Participants: Patients aged 16 years and over receiving systemic anticancer therapy with fever (≥ 38°C), or symptoms and signs of sepsis, and neutropenia (≤ 1.0 × 10⁹/l) within 24 hours of randomisation, with a Multinational Association for Supportive Care in Cancer score of ≥ 21 and receiving intravenous piperacillin/tazobactam or meropenem for < 24 hours were eligible. Patients with acute leukaemia or stem cell transplant were excluded.

Intervention: Early switch to oral ciprofloxacin (750 mg twice daily) and co-amoxiclav (625 mg three times daily) within 12-24 hours of starting intravenous antibiotics to complete 5 days treatment in total. Control was standard care, that is, continuation of intravenous antibiotics for at least 48 hours with ongoing treatment at physician discretion.

Main outcome measures: Treatment failure, a composite measure assessed at day 14 based on the following criteria: fever persistence or recurrence within 72 hours of starting intravenous antibiotics; escalation from protocolised antibiotics; critical care support or death.

Results: The study was closed early due to under-recruitment with 129 patients recruited; hence, a definitive conclusion regarding non-inferiority cannot be made. Sixty-five patients were randomised to the early switch arm and 64 to the standard care arm with subsequent intention-to-treat and per-protocol analyses including 125 (intervention n = 61 and control n = 64) and 113 (intervention n = 53 and control n = 60) patients, respectively. In the intention-to-treat population the treatment failure rates were 14.1% in the control group and 24.6% in the intervention group, difference = 10.5% (95% confidence interval 0.11 to 0.22). In the per-protocol population the treatment failure rates were 13.3% and 17.7% in control and intervention groups, respectively; difference = 3.7% (95% confidence interval 0.04 to 0.148). Treatment failure predominantly consisted of persistence or recurrence of fever and/or physician-directed escalation from protocolised antibiotics with no critical care admissions or deaths. The median length of stay was shorter in the intervention group and adverse events reported were similar in both groups. Patients, particularly those with care-giving responsibilities, expressed a preference for early switch. However, differences in health-related quality of life and health resource use were small and not statistically significant.

Conclusions: Non-inferiority for early oral switch could not be proven due to trial under-recruitment. The findings suggest this may be an acceptable treatment strategy for some patients who can adhere to such a treatment regimen and would prefer a potentially reduced duration of hospitalisation while accepting increased risk of treatment failure resulting in re-admission. Further research should explore tools for patient stratification for low-risk de-escalation or ambulatory pathways including use of biomarkers and/or point-of-care rapid microbiological testing as an adjunct to clinical decision-making tools. This could include application to shorter-duration antimicrobial therapy in line with other antimicrobial stewardship studies.

Trial registration: This trial is registered as ISRCTN84288963.

Funding: This award was funded by the National Institute for Health and Care Research (NIHR) Health Technology Assessment programme (NIHR award ref: 13/140/05) and is published in full in Health Technology Assessment; Vol. 28, No. 14. See the NIHR Funding and Awards website for further award information.

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低风险中性粒细胞减少性败血症癌症患者早期从静脉注射转为口服抗生素治疗：EASI-SWITCH RCT。

背景：中性粒细胞败血症是全身抗癌治疗的常见并发症。在开始经验性静脉注射抗生素治疗后，改用口服抗生素的时机在实践中存在差异：目的：确定感染并发症风险较低的中性粒细胞减少性败血症患者早期改用口服抗生素的临床效果和成本效益：设计：一项随机、多中心、开放标签、分配隐藏、非劣效试验，以确定早期口服抗生素与标准治疗相比的临床和成本效益：19家英国肿瘤中心：年龄在16岁及以上、正在接受全身抗癌治疗的患者，随机分组后24小时内出现发热（≥ 38°C）或败血症症状和体征，以及中性粒细胞减少（≤ 1.0 × 109/l），多国癌症支持性治疗协会评分≥ 21分，并正在接受静脉注射哌拉西林/他唑巴坦或美罗培南治疗：在开始静脉注射抗生素的 12-24 小时内，尽早改用口服环丙沙星（750 毫克，每天两次）和共阿莫西林（625 毫克，每天三次），总共完成 5 天的治疗。对照组为标准护理，即继续静脉注射抗生素至少 48 小时，由医生决定是否继续治疗：治疗失败，根据以下标准在第14天进行综合评估：开始静脉注射抗生素后72小时内持续发热或复发；方案抗生素升级；重症监护支持或死亡：该研究因招募人数不足而提前结束，共招募了 129 名患者，因此无法得出非劣效性的明确结论。65名患者被随机分配到早期转换治疗组，64名患者被随机分配到标准护理组，随后进行的意向治疗和按协议分析分别包括125名（干预组n=61，对照组n=64）和113名（干预组n=53，对照组n=60）患者。在意向治疗人群中，对照组的治疗失败率为 14.1%，干预组为 24.6%，差异 = 10.5%（95% 置信区间为 0.11 至 0.22）。在按协议人群中，对照组和干预组的治疗失败率分别为 13.3% 和 17.7%，差异 = 3.7%（95% 置信区间为 0.04 至 0.148）。治疗失败的主要原因是发热持续或复发和/或在医生指导下不再使用方案规定的抗生素，但没有出现重症监护入院或死亡病例。干预组的中位住院时间较短，两组报告的不良事件相似。患者，尤其是有护理责任的患者，表示更倾向于尽早更换抗生素。然而，与健康相关的生活质量和医疗资源使用方面的差异较小，且无统计学意义：结论：由于试验招募不足，无法证明早期口服换药的非劣效性。研究结果表明，对于一些能够坚持这种治疗方案的患者来说，这可能是一种可以接受的治疗策略，他们更愿意选择缩短住院时间，同时接受治疗失败导致再次入院的风险增加。进一步的研究应探索低风险降级或非住院路径的患者分层工具，包括使用生物标志物和/或护理点快速微生物检测作为临床决策工具的辅助工具。这可能包括与其他抗菌药物管理研究一致，应用于持续时间较短的抗菌药物治疗：该试验的注册号为 ISRCTN84288963：该奖项由美国国家健康与护理研究所（NIHR）健康技术评估项目资助（NIHR奖项编号：13/140/05），全文发表于《健康技术评估》（Health Technology Assessment）第28卷第14期。更多奖项信息，请参阅 NIHR Funding and Awards 网站。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Health technology assessment 医学-卫生保健

CiteScore

6.90

自引率

0.00%

发文量

审稿时长

>12 weeks

期刊介绍： Health Technology Assessment (HTA) publishes research information on the effectiveness, costs and broader impact of health technologies for those who use, manage and provide care in the NHS.