早期给予右丙亚胺预防多柔比星诱导的心力衰竭(PHOENIX研究):右丙亚胺诱导拓扑异构酶2b降解的剂量反应和时间进程
Prevention of Heart Failure Induced by Doxorubicin with Early Administration of Dexrazoxane (PHOENIX Study): dose response and time course of dexrazoxane-induced degradation of topoisomerase 2b.
作者信息
Chang Hui-Ming, Hsu Jinn-Yuan, Ahn Chul, Yeh Edward T H
机构信息
Department of Pharmacology and Toxicology, University of Arkansas for Medical Sciences, Little Rock, AR, USA.
Department of Internal Medicine, University of Arkansas for Medical Sciences, Little Rock, Arkansas, USA.
出版信息
Cardiooncology. 2025 May 2;11(1):42. doi: 10.1186/s40959-025-00339-0.
BACKGROUND
Dexrazoxane, a putative iron chelator, is effective in preventing doxorubicin-induced cardiotoxicity. However, dexrazoxane is also a catalytic inhibitor of topoisomerase 2b (Top2b), a key mediator of doxorubicin toxicity. Preclinical studies have shown that dexrazoxane induces Top2b degradation, and early administration (8 h before doxorubicin) can prevent doxorubicin-induced cardiotoxicity. In this study, we investigated the dose-response relationship and time course of dexrazoxane-induced Top2b degradation in human volunteers.
METHODS
Twenty-five healthy female volunteers received an intravenous infusion of dexrazoxane at doses ranging from 100 mg/m to 500 mg/m. Blood samples were collected hourly from time zero to 12 h, as well as at 24- and 48-h post-infusion. Peripheral blood mononuclear cells (PBMCs) were isolated, nuclear fractions were extracted, and Top2b expression was analyzed by western blot using Lamin B1 as a control. A linear mixed-effects model was used to assess differences among the five dose groups.
RESULTS
Dexrazoxane infusion led to a rapid and sustained reduction of Top2b in PBMCs, lasting up to 12 h. Statistical analysis revealed a significant difference in Top2b levels among the five dose groups (p = 0.0002). Subgroup analysis identified a significant difference between the 100 mg/m and 500 mg/m groups (p = 0.005). However, topoisomerase 2a (Top2a), the molecular target of doxorubicin's tumor-killing effect, remained unchanged following dexrazoxane infusion.
CONCLUSIONS
Findings from this dose-response and time-course study can inform the design of future clinical trials investigating the efficacy of early dexrazoxane administration in preventing doxorubicin-induced cardiotoxicity while minimizing the risk of tumor protection.
TRIAL REGISTRATION
(Funded by the National Institute of Health, RO1HL151993; PHOENIX trials, ClinicalTrials.gov number, NCT03930680.).
背景
右丙亚胺是一种公认的铁螯合剂,可有效预防阿霉素诱导的心脏毒性。然而,右丙亚胺也是拓扑异构酶2b(Top2b)的催化抑制剂,而Top2b是阿霉素毒性的关键介质。临床前研究表明,右丙亚胺可诱导Top2b降解,早期给药(阿霉素给药前8小时)可预防阿霉素诱导的心脏毒性。在本研究中,我们调查了右丙亚胺诱导人类志愿者Top2b降解的剂量反应关系和时间进程。
方法
25名健康女性志愿者接受了静脉输注右丙亚胺,剂量范围为100mg/m至500mg/m。从0小时到12小时每小时采集血样,并在输注后24小时和48小时采集。分离外周血单核细胞(PBMC),提取细胞核组分,以Lamin B1为对照,通过蛋白质印迹法分析Top2b表达。使用线性混合效应模型评估五个剂量组之间的差异。
结果
输注右丙亚胺导致PBMC中Top2b迅速且持续降低,持续长达12小时。统计分析显示五个剂量组之间Top2b水平存在显著差异(p = 0.0002)。亚组分析确定100mg/m组和500mg/m组之间存在显著差异(p = 0.005)。然而,阿霉素杀伤肿瘤作用的分子靶点拓扑异构酶2a(Top2a)在输注右丙亚胺后保持不变。
结论
本剂量反应和时间进程研究的结果可为未来临床试验的设计提供参考,该试验旨在研究早期给予右丙亚胺预防阿霉素诱导的心脏毒性的疗效,同时将肿瘤保护风险降至最低。
试验注册
(由美国国立卫生研究院资助,RO1HL151993;PHOENIX试验,ClinicalTrials.gov编号,NCT03930680。)
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