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给予猴子与乳腺癌治疗剂量相似的阿霉素后出现长期QT间期延长。

Long-term QT prolongation in monkeys after doxorubicin administration at doses similar to breast cancer therapy.

作者信息

Bodziock George M, Meléndez Giselle C

机构信息

Department of Internal Medicine, Section of Cardiovascular Medicine, Cardiac Electrophysiology, Wake Forest University School of Medicine, Winston-Salem, NC, United States.

Department of Pathology, Section on Comparative Medicine, Wake Forest University School of Medicine, Winston-Salem, NC, United States.

出版信息

Front Cardiovasc Med. 2023 Dec 12;10:1247273. doi: 10.3389/fcvm.2023.1247273. eCollection 2023.

Abstract

BACKGROUND

Studies in small animals and human patients have suggested that anthracyclines may prolong cardiac repolarization, or at least inhibit repolarization reserve, predisposing to QT prolongation and dangerous arrhythmias such as Torsades de pointes. This association in humans is difficult to confirm due to multiple confounding variables such as the presence of other medications and concurrent illness.

OBJECTIVES

Identify a long-term association between anthracycline administration and repolarization prolongation in nonhuman primates, which can be measured as prolonged QT/QTc intervals on surface electrocardiogram.

METHODS

Five female African Green monkeys (AGMs) aged 13 ± 1 years received Doxorubicin (Dox) at doses similar to women treated for breast cancer (30-60 mg/m/biweekly IV, total cumulative dose: 240 mg/m) and underwent 12-lead electrocardiogram (ECG) before and 15 weeks after the final dose of Dox treatment. A blinded paired analysis was performed on ECG derived heart rate (HR), QRS, QT and QT corrected for HR (QTc) interval durations.

RESULTS

After Dox, all monkeys exhibited increased QT (BL: 323.2 ± 27.4 ms vs. Post-Dox: 366.4 ± 18.7 ms,  = 0.002) and QTc (BL: 440.2 ± 22.8 ms vs. Post-Dox: 500.8 ± 22.0 ms,  = 0.009) intervals, without any significant changes in HR or QRS duration ( = 0.92 and  = 0.47 respectively).

CONCLUSIONS

AGMs treated with Dox exhibited long-term QT and QTc prolongation, along with the expected cardiotoxicity (LVEF decrease). While similar findings were shown in small animal studies, confounders make human association difficult to prove. Our finding provides a valuable intermediary step, showing direct effect of Dox on repolarization in nonhuman primates.

摘要

背景

对小动物和人类患者的研究表明,蒽环类药物可能会延长心脏复极化时间,或者至少抑制复极化储备,从而导致QT间期延长以及诸如尖端扭转型室速等危险心律失常。由于存在其他药物和并发疾病等多种混杂变量,这种关联在人类中难以证实。

目的

确定在非人类灵长类动物中蒽环类药物给药与复极化延长之间的长期关联,复极化延长可通过体表心电图上QT/QTc间期延长来衡量。

方法

5只年龄为13±1岁的雌性非洲绿猴接受了与乳腺癌治疗女性相似剂量的阿霉素(30-60mg/m²/每两周静脉注射一次,总累积剂量:240mg/m²),并在阿霉素治疗的最后一剂之前和之后15周进行了12导联心电图(ECG)检查。对从ECG得出的心率(HR)、QRS、QT以及校正HR后的QT(QTc)间期持续时间进行了盲法配对分析。

结果

使用阿霉素后,所有猴子的QT(基线:323.2±27.4毫秒,阿霉素治疗后:366.4±18.7毫秒,P=0.002)和QTc(基线:440.2±22.8毫秒,阿霉素治疗后:500.8±22.0毫秒,P=0.009)间期均增加,而HR或QRS持续时间无任何显著变化(分别为P=0.92和P=0.47)。

结论

接受阿霉素治疗的非洲绿猴出现了长期的QT和QTc延长,以及预期的心脏毒性(左心室射血分数降低)。虽然在小动物研究中也有类似发现,但混杂因素使得在人类中的关联难以证明。我们的发现提供了一个有价值的中间步骤,表明了阿霉素对非人类灵长类动物复极化的直接影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/db05/10752656/956bdfbbb712/fcvm-10-1247273-g001.jpg

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