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基于HPMA共聚物的阿霉素共轭物的血流动力学效应:清醒大鼠的随机对照和比较光谱研究

Hemodynamic effects of HPMA copolymer based doxorubicin conjugate: A randomized controlled and comparative spectral study in conscious rats.

作者信息

Cheah Hoay Yan, Šarenac Olivera, Arroyo Juan J, Vasić Marko, Lozić Maja, Glumac Sofija, Hoe See Ziau, Hindmarch Charles Colin Thomas, Murphy David, Kiew Lik Voon, Lee Hong Boon, Vicent María J, Chung Lip Yong, Japundžić-Žigon Nina

机构信息

a Department of Pharmacology, Faculty of Medicine , University of Malaya , Kuala Lumpur , Malaysia.

b Institute of Pharmacology, Clinical Pharmacology and Toxicology, Faculty of Medicine , University of Belgrade , Republic of Serbia.

出版信息

Nanotoxicology. 2017 Mar;11(2):210-222. doi: 10.1080/17435390.2017.1285071. Epub 2017 Feb 9.

DOI:10.1080/17435390.2017.1285071
PMID:28098511
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5964453/
Abstract

Conjugation of Doxorubicin (DOX) to N-(2-hydroxypropyl) methylacrylamide copolymer (HPMA) has significantly reduced the DOX-associated cardiotoxicity. However, the reports on the impact of HPMA-DOX conjugates on the cardiovascular system such as blood pressure (BP) and heart rate (HR) were in restrained animals using tail cuff and/or other methods that lacked the resolution and sensitivity. Herein, we employed radiotelemetric-spectral-echocardiography approach to further understand the in vivo cardiovascular hemodynamics and variability post administration of free DOX and HPMA-DOX. Rats implanted with radio-telemetry device were administered intravenously with DOX (5 mg/kg), HPMA-DOX (5 mg DOX equivalent/kg) and HPMA copolymer and subjected to continuous cardiovascular monitoring and echocardiography for 140 days. We found that DOX-treated rats had ruffled fur, reduced body weight (BW) and a low survival rate. Although BP and HR were normal, spectral analysis indicated that their BP and HR variabilities were reduced. All rats exhibited typical signs of cardiotoxicity at histopathology. In contrast, HPMA-DOX rats gained weight over time and survived. Although BP, HR and related variabilities were unaffected, the left ventricular end diastolic volume (EDV) of these rats, as well as of the HPMA copolymer-treated rats, was found increased at the end of observation period. Additionally, HPMA copolymer caused microscopic injury of the heart tissue. All of these suggest the necessity of caution when employing HPMA as carrier for prolonged drug delivery. The current study also indicates the potential of radiotelemetric-spectral-echocardiography approach for improved preclinical cardiovascular risk assessment of polymer-drug conjugate and other nano-sized-drug constructs.

摘要

将阿霉素(DOX)与N-(2-羟丙基)甲基丙烯酰胺共聚物(HPMA)偶联可显著降低与DOX相关的心脏毒性。然而,关于HPMA-DOX偶联物对心血管系统如血压(BP)和心率(HR)影响的报道,是在使用尾袖带和/或其他缺乏分辨率和灵敏度的方法的受限动物中进行的。在此,我们采用无线电遥测-频谱-超声心动图方法,以进一步了解游离DOX和HPMA-DOX给药后体内的心血管血流动力学和变异性。给植入无线电遥测装置的大鼠静脉注射DOX(5 mg/kg)、HPMA-DOX(5 mg DOX当量/kg)和HPMA共聚物,并进行连续140天的心血管监测和超声心动图检查。我们发现,DOX处理的大鼠毛发粗糙、体重减轻(BW)且存活率低。尽管血压和心率正常,但频谱分析表明它们的血压和心率变异性降低。所有大鼠在组织病理学上均表现出典型的心脏毒性迹象。相比之下,HPMA-DOX大鼠随时间体重增加并存活。尽管血压、心率及相关变异性未受影响,但在观察期末发现这些大鼠以及HPMA共聚物处理的大鼠的左心室舒张末期容积(EDV)增加。此外,HPMA共聚物导致心脏组织的微观损伤。所有这些表明,在将HPMA用作延长药物递送的载体时需要谨慎。当前研究还表明,无线电遥测-频谱-超声心动图方法在改善聚合物-药物偶联物和其他纳米尺寸药物构建体的临床前心血管风险评估方面具有潜力。

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