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阿霉素在体内诱导的心脏毒性:自旋捕获剂α-苯基叔丁基硝酮的保护活性

Cardiotoxicity induced by doxorubicin in vivo: protective activity of the spin trap alpha-phenyl-tert-butyl nitrone.

作者信息

Jotti A, Paracchini L, Perletti G, Piccinini F

机构信息

Istituto di Farmacologia, Università di Milano, Italy.

出版信息

Pharmacol Res. 1992 Sep;26(2):143-50. doi: 10.1016/s1043-6618(05)80127-6.

Abstract

The role of free radical generation in the development of the acute cardiotoxicity induced by doxorubicin (DXR) in the rat and the protective activity of anti-radical drugs were investigated in in vivo experiments by evaluating the body weight curve, ECG, contractile performance and coronary flow up to 10 days after DXR. A lipophilic spin trap (alpha-phenyl-tert-butyl nitrone, PBN) was continuously administered at a dose of 0.65 mg/kg every hour for 2 weeks by an intraperitoneal osmotic pump. DXR was administered i.v. at a dose of 9 mg/kg 3 days after beginning the PBN infusion. DXR impaired ECG and body weight gain after 3 days (partly reversible at later times), while contractility and coronary flow were significantly impaired throughout the experimental time. PBN was shown to prevent the DXR-induced alterations of contractility and coronary flow, while ECG was non-significantly improved. The body weight curve was not affected. Since the dose of PBN used does not produce pharmacological effects, the protective activity in rats receiving DXR indicates that free radicals may play a causal role in the acute cardiotoxicity in vivo. The use of suitable spin traps and administration schedules seems to be an interesting approach for the prevention of radical-dependent pathologies.

摘要

通过评估阿霉素(DXR)给药后长达10天的体重曲线、心电图、收缩性能和冠脉血流量,在体内实验中研究了自由基生成在大鼠阿霉素诱导的急性心脏毒性发展中的作用以及抗自由基药物的保护活性。一种亲脂性自旋捕获剂(α-苯基叔丁基硝酮,PBN)通过腹腔内渗透泵以每小时0.65mg/kg的剂量连续给药2周。在开始PBN输注3天后,静脉注射DXR,剂量为9mg/kg。3天后DXR损害了心电图和体重增加(后期部分可逆),而在整个实验期间收缩性和冠脉血流量均受到显著损害。结果表明,PBN可预防DXR诱导的收缩性和冠脉血流量改变,而心电图改善不显著。体重曲线未受影响。由于所用PBN剂量不产生药理作用,接受DXR的大鼠中的保护活性表明自由基可能在体内急性心脏毒性中起因果作用。使用合适的自旋捕获剂和给药方案似乎是预防自由基依赖性病变的一种有趣方法。

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