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新型一氧化氮供体匹昔多明的心血管效应。麻醉和清醒犬的血流动力学特征及耐受性研究。

Cardiovascular effects of the new nitric oxide donor, pirsidomine. Hemodynamic profile and tolerance studies in anesthetized and conscious dogs.

作者信息

Bohn H, Martorana P A, Schönafinger K

机构信息

Department of Pharmacology, Cassella AG, Frankfurt/Main, Germany.

出版信息

Eur J Pharmacol. 1992 Sep 10;220(1):71-8. doi: 10.1016/0014-2999(92)90013-t.

DOI:10.1016/0014-2999(92)90013-t
PMID:1425982
Abstract

The hemodynamic profile of pirsidomine, a new donor of NO (nitric oxide), was evaluated in dogs. In anesthetized dogs, the intravenous or intraduodenal administration of pirsidomine (0.3-10 mg/kg) decreased dose relatedly the preload and afterload of the heart, total peripheral resistance, cardiac output, left ventricular work and myocardial oxygen consumption. In conscious renal-hypertensive dogs, oral administration of pirsidomine (1.0-10 mg/kg) caused a marked and sustained decrease in systolic blood pressure and left ventricular end-diastolic pressure, which was accompanied by a slight and transient increase in heart rate and contractility. The diastolic blood pressure was affected less than in anesthetized dogs. Similar hemodynamic effects were obtained with M1 (3-(1-(2,6-dimethylpiperidino))-sydnonimine; 0.3-1 mg/kg), the main metabolite of pirsidomine, and with the known NO donor, isosorbide-5-mononitrate (IS-5-MN; 2-10 mg/kg). Tolerance development after repeated administration of pirsidomine and IS-5-MN was also investigated. In anesthetized dogs, repeated intraduodenal administrations of pirsidomine did not attenuate the response whereas tolerance occurred with hemodynamically equieffective doses of IS-5-MN. In conscious dogs, long term oral treatment, three times daily every 8th h for 5 days, revealed tolerance to IS-5-MN, slight or no tolerance to pirsidomine, and no cross-tolerance between the two agents. The results indicate that pirsidomine possesses an antianginal hemodynamic profile similar to that of its main metabolite, M1, and of IS-5-MN. This suggests a common mode of action via the release of NO.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在犬类动物中评估了新型一氧化氮(NO)供体匹西多明的血流动力学特征。在麻醉犬中,静脉内或十二指肠内给予匹西多明(0.3 - 10毫克/千克)可剂量依赖性地降低心脏的前负荷和后负荷、总外周阻力、心输出量、左心室作功以及心肌耗氧量。在清醒的肾性高血压犬中,口服匹西多明(1.0 - 10毫克/千克)可使收缩压和左心室舒张末期压力显著且持续降低,同时伴有心率和收缩力轻微短暂增加。舒张压受到的影响小于麻醉犬。匹西多明的主要代谢产物M1(3 - (1 - (2,6 - 二甲基哌啶基)) - 西多明;0.3 - 1毫克/千克)以及已知的NO供体5 - 单硝酸异山梨酯(IS - 5 - MN;2 - 10毫克/千克)也产生了类似的血流动力学效应。还研究了重复给予匹西多明和IS - 5 - MN后的耐受性发展情况。在麻醉犬中,重复十二指肠内给予匹西多明并未减弱反应,而给予血流动力学等效剂量的IS - 5 - MN则出现了耐受性。在清醒犬中,长期口服治疗,每8小时一次,每日三次,持续5天,结果显示对IS - 5 - MN产生耐受性,对匹西多明耐受性轻微或无耐受性,且两种药物之间无交叉耐受性。结果表明,匹西多明具有与主要代谢产物M1以及IS - 5 - MN相似的抗心绞痛血流动力学特征。这提示通过释放NO存在共同的作用模式。(摘要截短于250字)

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