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Selepressin, a new V1A receptor agonist: hemodynamic comparison to vasopressin in dogs.

机译:Selepressin,一个新的V1A受体激动剂:血流动力学相比,抗利尿激素的狗。

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摘要

Selepressin is a new selective vasopressin V1a agonist for treatment of vasodilatory hypotension in shock. Its effect on coronary and aortic blood flow, hemodynamics, and electrocardiogram as an indication of drug safety in healthy dogs was compared with arginine vasopressin (AVP). Eight dogs were fasted, anesthetized, intubated, and ventilated. Following thoracotomy, coronary and aortic blood flows were monitored, left ventricular and peripheral arterial blood pressures were measured, and electrocardiogram was recorded. Selepressin or AVP was administered by dose-escalating infusions (1-300, 0.3-100 ng · kg(-1) · min(-1), respectively). Drug formulation analysis and plasma bioanalysis confirmed exposure. For each dose level, hemodynamic parameters, drug potency, and efficacy were determined. Selepressin and AVP induced a similar increase in mean blood pressure (+13% to 18%), a moderate decrease in aortic blood flow (-40% to 45%), and a slight decrease in coronary blood flow (-16% to 22%). These vasopressors displayed similar hemodynamic characteristics, with peripheral vasoconstriction and decreased aortic blood flow being more pronounced than the increase in coronary resistance and decrease in coronary blood flow. Importantly, selepressin bore no relevant coronary ischemic liability, suggesting that V1a receptor agonists are a potential pharmacological target for treatment of vasodilatory hypotension in shock.
机译:Selepressin是一个新的选择性抗利尿激素V1a受体激动剂用于治疗血管扩张性低血压在冲击。流、血流动力学和心电图作为一个指示的药品安全健康的狗与精氨酸加压素(AVP)。狗是禁食,麻醉,气管插管,通风。主动脉血流量监控,离开了心室和外周动脉血液压力测量和心电图被记录。由dose-escalating注入(-100 1 - 300、0.3 ng·公斤(1)·分钟(1),分别)。分析和等离子体生物分析法证实曝光。参数、药物效力和有效性确定。增加意味着血压(18% + 13%),中度主动脉血流量下降(-40%45%),轻微下降,冠状动脉的血液流(-16%对22%)。类似的血流动力学特征,周边血管收缩和减少主动脉血流量比更明显冠状动脉阻力增加和减少冠状动脉血液流动。无相关冠状动脉缺血性责任,这表明V1a受体受体激动剂是一个潜在的药物治疗的目标血管扩张性休克低血压。

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