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前列环素诱导犬动脉低血压的全身及脑部影响

Systemic and cerebral effects of prostacyclin-induced arterial hypotension in the dog.

作者信息

Boarini D J, Kassell N F, Olin J J, Sprowell J A

出版信息

J Neurosurg. 1984 Jun;60(6):1201-6. doi: 10.3171/jns.1984.60.6.1201.

Abstract

Prostacyclin has strong vasodilating and antiplatelet properties. This study was performed to investigate its potential for producing profound intraoperative hypotension. Five dogs were anesthetized with morphine, nitrous oxide, and oxygen, paralyzed with pancuronium, and ventilated to a PaCO2 of 40 torr. Mean arterial blood pressure (MABP) was lowered to 40 mm Hg with an intravenous infusion of prostacyclin in 0.05 M Tris buffer (average rate of infusion 3 +/- 1 micrograms/kg/min). Blood flow was determined using the radioactive microsphere technique. Measurements were made before and after 20, 40, and 60 minutes of hypotension; and after a 40-minute recovery period. Infusion of prostacyclin reduced MABP 63% while increasing heart rate 51%. Tachyarrhythmias occurred in all dogs, and cardiac index decreased 18%. Myocardial blood flow decreased an average of 29%, cerebral blood flow decreased 30%, cerebellar blood flow decreased 18%, and blood flow in the brain stem and spinal cord was unchanged. Cerebral metabolic rate of oxygen, determined by measuring the oxygen content of the sagittal sinus, was unchanged. Hypotension was easily induced and maintained using prostacyclin, without apparent tachyphylaxis. However, the cardiac changes caused by this drug are more severe than those accompanying hypotension induced by most other agents, and may represent a serious contraindication to its clinical use.

摘要

前列环素具有强大的血管舒张和抗血小板特性。本研究旨在探讨其导致术中严重低血压的可能性。五只犬用吗啡、氧化亚氮和氧气麻醉,泮库溴铵使其麻痹,并通气使动脉血二氧化碳分压(PaCO2)维持在40托。通过静脉输注0.05M三羟甲基氨基甲烷缓冲液中的前列环素(平均输注速率3±1微克/千克/分钟)将平均动脉血压(MABP)降至40毫米汞柱。使用放射性微球技术测定血流量。在低血压20、40和60分钟前后以及40分钟恢复期后进行测量。输注前列环素使MABP降低63%,同时心率增加51%。所有犬均出现快速心律失常,心脏指数降低18%。心肌血流量平均降低29%,脑血流量降低30%,小脑血流量降低18%,脑干和脊髓血流量未改变。通过测量矢状窦氧含量测定的脑氧代谢率未改变。使用前列环素容易诱导并维持低血压,且无明显快速耐受性。然而,该药物引起的心脏变化比大多数其他药物引起的低血压所伴随的变化更为严重,可能是其临床应用的严重禁忌证。

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