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奥曲肽诱导肝硬化患者局部动脉血管收缩

Local arterial vasoconstriction induced by octreotide in patients with cirrhosis.

作者信息

Chatila R, Ferayorni L, Gupta T, Groszmann R J

机构信息

Section of Digestive Diseases, Yale University School of Medicine, and the Hepatic Hemodynamic Laboratory at the Veterans Administration Medical Center, West Haven, CT 06516, USA.

出版信息

Hepatology. 2000 Mar;31(3):572-6. doi: 10.1002/hep.510310304.

Abstract

Peripheral vasodilation initiates the hyperdynamic circulation in cirrhosis. Somatostatin and its analogues, such as octreotide, have a vasoconstrictive effect in cirrhotic patients and experimental animals with portal hypertension. The exact mechanism of octreotide-induced vasoconstriction remains unknown. To investigate whether octreotide produces vasoconstriction through suppression of vasodilatory peptides, such as glucagon, or through a local effect, we evaluated the effect of an intra-arterial dose on forearm blood flow (FBF), while measuring systemic glucagon levels. FBF was measured in 10 cirrhotic patients by venous occlusion plethysmography. The brachial artery of the nondominant arm was catheterized, and vasoactive drugs were administered: methacholine 4 microg/min; octreotide 20 microg/h, and octreotide 20 microg/h + methacholine 4 microg/min. Each infusion, lasting 5 minutes, was followed by saline for washout. FBF was measured in both arms during the last minute of each infusion and at the end of washout, with the uninfused arm acting as the control. Nitrates and nitrites, octreotide, and glucagon blood levels were determined at baseline and after each infusion. Percent change in flow (%triangle up) was obtained by comparing the flow during drug administration to that during the preceding saline infusion. Saline infusion did not alter FBF, but octreotide infusion resulted in a 34% +/- 7.7 (P <.005) reduction in FBF in the infused arm. FBF in the control arm was unchanged despite a significant decrease in systemic glucagon levels. Methacholine infusion increased FBF around 300%, which was not altered by the concomitant infusion of octreotide. Octreotide has a local vasoconstrictive effect that seems nitric oxide (NO)-independent. Octreotide probably has a facilitating effect over vasoconstrictors increased in chronic liver diseases.

摘要

外周血管舒张引发肝硬化患者的高动力循环。生长抑素及其类似物,如奥曲肽,对肝硬化患者及门静脉高压实验动物具有血管收缩作用。奥曲肽诱导血管收缩的确切机制尚不清楚。为研究奥曲肽是否通过抑制血管舒张肽(如胰高血糖素)或通过局部作用产生血管收缩,我们在测量全身胰高血糖素水平的同时,评估动脉内给药剂量对前臂血流量(FBF)的影响。通过静脉阻断体积描记法在10例肝硬化患者中测量FBF。将非优势臂的肱动脉插管,并给予血管活性药物:乙酰甲胆碱4微克/分钟;奥曲肽20微克/小时,以及奥曲肽20微克/小时 + 乙酰甲胆碱4微克/分钟。每次输注持续5分钟,随后用生理盐水冲洗。在每次输注的最后一分钟及冲洗结束时,测量双臂的FBF,未输注药物的手臂作为对照。在基线及每次输注后测定硝酸盐、亚硝酸盐、奥曲肽和胰高血糖素的血药浓度。通过比较给药期间与前一次生理盐水输注期间的血流量,得出流量变化百分比(%△)。生理盐水输注未改变FBF,但奥曲肽输注使输注臂的FBF降低了34%±7.7(P<.005)。尽管全身胰高血糖素水平显著降低,但对照臂的FBF未改变。乙酰甲胆碱输注使FBF增加约300%,同时输注奥曲肽对此无影响。奥曲肽具有局部血管收缩作用,似乎不依赖一氧化氮(NO)。奥曲肽可能对慢性肝病中增加的血管收缩剂具有促进作用。

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