Role of endothelin-converting enzyme in the systemic hemodynamics and regional circulatory effects of proendothelin-1 (1-38) and diaspirin cross-linked hemoglobin in rats.

A Gulati, R Singh, S M Chung, A P Sen
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Abstract

Diaspirin cross-linked hemoglobin (DCLHb) is a promising hemoglobin-based, oxygen-carrying resuscitative solution. DCLHb (400 mg/kg, iv) produces significant cardiovascular effects, along with an increase in plasma endothelin-1 (ET-1) level, when administered to conscious or anesthetized rats. Present studies were performed to determine whether the cardiovascular effects of DCLHb are due to an increase in the conversion of proendothelin-1 (1-38) (proET-1) to ET-1 by endothelin-converting enzyme (ECE). The regional circulatory and systemic hemodynamic effects of proET-1 (20 micrograms/kg, iv) and DCLHb (400 mg/kg, iv) were determined by using a radioactive microsphere technique in control rats and rats pretreated with phosphoramidon (ECE inhibitor). Administration of proET-1 produced an immediate increase in mean arterial pressure (MAP)(52%) and total peripheral resistance (TPR) (55%); stroke volume (SV) and cardiac output were not affected in the initial phase but were decreased subsequently. Heart rate (HR) was not affected after administration of proET-1. A significant increase in blood flow to the heart (39%), brain (46%), kidneys (74%), portal system (40%), and gastrointestinal tract (GIT) (42%) was also observed after administration of proET-1. Vascular resistance was found to be significantly increased in the mesentery and pancreas (168%) and in the musculoskeletal system (147%) and decreased in the kidneys (-11%) after administration of proET-1. Phosphoramidon (4 mg/kg, iv) pretreatment attenuated the increase in MAP and TPR induced by proET-1. Phosphoramidon pretreatment significantly attenuated the proET-1-induced increase in blood flow to the heart, brain, kidneys, portal system, and GIT. The increase in vascular resistance induced by proET-1 in the mesentery and pancreas and in the musculoskeletal system was also attenuated by phosphoramidon. DCLHb increased MAP (63%) and TPR (54%) without affecting HR. DCLHb increased blood flow to the heart (95%), GIT (45%), portal system (43%), and skin (79%) and increased vascular resistance in the musculoskeletal system (58%). In phosphoramidon-treated rats, DCLHb increased MAP (99%), HR (25%), cardiac output (37%), and TPR (60%). DCLHb increased blood flow to the heart (104%), brain (66%), kidneys (49%), GIT (59%), portal system (63%), and skin (100%) when administered to phosphoramidon-treated rats. Phosphoramidon did not attenuate any of the DCLHb-induced cardiovascular effects. It is concluded that proET-1 increases blood flow to various organs and that phosphoramidon, an ECE inhibitor, could block the proET-1-induced increases in regional blood flow.(ABSTRACT TRUNCATED AT 400 WORDS)

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内皮素转换酶在大鼠全身血流动力学中的作用及内皮素-1(1-38)和双阿司匹林交联血红蛋白的局部循环作用。
双阿司匹林交联血红蛋白(DCLHb)是一种很有前途的以血红蛋白为基础的携氧复苏溶液。DCLHb (400mg /kg, iv)对清醒或麻醉大鼠产生显著的心血管作用,同时血浆内皮素-1 (ET-1)水平升高。目前的研究是为了确定DCLHb对心血管的影响是否由于内皮素转换酶(ECE)将内皮素-1 (1-38)(proET-1)转化为ET-1的增加。采用放射性微球法测定proET-1(20微克/千克,iv)和DCLHb(400毫克/千克,iv)对对照大鼠和经ECE抑制剂磷酰胺预处理的大鼠的局部循环和全身血流动力学的影响。给予proET-1可立即增加平均动脉压(MAP)(52%)和总外周阻力(TPR) (55%);卒中容积(SV)和心输出量在初始阶段不受影响,但随后下降。给药后心率(HR)不受影响。在给予proET-1后,还观察到流向心脏(39%)、脑(46%)、肾脏(74%)、门静脉系统(40%)和胃肠道(42%)的血流显著增加。研究发现,在给予proET-1后,肠系膜和胰腺(168%)以及肌肉骨骼系统(147%)的血管阻力显著增加,肾脏(-11%)的血管阻力显著降低。磷酸酰胺(4 mg/kg, iv)预处理可减弱proET-1诱导的MAP和TPR的升高。磷酰胺预处理可显著减弱proet -1诱导的心脏、脑、肾脏、门静脉系统和胃肠道血流量的增加。由proET-1引起的肠系膜、胰腺和肌肉骨骼系统血管阻力的增加也被磷酰胺减弱。DCLHb增加MAP(63%)和TPR(54%),但不影响HR。DCLHb增加了流向心脏(95%)、GIT(45%)、门静脉系统(43%)和皮肤(79%)的血流量,并增加了肌肉骨骼系统的血管阻力(58%)。在磷酰胺处理的大鼠中,DCLHb增加MAP(99%)、HR(25%)、心输出量(37%)和TPR(60%)。DCLHb增加了流向心脏(104%)、大脑(66%)、肾脏(49%)、胃肠道(59%)、门静脉系统(63%)和皮肤(100%)的血流量。磷酰胺没有减弱dclhb诱导的任何心血管效应。由此可见,proET-1增加了各器官的血流量,而ECE抑制剂磷酰胺可以阻断proET-1引起的局部血流量增加。(摘要删节为400字)
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