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大内皮素-1在动脉和静脉中加工成血管活性肽。

Big ET-1 processing into vasoactive peptides in arteries and veins.

作者信息

Watts Stephanie W, Thakali Keshari, Smark Chuck, Rondelli Catherine, Fink Gregory D

机构信息

Department of Pharmacology and Toxicology, Michigan State University, East Lansing, MI 48824-1317, USA.

出版信息

Vascul Pharmacol. 2007 Nov-Dec;47(5-6):302-12. doi: 10.1016/j.vph.2007.08.006. Epub 2007 Sep 7.

DOI:10.1016/j.vph.2007.08.006
PMID:17904426
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2719821/
Abstract

The endothelin (ET) peptides are more potent in contracting veins than arteries. The precursor big ET-1 is metabolized by endothelin converting enzyme [ECE; to ET-1 (1-21)], matrix metalloproteases [MMPs; to ET-1 (1-32)] and chymase [to ET-1(1-31)]. We hypothesized that arteries and veins were differently dependent in conversion of big ET-1 to vasoconstrictors. Immunohistochemical, western, zymographic and isometric contractile assays in rat aorta and vena cava were used. Big ET-1 contracted aorta [60+/-17% phenylephrine contraction] but was more efficacious in vena cava [478+/-61% norepinephrine contraction]. ECE and its product ET-1(1-21) were detected in aorta and vena cava, and the ECE inhibitors phosphoramidon and CGS-26393 reduced big ET-1-induced contraction. ET-1 (1-32) contracted aorta and vena cava but inhibition of MMPs with minocycline or GM6001 did not reduce big ET-1-induced contraction; zymography confirmed active tissue MMPs. Aorta and vena cava contracted to the product of chymase, ET-1 (1-31). Chymase was detected in aorta and only weakly in vena cava. Inhibition of chymase (chymostatin, 100 muM) reduced arterial (19% control) but not venous constriction to big ET-1. These results suggest at least one potential significant difference - the role of chymase - in in vitro enzymatic processing of big ET-1 in arteries and veins.

摘要

内皮素(ET)肽类在使静脉收缩方面比动脉更有效。前体大ET-1由内皮素转换酶[ECE;转化为ET-1(1-21)]、基质金属蛋白酶[MMPs;转化为ET-1(1-32)]和糜酶[转化为ET-1(1-31)]代谢。我们推测动脉和静脉在将大ET-1转化为血管收缩剂方面存在不同的依赖性。采用大鼠主动脉和腔静脉的免疫组织化学、蛋白质印迹、酶谱分析和等长收缩试验。大ET-1使主动脉收缩[去氧肾上腺素收缩的60±17%],但在腔静脉中更有效[去甲肾上腺素收缩的478±61%]。在主动脉和腔静脉中检测到ECE及其产物ET-1(1-21),ECE抑制剂磷酰胺素和CGS-26393可减少大ET-1诱导的收缩。ET-1(1-32)使主动脉和腔静脉收缩,但用米诺环素或GM6001抑制MMPs并不能减少大ET-1诱导的收缩;酶谱分析证实组织中有活性MMPs。主动脉和腔静脉对糜酶产物ET-1(1-31)收缩。在主动脉中检测到糜酶,在腔静脉中仅微弱检测到。抑制糜酶(抑糜酶素,100μM)可减少动脉对大ET-1的收缩(对照组的19%),但不减少静脉收缩。这些结果表明,在动脉和静脉中,大ET-1的体外酶促加工过程中至少存在一个潜在的显著差异——糜酶的作用。

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