在体内存在白细胞介素-1β的猪模型中，冠状动脉痉挛并不依赖于细胞内钙库，而是主要由蛋白激酶C介导的途径介导。

Coronary artery spasm does not depend on the intracellular calcium store but is substantially mediated by the protein kinase C-mediated pathway in a swine model with interleukin-1 beta in vivo.

作者信息

Kadokami T, Shimokawa H, Fukumoto Y, Ito A, Takayanagi T, Egashira K, Takeshita A

机构信息

Research Institute of Angiocardiology, Kyushu University School of Medicine, Fuknoka, Japan.

出版信息

Circulation. 1996 Jul 15;94(2):190-6. doi: 10.1161/01.cir.94.2.190.

DOI:10.1161/01.cir.94.2.190

PMID:8674178

Abstract

BACKGROUND

The intracellular mechanism for coronary artery spasm is still unknown. Since the protein kinase C (PKC)-mediated pathway and Ca2+ release from sarcoplasmic reticulum (SR) are important intracellular mechanisms of vascular smooth muscle contraction, we examined the possible role of these two mechanisms in the pathogenesis of coronary spasm in our swine model in vivo.

METHODS AND RESULTS

In 25 pigs, interleukin-1 beta (IL-1 beta) was applied chronically to the coronary arteries from the adventitia to induce an inflammatory/proliferative lesion. Two weeks after the operation, either intracoronary serotonin or histamine repeatedly induced coronary spasm at the IL-1 beta-treated site. At those spastic sites, phorbol-12, 13-dibutyrate, a PKC-activating phorbol ester, also induced coronary spasm, which was blocked by pretreatment with the PKC inhibitors staurosporine and sphingosine. Serotonin- and histamine-induced coronary spasm was also significantly inhibited by pretreatment with staurosporine, sphingosine, or nifedipine (an L-type Ca2+ channel antagonist) but not by ryanodine (an inhibitor of Ca(2+)-induced Ca2+ release from SR) or thapsigargin (an inhibitor of Ca(2+)-ATPase of SR). Bay K 8644 (an L-type Ca2+ channel agonist) also induced coronary spasm at the IL-1 beta-treated site, which was significantly inhibited by pretreatment with staurosporine, sphingosine, and nifedipine. In contrast, coronary vasoconstriction induced by prostaglandin F2 alpha was not affected by pretreatment with staurosporine or sphingosine but was significantly inhibited by pretreatment with ryanodine, thapsigargin, or nifedipine.

CONCLUSIONS

These results suggest that (1) PKC activation largely accounts for the serotonin- and histamine-induced coronary spasm; (2) at the spastic site, the calcium influx through L-type Ca2+ channels may be augmented via the PKC-mediated pathway; and (3) the Ca2+ release from the SR into the cytosol may not play a primary role in coronary spasm.

摘要

背景

冠状动脉痉挛的细胞内机制尚不清楚。由于蛋白激酶C（PKC）介导的途径和肌浆网（SR）释放Ca2+是血管平滑肌收缩的重要细胞内机制，我们在体内猪模型中研究了这两种机制在冠状动脉痉挛发病机制中的可能作用。

方法与结果

在25头猪中，将白细胞介素-1β（IL-1β）从外膜长期应用于冠状动脉以诱导炎症/增殖性病变。术后两周，冠状动脉内注射5-羟色胺或组胺可在IL-1β处理部位反复诱发冠状动脉痉挛。在这些痉挛部位，佛波醇-12,13-二丁酸酯（一种激活PKC的佛波酯）也可诱发冠状动脉痉挛，该作用可被PKC抑制剂星形孢菌素和鞘氨醇预处理所阻断。星形孢菌素、鞘氨醇或硝苯地平（一种L型Ca2+通道拮抗剂）预处理也可显著抑制5-羟色胺和组胺诱发的冠状动脉痉挛，但ryanodine（一种抑制Ca2+诱导的Ca2+从SR释放的抑制剂）或毒胡萝卜素（一种抑制SR的Ca2+ -ATP酶的抑制剂）预处理则无此作用。Bay K 8644（一种L型Ca2+通道激动剂）也可在IL-1β处理部位诱发冠状动脉痉挛，该作用可被星形孢菌素、鞘氨醇和硝苯地平预处理显著抑制。相比之下，前列腺素F2α诱导的冠状动脉收缩不受星形孢菌素或鞘氨醇预处理的影响，但可被ryanodine、毒胡萝卜素或硝苯地平预处理显著抑制。