Cilostazol induces vasorelaxation through the activation of the eNOS/NO/cGMP pathway, prostanoids, AMPK, PKC, potassium channels, and calcium channels

IF 2.5 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Serdar Sahinturk
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引用次数: 0

Abstract

Objective

This study aimed to investigate vasoactive effect mechanisms of cilostazol in rat thoracic aorta.

Materials and methods

The vessel rings prepared from the thoracic aortas of the male rats were placed in the chambers of the isolated tissue bath system. The resting tone was adjusted to 1 g. Following the equilibration phase, potassium chloride or phenylephrine was used to contract the vessel rings. When achieving a steady contraction, cilostazol was applied cumulatively (10−8–10−4 M). In the presence of potassium channel blockers or signaling pathway inhibitors, the same experimental procedure was performed.

Results

Cilostazol exhibited a significant vasorelaxant effect in a concentration-dependent manner (pD2: 5.94 ± 0.94) (p < .001). The vasorelaxant effect level of cilostazol was significantly reduced by the endothelial nitric oxide synthase inhibitor L-NAME (10−4 M), soluble guanylate cyclase inhibitor methylene blue (10 µM), cyclooxygenase 1/2 inhibitor indomethacin (5 µM), adenosine monophosphate-activated protein kinase inhibitor compound C (10 µM), non-selective potassium channel blocker tetraethylammonium chloride (10 mM), large-conductance calcium-activated potassium channel blocker iberiotoxin (20 nM), voltage-gated potassium channel blocker 4-Aminopyridine (1 mM), and inward-rectifier potassium channel blocker BaCl2 (30 µM) (p < .001). Moreover, incubation of cilostazol (10−4 M) significantly reduced caffeine (10 mM), cyclopiazonic acid (10 µM), and phorbol 12-myristate 13-acetate-induced (100 µM) vascular contractions (p < .001).

Conclusions

In the rat thoracic aorta, the vasodilator action level of cilostazol is quite noticeable. The vasorelaxant effects of cilostazol are mediated by the eNOS/NO/cGMP pathway, prostanoids, AMPK pathway, PKC, potassium channels, and calcium channels.

Abstract Image

西洛他唑通过激活eNOS/NO/cGMP途径、前列腺素、AMPK、PKC、钾通道和钙通道诱导血管舒张。
目的:探讨西洛他唑对大鼠胸主动脉的血管活性作用机制。材料和方法:将雄性大鼠胸主动脉制备的血管环置于离体组织浴系统的腔内。将静息音调整为1g。在平衡阶段之后,使用氯化钾或苯肾上腺素来收缩血管环。当达到稳定收缩时,西洛他唑被累计使用(10-8-10-4M)。在钾通道阻断剂或信号通路抑制剂存在的情况下,进行相同的实验程序。结果:西洛他唑(pD2:5.94±0.94)(p-4M)、可溶性鸟苷酸环化酶抑制剂亚甲基蓝(10µM)、环氧合酶1/2抑制剂吲哚美辛(5µM)和腺苷活化蛋白激酶抑制剂化合物C(10µM)具有显著的浓度依赖性血管舒张作用,非选择性钾通道阻滞剂四乙基氯化铵(10mM)、大电导钙激活钾通道阻滞剂伊贝托毒素(20nM)、电压门控钾通道阻滞剂4-氨基吡啶(1mM)和内向整流钾通道阻滞剂BaCl2(30µM),和佛波醇12-肉豆蔻酸13-乙酸酯诱导的(100µM)血管收缩(p结论:在大鼠胸主动脉中,西洛他唑的血管舒张作用水平非常显著。西洛他zol的血管舒张效应由eNOS/NO/cGMP途径、前列腺素、AMPK途径、PKC、钾通道和钙通道介导。
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来源期刊
Prostaglandins & other lipid mediators
Prostaglandins & other lipid mediators 生物-生化与分子生物学
CiteScore
5.80
自引率
3.40%
发文量
49
审稿时长
2 months
期刊介绍: Prostaglandins & Other Lipid Mediators is the original and foremost journal dealing with prostaglandins and related lipid mediator substances. It includes basic and clinical studies related to the pharmacology, physiology, pathology and biochemistry of lipid mediators. Prostaglandins & Other Lipid Mediators invites reports of original research, mini-reviews, reviews, and methods articles in the basic and clinical aspects of all areas of lipid mediator research: cell biology, developmental biology, genetics, molecular biology, chemistry, biochemistry, physiology, pharmacology, endocrinology, biology, the medical sciences, and epidemiology. Prostaglandins & Other Lipid Mediators also accepts proposals for special issue topics. The Editors will make every effort to advise authors of the decision on the submitted manuscript within 3-4 weeks of receipt.
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