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KCI과 phenylephrine에 의한 대동맥 수축에서 $Ca^{2+}$ 길항제와 protein kinase 억제제들의 비교 효과
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  • KCI과 phenylephrine에 의한 대동맥 수축에서 $Ca^{2+}$ 길항제와 protein kinase 억제제들의 비교 효과
  • Comparative Effects of $Ca^{2+}$ Antagonists and Protein Kinase Inhibitors on Rat Aorta Contraction Induced by KCI and Phenylephrine
저자명
심상수,문성원,이윤혜,이정근,김현준,박진형,이준한,조중형,김창종
간행물명
약학회지
권/호정보
1999년|43권 5호|pp.659-664 (6 pages)
발행정보
대한약학회
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정기간행물|
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이 논문은 한국과학기술정보연구원과 논문 연계를 통해 무료로 제공되는 원문입니다.
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기타언어초록

To investigate the difference of contractile mechanism between KCI and phenylephrine-induced contraction, we observed effects of $Ca^{2+}$ antagonists and protein kinase inhibitors on aorta contraction of rats. Verapamil dose-dependently inhibited the contraction induced by KCI and phenylephrine, the inhibitory effect of verapamil was more potent in KCI-induced contraction than phenylephrine-induced contraction. Econazole and TMB-8 significantly inhibited CKI-induced contraction but did not inhibit phenylephrine-induced contraction. Staurosporine dose-dependently inhibited both KCI and phenylephrine-induced contraction. Genistein and calmodulin antagonists (W-7 and trifluoperazine) also inhibited both contraction in a dose dependent manner. However, the inhibitory effects of genistein and calmodulin antagonists were more potent in phenylephrine-induced contraction than KCI-induced contraction. These results suggest that involvements of $Ca^{2+}$ channel and protein kinase in rat aorta contraction were dependent on agonist causing aorta smooth muscle contraction.