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Vasorelaxant effect of a newly synthesized dihydropyridine ethyl ester (DHPEE) on rat thoracic aorta: Dual mechanism of action

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APB-1-10.pdf (514.6Kb)
تاریخ
2011
نویسنده
Babaei, H
Ebrahimi, F
Mojarrad, JS
Azarmi, Y
Gharehbagheri, A
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نمایش پرونده کامل آیتم
چکیده
Introduction: DHPEE is a newly synthesized compound by merging the key structural elements in an angiotensin receptor blocker (Telmisartan) with key structural elements in 1,4- dihydropyridine calcium channel blocker (Nifedipine). In this study, we examined dual calcium channel blocking and AT1 antagonist activity for DHPEE. Methods: The functional inhibitory characteristics of DHPEE were studied in vitro in rat thoracic aorta preparations precontracted by phenylephrine (1?M) or KCl (80?M) or Ang II in normal or calcium-free solutions. Results: Concentration-dependent significant relaxation was observed in aortic rings precontracted with phenylephrine, KCl or Ang II. The tension increment produced by increasing external calcium was also reduced by DHPEE. DHPEE caused a marked decrease in the maximal contractile response of the vasoactive agents and shifted their concentration-response curves to the right. Conclusion: DHPEE possesses dual characteristics and cause vasorelaxation by blocking the L-type calcium channels and blocking Ang II receptors (AT1) in rat aortic smooth muscle. ط¢آ© 2011 by Tabriz University of Medical Sciences.
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http://dspace.tbzmed.ac.ir:8080/xmlui/handle/123456789/58693
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