Synthesis and Biological Activity of a Bis-steroid-methanocyclobutanaphthalene- dione Derivative against Ischemia/Reperfusion Injury via Calcium Channel Activation

Author:

Lauro Figueroa-Valverde1,Francisco Diaz-Cedillo2,Marcela Rosas-Nexticapa3,Virginia Mateu-Armand3,Alejandra Garcimarero-Espino E.4,Maria Lopez-Ramos1,Lenin Hau-Heredia1,Yaritza Borges-Ballote1,Jhair Cabrera-Tuz1

Affiliation:

1. Laboratory of Pharmaco-Chemistry at the Faculty of Chemical Biological Sciences of the University Autonomous of Campeche, Av. Agustin Melgar s/n, Col Buenavista C.P.24039 Campeche Cam., Mexico

2. Escuela Nacional de Ciencias Biologicas del Instituto Politecnico Nacional, Prol, Carpio y Plan de Ayala s/n Col. Santo Tomas, D.F. C.P. 11340, Mexico

3. Facultad de Nutricion, Universidad Veracruzana, Medicos y Odontologos s/n, 91010, Xalapa, Veracruz, Mexico

4. Facultad de Medicina, Universidad Veracruzana, Medicos y Odontologos s/n, 91010, Xalapa, Veracruz, Mexico

Abstract

Background: There is some experimental data on the effect exerted by some steroid derivatives against ischemia/reperfusion injury; however, the molecular mechanism is very confusing, perhaps this phenomenon could be due to the protocols used and/or differences in the chemical structure of each one of the steroid derivatives. Objective: The aim of this study was to synthesize a new bis-steroid-methanocyclobutanaphthalene- dione derivative using some tools chemical. Methodology: The biological activity exerted by the bis-steroid-methanocyclobutanaphthalene- dione derivative against ischemia/reperfusion injury was evaluated in an isolated heart model using noradrenaline, milrinone, dobutamine, levosimendan, and Bay-K- 8644 as controls. In addition, other alternative experiments were carried out to evaluate the biological activity induced by the bis-steroid-methanocyclobuta-naphthalene-dione derivative against left ventricular pressure in the absence or presence of nifedipine. Results: The results showed that 1) the bis-steroid-methanocyclobuta-naphthalene-dione derivative significantly decreases the ischemia-reperfusion injury translated as a decrease in the the infarct area in a similar manner to levosimendan drug; 2) both bis-steroidmethanocyclobuta- naphthalene-dione and Bay-K-8644 increase the left ventricular pressure and 3) the biological activity exerted by bis-steroid-methanocyclobuta-naphthalenedione derivative against left ventricular pressure is inhibited by nifedipine. Conclusion: In conclusion, the bis-steroid-methanocyclobuta-naphthalene-dione derivative decreases the area of infarction and increases left ventricle pressure via calcium channels activation; this phenomenon could constitute a new therapy for ischemia/reperfusion injury.

Publisher

Bentham Science Publishers Ltd.

Subject

Pharmacology,General Medicine,Immunology,Immunology and Allergy

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