Drug research2022,Vol.72Issue(4) :6.DOI:10.1055/a-1766-5491

Carvacrol Enhance Apoptotic Effect of 5-FU on MCF-7 Cell Line via inhibiting P-glycoprotein: An In-silco and In-vitro Study

Vajihe Ghorbanzadeh Karwan Anwar Hassan Aljaf Hunar Mustafa Wasman Lale Pirzeh Saleh Azimi Hassan Dariushnejad
Drug research2022,Vol.72Issue(4) :6.DOI:10.1055/a-1766-5491

Carvacrol Enhance Apoptotic Effect of 5-FU on MCF-7 Cell Line via inhibiting P-glycoprotein: An In-silco and In-vitro Study

Vajihe Ghorbanzadeh 1Karwan Anwar Hassan Aljaf 2Hunar Mustafa Wasman 3Lale Pirzeh 4Saleh Azimi 5Hassan Dariushnejad1
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作者信息

  • 1. Cardiovascular Research Center, Shahid Rahimi Hospital, Lorestan University of Medical Sciences
  • 2. Medical Laboratory Analysis, Cihan University-Sulaimaniya
  • 3. Medical Laboratory Science Department, University of Raparin, Kurdistan Region
  • 4. Institute for Vascular Signaling, Center for Molecular Medicine, Johann Wolfgang Goethe University
  • 5. Razi Herbal Medicines Research Center, Lorestan University of Medical Sciences
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Abstract

Background P-glycoprotein (P-gp), is an ATP-dependent efflux transporter and overexpressed in cancer cells which is responsible for drug resistance and transportation of anticancer agents out of cells. Hence, P-gp inhibition is a promising way to reverse multi-drug resistance, finding a suitable inhibitor is essential. Carvacrol, an active compound of thyme, has been shown anticancer properties in several types of cancers but the mechanisms underlying this effect remain unclear. Here, we evaluated the inhibitory effects of carvacrol on P-gp by In-silco and in-vitro studies. Method carvacrol was docked against P-gp via autodock vina software to identify the potential binding of this agent. Verapamil, a well-known P-gp inhibitor, was selected as the control ligands. Cell proliferation and apoptosis were assessed using MTT assay and ELISA cell death assay, respectively. Results It was observed that carvacrol exhibited appropriate affinity (?7?kcal/mol) to drug binding pocket of P-gp when compared with verapamil that showed binding affinities of ?8?kcal/mol. The result of MTT assay showed a dose-dependent inhibitory effect of carvacrol and 5-FU. Data of apoptosis assay showed that combining carvacrol with 5-FU increased apoptotic effect of 5-FU 6.7-Fold rather than the control group. This ability to enhance apoptosis is more than the combination of verapamil and 5-FU (4.26-Fold). Conclusion These results provide important evidence that carvacrol may be a promising agent able to overcome P-gp-mediated MDR.

Key words

Breast cancer/Carvacrol/Molecular docking/Multi Dug Resistance/P-glycoprotein

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出版年

2022
Drug research

Drug research

ESCI
ISSN:2194-9379
被引量3
参考文献量27
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