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Potential Anticancer Effect of Carvacrol Codrugs on Human Glioblastoma Cells. | LitMetric
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Potential Anticancer Effect of Carvacrol Codrugs on Human Glioblastoma Cells.

Ayşenur Yazici Lisa Marinelli Ivana Cacciatore Bugrahan Emsen Piera Eusepi Giuseppe Di Biase Antonio Di Stefano Adil Mardinoğlu Hasan Türkez

Curr Drug Deliv

Department of Medical Biology, Faculty of Medicine, Ataturk University, Erzurum, Turkey.

Published: October 2021

AI Article Synopsis

  • Essential oils, particularly carvacrol (CVC) found in oregano and thyme, show potential as novel anticancer agents, especially against cancers like liver, colon, and lung, but limited research exists on its effect on brain cancers such as Glioblastoma Multiforme (GBM).
  • This study focused on investigating the effect of synthesized CVC codrugs (CVC1-8) on human glioblastoma cells (U87-MG) for the first time, utilizing cell viability assays and gene expression analysis.
  • Findings indicate that CVC3 and CVC8 not only induced cytotoxic effects on glioblastoma cells but also positively modulated key molecular pathways associated with GBM, suggesting their potential as candidates for further research

Article Abstract

Background: Essential oils are considered as promising sources of novel anticancer compounds. Carvacrol (CVC), the major constituent of many aromatic plants including oregano and thymus, is endowed with curative properties on different cancers, including liver, colon, and lung. Little information is available regarding the potential of CVC for the treatment of brain cancers, notably Glioblastoma Multiforme (GBM).

Objective: In this work, we investigated the in vitro effect of CVC codrugs (CVC1-8), synthesized by direct-coupled co-drug strategies, on human glioblastoma cell line (U87-MG) for the first time.

Methods: Cell viability was detected by MTT and LDH assays while expression levels of important genes (such as EGFR, NFKB1A, AKT1, AKT2, and others) associated with GBM and inflammatory pathways were detected by PCR array.

Results: Results showed that CVC1-8 codrugs induced cytotoxicity and positive alterations in molecular responses on U87MG cells. Particularly, important pathways (such as PI3K/PTEN/AKT) involved in the onset and progression of GBM resulted in modulation by CVC3 and CVC8.

Conclusion: Our results suggest that CVC3 and CVC8 could be suitable candidates for further investigation to develop new strategies for the prevention and/or treatment of GBM.

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 Source
http://dx.doi.org/10.2174/1567201817666201027123424DOI Listing

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