Design and synthesis of novel caffeic acid phenethyl ester (CAPE) derivatives and their biological activity studies in glioblastoma multiforme (GBM) cancer cell lines

Bilgesu Onur Sucu; Elif Beyza Koc; Ozgecan Savlug Ipek; Afranur Mirat; Furkan Almas; Melike Aybala Guzel; Berna Dogan; Damla Uludag; Nihal Karakas; Serdar Durdagi; Mustafa Guzel

doi:10.1016/j.jmgm.2022.108160

Design and synthesis of novel caffeic acid phenethyl ester (CAPE) derivatives and their biological activity studies in glioblastoma multiforme (GBM) cancer cell lines

J Mol Graph Model. 2022 Jun:113:108160. doi: 10.1016/j.jmgm.2022.108160. Epub 2022 Feb 20.

Authors

Affiliations

¹ Istanbul Medipol University, Research Institute for Health Sciences and Technologies SABITA, Center of Drug Discovery and Development, Istanbul, Turkey; Istanbul Medipol University, Vocational School of Health Services, Department of Medical Services and Techniques, Istanbul, Turkey.
² Istanbul Medipol University, Research Institute for Health Sciences and Technologies SABITA, Center of Drug Discovery and Development, Istanbul, Turkey; Istanbul Medipol University, Health Sciences Institute, Department of Molecular Medicine and Biotechnology, Istanbul, Turkey.
³ Istanbul Medipol University, Research Institute for Health Sciences and Technologies SABITA, Center of Drug Discovery and Development, Istanbul, Turkey; Yildiz Technical University, Department of Chemistry, Faculty of Arts and Sciences, Istanbul, Turkey.
⁴ Istanbul Medipol University, Research Institute for Health Sciences and Technologies SABITA, Center of Drug Discovery and Development, Istanbul, Turkey.
⁵ Bahcesehir University, School of Medicine, Department of Biochemistry, Istanbul, Turkey.
⁶ Istanbul Medipol University, Research Institute for Health Sciences and Technologies SABITA, Cancer Research Center, Istanbul, Turkey.
⁷ Istanbul Medipol University, Research Institute for Health Sciences and Technologies SABITA, Cancer Research Center, Istanbul, Turkey; Istanbul Medipol University, School of Medicine, Department of Medical Biology, Istanbul, Turkey.
⁸ Bahcesehir University, School of Medicine, Department of Biophysics, Computational Biology and Molecular Simulations Laboratory, Istanbul, Turkey.
⁹ Istanbul Medipol University, Research Institute for Health Sciences and Technologies SABITA, Center of Drug Discovery and Development, Istanbul, Turkey; Istanbul Medipol University, Health Sciences Institute, Department of Molecular Medicine and Biotechnology, Istanbul, Turkey; Istanbul Medipol University, International School of Medicine, Department of Medical Pharmacology, Istanbul, Turkey. Electronic address: mguzel@medipol.edu.tr.

PMID: 35248814
DOI: 10.1016/j.jmgm.2022.108160

Abstract

Glioblastoma Multiforme (GBM) is the most aggressive brain tumor and classified as one of the deadliest cancers. The current treatment plans for GBM remains to be ineffective because of its rapid progress and inability of the drugs used to cross the blood-brain barrier (BBB). Thus, developing more effective and potent medicines for GBM are needed. There have been several reports demonstrating that CAPE presents reasonably good anti-cancer activity in certain cancer cell lines and can penetrate the blood-brain barrier. Accordingly, in this study we synthesized several novel CAPE analogs with the addition of more druggable handles and solubilizing entities and subsequently evaluated their in vitro therapeutic efficacies in GBM cell lines (T98G and LN229). The most potent compound was then examined extensively and results showed that the 50 μM novel CAPE analog (compound 10) significantly decreases the viability of both T98G and LN229 GBM cells as compared to CAPE itself. Moreover, the compound 10 was not cytotoxic to healthy human cells (fibroblast-like mesenchymal stem cells) at the same concentration. Apoptotic (32.8%, and 44.6%) cell populations were detected in the compound 10 treated groups for LN229 and T98G, respectively. As an indication of apotosis, significantly increased PARP cleavage was detected in compound 10 versus CAPE treated LN229. In addition, we conducted molecular docking and molecular dynamics (MD) simulations studies on certain targets playing roles on GBM disease pathway such as NF-κB, EGFR, TNF-α, ERK2, PAPR1, hCA IX and hCA XII. Our findings demonstrated that designed CAPE analogs have anti-cancer activity on GBM cells and in silico studies also demonstrate the inhibitory ability of suggested compounds via interactions with critical residues in binding pockets of studied targets. Here, we suggest the novel CAPE analog to study further against GBM. Therefore, identification of the compound related molecular signature may provide more to understand the mechanism of action.

Keywords: Anti-cancer activity; Caffeic acid phenethyl ester (CAPE); Glioblastoma multiforme (GBM); In silico molecular modeling; Novel heterocyclic CAPE analogs.

MeSH terms

Caffeic Acids
Cell Line
Cell Line, Tumor
Cell Proliferation
Glioblastoma* / drug therapy
Glioblastoma* / metabolism
Glioblastoma* / pathology
Humans
Molecular Docking Simulation
Phenylethyl Alcohol / analogs & derivatives

Substances

Caffeic Acids
caffeic acid phenethyl ester
Phenylethyl Alcohol