Issue 32, 2019
From the journal:

RSC Advances

Induction of cell cycle arrest and apoptosis by copper complex Cu(SBCM)2 towards oestrogen-receptor positive MCF-7 breast cancer cells

Jhi Biau Foo, ORCID logo *ab   Li Shan Ng,a   Ji Hui Lim,a   Pau Xien Tan,a   Yan Zhi Lor,a   Jason Siau Ee Loo, ORCID logo b   May Lee Low,c   Lee Chin Chan,d   Chaw Yee Beh,e   Sze Wei Leong,d   Latifah Saiful Yazan,gh   Yin Sim Tor*f  and  Chee Wun Howa  

* Corresponding authors

a Faculty of Pharmacy, MAHSA University, Jalan SP2, Bandar Saujana Putra, 42610 Jenjarom, Kuala Langat, Selangor, Malaysia
E-mail: foojhibiau@gmail.com

b School of Pharmacy, Faculty of Health & Medical Sciences, Taylor's University, No. 1 Jalan Taylor's, 47500 Subang Jaya, Selangor Darul Ehsan, Malaysia
E-mail: JhiBiau.Foo@taylors.edu.my

c Department of Pharmaceutical Chemistry, School of Pharmacy, International Medical University, No. 126, Jalan Jalil Perkasa 19, 57000 Bukit Jalil, Kuala Lumpur, Malaysia

d Virology Lab 1, Faculty of Biotechnology and Biomolecular Sciences, Universiti Putra Malaysia (UPM), 43400 Serdang, Selangor, Malaysia

e Laboratory of Vaccines and Immunotherapeutics, Institute of Bioscience, Universiti Putra Malaysia (UPM), 43400 Serdang, Selangor, Malaysia

f School of Biosciences, Faculty of Health & Medical Sciences, Taylor's University, No. 1 Jalan Taylor's, 47500 Subang Jaya, Selangor Darul Ehsan, Malaysia
E-mail: YinSim.Tor@taylors.edu.my

g Laboratory of Molecular Biomedicine, Institute of Bioscience, Universiti Putra Malaysia, 43400 UPM Serdang, Selangor, Malaysia

h Department of Biomedical Sciences, Faculty of Medicine and Health Sciences, Universiti Putra Malaysia (UPM), 43400 Serdang, Selangor, Malaysia

Abstract

Copper complexes have the potential to be developed as targeted therapy for cancer because cancer cells take up larger amounts of copper than normal cells. Copper complex Cu(SBCM)2 has been reported to induce cell cycle arrest and apoptosis towards triple-negative breast cancer cells. Nevertheless, its effect towards other breast cancer subtypes has not been explored. Therefore, the present study was conducted to investigate the effect of Cu(SBCM)2 towards oestrogen-receptor positive MCF-7 breast cancer cells. Growth inhibition of Cu(SBCM)2 towards MCF-7 and human non-cancerous MCF-10A breast cells was determined by MTT assay. Morphological changes of Cu(SBCM)2-treated-MCF-7 cells were observed under an inverted microscope. Annexin V/PI apoptosis assay and cell cycle analysis were evaluated by flow cytometry. The expression of wild-type p53 protein was evaluated by Western blot analysis. The intracellular ROS levels of MCF-7 treated with Cu(SBCM)2 were detected using DCFH-DA under a fluorescence microscope. The cells were then co-treated with Cu(SBCM)2 and antioxidants to evaluate the involvement of ROS in the cytotoxicity of Cu(SBCM)2. Docking studies of Cu(SBCM)2 with DNA, DNA topoisomerase I, and human ribonucleotide reductase were also performed. The growth of MCF-7 cells was inhibited by Cu(SBCM)2 in a dose-dependent manner with less toxicity towards MCF-10A cells. It was found that Cu(SBCM)2 induced G2/M cell cycle arrest and apoptosis in MCF-7 cells, possibly via a p53 pathway. Induction of intracellular ROS was not detected in MCF-7 cells. Interestingly, antioxidants enhance the cytotoxicity of Cu(SBCM)2 towards MCF-7 cells. DNA topoisomerase I may be the most likely target that accounts for the cytotoxicity of Cu(SBCM)2.

Graphical abstract: Induction of cell cycle arrest and apoptosis by copper complex Cu(SBCM)2 towards oestrogen-receptor positive MCF-7 breast cancer cells

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Article information

DOI
https://doi.org/10.1039/C9RA03130H
Article type
Paper
Submitted
26 Apr 2019
Accepted
03 Jun 2019
First published
11 Jun 2019
This article is Open Access
Creative Commons BY-NC license

RSC Adv., 2019,9, 18359-18370

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Induction of cell cycle arrest and apoptosis by copper complex Cu(SBCM)2 towards oestrogen-receptor positive MCF-7 breast cancer cells

J. B. Foo, L. S. Ng, J. H. Lim, P. X. Tan, Y. Z. Lor, J. S. E. Loo, M. L. Low, L. C. Chan, C. Y. Beh, S. W. Leong, L. Saiful Yazan, Y. S. Tor and C. W. How, RSC Adv., 2019, 9, 18359 DOI: 10.1039/C9RA03130H

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