Cell death caused by quinazolinone HMJ-38 challenge in oral carcinoma CAL 27 cells: dissections of endoplasmic reticulum stress,mitochondrial dysfunction and tumor xenografts |
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| Authors: | Chi-Cheng Lu Jai-Sing Yang Jo-Hua Chiang Mann-Jen Hour Kuei-Li Lin Tsung-Han Lee Jing-Gung Chung |
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| Affiliation: | 1. Department of Life Sciences, National Chung Hsing University, Taichung 40227, Taiwan;2. Department of Pharmacology, China Medical University, Taichung 40402, Taiwan;3. School of Pharmacy, China Medical University, Taichung 40402, Taiwan;4. Department of Radiation Oncology, Chi Mei Medical Center, Tainan 71004, Taiwan;5. Department of Biological Science and Technology, China Medical University, Taichung 40402, Taiwan;6. Department of Biotechnology, Asia University, Taichung 41354, Taiwan |
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| Abstract: | BackgroundThis investigation clearly clarified the synthesized and antimitotic compound, 2-(3′-methoxyphenyl)-6-pyrrolidinyl-4-quinazolinone (HMJ-38), addressing its target and precise mechanism of action. We hypothesized that HMJ-38 might sensitize apoptotic death of human oral carcinoma CAL 27 cells in vitro and inhibit xenograft tumor growth in vivo.MethodsCell viability was assessed utilizing MTT assay. HMJ-38-treated cells represented DNA fragmentation using agarose gel electrophoresis as further evidenced using TUNEL staining. Flow cytometric analyses, immunoblotting and quantitative RT-PCR were applied for protein and gene expression. Antitumor xenograft study was employed.ResultsHMJ-38 concentration- and time-dependently reduced viability of CAL 27 cells. The effect of intrinsic molecules was signalized during HMJ-38 exposure with disruption of ΔΨm, MPT pore opening and the release of various events from mitochondria undergoing cell apoptosis. HMJ-38 also markedly facilitated G2/M phase arrest. HMJ-38 stimulated the activation of CDK1 activity that modulated phosphorylation on Ser70 of Bcl-2-mediated mitotic arrest and apoptosis. HMJ-38 triggered intracellular Ca2 + release and activated related pivotal hallmarks of ER stress. HMJ-38 in nude mice bearing CAL 27 tumor xenografts decreased tumor growth. Furthermore, HMJ-38 enhanced caspase-3 gene expression and protein level in xenotransplanted tumors.ConclusionsEarly roles of mitotic arrest, unfolded protein response and mitochondria-dependent signaling contributed to apoptotic CAL 27 cell demise induced by HMJ-38. In in vivo experiments, HMJ-38 also efficaciously suppressed tumor volume in a xenotransplantation model.General significanceThis finding might fully support a critical event for HMJ-38 via induction of apoptotic machinery and ER stress against human oral cancer cells. |
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| Keywords: | HMJ-38 Human oral carcinoma cells Endoplasmic reticulum stress Mitochondrial dysfunction Tumor xenografts |
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