Combination treatment strategy for pancreatic cancer involving the novel HDAC inhibitor MPT0E028 with a MEK inhibitor beyond K-Ras status

Min-Wu Chao; Li-Hsun Chang; Huang-Ju Tu; Chao-Di Chang; Mei-Jung Lai; Yi-Ying Chen; Jing-Ping Liou; Che-Ming Teng; Shiow-Lin Pan

doi:10.1186/s13148-019-0681-6

Clinical Epigenetics (May 2019)

Combination treatment strategy for pancreatic cancer involving the novel HDAC inhibitor MPT0E028 with a MEK inhibitor beyond K-Ras status

Min-Wu Chao,
Li-Hsun Chang,
Huang-Ju Tu,
Chao-Di Chang,
Mei-Jung Lai,
Yi-Ying Chen,
Jing-Ping Liou,
Che-Ming Teng,
Shiow-Lin Pan

Affiliations

Min-Wu Chao: Graduate Institute of Cancer Molecular Biology and Drug Discovery, College of Medical Science and Technology, Taipei Medical University
Li-Hsun Chang: Pharmacological Institute, College of Medicine, National Taiwan University
Huang-Ju Tu: School of Pharmacy, College of Pharmacy, Taipei Medical University
Chao-Di Chang: Ph.D. Program in Biotechnology Research and Development, College of Pharmacy, Taipei Medical University
Mei-Jung Lai: Biomedical Commercialization Center, Taipei Medical University
Yi-Ying Chen: Graduate Institute of Cancer Molecular Biology and Drug Discovery, College of Medical Science and Technology, Taipei Medical University
Jing-Ping Liou: Ph.D. Program in Biotechnology Research and Development, College of Pharmacy, Taipei Medical University
Che-Ming Teng: Pharmacological Institute, College of Medicine, National Taiwan University
Shiow-Lin Pan: Graduate Institute of Cancer Molecular Biology and Drug Discovery, College of Medical Science and Technology, Taipei Medical University

DOI: https://doi.org/10.1186/s13148-019-0681-6
Journal volume & issue: Vol. 11, no. 1
pp. 1 – 14

Abstract

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Abstract Background Oncogenic K-Ras signaling highly relies on the canonical Ras/MEK/ERK pathway to contribute to pancreatic cancer progression. However, numerous efforts of MEK inhibitors have failed to provide an optimal antitumor effect for pancreatic cancer in practice. The aim of the present work was to develop a more efficacious therapeutic intervention for MEK inhibitors through combination with histone deacetylase (HDAC) inhibitor MPT0E028. Methods The effects of combined therapy on cell viability, apoptosis, protein, and RNA expressions were determined by MTT assay, flow cytometry, western blotting, and quantitative PCR analysis. The AsPC-1 xenograft was used to assess antitumor effects in vivo. Results The co-administration of MPT0E028 and MEK inhibitor yielded synergistic effects on cell viability suppression both in K-Ras mutated and wild-type pancreatic cancer cells and also markedly triggered cell apoptosis. Surprisingly, ERK and epidermal growth factor receptor (EGFR) were activated by the long-term and low-concentration treatment of MPT0E028 or another HDAC inhibitor alone. Whereas, the pharmacological attenuation of ERK signaling dramatically abolished the MPTE028-induced p-ERK and EGFR expression. Overexpression of HDAC4, HDAC6, and MEK, respectively, reversed the cell death induced by the combined treatment. Finally, the combined treatment decreased the tumor volume in an AsPC-1 xenograft model compared to each individual treatment alone. Conclusions The synergistic anti-survival effect of the combination was suggested to occur via compensation of the MEK inhibitor for activated ERK. Our results indicate that this combination strategy could benefit patients with pancreatic cancer beyond K-Ras status.

Published in Clinical Epigenetics

ISSN: 1868-7083 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine; Science: Biology (General): Genetics
Website: https://clinicalepigeneticsjournal.biomedcentral.com/

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Abstract

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