Involvement of clusterin expression in the refractory response of pancreatic cancer cells to a MEK inhibitor

Author:

Amada Kohei12,Hijiya Naoki1ORCID,Ikarimoto Sawa3,Yanagihara Kazuyoshi4,Hanada Toshikatsu5,Hidano Shinya67,Kurogi Shusaku1,Tsukamoto Yoshiyuki1,Nakada Chisato18,Kinoshita Keisuke19,Hirashita Yuka19,Uchida Tomohisa110,Shin Toshitaka8,Yada Kazuhiro11,Hirashita Teijiro11,Kobayashi Takashi6,Murakami Kazunari9,Inomata Masafumi11ORCID,Shirao Kuniaki2,Aoki Masahiro12ORCID,Takekawa Mutsuhiro13,Moriyama Masatsugu1

Affiliation:

1. Department of Molecular Pathology, Faculty of Medicine Oita University Oita Japan

2. Department of Medical Oncology and Hematology, Faculty of Medicine Oita University Oita Japan

3. Department of Plastic Surgery Kagoshima City Hospital Kagoshima Japan

4. Division of Rare Cancer Research National Cancer Center Research Institute Tokyo Japan

5. Department of Cell Biology, Faculty of Medicine Oita University Oita Japan

6. Department of Infectious Disease Control, Faculty of Medicine Oita University Oita Japan

7. Department of Immune Regulation, The Research Center for Hepatitis and Immunology National Center for Global Health and Medicine Chiba Japan

8. Department of Urology, Faculty of Medicine Oita University Oita Japan

9. Department of Gastroenterology, Faculty of Medicine Oita University Oita Japan

10. Department of Forensic Medicine, Faculty of Medicine Oita University Oita Japan

11. Department of Gastroenterological and Pediatric Surgery, Faculty of Medicine Oita University Oita Japan

12. Division of Pathophysiology Aichi Cancer Center Aichi Japan

13. Division of Cell Signaling and Molecular Medicine, Institute of Medical Sciences University of Tokyo Tokyo Japan

Abstract

AbstractConstitutive activation of the mitogen‐activated protein kinase (MAPK) signaling pathway is essential for tumorigenesis of pancreatic ductal adenocarcinoma (PDAC). To date, however, almost all clinical trials of inhibitor targeting this pathway have failed to improve the outcome of patients with PDAC. We found that implanted MIA Paca2, a human PDAC cell line sensitive to a MAPK inhibitor, PD0325901, became refractory within a week after treatment. By comparing the expression profiles of MIA Paca2 before and after acquisition of the refractoriness to PD0325901, we identified clusterin (CLU) as a candidate gene involved. CLU was shown to be induced immediately after treatment with PD0325901 or expressed primarily in more than half of PDAC cell lines, enhancing cell viability by escaping from apoptosis. A combination of PD0325901 and CLU downregulation was found to synergistically or additively reduce the proliferation of PDAC cells. In surgically resected PDAC tissues, overexpression of CLU in cancer cells was observed immunohistochemically in approximately half of the cases studied. Collectively, our findings highlight the mechanisms responsible for the rapid refractory response to MEK inhibitor in PDAC cells, suggesting a novel therapeutic strategy that could be applicable to patients with PDAC using inhibitor targeting the MAPK signaling pathway and CLU.

Funder

Japan Society for the Promotion of Science

Publisher

Wiley

Subject

Cancer Research,Oncology,General Medicine

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