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Resistance mechanisms for anti-tubulin agents in malignant melanomas

Research Project

Project/Area Number 24791171
Research Category

Grant-in-Aid for Young Scientists (B)

Allocation TypeMulti-year Fund
Research Field Dermatology
Research InstitutionIwate Medical University

Principal Investigator

AKASAKA K  岩手医科大学, 医学部, 研究員 (90552753)

Project Period (FY) 2012-04-01 – 2014-03-31
Project Status Completed (Fiscal Year 2013)
Budget Amount *help
¥4,290,000 (Direct Cost: ¥3,300,000、Indirect Cost: ¥990,000)
Fiscal Year 2013: ¥1,560,000 (Direct Cost: ¥1,200,000、Indirect Cost: ¥360,000)
Fiscal Year 2012: ¥2,730,000 (Direct Cost: ¥2,100,000、Indirect Cost: ¥630,000)
Keywords悪性黒色腫 / BCL2 / BCLxL / 抗微小管薬 / 皮膚腫瘍学 / MCL1 / apoptosis
Research Abstract

Previous studies have suggested a link between TUBB3 overexpression and paclitaxel resistance through alterations in the properties of the mitotic spindle. We found that paclitaxel treatment induced temporary mitotic arrest in 7 melanoma cell lines irrespective of the TUBB3 level, suggesting that TUBB3 had no significant influence on spindle properties. On the other hand, the amount of BCL2, an anti-apoptotic protein, was well correlated with paclitaxel resistance. Treatment of the paclitaxel-resistant cell lines with ABT-737, an inhibitor of BCL2 and BCLxL, or simultaneous knock-down of BCL2 and BCLxL dramatically increased the cells' sensitivity, while knock-down of MCL1, another member of the BCL2 family, had only a minimal effect. Our results suggest that the paclitaxel sensitivity of melanoma cells is attributable to apoptosis susceptibility rather than a change in spindle properties and that BCL2 and BCLxL play a pivotal role in the former.

Report

(3 results)
  • 2013 Annual Research Report   Final Research Report ( PDF )
  • 2012 Research-status Report
  • Research Products

    (5 results)

All 2014 2013 2012

All Journal Article (4 results) (of which Peer Reviewed: 4 results,  Open Access: 1 results) Presentation (1 results)

  • [Journal Article] Immunohistochemistry for histone h3 lysine 9 methyltransferase and demethylase proteins in human melanomas.2014

    • Author(s)
      Miura S, Maesawa C, Shibazaki M, Yasuhira S, Kasai S, Tsunoda K, Maeda F, Takahashi K, Akasaka T, Masuda T. Immunohistochemistry for histone h3 lysine 9 methyltransferase and demethylase proteins in human melanomas.
    • Journal Title

      Am J Dermatopathol

      Volume: 36(3) Issue: 3 Pages: 211-216

    • DOI

      10.1097/dad.0b013e3182964e02

    • Related Report
      2013 Final Research Report
    • Peer Reviewed / Open Access
  • [Journal Article] BCL2 and BCLxL are key determinants of resistance to antitubulin chemotherapeutics in melanoma cells.2013

    • Author(s)
      Watanabe A, Yasuhira S, Inoue T, Kasai S, Shibazaki M, Takahashi K, Akasaka T, Masuda T, Maesawa C.
    • Journal Title

      Exp Dermatol

      Volume: 22(8) Issue: 8 Pages: 518-523

    • DOI

      10.1111/exd.12185

    • Related Report
      2013 Final Research Report
    • Peer Reviewed
  • [Journal Article] Transcriptional and post-transcriptional regulation of βIII-tubulin protein expression in relation with cell cycle-dependent regulation of tumor cells2012

    • Author(s)
      Shibazaki M, Maesawa C, Akasaka K, Kasai S, Yasuhira S, Kanno K, Nakayama I, Sugiyama T, Wakabayasi G, Masuda T, Mori N
    • Journal Title

      Int.J.Oncol.

      Volume: 40(3) Pages: 695-702

    • DOI

      10.3892/ijo.2011.1291

    • Related Report
      2013 Final Research Report
    • Peer Reviewed
  • [Journal Article] Downregulation of cylindromatosis gene, CYLD, confers a growth advantage on malignant melanoma cells while negatively regulating their migration activity2012

    • Author(s)
      Ishikawa Y
    • Journal Title

      Int J Oncol

      Volume: (in press) Issue: 3 Pages: 314-5

    • DOI

      10.1111/j.1346-8138.2011.01259.x

    • Related Report
      2013 Final Research Report
    • Peer Reviewed
  • [Presentation] 悪性黒色腫におけるβIII-tubulinの発現とタキサン系抗がん剤感受性に対する影響の解析2012

    • Author(s)
      赤坂 季代美
    • Organizer
      日本病理学会総会
    • Place of Presentation
      東京
    • Related Report
      2012 Research-status Report

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Published: 2013-05-31   Modified: 2019-07-29  

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