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2017 Fiscal Year Final Research Report

Development of high accuracy multidrug resistance prediction method using SPECT imaging for individualized anticancer therapy

Research Project

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Project/Area Number 15K09949
Research Category

Grant-in-Aid for Scientific Research (C)

Allocation TypeMulti-year Fund
Section一般
Research Field Radiation science
Research InstitutionKanazawa University

Principal Investigator

KOBAYASHI Masato  金沢大学, 健康増進科学センター, 助教 (30444235)

Co-Investigator(Kenkyū-buntansha) 川井 恵一  金沢大学, 保健学系, 教授 (30204663)
Co-Investigator(Renkei-kenkyūsha) TAMAI Ikumi  金沢大学, 薬学系, 教授 (20155237)
OKAZAWA Hidehiko  福井大学, 高エネルギー医学研究センター, 教授 (50360813)
KUNISHIMA Munetaka  金沢大学, 薬学系, 教授 (10214975)
NISHII Ryuichi  放射線医学総合研究所, 分子イメージング診断治療研究部, 主任研究員 (60463212)
SHIKANO Naoto  茨城県立医療大学, 保健医療学部, 准教授 (80295435)
NISHI Kodai  長崎大学, 原爆後障害医療研究所, 助教 (10719496)
Research Collaborator INNIS B Robert  National Institute of Mental Health, Molecular Imaging Branch, Chief
Project Period (FY) 2015-04-01 – 2018-03-31
Keywords核医学 / 分子イメージング / 個別化治療 / 多剤耐性 / 薬物トランスポータ
Outline of Final Research Achievements

We developed high an accuracy multidrug resistance prediction method using SPECT imaging for individualized anticancer therapy. Although [99mTc]sestamibi and [99mTc]tetrofosmin has been reported to be the same method, we clarified that [99mTc]sestamibi had affinity to MDR1 and MRP1, whereas [99mTc]tetrofosmin had affinity to MDR1 and MRP1-3. Thus, these SPECT tracers had different method for multidrug resistance prediction in this study. Additionally, [131I]adsterol was possibility to be higher accuracy multidrug resistance prediction method than [99mTc]sestamibi and [99mTc]tetrofosmin because [131I]adsterol had only affinity to BCRP.

Free Research Field

放射線科学

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Published: 2019-03-29  

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