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Inhibition of Importin beta 1 With a 2-Aminothiazole Derivative Resulted in G(2)/M Cell-cycle Arrest and Apoptosis

Authors
Ha, SiyoungChoi, JaesungMin, Na YoungLee, Kwang-HoHam, Seung Wook
Issue Date
May-2017
Publisher
INT INST ANTICANCER RESEARCH
Keywords
KPNB1 inhibitor; 2-aminothiazole derivative; cell cycle; apoptosis; mitotic defects
Citation
ANTICANCER RESEARCH, v.37, no.5, pp 2373 - 2379
Pages
7
Journal Title
ANTICANCER RESEARCH
Volume
37
Number
5
Start Page
2373
End Page
2379
URI
https://scholarworks.bwise.kr/cau/handle/2019.sw.cau/4525
DOI
10.21873/anticanres.11575
ISSN
0250-7005
1791-7530
Abstract
Background: The design and synthesis of novel chemotherapeutic agents that can induce apoptosis and cell-cycle arrest has emerged as an attractive approach for the treatment of cancer, because they can limit possible nonspecific effects of compound treatment. Previous studies established that the expression of KPNB1 was increased in several cancer cells and transformed cell lines and inhibition of KPNB1 using siRNA significantly inhibited cervical tumour proliferation, but did not affect normal cervical epithelium. Recently, we reported that a KPNB1 inhibitor, the 2-aminothiazole derivative 1, possesses strong anti-proliferative effects against several cancer cells in the nanomolar concentration range. Results: Treatment with compound 1 interferes with cell-cycle progression in the G2/M phase, as detected by flow cytometry analysis and results in apoptosis by the intrinsic pathway. Fluorescence microscopic analysis of mitotic cells predominantly mitotic abnormal cells with monopolar spindles and treatment with compound 1 did not affect polymerization of microtubules. Conclusion: Compound 1, as a KPNB1 inhibitor, might be a good target for future development of anticancer agents showing the activities of apoptosis and cell cycle arrest.
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Ham, Seung Wook
자연과학대학 (화학과)
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