상세 보기
- Park, Mina;
- Hwang, Jee Won;
- Cho, Yena;
- Kim, Saegun;
- Han, Sang Hoon;
- ... Kim, Woo-Young;
- ... Kim, Yong Kee;
- 외 4명
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19SCOPUS
18초록
The success of cancer chemotherapy is limited by multidrug resistance (MDR), which is mainly caused by P-glycoprotein (P-gp) overexpression. In the present study, we describe a novel microtubule inhibitor, 5-(N-methylmaleimid-3-yl)-chromone (SPC-160002), that can be used to overcome MDR. A synthetic chromone derivative, SPC-160002, showed a broad spectrum of anti-proliferative effects on various human cancer cells without affecting P-gp expression and its drug efflux function. Treatment with SPC-160002 arrested the cell cycle at the M phase, as evidenced using fluorescence-activated cell sorting analysis, and increased the levels of mitotic marker proteins, including cyclin B, pS10-H3, and chromosomal passenger complex. This mitotic arrest by SPC-160002 was mediated by promoting and stabilizing microtubule polymerization, similar to the mechanism observed in case of taxane-based drugs. Furthermore, SPC-160002 suppressed the growth and sphere-forming activity of cancer stem cells. Our data herein strongly suggest that SPC-160002, a novel microtubule inhibitor, can be used to overcome MDR and can serve as an attractive candidate for anticancer drugs.
키워드
- 제목
- A novel synthetic microtubule inhibitor exerts antiproliferative effects in multidrug resistant cancer cells and cancer stem cells
- 저자
- Park, Mina; Hwang, Jee Won; Cho, Yena; Kim, Saegun; Han, Sang Hoon; Yu, Jinsuh; Ha, Sojung; Kim, Woo-Young; Kim, Su-Nam; Kim, In Su; Kim, Yong Kee
- 발행일
- 2021-05
- 유형
- Article
- 권
- 11
- 호
- 1
- 페이지
- 1 ~ 11