상세 보기
- Yoon, Kyoung Bin;
- Lee, Hyo Jeong;
- Chung, Hye Jin;
- Lee, Jungeun;
- Choi, Jungil;
- ... Han, Sun-Young;
- 외 2명
WEB OF SCIENCE
4SCOPUS
4초록
Fms-like tyrosine kinase 3 (FLT3) is a valuable pharmacological target in the treatment of acute myeloid leukemia (AML). LDD-1075 and LDD-1076 are indirubin derivatives, and LDD-1075 is the ester form of LDD-1076. LDD-1076 exhibited a potent in vitro FLT3 kinase activity inhibition with an IC50 of 7.89 nM, whereas, LDD-1075 demonstrated a relatively weak activity against FLT3 (IC50 of 3.19 mu M). In contrast with the results of the FLT3 kinase activity inhibition assay, the LDD-1076 did not affect the growth of the MV4-11 cell line, which harbors the constitutively activated form of the FLT3 mutation. Notably, LDD-1075 exhibited a strong cytotoxic effect against the MV4-11 cells. When LDD-1075 was incubated with the MV4-11 cell lysate, the formation of LDD-1076 was observed. Treatment with LDD-1075 inhibited the FLT3 phosphorylation along with the phosphorylation of the signal transducer and activator of transcription 5 protein, which is a downstream signal transducer of FLT3. Treatment with LDD-1075 induced apoptosis and cell cycle arrest at the G1 phase. The present study demonstrated that the LDD-1076 formed by the bioconversion of LDD-1075 is a potent FLT3 inhibitor with anti-leukemic activity.
키워드
- 제목
- Discovery of LDD-1075 as a potent FLT3 inhibitor
- 저자
- Yoon, Kyoung Bin; Lee, Hyo Jeong; Chung, Hye Jin; Lee, Jungeun; Choi, Jungil; Heo, Jeong Doo; Kim, Yong-Chul; Han, Sun-Young
- 발행일
- 2019-05
- 유형
- Article
- 저널명
- Oncology Letters
- 권
- 17
- 호
- 5
- 페이지
- 4735 ~ 4741