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Identification and biological evaluation of novel indole-2-one derivatives as BRD4-BD2 inhibitors.

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Bioorganic & medicinal chemistry 📖 저널 OA 5.3% 2024: 0/3 OA 2025: 0/27 OA 2026: 4/43 OA 2024~2026 2025 Vol.130() p. 118379
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Yang CJ, Cui QH, Lyu HJ, Wang ZY, Wang QS, Xiang R

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Pan-inhibitions of Bromodomain and Extra Terminal Domain (BET) proteins have shown great potential in anti-tumor therapy but exhibited clinical toxicities, while selective inhibition of BRD4-BD2 could

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APA Yang CJ, Cui QH, et al. (2025). Identification and biological evaluation of novel indole-2-one derivatives as BRD4-BD2 inhibitors.. Bioorganic & medicinal chemistry, 130, 118379. https://doi.org/10.1016/j.bmc.2025.118379
MLA Yang CJ, et al.. "Identification and biological evaluation of novel indole-2-one derivatives as BRD4-BD2 inhibitors.." Bioorganic & medicinal chemistry, vol. 130, 2025, pp. 118379.
PMID 40929782 ↗

Abstract

Pan-inhibitions of Bromodomain and Extra Terminal Domain (BET) proteins have shown great potential in anti-tumor therapy but exhibited clinical toxicities, while selective inhibition of BRD4-BD2 could improve specificity and have better safety. Herein, a series of indole-2-one derivatives were designed and synthesized as novel BD2-selective inhibitors. The representative compound 47 showed good inhibitory effect on BRD4-BD2 with the IC of 27 nM and displayed 102-fold selectivity over BRD4-BD1, and exhibited extensive anti-tumor proliferation activities in vitro, especially against tumor cells, such as K562 and HGC-27 (IC = 0.15 and 3 μM), and it was less toxic to normal cell in GES-1 (IC = 71 μM). Further biological studies revealed that 47 could down-regulate c-Myc and up-regulate p21, arrest cell cycle at G/G phase and induce apoptosis in HGC-27 cells. More importantly, 47 showed moderate pharmacokinetic properties and low toxicity in vivo. These results demonstrated that 47 might serve as a potent lead compound with potential for the treatment of cancers such as gastric cancer.

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