Development of a Polo-like Kinase-1 Polo-Box Domain Inhibitor as a Tumor Growth Suppressor in Mice Models.
Pethaiah GunasekaranMin Su YimMija AhnNak-Kyun SoungJung-Eun ParkJaehi KimGeul BangSang Chul ShinJoonhyeok ChoiMinkyoung KimHak Nam KimYoung-Ho LeeYoung-Ho ChungKyeong LeeEunice EunKyeong KimYoung-Ho JeonMin Ju KimKyeong-Ryoon LeeBo-Yeon KimKyung S LeeEun Kyoung RyuJeong Kyu BangPublished in: Journal of medicinal chemistry (2020)
Polo-like kinase-1 (Plk1) plays a key role in mitosis and has been identified as an attractive anticancer drug target. Plk1 consists of two drug-targeting sites, namely, N-terminal kinase domain (KD) and C-terminal polo-box domain (PBD). As KD-targeting inhibitors are associated with severe side effects, here we report on the pyrazole-based Plk1 PBD inhibitor, KBJK557, which showed a remarkable in vitro anticancer effect by inducing Plk1 delocalization, mitotic arrest, and apoptosis in HeLa cells. Further, in vivo optical imaging analysis and antitumorigenic activities in mouse xenograft models demonstrate that KBJK557 preferentially accumulates in cancer cells and selectively inhibits cancer cell proliferation. Pharmacokinetic profiles and partition coefficients suggest that KBJK557 was exposed in the blood and circulated through the organs with an intermediate level of clearance (t1/2, 7.73 h). The present investigation offers a strategy for specifically targeting cancer using a newly identified small-molecule inhibitor that targets the Plk1 PBD.
Keyphrases
- cell cycle arrest
- small molecule
- papillary thyroid
- cell proliferation
- cell cycle
- cancer therapy
- high resolution
- protein kinase
- squamous cell
- transcription factor
- pi k akt
- induced apoptosis
- tyrosine kinase
- oxidative stress
- endoplasmic reticulum stress
- binding protein
- drug induced
- molecular docking
- early onset
- childhood cancer
- adipose tissue
- young adults
- signaling pathway
- drug delivery
- adverse drug
- type diabetes
- metabolic syndrome
- electronic health record