posted on 2021-06-03, 21:47authored byLun Wang, Yunhua Zheng, Dan Li, Jianhong Yang, Lei Lei, Wei Yan, Wei Zheng, Minghai Tang, Mingsong Shi, Ruijia Zhang, Xiaoying Cai, Hengfan Ni, Xu Ma, Na Li, Feng Hong, Haoyu Ye, Lijuan Chen
Klisyri (KX01) is a dual tubulin/Src
protein inhibitor that has
shown potential therapeutic effects in several tumor models. However,
a phase II clinical trial in patients with bone-metastatic castration-resistant
prostate cancer was halted because of lack of efficacy. We previously
reported that KX01 binds to the colchicine site of β-tubulin
and its morpholine group lies close to α-tubulin’s surface.
Thus, we hypothesized that enhancing the interaction of KX01 with
α-tubulin could increase tubulin inhibition and synthesized
a series of KX01 derivatives directed by docking studies. Among these
derivatives, 8a exhibited more than 10-fold antiproliferation
activity in several tumor cells than KX01 and significantly improved in vivo antitumor effects. The X-ray crystal structure suggested
that 8a both bound to the colchicine site and extended
into the interior of α-tubulin to form potent interactions,
presenting a novel binding mode. A potential clinical candidate for
cancer therapy was identified in this study.