| Literature DB >> 28228362 |
Zhongpeng Ding1, Hejuan Cheng1, Shixiao Wang2, Yingwei Hou3, Jianchun Zhao3, Huashi Guan3, Wenbao Li4.
Abstract
Plinabulin, a drug targeting microtubule of cancer cells, has been currently tried in its phase III clinical study. However, low efficacy caused by poor pharmacokinetic (PK) properties has been considered to be the main obstacle to approved by the Food and Drug Administration. Herein, we introduced a deuterium atom as an isostere in its structure to become a new compound named (MBRI-001, No. 9 in a series of deuterium-substituted compounds). The structure of MBRI-001 was characterized by HRMS, NMR, IR and a single crystal analysis. MBRI-001 exhibited better pharmacokinetic characteristics than that of plinabulin. Additionally, its antitumor activity is in a low nanomolar level for a variety of cancer cell lines and high activity against human NCI-H460 xenograted in mice intravenous administration. Importantly, continuous administration of MBRI-001 exhibited lower toxicity compared to docetaxel. We thus suggest that MBRI-001 could be developed as a promising anti-cancer agent in near future.Entities:
Keywords: Deuterium substituted; Docetaxel; Microtubule; Pharmacokinetic properties; Plinabulin
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Year: 2017 PMID: 28228362 DOI: 10.1016/j.bmcl.2017.01.096
Source DB: PubMed Journal: Bioorg Med Chem Lett ISSN: 0960-894X Impact factor: 2.823