Structure-antitumor activity relationship of hybrid acetogenins focusing on connecting groups between heterocycles and the linker moiety

Kaito Ohta; Tetsuya Fushimi; Mutsumi Okamura; Akinobu Akatsuka; Shingo Dan; Hiroki Iwasaki; Masayuki Yamashita; Naoto Kojima

doi:10.1039/d2ra02399g

Structure-antitumor activity relationship of hybrid acetogenins focusing on connecting groups between heterocycles and the linker moiety

RSC Adv. 2022 May 25;12(25):15728-15739. doi: 10.1039/d2ra02399g. eCollection 2022 May 23.

Authors

Kaito Ohta¹, Tetsuya Fushimi², Mutsumi Okamura³, Akinobu Akatsuka³, Shingo Dan³, Hiroki Iwasaki¹, Masayuki Yamashita¹, Naoto Kojima¹

Affiliations

¹ Kyoto Pharmaceutical University 1 Misasagi-Shichono-cho, Yamashina-ku Kyoto 607-8412 Japan kojima@mb.kyoto-phu.ac.jp.
² Graduate School of Pharmaceutical Sciences, Osaka University 1-6 Yamadaoka Suita Osaka 565-0871 Japan.
³ Cancer Chemotherapy Center, Japanese Foundation for Cancer Research 3-8-1 Ariake-ku Tokyo 135-8550 Japan.

Abstract

We studied hybrid molecules of annonaceous acetogenins and mitochondrial complex I-inhibiting insecticides to develop a novel anticancer agent. A structure-antitumor activity relationship study focusing on the connecting groups between the heterocycles and the linker moiety bearing the tetrahydrofuran moiety was conducted. Eleven hybrid acetogenins with 1-methylpyrazole instead of γ-lactone were synthesized and their growth inhibitory activities against 39 human cancer cell lines were evaluated. The nitrogen atom at the 2'-position of the linker moiety was essential for inhibiting cancer growth. The 1-methylpyrazole-5-sulfonamide analog showed potent growth inhibition of NCI-H23, a human lung cancer cell line, in a xenograft mouse assay without critical toxicity. Hence, the results of this study may pave the way for the development of novel anticancer agents, with both selective and broad anticancer activities.