In vitro cytotoxicity on human ovarian cancer cells by T-type calcium channel blockers

The growth inhibition of human Cancer cells via T-type CA(2+) channel blockade has been well known. Herein, a series of new 3,4-dihydroquinazoline derivatives were synthesized via a brief SAR study on KYS05090 template and evaluated for both T-type CA(2+) channel (Cav3.1) blockade and cytotoxicity on three human ovarian Cancer cells (SK-OV-3, A2780 and A2780-T). Most of compounds except 6i generally exhibited more potent cytotoxicity on SK-OV-3 than mibefradil as a positive control regardless of the degree of T-type channel blockade. In particular, eight compounds (KYS05090, 6a and 6c-6h) showing strong channel blockade exhibited almost equal and more potent cytotoxicity on A2780 when compared to mibefradil. On A2780-T paclitaxel-resistant human ovarian carcinoma, two compounds (KYS05090 and 6d) were 20-fold more active than mibefradil. With respect to cell cycle arrest effect on A2780 and A2780-T cells, KYS05090 induced large proportion of sub-G1 phase in the cell cycle progression of A2780 and A2780-T, meaning the induction of Cancer cell death instead of cell cycle arrest via blocking T-type CA(2+) channel. Among new analogues, compounds 6g and 6h induced cell cycle arrest at G1 phase of A2780 and A2780-T cells in dose-dependent manner and exhibited strong anti-proliferation effects of ovarian Cancer cells by blocking T-type CA(2+) channel. Furthermore, 6g and 6h possessing strong cytotoxic effects could induce Apoptosis of A2780 cells, which was detected by confocal micrographs using DAPI staining.

Apoptosis; Cell cycle arrest; Cytotoxicity; Ovarian cancer; T-type Ca(2+) channel.