Antitumor activity of cis-malonato[(4R,5R)-4,5-bis(aminomethy1)-2-isopropyl-1,3-dioxolanelplatinum(II), a new platinum analogue,as an anticancer agent |
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| Authors: | Dae-Kee Kim Hun-Taek Kim Yong-Baik Cho Joo Ho Tai Jae Suk Ahn Taek-Soo Kim Key H Kim Weon-Seon Hong |
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| Institution: | (1) Life Science Research Center, Sunkyong Industries, 600, Jungja-Dong, Changan-Ku, Suwon-Si, Kyungki-Do 440–745, Korea, KR;(2) Department of Medicine, Asan Medical Center, College of Medicine, Ulsan University, Seoul 138–040, Korea, KR |
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| Abstract: | The in vitro and in vivo antitumor activity of a new antitumor platinum complex, cis-malonato(4R, 5R)-4, 5-bis(aminomethyl)-2-isopropyl-1,3-dioxolane]platinum(II) (SKI 2053R, NSC D644591), were evaluated and compared with
those of cisplatin (CDDP) and carboplatin (CBDCA) using murine tumors. SKI 2053R was highly active in vitro against both L1210
murine leukemia and its CDDP-resistant subline, L1210/DDP; the relative resistances were 20.0-, 14.5-, and 2.7-fold for CDDP,
CBDCA, and SKI 2053R, respectively. SKI 2053R showed activity comparable with or superior to either CDDP or CBDCA in mice
implanted with L1210. In mice implanted with L1210/DDP, as compared with CBDCA, SKI 2053R showed high values for the percentage
of treated survivors relative to controls and for numbers of cured mice, whereas CDDP had virtually no activity. In mice implanted
with P388, all three drugs were highly active, but the intensity of activity was shown to be ranked in the following order:
SKI 2053R > CDDP > CBDCA. The antitumor activity of SKI 2053R against Lewis lung carcinoma was comparable with that of both
CDDP and CBDCA. The antitumor activity of SKI 2053R was further investigated against two human tumor xenografts, KATO III
(stomach adenocarcinoma) and WiDr (colon adenocarcinoma), implanted s.c. in nude mice and was compared with that of CDDP.
In SKI 2053R-treated groups, the time required for a mean tumor weight of 1,000 mg was 33.1 days in KATO III xenografts and
35.0 days in WiDr xenografts as compared with 30.2 and 27.2 days in CDDP-treated groups, respectively. SKI 2053R achieved
growth-inhibition rates comparable with those of CDDP against KATO III (65% versus 59%) and WiDr xenografts (64% versus 54%)
on day 35. These results indicate that SKI 2053R is an attractive candidate for further development as a clinically useful
anticancer drug.
Received: 7 June 1994 / Accepted: 27 September 1994 |
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| Keywords: | SKI 2053R Antitumor activity |
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