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Relative cardiotoxicity and cytotoxicity of anthraquinonyl glucosaminosides
Authors:Jon W. Banning  Hanley N. Abramson  Henry C. Wormser  Jender Wu  Thomas H. Corbett
Affiliation:(1) Department of Pharmaceutical Sciences, College of Pharmacy and Allied Health Professions, Wayne State University, 48202 Detroit, MI, USA;(2) Division of Medical Oncology, Dept. of Internal Medicine, School of Medicine, Wayne State University, 48202 Detroit, MI, USA
Abstract:Summary The cardiotoxicity and cytotoxicity for tumor cells of four new synthetic anthraquinonyl glucosaminosides were compared in vitro. The nonhydroxylated anthraquinone was not cardiotoxic, and its cytotoxic activity was the weakest of the compounds in the series. Increasing the number of hydroxyl groups on the anthraquinone moiety increased the inhibition of growth of L-1210 leukemia cells and pancreatic or colonic adenocarcinomas in a soft agar colony formation assay. However, cardiotoxicity was also increased in proportion to the number of hydroxyl groups present. The adenocarcinomas were slightly more sensitive than the leukemias to the inhibitory action of the dihydroxylated anthraquinonyl glucosaminosides on cell growth.
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