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Experimental antitumor activity of BMY-28175 a new fermentation derived antitumor agent
Authors:John E Schurig  William C Rose  Hideo Kamei  Yuji Nishiyama  William T Bradner  Dale A Stringfellow
Institution:(1) Bristol-Myers Co., Inc., Pharmaceutical Research and Development Division, 06492 Wallingford, CT, USA;(2) Bristol-Myers Research Institute, Tokyo, Japan;(3) Bristol-Myers Co., Inc., P.O. Box 5100, 06492 Wallingford, CT, USA
Abstract:Summary BMY-28175 is a novel antitumor antibiotic produced in fermentation by Actinomadura verrucosospora. The cytotoxic effects of BMY-28175 were determined using murine and human tumor cell lines in vitro. Following 72 hour exposure, the drug had IC50 values 1.5 to 13.5 ng/ml in a microtiter assay. BMY-28175 was evaluated for antitumor activity against several experimental murine and human tumor models. The drug administered ip was active against ip implanted P388 leukemia, L1210 leukemia, B16 melanoma, M109 lung carcinoma, C26 colon carcinoma, M5076 sarcoma and Lewis lung carcinoma. In addition, BMY-28175 administered iv was active against iv implanted P388 and L1210 leukemias. BMY-28175 was active against sc implanted B16 melanoma (increased lifespan and/or inhibition of primary tumor growth) in about 60% of the tests. The growth of sc implanted M109 was inhibited by BMY-28175 in a single experiment. BMY-28175 was also active against the MX-1 human mammary xenograft implanted in the subrenal capsule of nude mice. The optimal dose for BMY-28175 in these various studies ranged from 0.16 mgrg/kg per injection with consecutive daily (qd1-9) administration, to 51.2 mgrg/kg with single dose administration. The results of these studies indicate that BMY-28175 is one of the most potent antitumor agents yet observed, with a broad spectrum of activity against tumors of murine and human origin and activity against tumors located distal to the site of drug administration.
Keywords:antitumor  antibiotic  cytotoxicity
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