Abstract |
The efficacy of cisplatin (CDDP) in combination with the protein synthesis inhibitor ethyldeshydroxysparsomycin ( EDSM) has been tested in two tumor models at various schedules. Mice with L1210 leukemia or B16 melanoma were treated with CDDP alone or in combination with EDSM. Against L1210 leukemia, which is sensitive to CDDP, combinations elicited increases in life-span for all treatment schedules compared to those achieved with the corresponding dose of CDDP. Moreover, the combination of EDSM with this platinum compound yielded a cure rate > 80%, compared to < 35% for single CDDP treatment. Although the B16 melanoma is rather resistant to both CDDP and EDSM, combinations of these agents against B16 melanoma showed schedule dependent efficacy and in certain schedules significant therapeutic advantage over individual drug treatment, but cures were not observed. Our results suggest that EDSM has significant synergistic capabilities in both animal tumor models, but strong therapeutic enhancement of cisplatin efficacy is only seen when the tumor is sensitive to CDDP.
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Authors | H P Hofs, D J Wagener, V De Valk-Bakker, H Van Rennes, D De Vos, W H Doesburg, H C Ottenheijm, W J De Grip |
Journal | Investigational new drugs
(Invest New Drugs)
Vol. 13
Issue 1
Pg. 23-32
( 1995)
ISSN: 0167-6997 [Print] United States |
PMID | 7499104
(Publication Type: Journal Article, Research Support, Non-U.S. Gov't)
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Chemical References |
- ethyldeshydroxysparsomycin
- Sparsomycin
- Cisplatin
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Topics |
- Animals
- Antineoplastic Combined Chemotherapy Protocols
(therapeutic use)
- Cisplatin
(therapeutic use)
- Drug Screening Assays, Antitumor
- Leukemia L1210
(drug therapy)
- Melanoma, Experimental
(drug therapy)
- Mice
- Sparsomycin
(analogs & derivatives, therapeutic use)
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