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Synthesis, physical properties, and antitumor activity of tetraplatin and related tetrachloroplatinum(IV) stereoisomers of 1,2-diaminocyclohexane

  • W. K. Anderson
  • , D. A. Quagliato
  • , R. D. Haugwitz
  • , V. L. Narayanan
  • , M. K. Wolpert-DeFilippes
  • National Institutes of Health

Research output: Contribution to journalArticlepeer-review

97 Scopus citations

Abstract

The synthesis, physical properties, and antitumor activity of the cis-, d,l-trans, d-trans-, and l-trans- stereoisomers of 1,2-diaminocyclohexane tetrachloroplatinum (IV) are described. The objective of the study was to produce a platinum complex with activity against cisplatin-resistant tumor cells and with suitable pharmaceutical properties for formulation development. The isomers had the following solubilities in saline: cis-, 2 mg/ml; d,l-trans-, 6.5 mg/ml; and d-trans- and l-trans-, 15-16 mg/ml. The four complexes showed slightly better activity than cisplatin against the ip implanted murine L1210 leukemia. In contrast to cisplatin, all complexes produced significant increases in life span against L1210/cisplatin, a subline of L1210 with acquired resistance to cisplatin. However, the cis- isomer was less active against L1201/cisplatin. The d,l-trans- isomer (tetraplatin) was selected for further studies based on greater ease for large-scale synthesis. It showed superior activity to cisplatin against P388/cisplatin and like cisplatin showed significant and reproducible activity against the ip implanted B16 melanoma, ip implanted M5076 sarcoma, ip implanted P388 leukemia, and MX-1 human breast xenograft implanted under the renal capsule. Purity and stability (> 24 hours in saline) were evaluated by high-performance liquid chromatography and found to be suitable for development of a parenteral dosage form. Preliminary studies in a rat model (to be reported elsewhere) showed it to be less nephrotoxic than cisplatin on a molar basis and worthy of further study.

Original languageEnglish
Pages (from-to)997-1002
Number of pages6
JournalCancer Treatment Reports
Volume70
Issue number8
StatePublished - 1986

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