In Vitro Activity of Bleomycin, Tallysomycin SlOb, and Liblomycin against Fresh Human Tumor Cells

Elias A. Tueni, Robert A. Newman, Fraser L. Baker, Jaffer A. Ajani, Dominic Fan, Gary Spitzer

Research output: Contribution to journalArticlepeer-review

7 Scopus citations

Abstract

The objective of this study was to compare the relative in vitro cytotoxicity of bleomycin to that of two newer-generation analogues, tallysomycin SI Ob and liblomycin. The latter compound is of particular interest as it has recently been shown in preclinical studies to be free of a potential to cause pulmonary injury and yet to possess only a minor potential to produce myelotoxicity. Using the adhesive tumor cell culture system, we evaluated the activity of these three drugs against a panel of 13 human tumors of various types. The range of concentrations chosen was determined and normalized using a nonleukemic permanent mouse hematopoietic progenitor cell line. Those drug concentrations achieving 90% inhibition of growth (IC90) against the murine cell line were: 6.11 pM bleomycin; 7.53 pM tallysomycin S10b; and 0.6 mm liblomycin. When tested against fresh human tumors at equally myelotoxic IC90 concentrations, bleomycin and tallysomycin S10b (nonmyelotoxic compounds) both achieved 90% growth inhibition of all tumors, while liblomycin (a myelotoxic compound) produced an IC90 inhibition in 69% of all tumors. A comparison of drug IC90 values against individual fresh tumors indicated a correlation between bleomycin and its structurally related analogue tallysomycin SlOb. No such correlation, however, was seen with liblomycin in comparison to either bleomycin or tallysomycin S10b. The relative activity of liblomycin versus that of bleomycin and tallysomycin SlOb varied with individual tumors tested. The response rate of liblomycin, a myelotoxic compound within this normalized range, appears promising. These data represent the first comparison of liblomycin to bleomycin against a spectrum of fresh human tumors using a stem cell assay technique.

Original languageEnglish (US)
Pages (from-to)1099-1102
Number of pages4
JournalCancer Research
Volume49
Issue number5
StatePublished - Mar 1 1989

ASJC Scopus subject areas

  • Oncology
  • Cancer Research

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