Induction of the differentiation of WEHI-3B D+ monomyelocytic leukemia cells by inhibitors of topoisomerase II
- PMID: 2170008
Induction of the differentiation of WEHI-3B D+ monomyelocytic leukemia cells by inhibitors of topoisomerase II
Abstract
Topoisomerase II has been suggested to have a role in the early events of differentiation. This possibility was evaluated by measuring the effects of inhibitors of topoisomerase II on the induction of the differentiation of WEHI-3B D+ monomyelocytic leukemia cells. Differentiation of this cell line was induced along the granulocytic pathway by treatment with the topoisomerase II inhibitors novobiocin (150-300 microM), teniposide (20-50 nM), etoposide (0.1 microM), elsamicin (0.5 microM), and doxorubicin (40 nM). Maturation was assessed by the morphological appearance of mature forms of the granulocytic lineage, an increase in cell surface Fc receptors, the ability to reduce nitroblue tetrazolium, and the loss of proliferative capacity. In contrast, the non-topoisomerase II-reactive agent cisplatin and the topoisomerase I-reactive drug camptothecin did not cause the maturation of WEHI-3B D+ cells. Aclacinomycin A and retinoic acid, which are known efficacious inducers of the differentiation of this cell line, affected topoisomerase II extracted from WEHI-3B D+ cells in vitro, causing concentration-dependent inhibition of the strand-passing activity of the enzyme. Treatment of WEHI-3B D+ cells with novobiocin at 150 microM for 3 h or with teniposide at 50 nM for 24 h resulted in a 2- to 3-fold increase in etoposide-induced protein-DNA cross-links. Nuclear proteins in 0.35 M NaCl extracts from cells treated with novobiocin at 150 microM for 3 h or with teniposide at 50 nM for 24 h showed a slight increase in topoisomerase II activity compared to untreated cells. No changes in topoisomerase II levels, as measured by immunoblotting, were detected after treatment of WEHI-3B D+ cells with 150 microM novobiocin or 50 nM teniposide during the first 2 days of treatment. At day 3 of treatment, however, a decrease in topoisomerase II was observed in cells treated with either drug, possibly due to decreased cellular proliferation consequent to cell differentiation. The findings support the conclusion that topoisomerase II may have a role in the induction of granulocytic differentiation of WEHI-3B D+ leukemia cells.
Similar articles
-
Development and characterization of a WEHI-3B D+ monomyelocytic leukemia cell line resistant to novobiocin and cross-resistant to other topoisomerase II-targeted drugs.Cancer Res. 1992 May 15;52(10):2782-90. Cancer Res. 1992. PMID: 1316227
-
Differentiation of WEHI-3B D+ monomyelocytic leukemia cells by retinoic acid and aclacinomycin A.Cancer Res. 1986 Mar;46(3):1189-94. Cancer Res. 1986. PMID: 3455881
-
Increased rate of adenosine triphosphate-dependent etoposide (VP-16) efflux in a murine leukemia cell line overexpressing the multidrug resistance-associated protein (MRP) gene.Cancer Res. 1995 Oct 1;55(19):4352-60. Cancer Res. 1995. PMID: 7671247
-
[Mechanisms of resistance to DNA topoisomerase II inhibitors].Gan To Kagaku Ryoho. 1991 Aug;18(10):1568-73. Gan To Kagaku Ryoho. 1991. PMID: 1651684 Review. Japanese.
-
Topoisomerase II can relax; novobiocin is a mitochondrial poison after all.Bioessays. 1990 Oct;12(10):493-4. doi: 10.1002/bies.950121008. Bioessays. 1990. PMID: 1964558 Review. No abstract available.
Cited by
-
Novobiocin-induced anti-proliferative and differentiating effects in melanoma B16.Br J Cancer. 1992 Feb;65(2):183-8. doi: 10.1038/bjc.1992.38. Br J Cancer. 1992. PMID: 1739614 Free PMC article.
-
Sphinganine potentiation of cellular differentiation induced by various anti-leukemia drugs in human leukemia cell line HL-60.Naunyn Schmiedebergs Arch Pharmacol. 1994 Nov;350(5):575-81. doi: 10.1007/BF00173029. Naunyn Schmiedebergs Arch Pharmacol. 1994. PMID: 7870198
-
Multiple resistance modulators combined with carboplatin for resistant malignancies: a pilot study.Invest New Drugs. 1997;15(4):267-77. doi: 10.1023/a:1005993705237. Invest New Drugs. 1997. PMID: 9547669 Clinical Trial.