Enhanced etoposide sensitivity following adenovirus-mediated human topoisomerase IIα gene transfer is independent of topoisomerase IIβ

Z. Zhou, L. A. Zwelling, R. Ganapathi, E. S. Kleinerman

Research output: Contribution to journalArticlepeer-review

11 Scopus citations

Abstract

The roles that the α and β isoforms of topoisomerase II (topo II) play in anticancer drug action were determined using MDA-VP etoposide-resistant human breast cancer cells and a newly constructed adenoviral vector containing the topo IIα gene (Ad-topo IIα). MDA-VP cells were more resistant to etoposide than to amsacrine and had more resistance to etoposide than did MDA-parental cells. MDA-VP cells also expressed lower topo IIα RNA and protein levels than parental cells but had comparable topo IIβ levels. After infection with Ad-topo IIα, topo IIα, RNA and protein levels increased significantly, as did the cells' sensitivity to etoposide. In contrast, topo IIβ levels remained constant with little alteration in the cells' sensitivity to amsacrine. Band-depletion immunoblotting assays indicated that topo IIα was depleted in etoposide-treated, Ad-topo IIα-transduced MDA-VP cells but not in amsacrine-treated cells. Topo IIβ was depleted in amsacrine-treated, Adtopo IIα-MDA-VP cells, with little change in the topo IIα levels. These results suggest that topo IIα gene transfer does not alter topo IIβ expression and that enhanced sensitivity to etoposide is therefore secondary to change in topo IIα levels. These studies support the theory that etoposide preferentially targets topo IIα, while amsacrine targets topo IIα.

Original languageEnglish (US)
Pages (from-to)747-751
Number of pages5
JournalBritish journal of cancer
Volume85
Issue number5
DOIs
StatePublished - Sep 1 2001

Keywords

  • Amsacrine
  • Drug targetting
  • Etoposide
  • Topoisomerase IIα
  • Topoisomerase IIβ

ASJC Scopus subject areas

  • Oncology
  • Cancer Research

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