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The role of topoisomerase IIα and HER-2 in predicting sensitivity to anthracyclines in breast cancer patients

Journal

CANCER TREATMENT REVIEWS
Volume 35, Issue 8, Pages 662-667

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.ctrv.2009.08.006

Keywords

Topoisomerase II alpha; HER-2; Anthracycline; Breast cancer; Prediction

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Funding

  1. Associazione Prato, Italy
  2. Associazione Italiana Ricerca Cancro, Milan, Italy

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Human epidermal growth factor receptor-2 (HER-2) and topoisomerase II alpha (topo Hot) co-inhabit chromosome 17. In the search for predictive biomarkers to refine clinical prescription of cytotoxic agents. both HER-2 and topo II alpha are under exploration for their potential role in identifying individuals with early breast cancer who may benefit from anthracycline therapy. Whilst recent meta-analyses support a predictive role for HER-2 amplification, it remains unclear whether HER-2 is the critical biomarker or whether it is a surrogate marker for topo II alpha alteration, a known drug target of anthracyclines. The major limitation in considering HER-2 as a single marker is heterogeneity within the subgroups of HER-2 positive and HER-2 negative disease. For topo II alpha, current data is inconclusive. Issues plaguing this field are technical variability in marker definition, complex regulation pathway of topo II alpha and lack of prospective, adequately powered studies. With current evidence, neither HER-2 nor topo II alpha gene status can be considered clinically valuable markers for anthracycline benefit. This paper will focus on issues relating to reliable detection and predictive analyses of HER-2 and topo II alpha, and highlight potential developments in improving individualized approach to anthracycline use in early breast cancer patients. (C) 2009 Elsevier Ltd. All rights reserved.

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