Breast cancer angiogenesis - New approaches to therapy via antiangiogenesis, hypoxic activated drugs, and vascular targeting

Adrian L. Harris, Huatang Zhang, Amir Moghaddam, Steve Fox, Prudence Scott, Adam Pattison, Kevin Gatter, Ian Stratford, Roy Bicknell

    Research output: Contribution to journalArticlepeer-review

    Abstract

    Several groups have shown that quantitation of tumor angiogenesis by counting blood vessels in primary breast cancer gives an independent assessment of prognosis. Poor prognosis is associated with high blood vessel counts. We have shown that the rate of cell division in endothelial cells is much higher in breast tumours than in normal breast. Breast cancer cell lines and primary human breast tumours express a wide range of vascular growth factors, including VEGF, placenta growth factor, pleiotrophin, TGFβ1, acidic and basic FGF, and platelet-derived endothelial cell growth factor. Inhibiting angiogenesis by blocking vascular growth factors would be difficult with highly specific agents, but drugs with a broader spectrum of antagonism may be effective. We have developed several suramin analogues which are less toxic than suramin in vivo but more potent in inhibiting angiogenesis, and these have been developed for Phase I. A combination of anti-angiogenesis agents with drugs activated by hypoxia may also be useful, because anti-angiogenesis alone may not kill cells, whereas activation of hypoxic drugs could synergize. New endpoints may be necessary because inhibition of new blood vessel formation may not cause tumour regression. Thus, the endpoint of stable disease and biochemical assessment of inhibition of angiogenesis may be much more important in therapeutic studies and for drug development in the future. The prognostic importance of angiogenesis suggests that this should be a major new therapeutic target.
    Original languageEnglish
    Pages (from-to)97-108
    Number of pages11
    JournalBreast Cancer Research and Treatment
    Volume38
    Issue number1
    DOIs
    Publication statusPublished - 1996

    Keywords

    • Angiogenesis
    • Angiogenesis inhibitors
    • Gene therapy
    • Hypoxic activated pro-drugs
    • Prognosis
    • Vascular targeting

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