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Initiation of Aspirin Therapy Modulates Angiogenic Protein Levels in Women with Breast Cancer Receiving Tamoxifen Therapy
Authors:Chris E Holmes  Jagoda Jasielec  Jamie E Levis  Joan Skelly  Hyman B Muss
Institution:1.Department of Medicine, University of Vermont, Burlington, Vermont, USA;2.Department of Biostatistics, University of Vermont, Burlington, Vermont, USA;3.Department of Medicine, University of North Carolina, Chapel Hill, North Carolina, USA
Abstract:Aspirin has a range of antineoplastic properties linked to inhibition of cyclooxygenase enzymes in tumor cells, platelet inhibition and to inhibition of angiogenesis. We undertook a prospective study to determine the influence of a 45‐day course of aspirin therapy on circulating and intraplatelet levels of selected proangiogenic (vascular endothelial growth factor VEGF]) and antiangiogenic (thrombospondin‐1 TSP‐1]) proteins, and platelet protein release in women diagnosed with breast cancer who were receiving tamoxifen therapy. Initiation of aspirin therapy increases serum and intraplatelet levels of TSP‐1 without a corresponding increase in VEGF levels. Following aspirin therapy, VEGF levels decreased (relative to pretreatment levels) while TSP‐1 returned to pretreatment levels. Plasma TSP‐1 and VEGF levels did not change on aspirin therapy. Aspirin use also decreased thrombin receptor mediated release of TSP‐1 and VEGF from platelets. The selective impact on platelet angiogenic protein content and release supports one mechanism by which aspirin can modify the angiogenic balance in women receiving tamoxifen therapy. Aspirin therapy appears to favor an overall antiangiogenic balance in women with breast cancer who are receiving tamoxifen therapy.
Keywords:platelet activation  VEGF  TSP‐  1 tamoxifen  breast cancer
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