Abstract
Platelet inhibition has been considered an effective strategy for combating cancer metastasis and compromising disease malignancy although recent clinical data provided evidence that long-term platelet inhibition might increase incidence of cancer deaths in initially cancer-free patients. In the present study we demonstrated that dual anti-platelet therapy based on aspirin and clopidogrel (ASA+Cl), a routine regiment in cardiovascular patients, when given to cancer-bearing mice injected orthotopically with 4T1 breast cancer cells, promoted progression of the disease and reduced mice survival in association with induction of vascular mimicry (VM) in primary tumour. In contrast, treatment with ASA+Cl or platelet depletion did reduce pulmonary metastasis in mice, if 4T1 cells were injected intravenously. In conclusion, distinct platelet-dependent mechanisms inhibited by ASA+Cl treatment promoted cancer malignancy and VM in the presence of primary tumour and afforded protection against pulmonary metastasis in the absence of primary tumour. In view of our data, long-term inhibition of platelet function by dual anti-platelet therapy (ASA+Cl) might pose a hazard when applied to a patient with undiagnosed and untreated malignant cancer prone to undergo VM.
Highlights
Platelets contribute to tumour cell growth as well as metastatic spread [1]
In the present study we demonstrated that dual anti-platelet therapy based on aspirin and clopidogrel (ASA+Cl), a routine regiment in cardiovascular patients, when given to cancer-bearing mice injected orthotopically with 4T1 breast cancer cells, promoted progression of the disease and reduced mice survival in association with induction of vascular mimicry (VM) in primary tumour
Survival of tumour-bearing mice receiving dual antiplatelet therapy based on aspirin (ASA) and clopidogrel (Cl) (4T1+ASA/Cl group, n=40) was diminished as compared with control tumour-bearing mice not subjected to the ASA+Cl treatment (4T1 control group, n=80) (P=0.0259) (Figure 1)
Summary
An increase in platelet number inversely correlates with cancer patient survival [2]. Defective platelet function or reduced platelet count is associated with decreased metastasis [3,4,5]. Given the possible role of platelets in promotion of malignant diseases and metastatic spread, effects of anti-platelet therapy on metastasis have been intensively studied in animal models [3, 6, 7] as well as in humans. Aspirin, inhibiting cyclooxygenase-1 (COX-1) – derived thromboxane A2 (TXA2) synthesis in platelets (and platelet aggregation and degranulation) was the first anti-platelet drug used to combat cancer metastasis [15] Today there is overwhelming evidence from epidemiological studies [8,9,10,11,12] and clinical trials [13, 14] that supports the involvement of platelets in metastatic spread.
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