Abstract
Angiogenesis is an important event in tumor growth. We evaluated the contribution of endogenous bradykinin to tumor-associated angiogenesis and tumor growth using pharmacological approaches in mice bearing sarcoma 180 cells. The weight of implanted tumors increased in parallel with increased hemoglobin contents (a parameter to evaluate angiogenesis) over a 20-day experimental period. Daily administration of bradykinin B2-receptor antagonists, Hoe140 (0.1 and 1 mg /kg per day, local injection) or FR173657 (30 mg /kg per day, p.o.), significantly suppressed the increment in angiogenesis and tumor weight, but a Bi -receptor antagonist, desArg10-Hoe140 (1 mg /kg per day), did not. Administration of a plasma kallikrein inhibitor, soybean trypsin inhibitor (3 mg/site per day), significantly suppressed angiogenesis and tumor growth. In contrast, bradykinin-degrading enzyme inhibitors, Captopril and phosphoramidon (500 μg/site per day), enhanced angiogenesis and increased tumor weight. Our results suggest that brady-kinin, produced by plasma kallikrein or plasma kallikrein-like enzymes, promote tumor-associated angio-genesis and tumor growth in vivo.
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