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Fifty years with aspirin and platelets

期刊

BRITISH JOURNAL OF PHARMACOLOGY
卷 180, 期 1, 页码 25-43

出版社

WILEY
DOI: 10.1111/bph.15966

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aspirin; cardiac pharmacology; clinical pharmacology; cyclo-oxygenase; pharmacodynamics; platelets; thrombocytes; prostaglandins

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This passage describes the significant impact of Sir John Vane's publication on the pharmacological effects of aspirin and similar drugs, as well as the subsequent discovery of the platelet arachidonic acid metabolism pathway. It also emphasizes the importance of low-dose aspirin as an antiplatelet drug.
In 2021, we reached the 50th anniversary of the publication of Sir John Vane's seminal paper in Nature New Biology describing the experiments supporting his mechanistic hypothesis that inhibition of prostaglandin synthesis might explain the main pharmacological effects of aspirin and aspirin-like drugs, that is, reduction in pain, fever and inflammation. Bengt Samuelsson's subsequent discoveries elucidating the cyclooxygenase pathway of platelet arachidonic acid metabolism motivated my research interest towards measuring platelet thromboxane A(2) biosynthesis as a tool to investigate the clinical pharmacology of cyclooxygenase inhibition by aspirin in health and disease. What followed was a long, winding road of clinical research leading to the characterization of low-dose aspirin as a life-saving antiplatelet drug that still represents the cornerstone of antithrombotic therapy. Having witnessed and participated in these 50 years of aspirin research, I thought of providing a personal testimony of how things developed and eventually led to a remarkable success story of independent research.

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