Most heart attacks and strokes are caused by blood clots (thrombi) that block the vasculature. Because disease-causing arterial thrombosis depends on blood platelets, platelet inhibitors such as aspirin and clopidogrel effectively decrease the risk of thrombosis; however, they also impair platelet-dependent hemostasis that staunches bleeding from wounds and can therefore produce excessive bleeding. Experimental studies show that a reduction in the number of platelets also inhibits thrombosis, but these treatments also interfere with platelet function. Because normal hemostasis requires that the platelet concentration remain within a physiological range in the circulation, we evaluated whether lowering the number of circulating platelets--but only to a value still within the normal range--by inhibiting platelet formation in the bone marrow inhibits acute thrombogenesis in baboons. We reduced the platelet count with an inhibitor against the megakaryocyte-promoting hormone thrombopoietin and then showed that experimental occlusive thrombogenesis on collagen-coated vascular grafts was reduced, without impairment of primary hemostasis. These results suggest that suppressing platelet production without interfering with the hemostatic function of platelets may offer a safe alternative to current therapies for prevention of stroke and heart attack triggered by blood clotting.
Safety and antithrombotic efficacy of moderate platelet count reduction by thrombopoietin inhibition in primates.
抑制血小板生成素降低中度血小板计数在灵长类动物中的安全性和抗血栓疗效
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作者:Tucker Erik I, Marzec Ulla M, Berny Michelle A, Hurst Sawan, Bunting Stuart, McCarty Owen J T, Gruber András, Hanson Stephen R
| 期刊: | Science Translational Medicine | 影响因子: | 14.600 |
| 时间: | 2010 | 起止号: | 2010 Jun 23; 2(37):37ra45 |
| doi: | 10.1126/scitranslmed.3000697 | 研究方向: | 其它 |
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