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Primary hemostasis

机译:原发性止血

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摘要

Objective: To review the current understanding of the mechanisms responsible for primary hemostasis and to give an overview of primary hemostatic syndromes in small animal patients. Current and future therapeutic options for dysfunction of primary hemostasis are discussed. Data sources: A thorough search of the human and veterinary literature using the keywords platelets, primary hemostasis, von Willebrand factor (vWF), von Willebrand disease, aspirin, thromboxane, and aggregation, were performed. Databases searched included OVID Medline, Pubmed, and CAB abstracts. Conclusions: Primary hemostasis occurs when platelets adhere to an injured or disrupted endothelial surface. Adherence is followed by activation, or the release of platelet granule contents. The agonists released from platelet granules recruit additional platelets and induce their activation and aggregation. Adhesion, activation, and aggregation are mediated by different receptors and ligands depending on the local blood flow conditions.vWF and adenosine diphosphate are the primary mediators of adhesion, activation, and aggregation under high shear conditions. During low shear conditions collagen, fibronectin, and laminin mediate adhesion, thromboxane A_2 promotes activation, while aggregation is mediated by glycoprotein Ib-IX-V (GP Ib-IX-V) and fibrinogen. Knowledge of the receptor interactions during different blood flow conditions is crucial to the understanding of the various inhibitors of primary hemostasis available to clinicians.
机译:目的:回顾目前对引起原发性止血的机制的了解,并概述小动物患者的原发性止血综合症。讨论了目前和将来针对原发性止血功能障碍的治疗选择。数据来源:使用关键词血小板,原发性止血,von Willebrand因子(vWF),von Willebrand病,阿司匹林,血栓烷和聚集,对人类和兽医文献进行了彻底搜索。搜索的数据库包括OVID Medline,Pubmed和CAB摘要。结论:当血小板粘附于受损或破裂的内皮表面时,就会发生原发性止血。粘附之后是活化或血小板颗粒内容物的释放。从血小板颗粒释放的激动剂募集额外的血小板并诱导其活化和聚集。黏附,活化和聚集由不同的受体和配体介导,取决于局部血流状况。vWF和二磷酸腺苷是高剪切条件下黏附,活化和聚集的主要介质。在低剪切条件下,胶原蛋白,纤连蛋白和层粘连蛋白介导粘附,血栓烷A_2促进活化,而聚集由糖蛋白Ib-IX-V(GP Ib-IX-V)和纤维蛋白原介导。了解不同血流条件下的受体相互作用对于了解临床医生可利用的各种主要止血抑制剂至关重要。

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