Targeting the Contact Pathway of Coagulation for the Prevention and Management of Medical Device-Associated Thrombosis.

IF 3.6 2区 医学 Q2 HEMATOLOGY
Seminars in thrombosis and hemostasis Pub Date : 2024-10-01 Epub Date: 2023-04-12 DOI:10.1055/s-0043-57011
Abhishek Goel, Harsha Tathireddy, Si-Han Wang, Helen H Vu, Cristina Puy, Monica T Hinds, David Zonies, Owen J T McCarty, Joseph J Shatzel
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引用次数: 0

Abstract

Hemorrhage remains a major complication of anticoagulants, with bleeding leading to serious and even life-threatening outcomes in rare settings. Currently available anticoagulants target either multiple coagulation factors or specifically coagulation factor (F) Xa or thrombin; however, inhibiting these pathways universally impairs hemostasis. Bleeding complications are especially salient in the medically complex population who benefit from medical devices. Extracorporeal devices-such as extracorporeal membrane oxygenation, hemodialysis, and cardiac bypass-require anticoagulation for optimal use. Nonetheless, bleeding complications are common, and with certain devices, highly morbid. Likewise, pharmacologic prophylaxis to prevent thrombosis is not commonly used with many medical devices like central venous catheters due to high rates of bleeding. The contact pathway members FXI, FXII, and prekallikrein serve as a nexus, connecting biomaterial surface-mediated thrombin generation and inflammation, and may represent safe, druggable targets to improve medical device hemocompatibility and thrombogenicity. Recent in vivo and clinical data suggest that selectively targeting the contact pathway of coagulation through the inhibition of FXI and FXII can reduce the incidence of medical device-associated thrombotic events, and potentially systemic inflammation, without impairing hemostasis. In the following review, we will outline the current in vivo and clinical data encompassing the mechanism of action of drugs targeting the contact pathway. This new class of inhibitors has the potential to herald a new era of effective and low-risk anticoagulation for the management of patients requiring the use of medical devices.

以凝血接触途径为目标,预防和处理医疗器械相关血栓。
出血仍然是抗凝剂的主要并发症,在极少数情况下,出血会导致严重后果,甚至危及生命。目前可用的抗凝血剂要么针对多种凝血因子,要么专门针对凝血因子 (F) Xa 或凝血酶;然而,抑制这些途径会普遍影响止血效果。出血并发症在受益于医疗设备的复杂医疗人群中尤为突出。体外设备(如体外膜肺氧合、血液透析和心脏搭桥术)需要抗凝治疗才能达到最佳使用效果。然而,出血并发症很常见,某些设备的出血并发症发病率很高。同样,由于出血率高,许多医疗器械(如中心静脉导管)并不常用药物预防来防止血栓形成。接触途径成员 FXI、FXII 和前allkelikrein 是连接生物材料表面介导的凝血酶生成和炎症的纽带,可能是改善医疗器械血液相容性和血栓形成性的安全、可药用的靶点。最近的体内和临床数据表明,通过抑制 FXI 和 FXII 选择性地靶向凝血的接触途径,可以在不影响止血的情况下降低医疗器械相关血栓事件的发生率,并可能降低全身炎症的发生率。在下面的综述中,我们将概述目前的体内和临床数据,包括以接触途径为靶点的药物的作用机制。这一类新的抑制剂有可能预示着一个新时代的到来,即为需要使用医疗器械的患者提供有效、低风险的抗凝治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Seminars in thrombosis and hemostasis
Seminars in thrombosis and hemostasis 医学-外周血管病
CiteScore
8.80
自引率
21.10%
发文量
132
审稿时长
6-12 weeks
期刊介绍: Seminars in Thrombosis and Hemostasis is a topic driven review journal that focuses on all issues relating to hemostatic and thrombotic disorders. As one of the premiere review journals in the field, Seminars in Thrombosis and Hemostasis serves as a comprehensive forum for important advances in clinical and laboratory diagnosis and therapeutic interventions. The journal also publishes peer reviewed original research papers. Seminars offers an informed perspective on today''s pivotal issues, including hemophilia A & B, thrombophilia, gene therapy, venous and arterial thrombosis, von Willebrand disease, vascular disorders and thromboembolic diseases. Attention is also given to the latest developments in pharmaceutical drugs along with treatment and current management techniques. The journal also frequently publishes sponsored supplements to further highlight emerging trends in the field.
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