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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Advanced drug delivery systems for antithrombotic agents.
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Advanced drug delivery systems for antithrombotic agents.

机译:先进的抗血栓药物递送系统。

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摘要

Despite continued achievements in antithrombotic pharmacotherapy, difficulties remain in managing patients at high risk for both thrombosis and hemorrhage. Utility of antithrombotic agents (ATAs) in these settings is restricted by inadequate pharmacokinetics and narrow therapeutic indices. Use of advanced drug delivery systems (ADDSs) may help to circumvent these problems. Various nanocarriers, affinity ligands, and polymer coatings provide ADDSs that have the potential to help optimize ATA pharmacokinetics, target drug delivery to sites of thrombosis, and sense pathologic changes in the vascular microenvironment, such as altered hemodynamic forces, expression of inflammatory markers, and structural differences between mature hemostatic and growing pathological clots. Delivery of ATAs using biomimetic synthetic carriers, host blood cells, and recombinant fusion proteins that are activated preferentially at sites of thrombus development has shown promising outcomes in preclinical models. Further development and translation of ADDSs that spare hemostatic fibrin clots hold promise for extending the utility of ATAs in the management of acute thrombotic disorders through rapid, transient, and targeted thromboprophylaxis. If the potential benefit of this technology is to be realized, a systematic and concerted effort is required to develop clinical trials and translate the use of ADDSs to the clinical arena.
机译:尽管在抗血栓药物治疗方面取得了持续的成就,但是在处理血栓形成和出血高风险患者方面仍然存在困难。在这些情况下抗血栓形成剂(ATA)的使用受到药代动力学不足和治疗指标狭窄的限制。使用先进的药物输送系统(ADDS)可能有助于避免这些问题。各种纳米载体,亲和配体和聚合物涂层提供的ADDS具有帮助优化ATA药代动力学,将药物靶向血栓形成的位点以及感知血管微环境中病理变化的潜力,例如改变的血流动力学力,炎症标志物的表达和成熟的止血和生长中的病理性凝块之间的结构差异。使用仿生合成载体,宿主血细胞和在血栓形成部位优先被激活的重组融合蛋白递送ATA在临床前模型中已显示出令人鼓舞的结果。多余的止血纤维蛋白凝块的ADDS的进一步开发和翻译有望通过快速,短暂和有针对性的血栓预防扩大ATA在急性血栓形成疾病管理中的应用。如果要实现该技术的潜在利益,则需要系统一致的努力来开展临床试验并将ADDS的使用转化到临床领域。

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