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定量研究多价纳米医学靶向

A quantitative view on multivalent nanomedicine targeting.

机构信息

Department of Biomedical Engineering, Institute of Complex Molecular Systems (ICMS), Eindhoven University of Technology (TUE), Eindhoven 5612 AZ, the Netherlands.

Electric Ant Lab, Science Park 106, 1098 XG Amsterdam, the Netherlands.

出版信息

Adv Drug Deliv Rev. 2021 Feb;169:1-21. doi: 10.1016/j.addr.2020.11.010. Epub 2020 Nov 29.

Abstract

Although the concept of selective delivery has been postulated over 100 years ago, no targeted nanomedicine has been clinically approved so far. Nanoparticles modified with targeting ligands to promote the selective delivery of therapeutics towards a specific cell population have been extensively reported. However, the rational design of selective particles is still challenging. One of the main reasons for this is the lack of quantitative theoretical and experimental understanding of the interactions involved in cell targeting. In this review, we discuss new theoretical models and experimental methods that provide a quantitative view of targeting. We show the new advancements in multivalency theory enabling the rational design of super-selective nanoparticles. Furthermore, we present the innovative approaches to obtain key targeting parameters at the single-cell and single molecule level and their role in the design of targeting nanoparticles. We believe that the combination of new theoretical multivalent design and experimental methods to quantify receptors and ligands aids in the rational design and clinical translation of targeted nanomedicines.

摘要

虽然选择性递药的概念早在 100 多年前就已被提出,但迄今为止,还没有靶向纳米药物被临床批准。已经广泛报道了用靶向配体修饰的纳米颗粒来促进治疗剂向特定细胞群的选择性递送。然而,选择性颗粒的合理设计仍然具有挑战性。造成这种情况的一个主要原因是缺乏对细胞靶向中涉及的相互作用的定量理论和实验理解。在这篇综述中,我们讨论了提供靶向定量观点的新理论模型和实验方法。我们展示了多价理论的新进展,使超选择性纳米颗粒的合理设计成为可能。此外,我们还介绍了在单细胞和单分子水平上获得关键靶向参数的创新方法及其在靶向纳米颗粒设计中的作用。我们相信,新的理论多价设计与定量受体和配体的实验方法相结合,有助于靶向纳米药物的合理设计和临床转化。

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