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不同凝血因子触发的抗凝血水凝胶中肝素的自适应释放。

Adaptive release of heparin from anticoagulant hydrogels triggered by different blood coagulation factors.

机构信息

Leibniz-Institute of Polymer Research Dresden, Max Bergmann Center of Biomaterials Dresden, Hohe Strasse 6, 01069 Dresden, Germany.

Leibniz-Institute of Polymer Research Dresden, Max Bergmann Center of Biomaterials Dresden, Hohe Strasse 6, 01069 Dresden, Germany.

出版信息

Biomaterials. 2017 Aug;135:53-61. doi: 10.1016/j.biomaterials.2017.04.044. Epub 2017 Apr 26.

Abstract

Feedback-controlled anticoagulant hydrogels were formed by crosslinking the anticoagulant heparin with star-shaped poly(ethylene glycol) using peptide linkers, which are selectively cleaved by different activated blood coagulation factors acting as proteolytic enzymes. Various cleavable peptide units, differing either in their thrombin turnover rates or in their responsiveness to factors activated earlier in the course of blood coagulation, were used for the formation of the biohybrid materials. Release triggered by the early coagulation factors Xa (FXa) or FXIIa/kallikrein was shown to enhance the efficiency of the released anticoagulant. Furthermore, FXa-cleavable gels enabled a faster release of heparin, which was attributed to the lower affinity of the factor for heparin. Combining early and fast responses, FXa-cleavable gels were shown to provide anticoagulant protection of biomaterial surfaces at low levels of released heparin in human whole-blood incubation experiments. The results demonstrate the potential for employing biomolecular circuits in the design of functional biomaterials to tailor the adaptive delivery of bioactive molecules.

摘要

通过使用肽接头将抗凝剂肝素与星形聚乙二醇交联,形成反馈控制的抗凝水凝胶,这些肽接头可被作为蛋白水解酶的不同激活的血液凝固因子选择性切割。使用各种可切割的肽单元,其在凝血过程早期被激活的因子的血栓周转率或对其的响应性不同,用于形成生物杂化材料。由早期凝血因子 Xa(FXa)或 FXIIa/激肽引发的释放被证明可提高释放的抗凝剂的效率。此外,FXa 可切割的凝胶可使肝素更快地释放,这归因于因子对肝素的亲和力较低。通过结合早期和快速反应,FXa 可切割的凝胶在人全血孵育实验中以低水平释放肝素的情况下,显示出对生物材料表面的抗凝保护作用。结果表明,在设计功能生物材料时,可以采用生物分子回路来定制生物活性分子的适应性输送。

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