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Sculpting the blank slate: How fibrin's support of vascularization can inspire biomaterial design

机译:雕刻空白板:纤维蛋白对血管化的支持如何激发生物材料设计

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摘要

Fibrin is the primary extracellular constituent of blood clots, and plays an important role as a provisional matrix during wound healing and tissue remodeling. Fibrin-based biomaterials have proven their utility as hemostatic therapies, scaffolds for tissue engineering, vehicles for controlled release, and platforms for culturing and studying cells in three dimensions. Nevertheless, fibrin presents a complex milieu of signals to embedded cells, many of which are not well understood. Synthetic extracellular matrices (ECMs) provide a blank slate that can ostensibly be populated with specific bioactive cues, including growth factors, growth factor binding motifs, adhesive peptides and peptide crosslinks susceptible to proteases, thereby enabling a degree of customization for specific applications. However, the continued evolution and improvement of synthetic ECMs requires parallel efforts to deconstruct native ECMs and decipher the cues they provide to constituent cells. The objective of this review is to reintroduce fibrin, a protein with a well-characterized structure and biochemistry, and its ability to support angiogenesis specifically. Although fibrin's structure function relationships have been studied for decades, opportunities to engineer new and improved synthetic hydrogels can be realized by further exploiting fibrin's inspiring design. (C) 2013 Acta Materialia Inc. Published by Elsevier Ltd. All rights reserved.
机译:纤维蛋白是血凝块的主要细胞外成分,在伤口愈合和组织重塑中作为临时基质发挥重要作用。基于纤维蛋白的生物材料已被证明可以用作止血疗法,组织工程支架,控释载体以及用于培养和研究三维细胞的平台。然而,血纤蛋白向嵌入细胞呈现出复杂的信号环境,其中许多还没有被很好地理解。合成的细胞外基质(ECM)提供了一块空白板块,表面上似乎可以布满特定的生物活性线索,包括生长因子,生长因子结合基序,粘附性肽和易受蛋白酶影响的肽交联,从而可以针对特定应用进行一定程度的定制。但是,合成ECM的不断发展和改进需要并行努力来解构天然ECM,并破译它们提供给组成细胞的线索。这篇综述的目的是重新引入纤维蛋白,一种具有良好特征的结构和生物化学的蛋白质,及其特异性支持血管生成的能力。尽管已经研究了纤维蛋白的结构功能关系数十年,但通过进一步利用纤维蛋白的启发性设计,可以实现设计新的和改良的合成水凝胶的机会。 (C)2013 Acta Materialia Inc.,由Elsevier Ltd.发行。保留所有权利。

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