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Peptide Amphiphile Nanostructure-Heparin Interactions and their Relationship to Bioactivity

机译:肽两亲物纳米结构-肝素相互作用及其与生物活性的关系

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摘要

Heparin-protein interactions are important in many physiological processes, including angiogenesis, the growth of new blood vessels from existing ones. We have previously developed a highly angiogenic self-assembling gel, wherein the self-assembly process is triggered by interactions between heparin and peptide amphiphiles (PAs) with a consensus heparin binding sequence. In this report, this consensus sequence was scrambled and incorporated into a new peptide amphiphile in order to study its importance in heparin interaction and bioactivity. Heparin was able to trigger gel formation of the scrambled peptide amphiphile (SPA). Furthermore, the affinity of the scrambled molecule for heparin was unchanged as shown by isothermal titration calorimetry and high Förster resonance emission transfer efficiency. However, both the mobile fraction and the dissociation rate constant of heparin, using fluorescence recovery after photobleaching, were markedly higher in its interaction with the scrambled molecule implying a weaker association. Importantly, the scrambled peptide amphiphile- heparin gel had significantly less angiogenic bioactivity as shown by decreased tubule formation of sandwiched endothelial cells. Hence, we believe that the presence of the consensus sequence stabilizes the interaction with heparin and is important for the bioactivity of these new materials.
机译:肝素与蛋白质的相互作用在许多生理过程中都很重要,包括血管生成,已有血管的生长。我们以前已经开发了一种高度血管生成的自组装凝胶,其中自组装过程是由肝素和具有共同肝素结合序列的肽两亲物(PAs)之间的相互作用触发的。在本报告中,为了研究其在肝素相互作用和生物活性中的重要性,对该共有序列进行了打乱并将其并入新的肽两亲物中。肝素能够触发加扰肽两亲物(SPA)的凝胶形成。此外,如等温滴定量热法和高福斯特共振发射转移效率所表明的,混乱分子对肝素的亲和力没有改变。然而,使用光漂白后的荧光回收,肝素的可移动分数和解离速率常数均显着高于其与混乱分子的相互作用,表明缔合较弱。重要的是,如夹心内皮细胞的小管形成减少所示,加扰的肽两亲肝素凝胶的血管生成生物活性明显较低。因此,我们相信共有序列的存在稳定了与肝素的相互作用,并且对于这些新材料的生物活性很重要。

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