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Solid State Self-Assembly Mechanism of RADA16-I Designer Peptide

机译:RADA16-I设计肽的固态自组装机制

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摘要

We report that synthetic RADA16-I peptide transforms to β-strand secondary structure and develops intermolecular organization into β-sheets when stored in the solid state at room temperature. Secondary structural changes were probed using solid state nuclear magnetic resonance spectroscopy (ssNMR) and Fourier transform infrared spectroscopy (FTIR). Intermolecular organization was analyzed viawide-angle X-ray diffraction (WAXD). Observed changes in molecular structure and organization occurred on the time scale of weeks during sample storage at room temperature. We observed structural changes on faster time scales by heating samples above room temperature or by addition of water. Analysis of hydration effects indicates that water can enhance the ability of the peptide to convert to β-strand secondary structure and assemble into β-sheets. However, temperature dependent FTIR and time dependent WAXD data indicate that bound water may hinder the assembly of β-strands into β-sheets. We suggest that secondary structural transformation and intermolecular organization together produce a water-insoluble state. These results reveal insights into the role of water,in self-assembly of polypeptides with hydrophilic side chains, and have implications on future optimization of RADA16-I nanofiber production.
机译:我们报告说,当在室温下以固态存储时,合成的RADA16-I肽会转变为β链二级结构,并将分子间组织发展为β-折叠。使用固态核磁共振波谱(ssNMR)和傅里叶变换红外光谱(FTIR)探测二级结构变化。通过广角X射线衍射(WAXD)分析分子间组织。在室温下保存样品的几周时间内,观察到分子结构和组织的变化。通过将样品加热到室温以上或加水,我们观察到了更快时间尺度上的结构变化。对水合作用的分析表明,水可以增强肽转化为β链二级结构并组装成β折叠的能力。但是,温度相关的FTIR和时间相关的WAXD数据表明,结合的水可能会阻碍β链组装成β折叠。我们建议二级结构转化和分子间组织一起产生水不溶状态。这些结果揭示了对水在具有亲水性侧链的多肽的自组装中所起的作用的洞察力,并且对RADA16-I纳米纤维生产的未来优化具有影响。

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