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Elastin-like Polypeptide Diblock Copolymers Self-Assemble into Weak Micelles

机译:弹性蛋白样多肽二嵌段共聚物自组装成弱胶束

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摘要

The self-assembly of synthetic diblock copolymers has been extensively studied experimentally and theoretically. In contrast, self-assembly of polypeptide diblock copolymers has so far been mostly studied experimentally. We discovered that the theory developed for synthetic diblock copolymer does not fully explain the self-assembly of elastin-like polypeptide diblock copolymers, leading us to generalize the theory to make it applicable for these polypeptides. We demonstrated that elastin-like polypeptide diblocks self-assemble into weak micelles with dense cores and almost unstretched coronas, a state not previously observed for synthetic diblock copolymers. Weak micelles form if the surface tension at the core–corona interface is low compared to that expected of a micelle with a dense core. The predictions of the theory of weak micelles for the critical micelle temperature, hydrodynamic radius, and aggregation number of elastin-like polypeptide diblocks are in reasonable agreement with the experimentally measured values. The unique and unprecedented control of amphiphilicity in these recombinant peptide polymers reveals a new micellar state that has not been previously observed in synthetic diblock copolymer systems.
机译:合成二嵌段共聚物的自组装已在实验和理论上进行了广泛的研究。相反,迄今为止,多肽二嵌段共聚物的自组装主要是通过实验研究的。我们发现,为合成二嵌段共聚物开发的理论不能完全解释弹性蛋白样多肽二嵌段共聚物的自组装,这使我们对其进行了概括以使其适用于这些多肽。我们证明,弹性蛋白样多肽二嵌段自组装成具有致密核心和几乎未拉伸的电晕的弱胶束,这种状态以前从未在合成二嵌段共聚物中观察到。如果在芯-电晕界面处的表面张力低于具有密集芯的胶束的预期表面张力,则会形成弱胶束。对于临界胶束温度,流体动力学半径和弹性蛋白样多肽二嵌段的聚集数,弱胶束理论的预测与实验测量值合理地吻合。这些重组肽聚合物中两亲性的独特而空前的控制揭示了新的胶束状态,这是以前在合成的二嵌段共聚物系统中尚未观察到的。

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