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首页> 外文期刊>Advanced Functional Materials >Functional and Well-Defined -Sheet-Assembled Porous Spherical Shells by Surface-Guided Peptide Formation
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Functional and Well-Defined -Sheet-Assembled Porous Spherical Shells by Surface-Guided Peptide Formation

机译:通过表面引导肽形成的功能完好的组装好的多孔球形壳

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Polypeptides have attracted widespread attention as building blocks for complex materials due to their ability to form higher-ordered structures such as -sheets. However, the ability to precisely control the formation of well-defined -sheet-assembled materials remains challenging as -sheet formation tends to lead to ill-defined and unprocessable aggregates. This work reports a simple, rapid, and robust strategy to form well-defined peptide -sheet-assembled shells (i.e., hollow spheres) by employing surface-initiated N-carboxyanhydride ring-opening polymerization under a highly efficient surface-driven approach. The concept is demonstrated by the preparation of enzyme-degradable rigid shell architectures composed of H-bonded poly(L-valine) (PVal) grafts with porous and sponge-like surface morphology. The porous PVal-shells exhibit a remarkable and unprecedented ability to non-covalently entrap metal nanoparticles, proteins, drug molecules, and biorelevant polymers, which could potentially lead to a diverse range of biodegradable and functional platforms for applications ranging from therapeutic delivery to organic catalysis.
机译:多肽由于具有形成更高层次结构(例如-薄片)的能力而作为复杂材料的构建基块吸引了广泛的关注。然而,精确地控制良好定义的片材组装材料的形成的能力仍然具有挑战性,因为片材的形成倾向于导致不明确的和不可加工的聚集体。这项工作报告了一种简单,快速和稳健的策略,通过在高效的表面驱动方法下采用表面引发的N-羧基酐开环聚合反应,形成定义明确的肽-片状组装壳(即中空球)。通过制备可酶降解的刚性壳结构(由具有多孔和海绵状表面形态的H键合聚(L-缬氨酸)(PVal)接枝组成)证明了这一概念。多孔的PVal壳具有非共价捕获金属纳米颗粒,蛋白质,药物分子和生物相关聚合物的卓越能力,这可能潜在地导致从治疗递送到有机催化的各种生物降解和功能平台。

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