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设计肽作为模型自组装纳米系统:表征及潜在生物医学应用

Designed peptides as model self-assembling nanosystems: characterization and potential biomedical applications.

作者信息

Panda Jiban J, Kaul Ankur, Alam Shadab, Babbar Anil K, Mishra Anil K, Chauhan Virander S

机构信息

International Centre for Genetic Engineering & Biotechnology, New Delhi, India.

出版信息

Ther Deliv. 2011 Feb;2(2):193-204. doi: 10.4155/tde.10.93.

Abstract

Synthesis of nanomaterials via 'molecular self-assembly' allows one to define the properties of the nanomaterial by rational design of the individual constituents. Use of peptides for self-assembly offers the ease of design and synthesis, and provides higher biofunctionality and biocompatibility to nanomaterials. Our work focused on the synthesis, characterization and potential biomedical applications of small self-assembled peptide-based nanosystems. We demonstrated that dipeptides containing the conformational restricting residue alpha,beta-dehydrophenylalanine, self-assembled into nanovesicular and nanotubular structures. The nanosystems could encapsulate and release anticancer drugs, showed enhanced stability to proteinase K degradation, a property crucial for them to have a high in vivo half-life, and exhibited no cytotoxicity towards cultured mammalian cells. The dipeptide nanostructures were easily taken up by cells and could evade uptake by reticuloendothelial systems when injected into healthy laboratory animals. Thus, small self-assembling peptides may offer novel scaffolds for the future design of nanostructures with potential applications in the field of drug delivery.

摘要

通过“分子自组装”合成纳米材料,能够通过合理设计单个成分来定义纳米材料的性质。使用肽进行自组装具有设计和合成简便的优点,并为纳米材料提供更高的生物功能性和生物相容性。我们的工作聚焦于基于小自组装肽的纳米系统的合成、表征及其潜在的生物医学应用。我们证明,含有构象限制残基α,β-脱氢苯丙氨酸的二肽能自组装成纳米囊泡和纳米管结构。这些纳米系统能够包封和释放抗癌药物,对蛋白酶K降解表现出增强的稳定性,这一特性对于它们具有高体内半衰期至关重要,并且对培养的哺乳动物细胞无细胞毒性。当注射到健康实验动物体内时,二肽纳米结构很容易被细胞摄取,并且能够逃避网状内皮系统的摄取。因此,小型自组装肽可能为未来设计具有药物递送领域潜在应用的纳米结构提供新型支架。

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