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Nucleic acid peptide nanogels for the treatment of bacterial keratitis

机译:核酸肽纳米凝胶治疗细菌性角膜炎

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Cage-shaped nucleic acid nanocarriers are promising molecular scaffolds for the organization of polypeptides. However, there is an unmet need for facile loading strategies that truly emulate nature's host-guest systems to drive encapsulation of antimicrobial peptides (AMPs) without loss of biological activity. Herein, we develop DNA nanogels with rapidin situloading of L12 peptide during the thermal annealing process. By leveraging the binding affinity of L12 to the polyanionic core, we successfully confine the AMPs within the DNA nanogel. We report that the thermostability of L12 in parallel with the high encapsulation efficiency, low toxicity and sustained drug release of the pre-loaded L12 nanogels can be translated into significant antimicrobial activity. Using anS. aureusmodel of infectious bacterial keratitis, we observe fast resolution of clinical symptoms and significant reduction of bacterial bioburden. Collectively, this study paves the way for the development of DNA nanocarriers for caging AMPs with immense significance to address the rise of resistance.
机译:Cage-shaped核酸人们有前途的分子的支架组织多肽。一个简单加载策略,未满足的需求真正模仿大自然的主-客体系统封装的抗菌肽(安培),而不失去生物活性。在此,我们发展与rapidin DNA纳米凝胶在热situloading L12肽退火过程。的亲和力L12阴离子的核心,我们成功地限制了安培在DNAnanogel。L12与高封装效率、低毒性和持续的药物发布的预装L12纳米凝胶翻译成显著的抗菌活动。细菌性角膜炎,我们观察到的快速解决临床症状和显著减少细菌的微生物污染水平。为DNA的发展铺平了道路人们与巨大的闭锁安培意义解决抗药性。

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