纳米载体
化学
神经炎症
胞浆
肽
生物物理学
细胞生物学
超分子化学
小胶质细胞
细胞内
药物输送
纳米凝胶
生物相容性材料
蛋白质聚集
生物化学
纳米技术
HDAC6型
双重角色
神经退行性变
HEK 293细胞
α分泌酶
转运蛋白
赖氨酸
作者
Doudou Hu,Tiandong Li,Jian He,Yujian Jiang,Yeyuan Wang,Jingchen Sun
摘要
Delivering protein therapeutics to the brain through nanocarriers requires overcoming both the blood-brain barrier (BBB) and intracellular lysosomal degradation. Here, we report a silk-based supramolecular protein delivery platform that addresses these dual physiological barriers. Two phenolic compounds are grafted onto silk sericin (SS), a biocompatible and bioactive natural protein, yielding phenolic SS capable of assembling with protein cargos via supramolecular interactions. To facilitate BBB penetration, the iRGD peptide is incorporated to enable transcytosis via the bystander effect. Phenolic modification alters the ratio of amino to carboxyl groups on SS, thereby tuning its isoelectric point. In acidic lysosomes, the nanocomplex undergoes a surface charge reversal from negative to positive, promoting lysosomal escape and cytosolic release of catalase. In parallel, phenolic SS exhibits intrinsic anti-inflammatory activity, repolarizing activated microglia toward an anti-inflammatory phenotype. In APP/PS1 transgenic mice, systemic administration of the nanocomplex reduces oxidative stress and neuroinflammation, leading to significant improvements in cognitive function, compared to a non-charge-reversal control. Collectively, this strategy provides a versatile and translatable framework for engineering protein-based nanocarriers to deliver protein therapeutics for neurodegenerative disease treatments.
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