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Utilizing Inverse Emulsion Polymerization To Generate Responsive Nanogels for Cytosolic Protein Delivery

机译:利用逆乳液聚合产生响应纳米孔,用于细胞溶蛋白递送

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摘要

Therapeutic biologics have various advantages over synthetic drugs in terms of selectivity, their catalytic nature, and, thus, therapeutic efficacy. These properties offer the potential for more effective treatments that may also overcome the undesirable side effects observed due to off-target toxicities of small molecule drugs. Unfortunately, systemic administration of biologics is challenging due to cellular penetration, renal clearance, and enzymatic degradation difficulties. A delivery vehicle that can overcome these challenges and deliver biologics to specific cellular populations has the potential for significant therapeutic impact. In this work, we describe a redox-responsive nanoparticle platform, which can encapsulate hydrophilic proteins and release them only in the presence of a reducing stimulus. We have formulated these nanoparticles using an inverse emulsion polymerization (IEP) methodology, yielding inverse nanoemulsions, or nanogels. We have demonstrated our ability to overcome the liabilities that contribute to activity loss by delivering a highly challenging cargo, functionally active caspase-3, a cysteine protease susceptible to oxidative and self-proteolytic insults, to the cytosol of HeLa cells by encapsulation inside a redox-responsive nanogel.
机译:治疗生物学在选择性,催化性质方面具有各种优于合成药物的优点,以及其催化性质,以及治疗效果。这些性质提供更有效治疗的可能性,这些处理也可能克服由于小分子药物的偏离毒性毒性而观察到的不希望的副作用。遗憾的是,由于细胞渗透,肾间隙和酶促降解困难,生物制剂的全身施用是挑战性的。可以克服这些挑战并向特定细胞群赋予生物学的递送车具有显着的治疗局部的可能性。在这项工作中,我们描述了一种氧化还原响应纳米粒子平台,其可以包封亲水蛋白质并仅在存在还原刺激的情况下释放它们。我们使用逆乳液聚合(IEP)方法,产生逆纳米乳液或纳米凝胶来配制这些纳米颗粒。我们证明了我们通过在氧化还原内部封装,通过包封氧化和自我蛋白水解损伤的半胱氨酸蛋白酶,通过包封氧化和自我蛋白水解损伤的半胱氨酸蛋白酶,通过包封在Hela细胞的细胞溶质,通过克服氧化和自我蛋白水解损伤的半胱氨酸蛋白酶,通过包封克服氧化和自我蛋白水解损伤,克服活动损失的负债能力 - 夸张的纳米凝胶。

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