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用于增强X射线相互作用的金-蛋白质复合纳米颗粒:一种触发释放的潜在制剂。

Gold-Protein Composite Nanoparticles for Enhanced X-ray Interactions: A Potential Formulation for Triggered Release.

作者信息

van Ballegooie Courtney, Man Alice, Pallaoro Alessia, Bally Marcel, Gates Byron D, Yapp Donald T

机构信息

Experimental Therapeutics, BC Cancer, Vancouver, BC V5Z 4E6, Canada.

Faculty of Medicine, University of British Columbia, Vancouver, BC V6T 1Z3, Canada.

出版信息

Pharmaceutics. 2021 Sep 4;13(9):1407. doi: 10.3390/pharmaceutics13091407.

Abstract

Drug-delivery vehicles have been used extensively to modulate the biodistribution of drugs for the purpose of maximizing their therapeutic effects while minimizing systemic toxicity. The release characteristics of the vehicle must be balanced with its encapsulation properties to achieve optimal delivery of the drug. An alternative approach is to design a delivery vehicle that preferentially releases its contents under specific endogenous (e.g., tissue pH) or exogenous (e.g., applied temperature) stimuli. In the present manuscript, we report on a novel delivery system with potential for triggered release using external beam radiation. Our group evaluated Zein protein as the basis for the delivery vehicle and used radiation as the exogenous stimulus. Proteins are known to react with free radicals, produced during irradiation in aqueous suspensions, leading to aggregation, fragmentation, amino acid modification, and proteolytic susceptibility. Additionally, we incorporated gold particles into the Zein protein matrix to create hybrid Zein-gold nanoparticles (ZAuNPs). Zein-only nanoparticles (ZNPs) and ZAuNPs were subsequently exposed to kVp radiation (single dose ranging from 2 to 80 Gy; fractionated doses of 2 Gy delivered 10 times) and characterized before and after irradiation. Our data indicated that the presence of gold particles within Zein particles was correlated with significantly higher levels of alterations to the protein, and was associated with higher rates of release of the encapsulated drug compound, Irinotecan. The aggregate results demonstrated a proof-of-principle that radiation can be used with gold nanoparticles to modulate the release rates of protein-based drug-delivery vehicles, such as ZNPs.

摘要

药物递送载体已被广泛用于调节药物的生物分布,目的是在使全身毒性最小化的同时最大化其治疗效果。载体的释放特性必须与其包封特性相平衡,以实现药物的最佳递送。另一种方法是设计一种递送载体,使其在特定的内源性(如组织pH值)或外源性(如施加的温度)刺激下优先释放其内容物。在本论文中,我们报道了一种具有利用外照射触发释放潜力的新型递送系统。我们团队评估了玉米醇溶蛋白作为递送载体的基础,并使用辐射作为外源性刺激。已知蛋白质会与水悬浮液辐照过程中产生的自由基发生反应,导致聚集、碎片化、氨基酸修饰和蛋白水解敏感性。此外,我们将金颗粒掺入玉米醇溶蛋白基质中,以制备玉米醇溶蛋白-金复合纳米颗粒(ZAuNPs)。随后将仅含玉米醇溶蛋白的纳米颗粒(ZNPs)和ZAuNPs暴露于千伏峰值辐射(单剂量范围为2至80 Gy;分10次给予2 Gy的分次剂量),并在辐照前后进行表征。我们的数据表明,玉米醇溶蛋白颗粒中金颗粒的存在与蛋白质更高水平的改变相关,并且与包封的药物化合物伊立替康的更高释放速率相关。总体结果证明了一个原理验证,即辐射可与金纳米颗粒一起用于调节基于蛋白质的药物递送载体(如ZNPs)的释放速率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3d21/8471296/dfce05b015aa/pharmaceutics-13-01407-g001.jpg

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