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通过冰模板法制备的用于疏水性药物控释的蛋白质纳米球和纳米纤维

Protein Nanospheres and Nanofibers Prepared by Ice-Templating for the Controlled Release of Hydrophobic Drugs.

作者信息

Zhang Meina, Cai Hong, Zhang Haifei

机构信息

Department of Chemistry, University of Liverpool, Crown Street, Liverpool L69 7ZD, U.K.

出版信息

ACS Appl Nano Mater. 2024 Sep 13;7(18):21692-21704. doi: 10.1021/acsanm.4c03657. eCollection 2024 Sep 27.

Abstract

Protein scaffolds play a vital role in drug delivery systems. However, few research studies have been focused on loading hydrophobic drugs on protein scaffolds in biomedical fields. Here, we report on the development of protein microspheres and nanofibers by a simple ice-templating approach and their use as scaffolds for the controlled release of hydrophobic drugs, with bovine serum albumin (BSA) as the model protein and curcumin as the model hydrophobic drug. The BSA scaffolds display the unique nanofibrous and microspherical structures. This is a surprising discovery because there has been no report on the formation of microspheres via simple ice-templating of solutions or suspensions. To further understand the formation of microspheres by this approach, lysozyme, papain, and their composites with BSA are also studied. It is speculated that nanoparticles are first formed in aqueous BSA solution, attributed to the overlapping of hydration layers and autoassembly of inner hydrophobic cores of BSA globular molecules. Nanoprecipitation and soaking evaporation approaches are then used to load curcumin into the BSA scaffolds, followed by cross-linking with glutaraldehyde vapor to improve stability in an aqueous medium. The controlled release of curcumin is demonstrated, paving the way for various hydrophobic drugs loaded into this biodegradable and nonimmunogenic protein scaffold for potential treatments of diverse diseases.

摘要

蛋白质支架在药物递送系统中起着至关重要的作用。然而,在生物医学领域,很少有研究关注在蛋白质支架上负载疏水性药物。在此,我们报道了通过一种简单的冰模板法制备蛋白质微球和纳米纤维,并将其用作疏水性药物控释的支架,以牛血清白蛋白(BSA)作为模型蛋白质,姜黄素作为模型疏水性药物。BSA支架呈现出独特的纳米纤维和微球结构。这是一个令人惊讶的发现,因为此前尚无通过简单的溶液或悬浮液冰模板法形成微球的报道。为了进一步了解通过这种方法形成微球的过程,还研究了溶菌酶、木瓜蛋白酶及其与BSA的复合材料。据推测,纳米颗粒首先在BSA水溶液中形成,这归因于水合层的重叠以及BSA球状分子内部疏水核心的自组装。然后采用纳米沉淀和浸泡蒸发法将姜黄素负载到BSA支架中,随后用戊二醛蒸汽交联以提高其在水性介质中的稳定性。姜黄素的控释得到了证实,为将各种疏水性药物负载到这种可生物降解且无免疫原性的蛋白质支架中用于多种疾病的潜在治疗铺平了道路。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2994/11443487/e7a888649846/an4c03657_0010.jpg

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