Elastin-like polypeptide-based micelles as a promising platform in nanomedicine

胶束 纳米医学 两亲性 药物输送 纳米材料 纳米颗粒 纳米技术 化学 原弹性蛋白 生物分子 生物物理学 共聚物 聚合物 靶向给药 材料科学 生物化学 有机化学 生物 水溶液 细胞外基质
作者
Jolinde van Strien,Oscar Escalona-Rayo,Wim Jiskoot,Bram Slütter,Alexander Kros
出处
期刊:Journal of Controlled Release [Elsevier BV]
卷期号:353: 713-726 被引量:13
标识
DOI:10.1016/j.jconrel.2022.12.033
摘要

New and improved nanomaterials are constantly being developed for biomedical purposes. Nanomaterials based on elastin-like polypeptides (ELPs) have increasingly shown potential over the past two decades. These polymers are artificial proteins of which the design is based on human tropoelastin. Due to this similarity, ELP-based nanomaterials are biodegradable and therefore well suited to drug delivery. The assembly of ELP molecules into nanoparticles spontaneously occurs at temperatures above a transition temperature (Tt). The ELP sequence influences both the Tt and the physicochemical properties of the assembled nanomaterial. Nanoparticles with desired properties can hence be designed by choosing the appropriate sequence. A promising class of ELP nanoparticles are micelles assembled from amphiphilic ELP diblock copolymers. Such micelles are generally uniform and well defined. Furthermore, site-specific attachment of cargo to the hydrophobic block results in micelles with the cargo shielded inside their core, while conjugation to the hydrophilic block causes the cargo to reside in the corona where it is available for interactions. Such control over particle design is one of the main contributing factors for the potential of ELP-based micelles as a drug delivery system. Additionally, the micelles are easily loaded with protein or peptide-based cargo by expressing it as a fusion protein. Small molecule drugs and other cargo types can be either covalently conjugated to ELP domains or physically entrapped inside the micelle core. This review aims to give an overview of ELP-based micelles and their applications in nanomedicine.
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