Taking advantage of cellular uptake of ferritin nanocages for targeted drug delivery

纳米载体 纳米笼 纳米技术 药物输送 靶向给药 生物制药 药品 化学 材料科学 药理学 医学 生物 生物技术 生物化学 催化作用
作者
Barbora Tesařová,Kamil Musílek,Simona Rex,Zbyněk Heger
出处
期刊:Journal of Controlled Release [Elsevier]
卷期号:325: 176-190 被引量:49
标识
DOI:10.1016/j.jconrel.2020.06.026
摘要

The search for ideal nanocarrier, which could be rapidly translated to clinical practice, isstill ongoing over the past few decades. However, many reviews are focused onimportant properties of ideal nanocarrier, including long circulation, high internalization efficiency ofadrug, surface charge of nanocarrier or the ability to encapsulate high amount of a drug. Indeed, theability to encapsulate wide variety of drugs, noimmunogenicity, biodegradability ornanocarrier monodispersity are very important aspects, therefore they are discussed in this review. The use of nanocarrier formulations able to innately form self-assembly cages ofuniform size and shape, employing protein-based structures naturally present inhuman body, seems to be very promising. Typical protein nanocarrier disposing all the above mentioned characteristics is represented by ferritin (FRT). Hence, the presented review provides detailed characterization of FRT structure, including its disassembly and reassembly properties, which are crucial for encapsulation ofdrugs, together with possibilities of active targeting, exploiting both the innate affinities of FRT nanocages towards selected receptors and the plethora of surface functional groups that can be used to attach a variety of targeting ligands. Finally, we discuss theopportunities of cutting-edge approaches to FRT-based nanotherapy and the challenges that must be overcome or avoided.
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