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Effects of Individual Amino Acids on the Blood Circulation of Biosynthetic Protein Nanocages: towards Guidance on Surface Engineering.

Ao LiangWei ZhouHui ZhangJuan ZhangXian-En ZhangTi FangFeng Li
Published in: Advanced healthcare materials (2023)
Protein nanocages (PNCs) hold great promise for developing multifunctional nanomedicines. Long blood circulation is a key requirement of PNCs for most in vivo application scenes. In addition to the classical PEGylation strategy, short peptides with a specific sequence screened via phage display are also very effective in prolonging the blood half-life (t 1/2 ) of PNCs. However, there is a lack of knowledge on how individual amino acids affect the circulation of PNCs. Here we explore the effects of the 20 proteinogenic amino acids in the form of an X 3 or X 5 tag (X represents an amino acid) on the pharmacokinetics of PNCs, which has led to the formation of a heatmap illustrating the extent of t 1/2 prolongation by each proteinogenic amino acid. Significantly, oligo-lysine and oligo-arginine can effectively prolong the t 1/2 of strongly negatively charged PNCs through charge neutralization, while oligo-cysteine can also do so, but via a different mechanism, mediating the covalent binding of PNCs with plasma albumin as a stealth material. These findings are extendible and offer guidance for surface-engineering biosynthetic PNCs and other nanoparticles. This article is protected by copyright. All rights reserved.
Keyphrases
  • amino acid
  • healthcare
  • pseudomonas aeruginosa
  • drug delivery
  • cancer therapy
  • nitric oxide
  • fluorescent probe
  • binding protein
  • single molecule