Nature Communications (Aug 2024)

Polyphenol-stabilized coacervates for enzyme-triggered drug delivery

  • Wonjun Yim,
  • Zhicheng Jin,
  • Yu-Ci Chang,
  • Carlos Brambila,
  • Matthew N. Creyer,
  • Chuxuan Ling,
  • Tengyu He,
  • Yi Li,
  • Maurice Retout,
  • William F. Penny,
  • Jiajing Zhou,
  • Jesse V. Jokerst

DOI
https://doi.org/10.1038/s41467-024-51218-8
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 11

Abstract

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Abstract Stability issues in membrane-free coacervates have been addressed with coating strategies, but these approaches often compromise the permeability of the coacervate. Here we report a facile approach to maintain both stability and permeability using tannic acid and then demonstrate the value of this approach in enzyme-triggered drug release. First, we develop size-tunable coacervates via self-assembly of heparin glycosaminoglycan with tyrosine and arginine-based peptides. A thrombin-recognition site within the peptide building block results in heparin release upon thrombin proteolysis. Notably, polyphenols are integrated within the nano-coacervates to improve stability in biofluids. Phenolic crosslinking at the liquid-liquid interface enables nano-coacervates to maintain exceptional structural integrity across various environments. We discover a pivotal polyphenol threshold for preserving enzymatic activity alongside enhanced stability. The disassembly rate of the nano-coacervates increases as a function of thrombin activity, thus preventing a coagulation cascade. This polyphenol-based approach not only improves stability but also opens the way for applications in biomedicine, protease sensing, and bio-responsive drug delivery.