Elucidation of Protonation Cooperativity of a STING-Activating Polymer

Adv Mater. 2023 Dec;35(51):e2305255. doi: 10.1002/adma.202305255. Epub 2023 Nov 10.

Abstract

Stimuli-responsive nanomaterials have the potential to improve the performance and overcome existing barriers of conventional nanotherapeutics. Molecular cooperativity design in stimuli-responsive nanomedicine can amplify physiological signals, enabling a cooperative response for improved diagnostic and therapeutic precision. Previously, this work reported an ultra-pH-sensitive polymer, PEG-b-PC7A, that possesses innate immune activating properties by binding to the stimulator of interferon genes (STING) through polyvalent phase condensation. This interaction enhances STING activation and synergizes with the endogenous STING ligand for robust cancer immunotherapy. Despite its successes in innate immune activation, the fundamental physicochemical and pH-responsive properties of PC7A require further investigation. Here, this study elucidates the protonation cooperativity driven by the phase transition of PC7A copolymer. The highly cooperative system displays an "all-or-nothing" proton distribution between highly charged unimer (all) and neutral micelle (nothing) states without gradually protonated intermediates. The binary protonation behavior is further illustrated in pH-precision-controlled release of a representative anticancer drug, β-lapachone, by PC7A micelles over a noncooperative PE5A polymer. Furthermore, the bimodal distribution of protons is represented by a high Hill coefficient (nH > 9), featuring strong positive cooperativity. This study highlights the nanoscale pH cooperativity of an immune activating polymer, providing insights into the physicochemical characterization and design parameters for future nanotherapeutics development.

Keywords: molecular cooperativity; nanomedicine; nanoscale self-assembly; ultra-pH-sensitive micelles.

MeSH terms

  • Antineoplastic Agents*
  • Hydrogen-Ion Concentration
  • Membrane Proteins* / agonists
  • Membrane Proteins* / metabolism
  • Micelles
  • Nanostructures*
  • Phase Transition
  • Polymers / chemistry

Substances

  • Antineoplastic Agents
  • Micelles
  • Polymers
  • STING1 protein, human
  • Membrane Proteins