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Elastin-like polypeptide coacervates as reversibly triggerable compartments for synthetic cells.

Chang ChenKetan A GanarRobbert J de HaasNele JarnotErwin HogeveenRenko de VriesSiddharth Deshpande
Published in: Communications chemistry (2024)
Compartmentalization is a vital aspect of living cells to orchestrate intracellular processes. In a similar vein, constructing dynamic and responsive sub-compartments is key to synthetic cell engineering. In recent years, liquid-liquid phase separation via coacervation has offered an innovative avenue for creating membraneless organelles (MOs) within artificial cells. Here, we present a lab-on-a-chip system to reversibly trigger peptide-based coacervates within cell-mimicking confinements. We use double emulsion droplets (DEs) as our synthetic cell containers while pH-responsive elastin-like polypeptides (ELPs) act as the coacervate system. We first present a high-throughput microfluidic DE production enabling efficient encapsulation of the ELPs. The DEs are then harvested to perform multiple MO formation-dissolution cycles using pH as well as temperature variation. For controlled long-term visualization and modulation of the external environment, we developed an integrated microfluidic device for trapping and environmental stimulation of DEs, with negligible mechanical force, and demonstrated a proof-of-principle osmolyte-based triggering to induce multiple MO formation-dissolution cycles. In conclusion, our work showcases the use of DEs and ELPs in designing membraneless reversible compartmentalization within synthetic cells via physicochemical triggers. Additionally, presented on-chip platform can be applied over a wide range of phase separation and vesicle systems for applications in synthetic cells and beyond.
Keyphrases
  • high throughput
  • induced apoptosis
  • single cell
  • cell cycle arrest
  • living cells
  • circulating tumor cells
  • cell therapy
  • stem cells
  • oxidative stress
  • mesenchymal stem cells
  • cancer therapy
  • ionic liquid