Chitosan Grafted with Thermoresponsive Poly(di(ethylene glycol) Methyl Ether Methacrylate) for Cell Culture Applications.
Natun DasguptaDuo SunMaud GorbetMario GauthierPublished in: Polymers (2023)
Chitosan is a polysaccharide extracted from animal sources such as crab and shrimp shells. In this work, chitosan films were modified by grafting them with a thermoresponsive polymer, poly(di(ethylene glycol) methyl ether methacrylate) (PMEO 2 MA). The films were modified to introduce functional groups useful as reversible addition-fragmentation chain transfer (RAFT) agents. PMEO 2 MA chains were then grown from the films via RAFT polymerization, making the chitosan films thermoresponsive. The degree of substitution of the chitosan-based RAFT agent and the amount of monomer added in the grafting reaction were varied to control the length of the grafted PMEO 2 MA chain segments. The chains were cleaved from the film substrates for characterization using 1 H NMR and a gel permeation chromatography analysis. Temperature-dependent contact angle measurements were used to demonstrate that the hydrophilic-hydrophobic nature of the film surface varied with temperature. Due to the enhanced hydrophobic character of PMEO 2 MA above its lower critical solution temperature (LCST), the ability of PMEO 2 MA-grafted chitosan films to serve as a substrate for cell growth at 37 °C (incubation temperature) was tested. Interactions with cells (fibroblasts, macrophages, and corneal epithelial cells) were assessed. The modified chitosan films supported cell viability and proliferation. As the temperature is lowered to 4 °C (refrigeration temperature, below the LCST), the grafted chitosan films become less hydrophobic, and cell adhesion should decrease, facilitating their removal from the surface. Our results indicated that the cells were detached from the films following a short incubation period at 4 °C, were viable, and retained their ability to proliferate.
Keyphrases
- room temperature
- drug delivery
- wound healing
- hyaluronic acid
- ionic liquid
- carbon nanotubes
- induced apoptosis
- cell adhesion
- mass spectrometry
- high resolution
- pseudomonas aeruginosa
- cell cycle arrest
- optical coherence tomography
- high speed
- cell death
- ms ms
- reduced graphene oxide
- signaling pathway
- pi k akt
- molecularly imprinted
- staphylococcus aureus
- simultaneous determination