We report the preparation and structural
and mechanical characterization
of a tough supramolecular hydrogel, based exclusively on hydrophobic
association. The system consists of a multiblock, segmented copolymer
of hydrophilic poly(ethylene glycol) (PEG) and hydrophobic dimer fatty
acid (DFA) building blocks. A series of copolymers containing 2K,
4K, and 8K PEG were prepared. Upon swelling in water, a network is
formed by self-assembly of hydrophobic DFA units in micellar domains,
which act as stable physical cross-link points. The resulting hydrogels
are noneroding and contain 75–92 wt % of water at swelling
equilibrium. Small-angle neutron scattering (SANS) measurements showed
that the aggregation number of micelles ranges from 2 × 102 to 6 × 102 DFA units, increasing with PEG
molecular weight. Mechanical characterization indicated that the hydrogel
containing PEG 2000 is mechanically very stable and tough, possessing
a tensile toughness of 4.12 MJ/m3. The high toughness,
processability, and ease of preparation make these hydrogels very
attractive for applications where mechanical stability and load bearing
features of soft materials are required.
End-stage liver diseases are an increasing health burden, and liver transplantations are currently the only curative treatment option. Due to a lack of donor livers, alternative treatments are urgently needed. Human liver organoids are very promising for regenerative medicine; however, organoids are currently cultured in Matrigel, which is extracted from the extracellular matrix of the Engelbreth-Holm-Swarm mouse sarcoma. Matrigel is poorly defined, suffers from high batch-to-batch variability and is of xenogeneic origin, which limits the clinical application of organoids. Here, a novel hydrogel based on polyisocyanopeptides (PIC) and laminin-111 is described for human liver organoid cultures. PIC is a synthetic polymer that can form a hydrogel with thermosensitive properties, making it easy to handle and very attractive for clinical applications. Organoids in an optimized PIC hydrogel proliferate at rates comparable to those observed with Matrigel; proliferation rates are stiffness-dependent, with lower stiffnesses being optimal for organoid proliferation. Moreover, organoids can be efficiently differentiated toward a hepatocyte-like phenotype with key liver functions. This proliferation and differentiation potential maintain over at least 14 passages. The results indicate that PIC is very promising for human liver organoid culture and has the potential to be used in a variety of clinical applications including cell therapy and tissue engineering.
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