Spatial and Temporal Modulation of Cell Instructive Cues in a Filamentous Supramolecular Biomaterial.

Supramolecular materials provide unique opportunities to mimic both the structure and mechanics of the biopolymer networks that compose the extracellular matrix. However, strategies to modify their filamentous structures in space and time in 3D cell culture to study cell behavior as encountered in development and disease are lacking. We herein disclose a multicomponent squaramide-based supramolecular material whose mechanics and bioactivity can be controlled by light through co-assembly of a 1,2-dithiolane (DT) monomer that forms disulfide cross-links. Remarkably, increases in storage modulus from ∼200 Pa to >10 kPa after stepwise photo-cross-linking can be realized without an initiator while retaining colorlessness and clarity. Moreover, viscoelasticity and plasticity of the supramolecular networks decrease upon photo-irradiation, reducing cellular protrusion formation and motility when performed at the onset of cell culture. When applied during 3D cell culture, force-mediated manipulation is impeded and cells move primarily along earlier formed channels in the materials. Additionally, we show photopatterning of peptide cues in 3D using either a photomask or direct laser writing. We demonstrate that these squaramide-based filamentous materials can be applied to the development of synthetic and biomimetic 3D in vitro cell and disease models, where their secondary cross-linking enables mechanical heterogeneity and shaping at multiple length scales.

Squaramide-Based Supramolecular Materials Drive HepG2 Spheroid Differentiation.

A major challenge in the use of HepG2 cell culture models for drug toxicity screening is their lack of maturity in 2D culture. 3D culture in Matrigel promotes the formation of spheroids that express liver-relevant markers, yet they still lack various primary hepatocyte functions. Therefore, alternative matrices where chemical composition and materials properties are controlled to steer maturation of HepG2 spheroids remain desired. Herein, a modular approach is taken based on a fully synthetic and minimalistic supramolecular matrix based on squaramide synthons outfitted with a cell-adhesive peptide, RGD for 3D HepG2 spheroid culture. Co-assemblies of RGD-functionalized squaramide-based and native monomers resulted in soft and self-recovering supramolecular hydrogels with a tunable RGD concentration. HepG2 spheroids are self-assembled and grown (≈150 µm) within the supramolecular hydrogels with high cell viability and differentiation over 21 days of culture. Importantly, significantly higher mRNA and protein expression levels of phase I and II metabolic enzymes, drug transporters, and liver markers are found for the squaramide hydrogels in comparison to Matrigel. Overall, the fully synthetic squaramide hydrogels are proven to be synthetically accessible and effective for HepG2 differentiation showcasing the potential of this supramolecular matrix to rival and replace naturally-derived materials classically used in high-throughput toxicity screening.

Photopatternable, Branched Polymer Hydrogels Based on Linear Macromonomers for 3D Cell Culture Applications.

Photochemical ligation strategies in hydrogel materials are crucial to model spatiotemporal phenomena that occur in the natural extracellular matrix. We here describe the use of cyclic 1,2-dithiolanes to cross-link with norbornene on linear poly(ethylene glycol) polymers through UV irradiation in a rapid and byproduct-free manner, resulting in branched macromolecular architectures and hydrogel materials from low-viscosity precursor solutions. Oscillatory rheology and NMR data indicate the one-pot formation of thioether and disulfide cross-links. Spatial and temporal control of the hydrogel mechanical properties and functionality was demonstrated by oscillatory rheology and confocal microscopy. A cytocompatible response of NIH 3T3 fibroblasts was observed within these materials, providing a foothold for further exploration of this photoactive cross-linking moiety in the biomedical field.

Smart Materials for Environmental Remediation Based on Two-Component Gels: Room-Temperature-Phase-Selective Gelation for the Removal of Organic Pollutants Including Nitrobenzene/O-Dichlorobenzene, and Dye Molecules from the Wastewater.

Novel two-component gel systems based on aliphatic acid-hydroxy/base interaction were developed as smart materials for environmental remediation. The G1-A16 gelator could be used directly as a powder form to selectively gel aromatic solvents (nitrobenzene and o-dichlorobenzene) from their mixtures with wastewater (containing 0.5 M sodium nitrate and 0.5 M sodium sulfate) via a simple shaking strategy at room temperature without employing co-solvents and a heating-cooling process. Meanwhile, the two-component gel system can efficiently remove the toxic dyes from the aqueous solution. The dominant factors that drive gelation in the case of the gelator and nitrobenzene or water have been studied using FT-IR, 1H NMR, and XRD. Overall, our research provides an efficient two-component approach for facilely tuning the properties of one-component gel for the realization of high-performance functionalities of gels. At the same time, our study demonstrates potential industrial application prospect in removing pollutants efficiently (such as aromatic solvents and toxic dye removal).

Squaramide-Based Supramolecular Materials for Three-Dimensional Cell Culture of Human Induced Pluripotent Stem Cells and Their Derivatives.

Synthetic hydrogel materials can recapitulate the natural cell microenvironment; however, it is equally necessary that the gels maintain cell viability and phenotype while permitting reisolation without stress, especially for use in the stem cell field. Here, we describe a family of synthetically accessible, squaramide-based tripodal supramolecular monomers consisting of a flexible tris(2-aminoethyl)amine (TREN) core that self-assemble into supramolecular polymers and eventually into self-recovering hydrogels. Spectroscopic measurements revealed that monomer aggregation is mainly driven by a combination of hydrogen bonding and hydrophobicity. The self-recovering hydrogels were used to encapsulate NIH 3T3 fibroblasts as well as human-induced pluripotent stem cells (hiPSCs) and their derivatives in 3D. The materials reported here proved cytocompatible for these cell types with maintenance of hiPSCs in their undifferentiated state essential for their subsequent expansion or differentiation into a given cell type and potential for facile release by dilution due to their supramolecular nature.

Application of solubility parameters in a D-sorbitol-based organogel in binary organic mixtures.

The gelation behaviour of a low molecular weight gelator 2,4-(3,4-dichlorobenzylidene)-D-sorbitol (DCBS) in a binary solvent system has been studied. DCBS was soluble in pure ethanol and insoluble in pure methylcyclohexane. However, DCBS formed opaque gels in ethanol-methylcyclohexane mixtures when the methylcyclohexane content varied from 50% to 80%. Within this range, an increase in the amount of methylcyclohexane reduced the gelation time and also caused the minimum gelation concentration to decrease. Scanning electron microscopy showed that the three-dimensional network structures of the xerogels became denser (from tape-like structures to uniform fibres) when the methylcyclohexane content increased from 40% to 80%. The precipitates that formed in 90% and 100% methylcyclohexane had rod-like structures. X-ray diffraction of the xerogels showed that in the gel state, the DCBS gelator had lamellar packing, which was different from the structure of the precipitate. Fourier transform infrared spectroscopy of the xerogels showed that H-bonding was a driving force for the self-aggregation of the DCBS and it was enhanced as the methylcyclohexane content increased. To estimate the gelator-solvent interactions, the Flory-Huggins parameter was calculated for the DCBS gelator in the binary mixed solvent systems. Based on the values of the Flory-Huggins parameter, the gelation behaviours could be grouped into four domains (solution, partial gel, gel and precipitation). This is a simple method to predict the gelation behaviour of DCBS in some mixed solvents.