Hydrophobized Hydrogels: Construction Strategies,Properties, and Biomedical Applications

Hydrogels, as 3D networks containing huge amount of water, display similarity to soft tissues, and thus they are of wide interest in tissue engineering. Hydrogels, due to biocompatibility and porous structure, are valuable therapeutic platforms for hydrophilic drugs. Over the last decade, there has been a strong emphasis on the development of hydrogel platforms with the ability to increase the solubility of hydrophobic drugs. However, the pronounced discrepancy between the hydrophilic character of hydrogels and the hydrophobic nature of numerous pharmacologically active compounds is problematic. In recent years, different strategies are applied using special polymer constructs or composite materials exploiting the advanced scientific knowledge in the area of polymer and lipid-based nano- and microcarriers hydrophobization of the hydrogel turns out to be not only valuable in terms of achieving the ability to dissolve poorly soluble drugs in water, but also proves to be crucial in obtaining bioadhesion in wet conditions, but also, unexpected abnormal water swelling behavior, as well as in mechanical properties such as the dissipation mechanism and self-healable hydrogel properties. This review is mainly focused on recent advances in the usage of hydrophobized hydrogels in biomedical applications.     

High‐Strength and High‐Toughness Double‐Cross‐Linked Cellulose Hydrogels: A New Strategy Using Sequential Chemical and Physical Cross‐Linking

Polysaccharide‐based hydrogels have multiple advantages because of their inherent biocompatibility, biodegradability, and non‐toxicic properties. The feasibility of using polysaccharide‐based hydrogels could be improved if they could simultaneously fulfill the mechanical property and cell compatibility requirements for practical applications. Herein, the construction of double‐cross‐linked (DC) cellulose hydrogels is described using sequential chemical and physical cross‐linking, resulting in DC cellulose hydrogels that are mechanically superior to single‐cross‐linked cellulose hydrogels. The formation and spatial distribution of chemically cross‐linked domains and physically cross‐linked domains within the DC cellulose hydrogels are demonstrated. The molar ratio of epichlorohydrin to anhydroglucose units of cellulose and the concentration of the aqueous ethanol solution are two critical parameters for obtaining mechanically strong and tough DC cellulose hydrogels. The mechanical properties of the DC cellulose hydrogels under loading‐unloading cycles are described using compression and tension models. The possible toughening mechanism of double‐cross‐linking is discussed.     

Bioinspired Structural Composite Hydrogels with a Combination of High Strength,Stiffness, and Toughness

In the development of artificial hydrogels, emulating the mechanical properties of biological tissues with a desirable combination of stiffness and toughness is crucial. To achieve such properties, a design principle inspired by a natural structural composite to wet hydrogels is applied. The bioinspired structural composite hydrogel consisting of layered microplatelets and polymer matrix with strong polymer–platelet interactions is fabricated by a facile method, that is, drying-induced unidirectional shrinkage and rehydration process coupled with secondary ionic crosslinking. The resulting hydrogels exhibit a combination of high tensile strength and elastic modulus (on the order of several MPa) and high fracture energy (up to ≈ 2 kJ·m⁻²). The results suggest the potential of the bioinspired approach that is limitedly applied in dry composites for developing mechanically robust composite hydrogels.     

Patterned Hydrogels for Controlled Platelet Adhesion from Whole Blood and Plasma

This work describes the preparation and properties of hydrogel surface chemistries enabling controlled and well‐defined cell adhesion. The hydrogels may be prepared directly on plastic substrates, such as polystyrene slides or dishes, using a quick and experimentally simple photopolymerization process, compatible with photolithographic and microfluidic patterning methods. The intended application for these materials is as substrates for diagnostic cell adhesion assays, particularly for the analysis of human platelet function. The non‐specific adsorption of fibrinogen, a platelet adhesion promoting protein, is shown to be completely inhibited by the hydrogel, provided that the film thickness is sufficient (>5 nm). This allows the hydrogel to be used as a matrix for presenting selected bioactive ligands without risking interference from non‐specifically adsorbed platelet adhesion factors, even in undiluted whole blood and blood plasma. This concept is demonstrated by preparing patterns of proteins on hydrogel surfaces, resulting in highly controlled platelet adhesion. Further insights into the protein immobilization and platelet adhesion processes are provided by studies using imaging surface plasmon resonance. The hydrogel surfaces used in this work appear to provide an ideal platform for cell adhesion studies of platelets, and potentially also for other cell types.     

Combining Mechanical Tuneability with Function: Biomimetic Fibrous Hydrogels with Nanoparticle Crosslinkers

Fibrous networks of biopolymers possess unique properties: mechanical stability at low concentrations, an extremely porous architecture, and strong stiffening at small deformations. An outstanding challenge is to find methods that allow to tailor the mechanical properties of these bionetworks or their synthetic equivalents without changing the polymer concentration, which simultaneously changes all other hydrogel properties. Here, networks of dilute (0.1 wt.%) fibrous hydrogels are prepared and crosslink them with functional rod-shaped nanoparticles. The crosslinking is observed to induce an architectural change that strongly affects the mechanical properties of the hydrogels with a 40-fold increase in stiffness. The effect is strongest at the lowest polymer and particle concentrations (99.8% water) and is tailorable through tuning the crosslink density. Moreover, the nanoparticle components in the composite offer the opportunity to introduce additional functions; gels with magnetic and conductive properties are reported. However, through the generic crosslinking approach of a fibrous network with decorated nanoparticle crosslinkers as presented in this work, virtually any functionality may be introduced in highly responsive hydrogels, providing a guide to design next generations of multi-functional soft materials.     

Bio‐Orthogonally Crosslinked,Engineered Protein Hydrogels with Tunable Mechanics and Biochemistry for Cell Encapsulation

Covalently‐crosslinked hydrogels are commonly used as 3D matrices for cell culture and transplantation. However, the crosslinking chemistries used to prepare these gels generally cross‐react with functional groups present on the cell surface, potentially leading to cytotoxicity and other undesired effects. Bio‐orthogonal chemistries have been developed that do not react with biologically relevant functional groups, thereby preventing these undesirable side reactions. However, previously developed biomaterials using these chemistries still possess less than ideal properties for cell encapsulation, such as slow gelation kinetics and limited tuning of matrix mechanics and biochemistry. Here, engineered elastin‐like proteins (ELPs) are developed that crosslink via strain‐promoted azide‐alkyne cycloaddition (SPAAC) or Staudinger ligation. The SPAAC‐crosslinked materials form gels within seconds and complete gelation within minutes. These hydrogels support the encapsulation and phenotypic maintenance of human mesenchymal stem cells, human umbilical vein endothelial cells, and murine neural progenitor cells. SPAAC‐ELP gels exhibit independent tuning of stiffness and cell adhesion, with significantly improved cell viability and spreading observed in materials containing a fibronectin‐derived arginine‐glycine‐aspartic acid (RGD) domain. The crosslinking chemistry used permits further material functionalization, even in the presence of cells and serum. These hydrogels are anticipated to be useful in a wide range of applications, including therapeutic cell delivery and bioprinting.     

Highly Efficient Self‐Healable and Dual Responsive Cellulose‐Based Hydrogels for Controlled Release and 3D Cell Culture

To face the increasing demand of self‐healing hydrogels with biocompatibility and high performances, a new class of cellulose‐based self‐healing hydrogels are constructed through dynamic covalent acylhydrazone linkages. The carboxyethyl cellulose‐graft‐dithiodipropionate dihydrazide and dibenzaldehyde‐terminated poly(ethylene glycol) are synthesized, and then the hydrogels are formed from their mixed solutions under 4‐amino‐DL‐phenylalanine (4a‐Phe) catalysis. The chemical structure, as well as microscopic morphologies, gelation times, mechanical and self‐healing performances of the hydrogels are investigated with ¹H NMR, Fourier transform infrared spectroscopy, atomic force microscopy, rheological and compression measurements. Their gelation times can be controlled by varying the total polymer concentration or 4a‐Phe content. The resulted hydrogels exhibit excellent self‐healing ability with a high healing efficiency (≈96%) and good mechanical properties. Moreover, the hydrogels display pH/redox dual responsive sol‐gel transition behaviors, and are applied successfully to the controlled release of doxorubicin. Importantly, benefitting from the excellent biocompatibility and the reversibly cross‐linked networks, the hydrogels can function as suitable 3D culture scaffolds for L929 cells, leading to the encapsulated cells maintaining a high viability and proliferative capacity. Therefore, the cellulose‐based self‐healing hydrogels show potential applications in drug delivery and 3D cell culture for tissue engineering.     

High Lubricity Meets Load Capacity: Cartilage Mimicking Bilayer Structure by Brushing Up Stiff Hydrogels from Subsurface

Natural articular cartilage has ultralow friction even at high squeezing pressure. Biomimicking cartilage with soft materials has been and remains a grand challenge in the fields of materials science and engineering. Inspired by the unique structural features of the articular cartilage, as well as by its remarkable lubrication mechanisms dictated by the properties of the superficial layers, a novel archetype of cartilage‐mimicking bilayer material by robustly entangling thick hydrophilic polyelectrolyte brushes into the subsurface of a stiff hydrogel substrate is developed. The topmost soft polymer layer provides effective aqueous lubrication, whereas the stiffer hydrogel layer used as a substrate delivers the load‐bearing capacity. Their synergy is capable of attaining low friction coefficients (order 0.010) under heavily loaded conditions (order 10 MPa contact pressure) in water environment, a performance incredibly close to that of natural articular cartilage. The bioinspired material can maintain low friction even when subjected to 50k reciprocating cycles under high contact pressure, with almost no wear observed on the sliding track. These findings are theoretically explained and compounded by multiscale simulations used to shed light on the mechanisms responsible for this remarkable performance. This work opens innovative technology routes for developing cartilage‐mimicking ultralow friction soft materials.     

Cationic Hybrid Hydrogels from Amino‐Acid‐Based Poly(ester amide): Fabrication,Characterization, and Biological Properties

A family of biodegradable, biocompatible, water soluble cationic polymer precursor, arginine‐based unsaturated poly (ester amide) (Arg‐UPEA), is reported. Its incorporation into conventional Pluronic diacrylate (Pluronic‐DA) to form hybrid hydrogels for a significant improvement of the biological performance of current synthetic hydrogels is shown. The gel fraction (G_f), equilibrium swelling ratio (Q_eq), compressive modulus, and interior morphology of the hybrid hydrogels as well as their interactions with human fibroblasts and bovine endothelial cells are fully investigated. It is found that the incorporation of Arg‐UPEA into Pluronic‐DA hydrogels significantly changes their Q_eq, mechanical strength, and interior morphology. The structure–property relationship of the newly fabricated hybrid hydrogels is studied in terms of the chemical structure of the Arg‐UPEA precursor, i.e., the number of methylene groups in the Arg‐UPEA repeating unit. The results indicate that increasing methylene groups in the Arg‐UPEA repeating unit increases Q_eq and decreases the compressive modulus of hydrogels. When compared with a pure Pluronic hydrogel, the cationic Arg‐UPEAs/Pluronic hybrid hydrogels greatly improve the attachment and proliferation of human fibroblasts on hydrogel surfaces. A bovine aortic endothelial cells (BAEC) viability test in the interior of the hydrogels shows that the positively charged hybrid hydrogels can significantly improve the viability of the encapsulated endothelial cell over a 2 week study period when compared with a pure Pluronic hydrogel.     

Hybrid Materials from Ultrahigh‐Inorganic‐Content Mineral Plastic Hydrogels: Arbitrarily Shapeable,Strong, and Tough

Natural mineralized structural materials such as nacre and bone possess a unique hierarchical structure comprising both hard and soft phases, which can achieve the perfect balance between mechanical strength and shape controllability. Nevertheless, it remains a great challenge to control the complex and predesigned shapes of artificial organic–inorganic hybrid materials at ambient conditions. Inspired by the plasticity of polymer‐induced liquid precursor phases that can penetrate and solidify in porous organic frameworks for biomineral formation, here a mineral plastic hydrogel is shown with ultrahigh silica content (≈95 wt%) that can be similarly hybridized into a porous delignified wood scaffold, and the resultant composite hydrogels can be manually made into arbitrary shapes. Subsequent air drying well preserves the designed shapes and produces fire‐retardant, ultrastrong, and tough structural organic–inorganic hybrids. The proposed mineral plastic hydrogel strategy opens an easy and eco‐friendly way for fabricating bioinspired structural materials that compromise both precise shape control and high mechanical strength.     

A Novel Design Strategy for Fully Physically Linked Double Network Hydrogels with Tough,Fatigue Resistant,and Self‐Healing Properties

Double network (DN) hydrogels with two strong asymmetric networks being chemically linked have demonstrated their excellent mechanical properties as the toughest hydrogels, but chemically linked DN gels often exhibit negligible fatigue resistance and poor self‐healing property due to the irreversible chain breaks in covalent‐linked networks. Here, a new design strategy is proposed and demonstrated to improve both fatigue resistance and self‐healing property of DN gels by introducing a ductile, nonsoft gel with strong hydrophobic interactions as the second network. Based on this design strategy, a new type of fully physically cross‐linked Agar/hydrophobically associated polyacrylamide (HPAAm) DN gels are synthesized by a simple one‐pot method. Agar/HPAAm DN gels exhibit excellent mechanical strength and high toughness, comparable to the reported DN gels. More importantly, because the ductile and tough second network of HPAAm can bear stress and reconstruct network structure, Agar/HPAAm DN gels also demonstrate rapid self‐recovery, remarkable fatigue resistance, and notable self‐healing property without any external stimuli at room temperature. In contrast to the former DN gels in both network structures and underlying association forces, this new design strategy to prepare highly mechanical DN gels provides a new avenue to better understand the fundamental structure‐property relationship of DN hydrogels, thus broadening current hydrogel research and applications.     

Injectable and Biodegradable Nanohybrid Polymers with Simultaneously Enhanced Stiffness and Toughness for Bone Repair

A series of novel injectable and photo‐crosslinkable poly(propylene fumarate) (PPF)‐co‐polyhedral oligomeric silsesquioxane (POSS) copolymers are synthesized via two‐step polycondensation to improve both stiffness and toughness and to promote biological performance of bone tissue engineering scaffolds. The viscoelastic behavior of uncrosslinked PPF‐co‐POSS and the thermal, mechanical, and surface characteristics of photo‐crosslinked PPF‐co‐POSS are investigated as well as the degradation behavior and microscopic POSS domain structures at various weight compositions of POSS (?_POSS). Tensile and compressive moduli and facture toughness are enhanced for crosslinked PPF‐co‐POSS when POSS nanocages are well distributed and their crystallinity is completely confined in the networks. Decreases in these mechanical properties are observed at higher ?_POSS because of decreased crosslinking density and larger POSS aggregates. The mechanical properties are correlated with in vitro mouse pre‐osteoblastic MC3T3‐E1 cell functions including cell attachment, spreading, proliferation, differentiation, and gene expression, which all maximize at ?_POSS of 10%.     

Healable,Stable and Stiff Hydrogels: Combining Conflicting Properties Using Dynamic and Selective Three‐Component Recognition with Reinforcing Cellulose Nanorods

Nanocomposite hydrogels are prepared combining polymer brush‐modified ‘hard’ cellulose nanocrystals (CNC) and ‘soft’ polymeric domains, and bound together by cucurbit[8]uril (CB[8]) supramolecular crosslinks, which allow dynamic host–guest interactions as well as selective and simultaneous binding of two guests, i.e., methyl viologen (the first guest) and naphthyl units (the second guest). CNCs are mechanically strong colloidal rods with nanometer‐scale lateral dimensions, which are functionalized by surface‐initiated atom transfer radical polymerization to yield a dense set of methacrylate polymer brushes bearing naphthyl units. They can then be non‐covalently cross‐linked through simple addition of poly(vinyl alcohol) polymers containing pendant viologen units as well as CB[8]s in aqueous media. The resulting supramolecular nanocomposite hydrogels combine three important criteria: high storage modulus (G′ > 10 kPa), rapid sol–gel transition (<6 s), and rapid self‐healing even upon aging for several months, as driven by balanced colloidal reinforcement as well as the selectivity and dynamics of the CB[8] three‐component supramolecular interactions. Such a new combination of properties for stiff and self‐healing hydrogel materials suggests new approaches for advanced dynamic materials from renewable sources.     

A Novel Double‐Crosslinking‐Double‐Network Design for Injectable Hydrogels with Enhanced Tissue Adhesion and Antibacterial Capability for Wound Treatment

Most photocrosslinkable hydrogels have inadequacy in either mechanical performance or biodegradability. This issue is addressed by adopting a novel hydrogel design by introducing two different chitosan chains (catechol‐modified methacryloyl chitosan, CMC; methacryloyl chitosan, MC) via the simultaneous crosslinking of carbon–carbon double bonds and catechol‐Fe³⁺ chelation. This leads to an interpenetrating network of two chitosan chains with high crosslinking‐network density, which enhances mechanical performance including high compressive modulus and high ductility. The chitosan polymers not only endow the hydrogels with good biodegradability and biocompatibility, they also offer intrinsic antibacterial capability. The quinone groups formed by Fe³⁺ oxidation and protonated amino groups of chitosan polymer further enhance antibacterial property of the hydrogels. Serving as one of the two types of crosslinking mechanisms, the catechol‐Fe³⁺ chelation can covalently link with amino, thiol, and imidazole groups, which substantially enhance the hydrogel's adhesion to biological tissues. The hydrogel's adhesion to porcine skin shows a lap shear strength of 18.1 kPa, which is 6‐time that of the clinically established Fibrin Glue's adhesion. The hydrogel also has a good hemostatic performance due to the superior tissue adhesion as demonstrated with a hemorrhaging liver model. Furthermore, the hydrogel can remarkably promote healing of bacteria‐infected wound.