ABSTRACT
Gelatin methacryloyl (GelMA), a photocrosslinkable gelatin-based hydrogel, has been immensely used for diverse applications in tissue engineering and drug delivery. Apart from its excellent functionality and versatile mechanical properties, it is also suitable for a wide range of fabrication methodologies to generate tissue constructs of desired shapes and sizes. Despite its exceptional characteristics, it is predominantly limited by its weak mechanical strength, as some tissue types naturally possess high mechanical stiffness. The use of high GelMA concentrations yields high mechanical strength, but not without the compromise in its porosity, degradability, and three-dimensional (3D) cell attachment. Recently, GelMA has been blended with various natural and synthetic biomaterials to reinforce its physical properties to match with the tissue to be engineered. Among these, nanomaterials have been extensively used to form a composite with GelMA, as they increase its biological and physicochemical properties without affecting the unique characteristics of GelMA and also introduce electrical and magnetic properties. This review article presents the recent advances in the formation of hybrid GelMA nanocomposites using a variety of nanomaterials (carbon, metal, polymer, and mineral-based). We give an overview of each nanomaterial's characteristics followed by a discussion of the enhancement in GelMA's physical properties after its incorporation. Finally, we also highlight the use of each GelMA nanocomposite for different applications, such as cardiac, bone, and neural regeneration.
Subject(s)
Gelatin , Tissue Engineering , Gelatin/chemistry , Hydrogels/chemistry , Methacrylates , Nanogels , Tissue Engineering/methods , Tissue Scaffolds/chemistryABSTRACT
Bioinks play a key role in determining the capability of the biofabricatoin processes and the resolution of the printed constructs. Excellent biocompatibility, tunable physical properties, and ease of chemical or biological modifications of gelatin methacryloyl (GelMA) have made it an attractive choice as bioinks for biomanufacturing of various tissues or organs. However, the current preparation methods for GelMA-based bioinks lack the ability to tailor their physical properties for desired bioprinting methods. Inherently, GelMA prepolymer solution exhibits a fast sol-gel transition at room temperature, which is a hurdle for its use in stereolithography (SLA) bioprinting. Here, synthesis parameters are optimized such as solvents, pH, and reaction time to develop GelMA bioinks which have a slow sol-gel transition at room temperature and visible light crosslinkable functions. A total of eight GelMA combinations are identified as suitable for digital light processing (DLP)-based SLA (DLP-SLA) bioprinting through systematic characterizations of their physical and rheological properties. Out of various types of GelMA, those synthesized in reverse osmosis (RO) purified water (referred to as RO-GelMA) are regarded as most suitable to achieve high DLP-SLA printing resolution. RO-GelMA-based bioinks are also found to be biocompatible showing high survival rates of encapsulated cells in the photocrosslinked gels. Additionally, the astrocytes and fibroblasts are observed to grow and integrate well within the bioprinted constructs. The bioink's superior physical and photocrosslinking properties offer pathways of tuning the scaffold microenvironment and highlight the applicability of developed GelMA bioinks in various tissue engineering and regenerative medicine applications.
Subject(s)
Bioprinting , Gelatin/pharmacology , Methacrylates/pharmacology , Stereolithography , Tissue Engineering , Cell Survival/drug effects , Gelatin/chemical synthesis , Gelatin/radiation effects , Humans , Hydrogels/chemistry , Hydrogels/pharmacology , Ink , Light , Methacrylates/chemical synthesis , Methacrylates/radiation effects , Printing, Three-Dimensional , Tissue Scaffolds/chemistryABSTRACT
Cells in vivo are constantly subjected to multiple microenvironmental mechanical stimuli that regulate cell function. Although 2D cell responses to the mechanical stimulation have been established, these methods lack relevance as physiological cell microenvironments are in 3D. Moreover, the existing platforms developed for studying the cell responses to mechanical cues in 3D either offer low-throughput, involve complex fabrication, or do not allow combinatorial analysis of multiple cues. Considering this, a stretchable high-throughput (HT) 3D cell microarray platform is presented that can apply dynamic mechanical strain to cells encapsulated in arrayed 3D microgels. The platform uses inkjet-bioprinting technique for printing cell-laden gelatin methacrylate (GelMA) microgel array on an elastic composite substrate that is periodically stretched. The developed platform is highly biocompatible and transfers the applied strain from the stretched substrate to the cells. The HT analysis is conducted to analyze cell mechano-responses throughout the printed microgel array. Also, the combinatorial analysis of distinct cell behaviors is conducted for different GelMA microenvironmental stiffnesses in addition to the dynamic stretch. Considering its throughput and flexibility, the developed platform can readily be scaled up to introduce a wide range of microenvironmental cues and to screen the cell responses in a HT way.
Subject(s)
Bioprinting , High-Throughput Screening Assays , Gelatin , Hydrogels , Methacrylates , Printing, Three-DimensionalABSTRACT
Microdroplets have been widely used in various biomedical applications. During droplet generation, parameters are manually adjusted to achieve the desired size of droplets. This process is tedious and time-consuming. In this paper, we present a fully automated system for controlling the size of droplets to optimize droplet generation parameters in a microfluidic flow-focusing device. The developed system employed a novel image processing program to measure the diameter of droplets from recorded video clips and correspondingly adjust the flow rates of syringe pumps to obtain the required diameter of droplets. The system was tested to generate phosphate-buffered saline and 8% polyethylene (glycol) diacrylate prepolymer droplets and regulate its diameters at various flow rates. Experimental results demonstrated that the difference between droplet diameters from the image processing and manual measurement is not statistically significant and the results are consistent over five repetitions. Taking the advantages of the accurate image processing method, the size of the droplets can be optimized in a precise and robust manner via automatically adjusting flow rates by the feedback control. The system was used to acquire quantitative data to examine the effects of viscosity and flow rates. Droplet-based experiments can be greatly facilitated by the automatic droplet generation and optimization system. Moreover, the system is able to provide quantitative data for the modelling and application of droplets with various conditions in a high-throughput way.
