Table 2.
Overview of advantages and disadvantages of various scaffolds
| Scaffold | Advantages | Disadvantages |
| Porous scaffolds | High porosity | Use of highly toxic solvent |
| Interconnected structure | Low pore interconnectivity | |
| Simple and easy to manufacture | Difficulty in homogenous cell seeding post scaffold fabrication | |
| Highly porous scaffolds can have weak mechanical properties | ||
| Lack of control over scaffold thickness | ||
| Fibrous scaffolds | Fiber meshes and fiber bonding are simple techniques | Fiber meshes lack mechanical integrity |
| Large surface area-volume ratio | Fiber bonding lacks control over porosity and pore size | |
| High inter-fiber distances for nutrition and gas exchange | Small pore sizes produced during fabrication processes such as electrospinning limit cell infiltration and 3-D cellular integration with host tissue after implantation | |
| Hydrogels | Can form stable and highly ordered scaffolds using self assembly | |
| Tissue like flexibility | Higher cost | |
| Viscoelasticity | Non-adherent and usually need to be secured by a secondary dressing, for in-vivo testing | |
| Custom scaffolds (Computer-aided design technique) | Intestinal flow and diffusive transport | Natural polymer hydrogels like collagen gelatin, alginate and agarose may evoke inflammatory responses |
| Controlled matrix architecture: size, shape, interconnectivity, branching, geometry and orientation | Low resolution of current systems | |
| Can control pore and pore size | Selective polymeric materials can only be used | |
| Controlled mechanical properties and degradation kinetics | ||
| Microspheres | Reproducible architecture and compositional variations | |
| Used as cell carriers, when fabricated using biodegradable and non-toxic materials | Difficult to remove once injected or implanted | |
| Large surface area for cell attachment and growth | Unknown toxicity associated with microsphere/beads | |
| Native/Extracellular matrix scaffolds | Applicable for 3-D cell culture in a stirred suspension bioreactor Simulates the cell's natural microenvironment in terms of composition, bioactive signal and mechanical properties | Difficult to control degree of decellularization and retain all ECM |
| Non-uniform distribution of cells | ||
| Immunogenicity upon incomplete decellularization |