Understanding the effect of mean pore size on cell activity in collagen-glycosaminoglycan scaffolds

Abstract

Mean pore size is an essential aspect of scaffolds for tissue-engineering. If pores are too small cells cannot migrate in towards the centre of the construct limiting the diffusion of nutrients and removal of waste products. Conversely, if pores are too large there is a decrease in specific surface area available limiting cell attachment. However the relationship between scaffold pore size and cell activity is poorly understood and as a result there are conflicting reports within the literature on the optimal pore size required for successful tissue-engineering. Previous studies in bone tissue-engineering have indicated a range of mean pore sizes (96 μm-150 μm) to facilitate optimal attachment. Other studies have shown a need for large pores (300 μm-800 μm) for successful bone growth in scaffolds. These conflicting results indicate that a balance must be established between obtaining optimal cell attachment and facilitating bone growth. In this commentary we discuss our recent investigations into the effect of mean pore size in collagen- glycosaminoglycan (CG) scaffolds with pore sizes ranging from 85 μm-325 μm and how it has provided an insight into the divergence within the literature. © 2010 Landes Bioscience.