Abstract
Tissue Engineering has expanded rapidly towards target applications of tissue repair and regeneration, whilst generating surprisingly novel models to study tissue modelling. However, clinical success in producing effective engineered tissues such as bone, skin, cartilage, and tendon, have been rare and limited. Problems tend to focus on how to stimulate the replacement of initial scaffold with mechanically functional, native extracellular matrix (principally collagen). Typical approaches have been to develop perfused and mechanically active bioreactors, with the use of native collagen itself as the initial scaffold, though the idea remains that cells do the fabrication (i.e. a cultivation process). We have developed a new, engineering approach, in which the final collagen template is fabricatedwithout cell involvement. The first part of this biomimetic engineering involves a plastic compression of cellular native collagen gels to form dense, strong, collagenous neotissues (in minutes). Further steps can be used to orientate and increase collagen fibril diameter, again by non-cell dependent engineering. This allows operator control of cell or matrix density and material properties (influencing biological half life and fate). In addition, this (non-cultivation) approach can incorporate techniques to generate localised 3D structures and zones at a meso-scale. In conclusion, the use of biomimetic engineering based on native collagen, rather than cell-cultivation approaches for bulk matrix fabrication, produces huge benefits. These include speed of fabrication (minutes instead of weeks and months), possibility of fine control of composition and 3D nano-micro scale structure and biomimetic complexity.
This is a preview of subscription content, log in via an institution to check access.
Similar content being viewed by others
References
Rheinwald, J. G. and H. Green (1975) Serial cultivation of strains of human epidermal keratinocytes: the formation of keratinizing colonies from single cells.Cell 6: 331–343.
Eastwood, M., V. C. Mudera, D. A. McGrouther, and R. A. Brown (1998) Effect of precise mechanical loading on fibroblast populated collagen lattices: morphological changes.Cell Motil. Cytoskeleton. 40: 13–21.
Bell, E., S. Sher, and B. Hull (1984) The living skin-equivalent as a structural and immunological model in skin grafting.Scan. Electron Microsc. 4: 1957–1962.
Falanga, V., D. Margolis, O. Alvarez, M. Auletta, F. Maggiacomo, M. Altman, J. Jensen, M. Sabolinski, and J. Hardin-Young (1998) Rapid healing of venous ulcers and lack of clinical rejection with an allogeneic cultured human skin equivalent.Arch. Dermatol. 134: 293–300.
Foroughi, F. and R. A. Brown, Collagen incorporation rates into bulk tissue engineering scaffolds: the rate limiting step. (in prep).
Ahsan, T., A. C. Chen, L. Chin, V. W. Wong, R. A. Bank, N. Verzijl, R. L. Sah, and A. Ratcliffe (2003) Effects of long term growth on tissue engineered cartilage.49th Annual Meeting of the Orthopaedic Research Society. Paper #0309.
Brown, R. A. (2006) Cytomechanics in connective tissue repair and engineering. pp. 7–24. In: C. Chaponnier, A. Desmoulière, and G. Gabbiani (eds.).Tissue Repair, Contraction and the Myofibroblast. Landes Bioscience, Georgetown, TX, USA.
Clark, L. D., R. K. Clark, and E. Heber-Katz (1998) A new murine model for mammalian wound repair and regeneration.Clin. Immunol. Immunopathol. 88: 35–45.
Elsdale, T. and J. Bard (1972) Collagen substrata for studies on cell behavior.J. Cell Biol. 54: 626–637.
Brown, R. A., M. Wiseman, C.-B. Chuo, U. Cheema, and S. N. Nazhat (2005) Ultra-rapid engineering of biomimetic tissues: A plastic compression fabrication process for nano-micro structures.Adv. Funct. Mater. 15: 1762–1770.
Dickinson, R. B., S. Guido, and R. T. Tranquillo (1994) Biased cell migration of fibroblasts exhibiting contact guidance in oriented collagen gels.Ann. Biomed. Eng. 22: 342–356.
Kostyuk, O. and R. A. Brown (2004) Novel spectroscopic technique forin situ monitoring of collagen fibril alignment in gels.Biophys. J. 87: 648–655.
Cheema, U., C.-B. Chuo, P. Sarathchandra, S. N. Nazhat, and R. A. Brown, Engineering collagen scaffolds: Cyclical loading increases material strength and fibril aggregation. (submitted).
Nazhat, S. N., E. A. Abou Neel, A. Kidane, I. Ahmed, C. Hope, M. Kershaw, P. D. Lee, E. Stride, N. Saffari, J. C. Knowles, and R. A. Brown (2007) Controlled microchanelling in dense collagen scaffolds by soluble phosphate glass fibers.Biomacromolecules 8: 543–551.
Frank, C., S. Woo, T. Andriacchi,et al. (1991) Normal ligament: structure, function and composition. pp. 45–101. In:Injury and Repair of the Musculoskeletal Soft Tissue, 2nd ed., American Academy of Orthopaedic Surgeons, Park Ridge, IL, USA.
Abou Neel, E. A., U. Cheema, J. C. Knowles, R. A. Brown, and S. N. Nazhat (2006) Use of multiple unconfined compression for control of collagen gel scaffold density and mechanical properties.Soft Matter 2: 986–992.
Author information
Authors and Affiliations
Corresponding author
Rights and permissions
About this article
Cite this article
Cheema, U., Nazhat, S.N., Alp, B. et al. Fabricating tissues: Analysis of farming versus engineering strategies. Biotechnol. Bioprocess Eng. 12, 9–14 (2007). https://doi.org/10.1007/BF02931797
Received:
Accepted:
Issue Date:
DOI: https://doi.org/10.1007/BF02931797