Combination of platelet‐rich plasma with polycaprolactone‐tricalcium phosphate scaffolds for segmental bone defect repair

Rai, Bina; Oest, Megan E.; Dupont, Ken M.; Ho, Kee H.; Teoh, Swee H.; Guldberg, Robert E.

Affiliations

¹Department of Oral and Maxillofacial Surgery, National University of Singapore, Singapore

²Department of Biomedical Engineering, Georgia Institute of Technology, Atlanta, Georgia

³School of Mechanical Engineering, Georgia Institute of Technology, Atlanta, Georgia

⁴Department of Mechanical Engineering, National University of Singapore, Singapore

Abstract and keywords

Porous scaffold biomaterials may offer a clinical alternative to bone grafts; however, scaffolds alone are typically insufficient to heal large bone defects. Numerous studies have demonstrated that osteoinductive growth factor or gene delivery significantly improves bone repair. However, given the important role of vascularization during bone regeneration, it may also be beneficial to incorporate factors that promote vascular ingrowth into constructs. In this study, a strategy combining structural polycaprolactone‐20% tricalcium phosphate (PCL‐TCP) composite scaffolds with platelet‐rich plasma (PRP) was tested. Following bilateral implantation of constructs into 8 mm rat nonunion femoral defects, 3D vascular and bone ingrowth were quantified at 3 and 12 weeks using contrast‐enhanced microcomputed tomography (micro‐CT) imaging. At week 3, PRP‐treated femurs displayed 70.3% higher vascular volume fraction than control femurs. Interestingly, bone volume fraction (BVF) was significantly higher for the empty scaffold group at the early time point. At 12 weeks, BVF measurements between the two groups were statiscally equivalent. However, a greater proportion of PRP‐treated femurs (83%) achieved bone union as compared to empty scaffold controls (33%). Consistent with this observation, biomechanical evaluation of functional integration also revealed a significantly higher torsional stiffness observed for PRP‐treated defects compared to empty scaffolds. Ultimate torque at failure was not improved, however, perhaps due to the slow resorption profile of the scaffold material. Histological evaluation illustrated infiltration of vascularized connective tissue and bone in both groups. Given that bone ingrowth into untreated defects in this model is minimal, PCL‐TCP scaffolds were clearly able to promote bone ingrowth but failed to consistently bridge the defect. The addition of PRP to PCL‐TCP scaffolds accelerated early vascular ingrowth and improved longer‐term functional integration. Taken together, the results of this study suggest that the use of PRP, alone or in combination with other bioactive components, may be an effective approach to augment the ability of porous biomaterial scaffolds to repair orthotopic defects.

Keywords: bone regeneration; vascularization; polycaprolactone; scaffold; growth factors

Links

DOI: 10.1002/jbm.a.31142

PubMed: 17236215

WoS: 000246636600013

History

Received: 2006-06-11

Revised: 2006-08-20

Accepted: 2006-10-09

Online: 2007-01-18

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Cited By (17)

Year	Entry
2011	Kolambkar YM, Dupont KM, Boerckel JD, Huebsch N, Mooney DJ, Hutmacher DW, Guldberg RE. An alginate-based hybrid system for growth factor delivery in the functional repair of large bone defects. Biomaterials. January 2011;32(1):65-74.
2012	Dupont KM, Boerckel JD, Stevens HY, Diab T, Kolambkar YM, Takahata M, Schwarz EM, Guldberg RE. Synthetic scaffold coating with adeno-associated virus encoding BMP2 to promote endogenous bone repair. Cell Tissue Res. March 2012;347(3):575-588.
2009	Boerckel JD, Dupont KM, Kolambkar YM, Lin ASP, Guldberg RE. In vivo model for evaluating the effects of mechanical stimulation on tissue-engineered bone repair. J Biomech Eng. August 2009;131(8):084502.
2010	Bouxsein ML, Boyd SK, Christiansen BA, Guldberg RE, Jepsen KJ, Müller R. Guidelines for assessment of bone microstructure in rodents using micro-computed tomography. J Bone Miner Res. July 2010;25(7):1468-1486.
2010	Dupont KM, Sharma K, Stevens HY, Boerckel JD, García AJ, Guldberg RE. Human stem cell delivery for treatment of large segmental bone defects. Proc Natl Acad Sci USA. February 23, 2010;107(8):3305-3310.
2011	Boerckel JD, Uhrig BA, Willett NJ, Huebsch N, Guldberg RE. Mechanical regulation of vascular growth and tissue regeneration in vivo. Proc Natl Acad Sci USA. September 13, 2011;108(37):E674-E680.
2013	Nebuloni L. Monitoring Angiogenesis in Tissue Engineering Through Time-Lapsed Vascular Imaging [PhD thesis]. Swiss Federal Institute of Technology Zürich; 2013.
2007	Oest ME. Dual Osteogenic and Angiogenic Growth Factor Delivery as a Treatment for Segmental Bone Defects [PhD thesis]. Atlanta, GA: Georgia Institute of Technology; August 2007.
2009	Deutsch ER. The Use of Stem Cell Synthesized Extracellular Matrix for Bone Repair [Master's thesis]. Atlanta, GA: Georgia Institute of Technology; December 2009.
2009	Wojtowicz AM. Genetically-Engineered Bone Marrow Stromal Cells and Collagen Mimetic Scaffold Modification for Healing Critically-Sized Bone Defects [PhD thesis]. Atlanta, GA: Georgia Institute of Technology; August 2009.
2009	Kolambkar YM. Electrospun Nanofiber Meshes for the Functional Repair of Bone Defects [PhD thesis]. Atlanta, GA: Georgia Institute of Technology; December 2009.
2010	Dupont KM. Human Stem Cell Delivery and Programming for Functional Regeneration of Large Segmental Bone Defects [PhD thesis]. Atlanta, GA: Georgia Institute of Technology; May 2010.
2010	Johnson MR. Delivery of BMP-2 for Bone Tissue Engineering Applications [PhD thesis]. Atlanta, GA: Georgia Institute of Technology; May 2010.
2011	Boerckel JD. Mechanical Regulation of Bone Regeneration and Vascular Growth in Vivo [PhD thesis]. Atlanta, GA: Georgia Institute of Technology; August 2011.
2015	Allen AB. Modulation of Stem Cell Delivery Strategy by Platelet Lysate Utilization and Cell Aggregation for Enhanced Bone Regeneration [PhD thesis]. Atlanta, GA: Georgia Institute of Technology; August 2015.
2017	Torstrick FB. Effects of Surface Chemistry and Surface Topography on Polyether-Ether-Ketone Osseointegration [PhD thesis]. Atlanta, GA: Georgia Institute of Technology; December 2017.
2011	Saito E. Designed Biodegradable and Osteoconductive Porous Scaffolds for Human Trabecular Bone [PhD thesis]. University of Michigan; 2011.