Porous scaffold architecture guides tissue formation

Porous scaffold architecture guides tissue formation

Critical‐sized bone defect regeneration is a remaining clinical concern. Numerous scaffold‐based strategies are currently being investigated to enable in vivo bone defect healing. However, a deeper understanding of how a scaffold influences the tissue formation process and how this compares to endog...

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Veröffentlicht in:Journal of bone and mineral research 2012-06, Vol.27 (6), p.1275-1288
Hauptverfasser: Cipitria, Amaia, Lange, Claudia, Schell, Hanna, Wagermaier, Wolfgang, Reichert, Johannes C, Hutmacher, Dietmar W, Fratzl, Peter, Duda, Georg N
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Biodegradation, Environmental - drug effects
Biological and medical sciences
Bone (cortical)
Bone growth
Bone healing
Calcification, Physiologic - drug effects
Calcium Phosphates - pharmacology
CRITICAL-SIZED DEFECT
Elastic Modulus - drug effects
Fundamental and applied biological sciences. Psychology
Guided Tissue Regeneration - methods
imaging
INDENTATION MODULUS
Mechanical properties
Mineralization
Osteogenesis
Osteogenesis - drug effects
OVINE DEFECT MODEL
Polyesters - pharmacology
Porosity - drug effects
Regeneration
SCAFFOLD-GUIDED BONE REGENERATION
scaffolds
SCANNING SMALL-ANGLE X-RAY SCATTERING
Scattering, Small Angle
Sheep
Skeleton and joints
Tibia - drug effects
Tibia - pathology
Tissue Scaffolds - chemistry
Vertebrates: osteoarticular system, musculoskeletal system
X-Ray Diffraction
X-ray scattering
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Zusammenfassung:Critical‐sized bone defect regeneration is a remaining clinical concern. Numerous scaffold‐based strategies are currently being investigated to enable in vivo bone defect healing. However, a deeper understanding of how a scaffold influences the tissue formation process and how this compares to endogenous bone formation or to regular fracture healing is missing. It is hypothesized that the porous scaffold architecture can serve as a guiding substrate to enable the formation of a structured fibrous network as a prerequirement for later bone formation. An ovine, tibial, 30‐mm critical‐sized defect is used as a model system to better understand the effect of the scaffold architecture on cell organization, fibrous tissue, and mineralized tissue formation mechanisms in vivo. Tissue regeneration patterns within two geometrically distinct macroscopic regions of a specific scaffold design, the scaffold wall and the endosteal cavity, are compared with tissue formation in an empty defect (negative control) and with cortical bone (positive control). Histology, backscattered electron imaging, scanning small‐angle X‐ray scattering, and nanoindentation are used to assess the morphology of fibrous and mineralized tissue, to measure the average mineral particle thickness and the degree of alignment, and to map the local elastic indentation modulus. The scaffold proves to function as a guiding substrate to the tissue formation process. It enables the arrangement of a structured fibrous tissue across the entire defect, which acts as a secondary supporting network for cells. Mineralization can then initiate along the fibrous network, resulting in bone ingrowth into a critical‐sized defect, although not in complete bridging of the defect. The fibrous network morphology, which in turn is guided by the scaffold architecture, influences the microstructure of the newly formed bone. These results allow a deeper understanding of the mode of mineral tissue formation and the way this is influenced by the scaffold architecture. © 2012 American Society for Bone and Mineral Research.
ISSN:0884-0431
1523-4681
DOI:10.1002/jbmr.1589