390                19. IMPACT OF MECHANOBIOLOGICAL PERTURBATION IN CARTILAGE TISSUE ENGINEERING

            [74] B.M. Baker, et al., The influence of an aligned nanofibrous topography on human mesenchymal stem cell fibrochondrogenesis, Biomaterials
                31 (24) (2010) 6190–6200.
            [75] J.K. Wise, et al., Chondrogenic differentiation of human mesenchymal stem cells on oriented nanofibrous scaffolds: engineering the superficial
                zone of articular cartilage, Tissue Eng. Part A 15 (4) (2009) 913–921.
            [76] W.J. Li, et al., Engineering controllable anisotropy in electrospun biodegradable nanofibrous scaffolds for musculoskeletal tissue engineering,
                J. Biomech. 40 (8) (2007) 1686–1693.
            [77] Y.N. Wu, et al., Substrate topography determines the fate of chondrogenesis from human mesenchymal stem cells resulting in specific cartilage
                phenotype formation, Nanomedicine 10 (7) (2014) 1507–1516.
            [78] Y. Wu, et al., The combined effect of substrate stiffness and surface topography on chondrogenic differentiation of mesenchymal stem cells,
                Tissue Eng. Part A 23 (1–2) (2017) 43–54.
            [79] S.D. McCullen, et al., Anisotropic fibrous scaffolds for articular cartilage regeneration, Tissue Eng. Part A 18 (19–20) (2012) 2073–2083.
            [80] J.A. Steele, et al., Combinatorial scaffold morphologies for zonal articular cartilage engineering, Acta Biomater. 10 (5) (2014) 2065–2075.
            [81] D. Kumar, A.B. Lassar, The transcriptional activity of Sox9 in chondrocytes is regulated by RhoA signaling and actin polymerization, Mol. Cell.
                Biol. 29 (15) (2009) 4262–4273.
            [82] A. Woods, F. Beier, RhoA/ROCK signaling regulates chondrogenesis in a context-dependent manner, J. Biol. Chem. 281 (19) (2006)
                13134–13140.
            [83] A. Woods, G. Wang, F. Beier, RhoA/ROCK signaling regulates Sox9 expression and actin organization during chondrogenesis, J. Biol. Chem.
                280 (12) (2005) 11626–11634.
            [84] Y. Wang, et al., Orientation and repositioning of chromosomes correlate with cell geometry-dependent gene expression, Mol. Biol. Cell 28 (14)
                (2017) 1997–2009.
            [85] C.H. Thomas, et al., Engineering gene expression and protein synthesis by modulation of nuclear shape, Proc. Natl. Acad. Sci. U. S. A. 99 (4)
                (2002) 1972–1977.
            [86] T.P. Driscoll, et al., Cytoskeletal to nuclear strain transfer regulates YAP signaling in mesenchymal stem cells, Biophys. J. 108 (12) (2015)
                2783–2793.
            [87] W. Zhong, et al., YAP-mediated regulation of the chondrogenic phenotype in response to matrix elasticity, J. Mol. Histol. 44 (5) (2013) 587–595.
            [88] A. Karystinou, et al., Yes-associated protein (YAP) is a negative regulator of chondrogenesis in mesenchymal stem cells, Arthritis Res. Ther.
                17 (2015) 147.
            [89] S. Wan, et al., FAK- and YAP/TAZ dependent mechanotransduction pathways are required for enhanced immunomodulatory properties of
                adipose-derived mesenchymal stem cells induced by aligned fibrous scaffolds, Biomaterials 171 (2018) 107–117.
            [90] J. Rieppo, et al., Changes in spatial collagen content and collagen network architecture in porcine articular cartilage during growth and mat-
                uration, Osteoarthr. Cartil. 17 (4) (2009) 448–455.
            [91] P. Julkunen, et al., Maturation of collagen fibril network structure in tibial and femoral cartilage of rabbits, Osteoarthr. Cartil. 18 (3) (2010)
                406–415.
            [92] A.J. Steward, D.J. Kelly, Mechanical regulation of mesenchymal stem cell differentiation, J. Anat. 227 (6) (2015) 717–731.
            [93] M. Wong, M. Siegrist, X. Cao, Cyclic compression of articular cartilage explants is associated with progressive consolidation and altered
                expression pattern of extracellular matrix proteins, Matrix Biol. 18 (4) (1999) 391–399.
            [94] R.L. Mauck, et al., Functional tissue engineering of articular cartilage through dynamic loading of chondrocyte-seeded agarose gels, J. Biomech.
                Eng. 122 (3) (2000) 252–260.
            [95] K.W. Ng, et al., Duty cycle of deformational loading influences the growth of engineered articular cartilage, Cell. Mol. Bioeng. 2 (3) (2009)
                386–394.
            [96] F. Guilak, et al., The effects of matrix compression on proteoglycan metabolism in articular cartilage explants, Osteoarthr. Cartil. 2 (2) (1994)
                91–101.
            [97] R.L. Smith, et al., Time-dependent effects of intermittent hydrostatic pressure on articular chondrocyte type II collagen and aggrecan mRNA
                expression, J. Rehabil. Res. Dev. 37 (2) (2000) 153–161.
            [98] R.L. Smith, et al., In vitro stimulation of articular chondrocyte mRNA and extracellular matrix synthesis by hydrostatic pressure, J. Orthop. Res.
                14 (1) (1996) 53–60.
            [99] C.Y. Huang, P.M. Reuben, H.S. Cheung, Temporal expression patterns and corresponding protein inductions of early responsive genes in
                rabbit bone marrow-derived mesenchymal stem cells under cyclic compressive loading, Stem Cells 23 (8) (2005) 1113–1121.
           [100] J.K. Mouw, et al., Dynamic compression regulates the expression and synthesis of chondrocyte-specific matrix molecules in bone marrow
                stromal cells, Stem Cells 25 (3) (2007) 655–663.
           [101] D. Pelaez, C.Y. Huang, H.S. Cheung, Cyclic compression maintains viability and induces chondrogenesis of human mesenchymal stem cells in
                fibrin gel scaffolds, Stem Cells Dev. 18 (1) (2009) 93–102.
           [102] Z. Li, et al., Chondrogenesis of human bone marrow mesenchymal stem cells in fibrin-polyurethane composites is modulated by frequency and
                amplitude of dynamic compression and shear stress, Tissue Eng. Part A 16 (2) (2010) 575–584.
           [103] P. Angele, et al., Cyclic hydrostatic pressure enhances the chondrogenic phenotype of human mesenchymal progenitor cells differentiated
                in vitro, J. Orthop. Res. 21 (3) (2003) 451–457.
           [104] K. Miyanishi, et al., Effects of hydrostatic pressure and transforming growth factor-beta 3 on adult human mesenchymal stem cell chondro-
                genesis in vitro, Tissue Eng. 12 (6) (2006) 1419–1428.
           [105] K. Sakao, et al., Induction of chondrogenic phenotype in synovium-derived progenitor cells by intermittent hydrostatic pressure, Osteoarthr.
                Cartil. 16 (7) (2008) 805–814.
           [106] Z. Li, et al., Mechanical load modulates chondrogenesis of human mesenchymal stem cells through the TGF-beta pathway, J. Cell. Mol. Med.
                14 (6A) (2010) 1338–1346.
           [107] A.H. Huang, et al., Long-term dynamic loading improves the mechanical properties of chondrogenic mesenchymal stem cell-laden hydrogel,
                Eur. Cell. Mater. 19 (2010) 72–85.
           [108] M.G. Haugh, et al., Temporal and spatial changes in cartilage-matrix-specific gene expression in mesenchymal stem cells in response to
                dynamic compression, Tissue Eng. Part A 17 (23–24) (2011) 3085–3093.



                                          II. MECHANOBIOLOGY AND TISSUE REGENERATION