4.5 Article

FUNCTIONAL CELL PHENOTYPE INDUCTION WITH TGF-β1 AND COLLAGEN-POLYURETHANE SCAFFOLD FOR ANNULUS FIBROSUS RUPTURE REPAIR

期刊

EUROPEAN CELLS & MATERIALS
卷 39, 期 -, 页码 1-17

出版社

AO RESEARCH INSTITUTE DAVOS-ARI
DOI: 10.22203/eCM.v039a01

关键词

Annulus fibrosus; annular rupture repair; tissue engineering; transforming growth factor beta 1; polyurethane scaffold; collagen type I hydrogel

资金

  1. AO Foundation
  2. AO Spine International
  3. National Natural Science Foundation of China [81772333, 51873069]
  4. National Institutes of Health [R01AR064157]
  5. European Union's Horizon 2020 research and innovation programme under Marie Sklodowska-Curie fellowship [642414]
  6. Whitaker Foundation

向作者/读者索取更多资源

Appropriate cell sources, bioactive factors and biomaterials for generation of functional and integrated annulus fibrosus (AF) tissue analogues are still an unmet need. In the present study, the AF cell markers, collagen type I, duster of differentiation 146 (CD146), mohawk (MKX) and smooth muscle protein 22 alpha (SM22 alpha) were found to be suitable indicators of functional AF cell induction. In vitro 2D culture of human AF cells showed that transforming growth factor beta 1 (TGF-beta 1) upregulated the expression of the functional AF markers and increased cell contractility, indicating that TGF-beta 1-pre-treated AF cells were an appropriate cell source for AF tissue regeneration. Furthermore, a tissue engineered construct, composed of polyurethane (PU) scaffold with a TGF-beta 1-supplemented collagen type I hydrogel and human AF cells, was evaluated with in vitro 3D culture and ex vivo predinical bioreactor-loaded organ culture models. The collagen type I hydrogel helped maintaining the AF functional phenotype. TGF-beta 1 supplement within the collagen I hydrogel further promoted cell proliferation and matrix production of AF cells within in vitro 3D culture. In the ex vivo IVD organ culture model with physiologically relevant mechanical loading, TGF-beta 1 supplement in the transplanted constructs induced the functional AF cell phenotype and enhanced collagen matrix synthesis. In conclusion, TGF-beta 1-containing collagen-PU constructs could induce the functional cell phenotype of human AF cells in vitro and in situ. This combined cellular, biomaterial and bioactive agent therapy has a great potential for AF tissue regeneration and rupture repair.

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