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The inhibition by interleukin 1 of MSC chondrogenesis and the development of biomechanical properties in biomimetic 3D woven PCL scaffolds

机译:MSC软骨发生的白细胞介素1的抑制与仿生3D编织PCL支架中的生物力学性能的发展

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摘要

Tissue-engineered constructs designed to treat large cartilage defects or osteoarthritic lesions may be exposed to significant mechanical loading as well as an inflammatory environment upon implantation in an injured or diseased joint. We hypothesized that a three-dimensionally (3D) woven poly(ε-caprolactone) (PCL) scaffold seeded with bone marrow-derived mesenchymal stem cells (MSCs) would provide biomimetic mechanical properties in early stages of in vitro culture as the MSCs assembled a functional, cartilaginous extracellular matrix (ECM). We also hypothesized that these properties would be maintained even in the presence of the pro-inflammatory cytokine interleukin-1 (IL-1), which is found at high levels in injured or diseased joints. MSC-seeded 3D woven scaffolds cultured in chondrogenic conditions synthesized a functional ECM rich in collagen and proteoglycan content, reaching an aggregate modulus of ~0.75 MPa within 14 days of culture. However, the presence of pathophysiologically relevant levels of IL-1 limited matrix accumulation and inhibited any increase in mechanical properties over baseline values. On the other hand, the mechanical properties of constructs cultured in chondrogenic conditions for 4 weeks prior to IL-1 exposure were protected from deleterious effects of the cytokine. These findings demonstrate that IL-1 significantly inhibits the chondrogenic development and maturation of MSC-seeded constructs; however, the overall mechanical functionality of the engineered tissue can be preserved through the use of a 3D woven scaffold designed to recreate the mechanical properties of native articular cartilage.
机译:在植入受伤或患病的关节后,旨在治疗大型软骨缺损或骨关节炎病变的组织工程化构造可能会暴露于明显的机械负荷以及炎性环境。我们假设,植入骨髓来源的间充质干细胞(MSC)的三维(3D)机织聚(ε-己内酯)(PCL)支架将在体外培养的早期阶段提供仿生机械性能,因为MSC组装了功能性软骨细胞外基质(ECM)。我们还假设即使存在促炎性细胞因子白介素-1(IL-1)(在受伤或患病的关节中含量很高)时,这些特性也能保持。在软骨形成条件下培养的带有MSC的3D编织支架合成了富含胶原蛋白和蛋白聚糖含量的功能性ECM,在培养的14天之内达到了约0.75 MPa的聚集模量。但是,IL-1的病理生理相关水平的存在限制了基质的积累,并抑制了机械性能超过基线值的任何增加。另一方面,保护了在暴露于IL-1之前在软骨形成条件下培养4周的构建体的机械性能不受细胞因子的有害影响。这些发现表明IL-1显着抑制了MSC接种的构建体的软骨形成和成熟。但是,可以通过使用3D编织支架来保留工程组织的整体机械功能,该3D编织支架旨在重建天然关节软骨的机械特性。

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