首页> 外文期刊>Tissue engineering, Part A >Differential morphology and homogeneity of tissue-engineered cartilage in hydrodynamic cultivation with transient exposure to insulin-like growth factor-1 and transforming growth factor-β1
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Differential morphology and homogeneity of tissue-engineered cartilage in hydrodynamic cultivation with transient exposure to insulin-like growth factor-1 and transforming growth factor-β1

机译:瞬时暴露于胰岛素样生长因子-1和转化生长因子-β1的水动力培养中组织工程软骨的形态和同质性差异

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Successful tissue-engineering strategies for cartilage repair must maximize the efficacy of chondrocytes within their limited life span. To that end, the combination of exogenous growth factors with mechanical stimuli holds promise for development of clinically relevant cartilage tissue substitutes. The current study aimed to determine whether incorporation of transient exposure to growth factors into a hydrodynamic bioreactor system can improve the functional maturation of tissue-engineered cartilage. Chondrocyte-seeded polyglycolic acid scaffolds were cultivated within a wavy-walled bioreactor that imparts fluid flow-induced shear stress for 4 weeks. Constructs were nourished with 100 ng/mL insulin-like growth factor-1 (IGF-1) or 10 ng/mL transforming growth factor-β1 (TGF-β1) either for the first 15 days of the culture (transient) or throughout the entire cultivation (continuous). Transiently treated constructs were found to exhibit better functional properties than continuously nourished constructs. The limited development of engineered tissues continuously stimulated by IGF-1 or TGF-β1 was related to massive growth factor leftovers in the environments that downregulated the expression of the associated receptors. Treatment with TGF-β1 eliminated the formation of a fibrous capsule at the construct periphery possibly through suppression of Smad3 phosphorylation, yielding constructs with greater homogeneity. Furthermore, TGF-β1 reversely regulated Smad2 and Smad3 pathways in articular chondrocytes under hydrodynamic stimuli partially via Smad7. Collectively, transient exposure to growth factors is likely to maintain chondrocyte homeostasis, and thus promotes their anabolic activities under hydrodynamic stimuli. The present work suggests that robust hydrodynamically engineered neocartilage with a reduced fibrotic response and enhanced tissue homogeneity can be achieved through optimization of growth factor supplementation protocols and potentially through manipulation of intracellular signals such as Smad.
机译:成功的软骨修复组织工程策略必须在有限的寿命内最大化软骨细胞的功效。为此,外源性生长因子与机械刺激的结合为开发临床相关的软骨组织替代物提供了希望。当前的研究旨在确定是否将暂时暴露于生长因子的流体动力学生物反应器系统并入可以改善组织工程软骨的功能成熟。在波状壁生物反应器中培养接种了软骨细胞的聚乙醇酸支架,该生物反应器可提供流体流动引起的剪切应力,持续4周。在培养的前15天(整个过程)或整个培养过程中,均用100 ng / mL胰岛素样生长因子-1(IGF-1)或10 ng / mL转化生长因子-β1(TGF-β1)滋养构建体。整个种植(连续)。发现与连续营养的构建体相比,瞬时处理的构建体表现出更好的功能特性。在下调相关受体表达的环境中,IGF-1或TGF-β1连续刺激的工程组织的有限发育与大量的生长因子残留有关。用TGF-β1处理可能通过抑制Smad3磷酸化消除了在构建体外围的纤维囊的形成,从而产生了具有更高同质性的构建体。此外,TGF-β1在流体动力刺激下通过Smad7反向调节关节软骨细胞中的Smad2和Smad3途径。总的来说,短暂暴露于生长因子可能会维持软骨细胞的稳态,从而在水动力刺激下促进其合成代谢活性。目前的工作表明,可以通过优化生长因子补充方案以及潜在地通过操纵细胞内信号(例如Smad)来实现具有降低的纤维化反应和增强的组织均匀性的强大的水动力工程化新软骨。

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