Department of Mechanical and Aerospace Engineering, Case Western Reserve University, Cleveland, OH 44106, USA.
Biomaterials. 2012 Mar;33(7):2137-44. doi: 10.1016/j.biomaterials.2011.11.066. Epub 2011 Dec 15.
Topographical cues from the extracellular microenvironment can influence cellular activity including proliferation and differentiation. Information on the effects of material topography on tenogenic differentiation of human mesenchymal stem cells (human MSCs) is limited. A methodology using the principles of isoelectric focusing has previously been developed in our laboratory to synthesize electrochemically aligned collagen (ELAC) threads that mimics the packing density, alignment and strength of collagen dense connective tissues. In the current study, human MSCs were cultured on ELAC and randomly oriented collagen threads and the effect of collagen orientation on cell morphology, proliferation and tenogenic differentiation was investigated. The results indicate that higher rates of proliferation were observed on randomly oriented collagen threads compared to ELAC threads. On the other hand, tendon specific markers such as scleraxis and tenomodulin, were significantly increased on ELAC threads compared to randomly oriented collagen threads. Additionally, osteocalcin, a specific marker of bone differentiation was suppressed on ELAC threads. Previous studies have reported that BMP-12 is a key growth factor to induce tenogenic differentiation of MSCs. To evaluate the synergistic effect of BMP-12 and collagen orientation, human MSCs were cultured on ELAC threads in culture medium supplemented with and without BMP-12. The results revealed that BMP-12 did not have an additional effect on the tenogenic differentiation of human MSCs on ELAC threads. Together, these results suggest that ELAC induces tenogenic differentiation of human MSCs by presenting an aligned and dense collagen substrate, akin to the tendon itself. In conclusion, ELAC has a significant potential to be used as a tendon replacement and in the development of an osteotendinous construct towards the regeneration of bone-tendon interfaces.
细胞外微环境的拓扑线索可以影响细胞的活动,包括增殖和分化。关于材料拓扑结构对人骨髓间充质干细胞(hMSC)腱向分化影响的信息有限。我们实验室之前采用等电聚焦原理开发了一种方法,合成电化学定向胶原(ELAC)纤维,这种纤维模拟了胶原致密结缔组织的堆积密度、取向和强度。在本研究中,hMSC 被培养在 ELAC 和随机定向胶原纤维上,研究胶原取向对细胞形态、增殖和腱向分化的影响。结果表明,与 ELAC 纤维相比,随机定向胶原纤维上观察到更高的增殖率。另一方面,与随机定向胶原纤维相比,ELAC 纤维上腱特异性标志物如 Scleraxis 和 Tenomodulin 显著增加。此外,骨钙素,一种骨分化的特异性标志物,在 ELAC 纤维上受到抑制。先前的研究报道 BMP-12 是诱导 MSC 腱向分化的关键生长因子。为了评估 BMP-12 和胶原取向的协同作用,将 hMSC 培养在补充有和没有 BMP-12 的 ELAC 纤维上的培养基中。结果表明,BMP-12 对 ELAC 纤维上 hMSC 的腱向分化没有额外作用。总之,ELAC 通过提供类似肌腱本身的定向和致密胶原基质来诱导 hMSC 的腱向分化。总之,ELAC 具有作为肌腱替代物和开发骨腱构建体以再生骨-腱界面的巨大潜力。
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