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A specific affinity cyclic peptide enhances the adhesion, expansion and proliferation of rat bone mesenchymal stem cells on beta-tricalcium phosphate scaffolds

机译:特定亲和力环肽增强大鼠骨间充质干细胞对β-三钙的磷酸钙细胞的粘附,膨胀和增殖

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摘要

Osteonecrosis of the femoral head (ONFH) is a common osteological disease. Treatment of ONFH prior to the collapse of the femoral head is critical for increasing therapeutic efficiency. Tissue engineering therapy using bone mesenchymal stem cells (BMSCs) combined with a scaffold is a promising strategy. However, it is currently unclear how to improve the efficiency of BMSC recruitment under such conditions. In the present study, a specific cyclic peptide for Sprague-Dawley rat BMSCs, CTTNPFSLC (known as C7), was used, which was identified via phage display technology. Its high affinity for BMSCs was demonstrated using flow cytometry and fluorescence staining. Subsequently, the cyclic peptide was placed on beta-tricalcium phosphate (beta-TCP) scaffolds using absorption and freeze-drying processes. Adhesion, expansion and proliferation of BMSCs was investigated in vitro on the C7-treated beta-TCP scaffolds and compared with pure beta-TCP scaffolds. The results revealed that C7 had a promoting effect on the adhesion, expansion and proliferation of BMSCs on beta-TCP scaffolds. Therefore, C7 may be effective in future tissue engineering therapy for ONFH.
机译:股骨头的骨折(ON​​FH)是一种常见的骨质疾病。在股骨头坍塌之前对ONFH进行治疗对于提高治疗效率至关重要。使用骨髓间充质干细胞(BMSC)与支架的组织工程治疗是一个有前途的策略。但是,目前不清楚如何在这种条件下提高BMSC招聘的效率。在本研究中,使用Sprague-Dawley大鼠BMSCs,CTTNPFSLC(称为C7)的特定环肽,通过噬菌体显示技术鉴定。使用流式细胞术和荧光染色来证明其对BMSC的高亲和力。随后,使用吸收和冷冻干燥方法将环肽置于β-三钙(β-TCP)支架上。对BMSCs的粘附,膨胀和增殖在C7处理的β-TCP支架上进行体外研究,并与纯β-TCP支架进行比较。结果表明,C7对BMSCs对β-TCP支架的粘附,膨胀和增殖具有促进作用。因此,C7可以在未来的组织工程治疗中有效。

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