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Biopanning of mouse bone marrow mesenchymal stem cell affinity for cyclic peptides

机译:循环肽的小鼠骨髓间充质干细胞亲和力的生物丙

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Osteonecrosis of the femoral head (ONFH) is a refractory disease present worldwide. In the development of therapies for this disease, mesenchymal stem cells (MSC) are a promising candidate cell source in tissue engineering (TE) and regenerative medicine. MSCs harvested from bone marrow (BM) are the gold standard. A significant barrier for BMMSC-based therapies is the inability and decreased number of BMMSCs in the tissues of interest. The ability to recruit BMMSCs efficiently to defective or injured sites in tissues or organs, for example the necrotic area of the femoral head in vivo, has been a major concern. In the present study, a peptide sequence (CDNVAQSVC), termed D7, was identified through phage display technology using C57BL/6 mouse BMMSCs. Subsequent analysis suggested that the identified loop-constrained heptapeptide exhibited a high specific affinity for mouse BMMSCs. Due to this specific affinity for BMMSCs, the present study provides a selective method to improve MSC-based TE strategies for the treatment of ONFH.
机译:股骨头的骨折(ON​​FH)是全世界呈现的难治性疾病。在该疾病的疗法的发展中,间充质干细胞(MSC)是组织工程(TE)和再生医学中的有希望的候选细胞来源。从骨髓(BM)收获的MSC是金标准。基于BMMSC的疗法的显着屏障是感兴趣组织中的BMMSC数量的无能和降低。能够有效地募集BMMSCs在组织或器官中有缺陷或受伤的部位,例如体内股骨头的坏死区域,这是一个主要问题。在本研究中,通过使用C57BL / 6小鼠BMMSCs通过噬菌体显示技术鉴定肽序列(CDNVAQSVC)。随后的分析表明,所识别的环状约束肽对小鼠BMMSCs表现出高特异性亲和力。由于对BMMSCs的这种特异性亲和力,本研究提供了一种选择性方法,以改善基于MSC的TE策略进行治疗ONFH。

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