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Mesenchymal Stem/Stromal Cells from Discarded Neonatal Sternal Tissue: In Vitro Characterization and Angiogenic Properties

机译:丢弃的新生儿胸骨组织间充质干/基质细胞:体外表征和血管生成特性。

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Autologous and nonautologous bone marrow mesenchymal stem/stromal cells (MSCs) are being evaluated as proangiogenic agents for ischemic and vascular disease in adults but not in children. A significant number of newborns and infants with critical congenital heart disease who undergo cardiac surgery already have or are at risk of developing conditions related to inadequate tissue perfusion. During neonatal cardiac surgery, a small amount of sternal tissue is usually discarded. Here we demonstrate that MSCs can be isolated from human neonatal sternal tissue using a nonenzymatic explant culture method. Neonatal sternal bone MSCs (sbMSCs) were clonogenic, had a surface marker expression profile that was characteristic of bone marrow MSCs, were multipotent, and expressed pluripotency-related genes at low levels. Neonatal sbMSCs also demonstrated in vitro proangiogenic properties. Sternal bone MSCs cooperated with human umbilical vein endothelial cells (HUVECs) to form 3D networks and tubes in vitro. Conditioned media from sbMSCs cultured in hypoxia also promoted HUVEC survival and migration. Given the neonatal source, ease of isolation, and proangiogenic properties, sbMSCs may have relevance to therapeutic applications.
机译:自体和非自体骨髓间充质干/基质细胞(MSC)被评估为成人而非儿童的局部缺血和血管疾病的促血管生成剂。大量接受心脏手术的患有先天性心脏病的新生儿和婴儿已经患有组织灌注不足或与之相关的风险。在新生儿心脏手术期间,通常会丢弃少量的胸骨组织。在这里,我们证明了可以使用非酶外植体培养方法从人的新生儿胸骨组织中分离出MSC。新生儿胸骨MSC(sbMSC)具有克隆性,具有骨髓MSC特有的表面标志物表达特征,具有多能性,并以低水平表达多能性相关基因。新生儿sbMSCs还显示出体外促血管生成特性。胸骨间质干细胞与人脐静脉内皮细胞(HUVEC)共同在体外形成3D网络和管。来自缺氧培养的sbMSC的条件培养基也促进了HUVEC的存活和迁移。考虑到新生儿的来源,易于分离和促血管生成的特性,sbMSCs可能与治疗应用有关。

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