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首页> 外文期刊>Tissue engineering >Autologous bone marrow-derived cultured mesenchymal stem cells delivered in a fibrin spray accelerate healing in murine and human cutaneous wounds.
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Autologous bone marrow-derived cultured mesenchymal stem cells delivered in a fibrin spray accelerate healing in murine and human cutaneous wounds.

机译:在纤维蛋白喷雾中递送的自体骨髓来源的培养的间充质干细胞可加速鼠和人皮肤伤口的愈合。

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The nonhematopoietic component of bone marrow includes multipotent mesenchymal stem cells (MSC) capable of differentiating into fat, bone, muscle, cartilage, and endothelium. In this report, we describe the cell culture and characterization, delivery system, and successful use of topically applied autologous MSC to accelerate the healing of human and experimental murine wounds. A single bone marrow aspirate of 35-50 mL was obtained from patients with acute wounds (n = 5) from skin cancer surgery and from patients with chronic, long-standing, nonhealing lower extremity wounds (n = 8). Cells were grown in vitro under conditions favoring the propagation of MSC, and flow cytometry and immunostaining showed a profile (CD29+, CD44+, CD105+, CD166+, CD34-, CD45-) highly consistent with published reports of human MSC. Functional induction studies confirmed that the MSC could differentiate into bone, cartilage, and adipose tissue. The cultured autologous MSC were applied up to four times to the wounds using a fibrin polymer spray system with a double-barreled syringe. Both fibrinogen (containing the MSC) and thrombin were diluted to optimally deliver a polymerized gel that immediately adhered to the wound, without run-off, and yet allowing the MSC to remain viable and migrate from the gel. Sequential adjacent sections from biopsy specimens of the wound bed after MSC application showed elongated spindle cells, similar to their in vitro counterparts, which immunostained for MSC markers. Generation of new elastic fibers was evident by both special stains and antibodies to human elastin. The application of cultured cells was safe, without treatment-related adverse events. A strong direct correlation was found between the number of cells applied (greater than 1 x 10(6) cells per cm2 of wound area) and the subsequent decrease in chronic wound size (p = 0.0058). Topical application of autologous MSC also stimulated closure of full-thickness wounds in diabetic mice (db/db). Tracking of green fluorescent protein (GFP)+ MSCin mouse wounds showed GFP+ blood vessels, suggesting that the applied cells may persist as well as act to stimulate the wound repair process. These findings indicate that autologous bone marrow-derived MSC can be safely and effectively delivered to wounds using a fibrin spray system.
机译:骨髓的非造血成分包括能够分化为脂肪,骨骼,肌肉,软骨和内皮的多能间充质干细胞(MSC)。在这份报告中,我们描述了细胞培养和表征,递送系统,以及成功地使用局部应用的自体MSC来加速人类和实验性小鼠伤口的愈合。从皮肤癌手术的急性伤口患者(n = 5)和慢性,长期不愈合的下肢伤口患者(n = 8)获得了35-50 mL的单个骨髓抽吸物。细胞在有利于MSC增殖的条件下体外生长,流式细胞仪和免疫染色显示与人MSC的已发表报道高度吻合的分布图(CD29 +,CD44 +,CD105 +,CD166 +,CD34-,CD45-)。功能诱导研究证实,MSC可以分化为骨骼,软骨和脂肪组织。使用带有双管注射器的纤维蛋白聚合物喷雾系统,将培养的自体MSC施加至伤口最多4次。纤维蛋白原(包含MSC)和凝血酶均被稀释,以最佳地递送聚合的凝胶,该凝胶立即粘附在伤口上,而不会流失,但仍使MSC保持活力并从凝胶中迁移出来。 MSC应用后,伤口床活检标本的连续相邻切片显示出细长的纺锤状细胞,类似于它们的体外对等体,对MSC标记物进行了免疫染色。新的弹性纤维的产生通过特殊的染色剂和抗人弹性蛋白的抗体而明显。应用培养的细胞是安全的,没有与治疗相关的不良事件。发现所施加的细胞数量(每平方厘米伤口面积大于1 x 10(6)个细胞)与随后的慢性伤口大小减少之间有很强的直接相关性(p = 0.0058)。自体MSC的局部应用也刺激了糖尿病小鼠(db / db)全层伤口的闭合。在小鼠伤口中跟踪绿色荧光蛋白(GFP)+ MSC显示出GFP +血管,表明所应用的细胞可能会持续存在并起到刺激伤口修复过程的作用。这些发现表明,使用血纤蛋白喷雾系统可以安全有效地将自体骨髓来源的MSC递送至伤口。

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