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Human multipotent adult progenitor cell-conditioned medium improves wound healing through modulating inflammation and angiogenesis in mice

机译:人类多能成人祖细胞条件培养基通过调节小鼠中的炎症和血管生成来改善伤口愈合

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BACKGROUND:Stem cell therapies have been widely investigated for their healing effects. However, the translation of these therapies has been hampered by the requirement to deliver live allogeneic or autologous cells directly to the wound in a clinical setting. Multipotent adult progenitor cells (MAPC? cells) are a subpopulation of bone marrow-derived adherent stem cells that secrete a wide range of factors known to accelerate the wound healing process. The aim of this study was to determine the impact of MAPC cells secretome on healing outcomes without the presence of MAPC cells.METHODS:The effect of MAPC-conditioned medium (MAPC-CM) on the capacity of keratinocytes, fibroblasts and endothelial cells to migrate and proliferate was determined in vitro using scratch wound closure and WST1 assay, respectively. The effect of MAPC-CM on collagen deposition and angiogenesis was also assessed using in vitro methods. Additionally, two excisional wounds were created on the dorsal surface of mice (n?=?8/group) and 100?μL of 20× MAPC-CM were intradermally injected to the wound margins. Wound tissues were collected at 3, 7 and 14?days post-wounding and stained with H&E for microscopic analysis. Immunohistochemistry was performed to investigate inflammation, angiogenesis and collagen deposition in the wounds.RESULTS:Skin fibroblasts, keratinocytes and endothelial cells treated with MAPC-CM all showed improved rates of scratch closure and increased cellular proliferation. Moreover, fibroblasts treated with MAPC-CM deposited more collagens I and III and endothelial cells treated with MAPC-CM showed increased capillary tube formation. Murine excisional wounds intradermally injected with MAPC-CM showed a significant reduction in the wound area and an increase in the rate of reepithelialisation. The results also showed that inflammatory cell infiltration was decreased while an increase in angiogenesis, as well as collagens I and III expressions, was observed.CONCLUSION:These findings suggest that factors produced by MAPC cells can have an important effect on cutaneous wound healing by affecting skin cell proliferation and migration, balancing inflammation and improving the formation of extracellular matrix and angiogenesis. Development of stem cell-free therapy for the treatment of wounds may be a more clinically translatable approach for improving healing outcomes.
机译:背景:干细胞疗法已被广泛研究其愈合效果。然而,这些疗法的翻译被要求阻碍了在临床环境中将活产物或自体细胞直接递送给伤口的活产物或自体细胞。多能成年祖细胞(Mapc?细胞)是骨髓衍生的粘附干细胞的亚群,其分泌着众所周知的各种因素来加速伤口愈合过程。本研究的目的是确定Mapc细胞沉淀对未存在Mapc细胞的愈合结果的影响。方法:Mapc条件培养基(MapC-cm)对角质形成细胞,成纤维细胞和内皮细胞的容量迁移的影响分别使用刮伤缠绕闭合和WST1测定法测定体外增殖。使用体外方法评估MapC-cm对胶原沉积和血管生成的影响。另外,在小鼠的背面(n≤=β8/组)上产生两种切除伤口,100μl20×mapc-cm的皮内注射到伤口边缘。在伤后3,7和14天收集伤口组织,并用H&E染色以进行微观分析。进行免疫组织化学以研究伤口中的炎症,血管生成和胶原沉积。结果:用MAPC-cm处理的皮肤成纤维细胞,角质形成细胞和内皮细胞所有均显示出划痕闭合和细胞增殖增加的提高速率。此外,用MAPC-CM处理的成纤维细胞沉积更多胶原蛋白I和III和用MAPC-CM处理的内皮细胞显示出增加的毛细管形成。用MAPC-CM皮内注射的鼠切除伤口显示出伤口面积显着降低,并增加了再皮率的增加。结果还表明,观察到炎症细胞浸润,同时观察到血管生成的增加,以及胶原蛋白I和III表达。结论:这些研究结果表明Mapc细胞产生的因素可以通过影响对皮肤伤口愈合产生重要影响皮肤细胞增殖和迁移,平衡炎症和改善细胞外基质和血管生成的形成。用于治疗伤口的干细胞治疗的发展可能是改善愈合结果的更具临床可翻译的方法。

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