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首页> 外文期刊>Cell biology international. >Stromal vascular fraction (svf) cells enhance long-term survival of autologous fat grafting through the facilitation of m2 macrophages
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Stromal vascular fraction (svf) cells enhance long-term survival of autologous fat grafting through the facilitation of m2 macrophages

机译:通过促进m2巨噬细胞,基质血管级分(svf)细胞可提高自体脂肪移植的长期存活率

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摘要

Optimum perfusion may be the key to the endurance, and hence survival, of autologous adipose tissue transportation. Stromal vascular fraction (SVF) cell therapy can greatly improve the survival of fat grafts by enhancing angiogenesis. However, SVF cells are poorly retained in later stages of SVF-assisted adipose tissue transplant. Therefore, it hardly defines the angiogenic effect through long-term transportation. Adipose tissue suffers from acute hypoxia in the early stage of transportation, leading to the recruitment of macrophages. M2 macrophages enhance angiogenesis in adipose transplantation by acting as an angiogenic signal source, promoting tip cell migration and assisting tip cell fusion. Furthermore, the angiogenic and anti-inflammatory micro-environment in the graft created by M2 macrophages may stimulate the transformation of infiltrating macrophages to M2 macrophages. These M2 macrophages may enhance the long-term retention of graft through angiogenesis. Based on these observations, we postulate that the long-term angiogenic effect of SVF cells may be achieved through the facilitation of the M2 macrophages.
机译:最佳灌注可能是自体脂肪组织运输的耐力和存活率的关键。基质血管级分(SVF)细胞疗法可通过增强血管生成而大大改善脂肪移植物的存活率。但是,SVF细胞在SVF辅助的脂肪组织移植的后期阶段很难保留。因此,它几乎不能定义通过长期运输的血管生成作用。脂肪组织在运输的初期遭受急性缺氧,导致巨噬细胞的募集。 M2巨噬细胞通过充当血管生成信号源,促进尖端细胞迁移并协助尖端细胞融合来增强脂肪移植中的血管生成。此外,由M2巨噬细胞产生的移植物中的血管生成和抗炎微环境可刺激浸润性巨噬细胞向M2巨噬细胞的转化。这些M2巨噬细胞可通过血管生成增强移植物的长期保留。基于这些观察,我们推测SVF细胞的长期血管生成作用可以通过促进M2巨噬细胞来实现。

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