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Fat extract promotes angiogenesis in a murine model of limb ischemia: a novel cell-free therapeutic strategy

机译:脂肪提取物在肢体缺血的小鼠模型中促进血管生成:一种新的无细胞治疗策略

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摘要

Abstract Background The proangiogenic capacity of adipose tissue and its derivatives has been demonstrated in a variety of studies. The paracrine mechanism of the cellular component is considered to play a critical role in the regenerative properties of these tissues. However, cell-based therapy for clinical application has been hindered by limitations such as safety, immunogenicity issues, and difficulties in cell preservation, transportation, and phenotype control. In the current study, we aimed to produce a cell-free extract directly from human fat tissue and evaluate its potential therapeutic efficacy. Methods We developed a novel physical approach to produce a cell-free aqueous extract from human fat tissue (fat extract (FE)). The therapeutic potential of FE was investigated in the ischemic hindlimb model of nude mice. After establishment of hindlimb ischemia with ligation of the left femoral artery and intramuscular injection of FE, blood perfusion was monitored at days 0, 7, 14, 21, and 28. Tissue necrosis and capillary density were evaluated. Enzyme-linked immunosorbent assay was used to analyze the growth factors contained in FE. Moreover, the proliferation, migration, and tube formation ability were tested on human umbilical vein endothelial cells (HUVECs) in vitro when treated with FE. The proangiogenic ability of FE was further assessed in an in-vivo Matrigel plug assay. Results FE was prepared and characterized. The intramuscular injection of FE into the ischemic hindlimb of mice attenuated severe limb loss and increased blood flow and capillary density of the ischemic tissue. Enzyme-linked immunosorbent assay showed that FE contained high levels of various growth factors. When added as a cell culture supplement, FE promoted HUVEC proliferation, migration, and tube formation ability in a dose-dependent manner. The subcutaneous injection of Matrigel infused with FE enhanced vascular formation. Conclusions We developed a novel cell-free therapeutic agent, FE, produced from human adipose tissue. FE was able to attenuate ischemic injury and stimulate angiogenesis in ischemic tissues. This study indicates that FE may represent a novel cell-free therapeutic agent in the treatment of ischemic disorders.
机译:摘要在各种研究中,已经证明了脂肪组织及其衍生物的诱发能力。细胞组分的邻静脉机理被认为在这些组织的再生性质中发挥着关键作用。然而,基于细胞的临床应用的疗法被诸如安全性,免疫原性问题和细胞保存,运输和表型对照中的困难的限制受到阻碍。在目前的研究中,我们旨在直接从人脂肪组织产生无细胞提取物,并评估其潜在的治疗效果。方法我们开发了一种新的物理方法,用于制备免于人脂肪组织的无细胞含水提取物(脂肪提取物(Fe))。在裸鼠的缺血性Hindlimb模型中研究了Fe的治疗潜力。在建立后肢缺血后,通过连接左股动脉和肌肉注射Fe,在0,7,14,21和28天监测血液灌注。评估组织坏死和毛细血管密度。酶联免疫吸附试验用于分析Fe中含有的生长因子。此外,当用Fe处理时,在体外对人脐静脉内皮细胞(HUVEC)进行增殖,迁移和管形成能力。在体内基质蛋白栓塞测定中进一步评估Fe的过致性能力。结果制备和表征。肌内注射到小鼠缺血性后肢的缺血性后肢减弱了缺血组织的严重肢体损失和增加的血流和毛细血管密度。酶联免疫吸附测定结果表明,Fe包含高水平的各种生长因子。当添加细胞培养补充剂时,Fe以剂量依赖性方式促进了Huvec增殖,迁移和管形成能力。皮下注射Matrigel注入Fe增强血管形成。结论我们开发了一种从人脂肪组织产生的新型无细胞治疗剂,Fe。 Fe能够衰减缺血性损伤并刺激缺血组织中的血管生成。该研究表明,Fe可以代表一种在治疗缺血性疾病的无细胞治疗剂。

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