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首页> 外文期刊>Acta biomaterialia >Human lung fibroblast-derived matrix facilitates vascular morphogenesis in 3D environment and enhances skin wound healing
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Human lung fibroblast-derived matrix facilitates vascular morphogenesis in 3D environment and enhances skin wound healing

机译:人肺成纤维细胞衍生的基质有利于3D环境中的血管形态发生,增强皮肤伤口愈合

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Extracellular matrix (ECM) is crucial to many aspects of vascular morphogenesis and maintenance of vasculature function. Currently the recapitulation of angiogenic ECM microenvironment is still challenging, due mainly to its diverse components and complex organization. Here we investigate the angiogenic potential of human lung fibroblast-derived matrix (hFDM) in creating a three-dimensional (3D) vascular construct. hFDM was obtained via decellularization of in vitro cultured human lung fibroblasts and analyzed via immunofluorescence staining and ELISA, which detect multiple ECM macromolecules and angiogenic growth factors (GFs). Human umbilical vein endothelial cells (HUVECs) morphology was more elongated and better proliferative on hFDM than on gelatin-coated substrate. To prepare 3D construct, hFDM is collected, quantitatively analyzed, and incorporated in collagen hydrogel (Col) with HUVECs. Capillary-like structure (CLS) formation at 7 day was significantly better with the groups containing higher doses of hFDM compared to the Col group (control). Moreover, the group (Col/hFDM/GFs) with both hFDM and angiogenic GFs (VEGF, bFGF, SDF-1) showed the synergistic activity on CLS formation and found much larger capillary lumen diameters with time. Further analysis of hFDM via angiogenesis antibody array kit reveals abundant biochemical cues, such as angiogenesis-related cytokines, GFs, and proteolytic enzymes. Significantly up-regulated expression of VE-cadherin and ECM-specific integrin sub-units was also noticed in Col/hFDM/GFs. In addition, transplantation of Col/hFMD/GFs with HUVECs in skin wound model presents more effective re-epithelialization, many regenerated hair follicles, better transplanted cells viability, and advanced neovascularization. We believe that current system is a very promising platform for 3D vasculature construction in vitro and for cell delivery toward therapeutic applications in vivo.
机译:细胞外基质(ECM)对于血管形态发生的许多方面至关重要和脉管系统的维持。目前,血管生成ECM微环境的概括仍然具有挑战性,主要是由于其各种组成部分和复杂组织。在这里,我们研究人肺成纤维细胞衍生基质(HFDM)的血管生成潜力在产生三维(3D)血管构建体中。通过体外培养的人肺成纤维细胞的脱细胞获得HFDM,并通过免疫荧光染色和ELISA分析,所述免疫荧光染色和抗肌肉,其检测多个ECM大分子和血管生成生长因子(GFS)。人的脐静脉内皮细胞(HUVECS)形态更细长,更具有比在明胶涂覆的基底上的HFDM的更好增殖。为了制备3D构建体,收集,定量分析HFDM,并在胶原蛋白水凝胶(Col)中掺入Huvecs。与含有Col组(对照)相比,含有较高剂量的HFDM的基团,毛细管样结构(CLS)形成明显更好。此外,具有HFDM和血管生成GFS(VEGF,BFGF,SDF-1)的组(COL / HFDM / GFS)显示了CLS形成的协同活性,并发现了大量较大的毛细管内腔直径。通过血管生成抗体阵列试剂盒的进一步分析HFDM揭示了丰富的生化线索,例如血管生成相关的细胞因子,GFS和蛋白水解酶。在Col / HFDM / GFS中还注意到了显着上调的Ve-Cadherin和ECM特异性整联蛋白子单元的表达。此外,Col / HFMD / GFS与皮肤伤口模型的Huvecs移植呈现更有效的重新上皮化,许多再生毛囊,更好的移植细胞活力和晚期新生血管化。我们认为,目前的系统是体外3D脉管系统建筑的一个非常有前途的平台,并用于细胞递送对体内治疗应用的细胞。

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