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首页> 外文期刊>Cytotherapy >Conditioned medium from amniotic membrane-derived cells prevents lung fibrosis and preserves blood gas exchanges in bleomycin-injured mice-specificity of the effects and insights into possible mechanisms
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Conditioned medium from amniotic membrane-derived cells prevents lung fibrosis and preserves blood gas exchanges in bleomycin-injured mice-specificity of the effects and insights into possible mechanisms

机译:羊膜来源细胞的条件培养基可预防肺纤维化并保持博来霉素损伤小鼠的血气交换-特异性作用及其对可能机制的见解

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Background and aims. We recently demonstrated that injection of conditioned medium (CM) generated from cells of the mesenchymal region of human amniotic membrane (AMTCs) reduces bleomycin-induced lung fibrosis in mice, suggesting a crucial role of paracrine factor(s) secreted by AMTCs in these beneficial effects. We further investigated this hypothesis, the mechanisms involved, the effects on some lung functional parameters and whether AMTC-secreted effector(s) are specific to these cells and not produced by other cell types, extending the time of analysis up to 28 days after treatment. Methods. Bleomycin-challenged mice were either treated with AMTC-CM or CM generated from human skin fibroblasts, human peripheral blood mononuclear cells or Jurkat cells, or were left untreated. Mouse lungs were analyzed for content of proinflammatory and pro-fibrotic molecules, presence of lymphocytes and macrophages and for fibrosis level (through histological semi-quantitative evaluation and quantitative measurement of collagen content). Arterial blood gas analysis was also performed. Results. Up to 28 days after delivery,AMTC-CM-treated mice developed reduced lung fibrosis with respect to mice treated with other CM types. AMTC-CM-treated mice had comparatively better preservation of blood gas parameters and showed lower lung content of interleukin-6, tumor necrosis factor-a, macrophage inflammatory protein-1a, monocyte chemoattractant protein-1 and transforming growth factor-b associated with reduced lung macrophage levels. Conclusions. AMTC-CMprevents lung fibrosis in bleomycin-challenged mice, improving survival and preserving lung functional parameters such as blood gas exchanges. The specificity of AMTC-CMaction was indicated by the absence of fibrosis reduction when other CM types were used. Finally, we provide some insights into the possible mechanisms underlying AMTC-CM-mediated control of fibrosis.
机译:背景和目标。我们最近证明,注射从人羊膜(AMTC)的间充质区域细胞产生的条件培养基(CM)可以减少博莱霉素诱导的小鼠肺纤维化,表明AMTC分泌的旁分泌因子在这些有益作用中起着至关重要的作用。效果。我们进一步研究了这一假设,涉及的机制,对某些肺功能参数的影响以及AMTC分泌的效应子是否对这些细胞具有特异性,而不是由其他细胞类型产生,从而将分析时间延长至治疗后28天。方法。用AMTC-CM或从人皮肤成纤维细胞,人外周血单核细胞或Jurkat细胞产生的CM处理博来霉素激发的小鼠,或不予治疗。分析小鼠肺中的促炎和纤维化分子含量,淋巴细胞和巨噬细胞的存在以及纤维化水平(通过组织学半定量评估和胶原蛋白含量的定量测量)。还进行了动脉血气分析。结果。分娩后长达28天,与接受其他CM类型治疗的小鼠相比,经AMTC-CM处理的小鼠肺纤维化程度降低。接受AMTC-CM处理的小鼠具有相对更好的血气参数保存,并显示较低的白细胞介素6,肿瘤坏死因子-a,巨噬细胞炎性蛋白1a,单核细胞趋化蛋白1和转化生长因子b的肺含量与降低有关肺巨噬细胞水平。结论AMTC-CM可以防止博来霉素攻击的小鼠出现肺纤维化,从而改善其存活率并保留肺功能参数,例如血气交换。当使用其他类型的CM时,无纤维化减少表明了AMTC-CMaction的特异性。最后,我们对AMTC-CM介导的纤维化控制的潜在机制提供了一些见解。

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