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Mesenchymal Stem Cells Promoted Lung Wound Repair through Hox A9 during Endotoxemia-Induced Acute Lung Injury

机译:间充质干细胞在内毒素血症引起的急性肺损伤中通过Hox A9促进了肺创面修复。

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摘要

Objectives. Acute lung injury (ALI) is a common clinical critical disease. Stem cells transplantation is recognized as an effective way to repair injured lung tissues. The present study was designed to evaluate the effects of mesenchymal stem cells (MSCs) on repair of lung and its mechanism. Methods. MSCs carrying GFP were administrated via trachea into wild-type SD rats 4 hours later after LPS administration. The lung histological pathology and the distribution of MSCs were determined by HE staining and fluorescence microscopy, respectively. Next, differentially expressed HOX genes were screened by using real-time PCR array and abnormal expression and function of Hox A9 were analyzed in the lung and the cells. Results. MSCs promoted survival rate of ALI animals. The expression levels of multiple HOX genes had obvious changes after MSCs administration and HOX A9 gene increased by 5.94-fold after MSCs administration into ALI animals. HOX A9 was distributed in endothelial cells and epithelial cells in animal models and overexpression of Hox A9 can promote proliferation and inhibit inflammatory adhesion of MSCs. Conclusion. HoxA9 overexpression induced by MSCs may be closely linked with lung repair after endotoxin shock.
机译:目标。急性肺损伤(ALI)是常见的临床危重疾病。干细胞移植被认为是修复受损肺组织的有效方法。本研究旨在评估间充质干细胞(MSCs)对肺部修复的作用及其机制。方法。在LPS施用后4小时,通过气管将携带GFP的MSC施用给野生型SD大鼠。肺组织病理学和MSCs的分布分别通过HE染色和荧光显微镜确定。接下来,使用实时PCR阵列筛选差异表达的HOX基因,并在肺和细胞中分析Hox A9的异常表达和功能。结果。 MSC提高了ALI动物的存活率。 MSCs给药后,多种HOX基因的表达水平发生了明显变化,而ALI动物中,MSCs给药后,HOX A9基因的表达增加了5.94倍。 HOX A9分布在动物模型的内皮细胞和上皮细胞中,Hox A9的过表达可以促进MSC的增殖和抑制炎症粘附。结论。内毒素休克后,MSCs诱导的HoxA9过表达可能与肺修复密切相关。

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