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首页> 外文期刊>Experimental and therapeutic medicine >Smad7-overexpressing rat BMSCs inhibit the fibrosis of hepatic stellate cells by regulating the TGF-beta 1/Smad signaling pathway
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Smad7-overexpressing rat BMSCs inhibit the fibrosis of hepatic stellate cells by regulating the TGF-beta 1/Smad signaling pathway

机译:Smad7过表达大鼠BMSC通过调节TGF-Beta 1 / Smad信号通路来抑制肝星状细胞的纤维化

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Mesenchymal stem cells (MSCs) are able to differentiate into hepatocytes, promote the regeneration of hepatic cells and inhibit the progression of hepatic fibrosis. Transforming growth factor (TGF)-beta 1 is one of the key factors in the development of liver fibrosis, which also promotes extra cellular matrix (ECM) formation. Drosophila mothers against decapentaplegic 7 (Smad7) is an essential negative regulator in the TGF-beta 1/Smad signaling pathway. In the present study, bone mesenchymal stem cells (BMSCs) were isolated from rat bone marrow and transfected with lentiviral vectors carrying the Smad7 gene. Smad7-enhanced green fluorescent protein (EGFP)-BMSCs stably expressing Smad7 were subsequently co-cultured with hepatic stellate cells (HSCs) for 48 h. Smad7 and TGF-beta 1 levels in the culture medium were detected using ELISA, and the levels of collagen (Col) I, Col III, laminin (LN) and hyaluronic acid (HA) were measured using immunoassays. The early apoptosis rates of HSCs were determined via flow cytometry. Reverse transcription-quantitative polymerase chain reaction and western blotting were performed to evaluate the mRNA and protein expression profiles, respectively. The results indicated that Smad7-EGFP-BMSCs stably expressing Smad7 were successfully constructed. Upon co-culturing with rat Smad7-EGFP-BMSCs, the early apoptotic rate of HSCs was significantly increased (P<0.05). Levels of Smad7 in the culture medium were also significantly increased (P<0.05), whereas the levels of TGF-(31, Col I, Col III, LN and HA were significantly decreased (P<0.05). Furthermore, the mRNA and protein levels of Smad7 and matrix metalloproteinase 1 were significantly increased (P<0.05), whereas those of TGF-beta 1, alpha-SMA, Smad2, smad3, TGF-beta receptor I, Col I, tissue inhibitors of metalloproteinase-1 and Col III were significantly decreased. The results of the present study suggest that rat BMSCs overexpressing Smad7 may inhibit the fibrosis of HSCs by regulating the TGF-beta 1/Smad signaling pathway. This provides a novel insight into future treatments for liver fibrosis.
机译:间充质干细胞(MSCs)能够分化成肝细胞,促进肝细胞的再生并抑制肝纤维化的进展。转化生长因子(TGF)-Beta 1是肝纤维化发育的关键因素之一,也促进了额外的细胞基质(ECM)形成。杜松星虫患者夫妇对抗甲板,7(SMAD7)是TGF-β1/ Smad信号通路中的必要负调节剂。在本研究中,从大鼠骨髓中分离骨间充质干细胞(BMSC),并用携带Smad7基因的慢病毒载体转染。 Smad7增强的绿色荧光蛋白(EGFP)-BMSCs稳定表达Smad7随后与肝星状细胞(HSC)共培养48小时。使用ELISA检测培养基中的SMAD7和TGF-β1水平,使用免疫测定法测量培养基的水平(COL)I,COL III,层粘连蛋白(LN)和透明质酸(HA)。通过流式细胞术确定HSC的早期凋亡率。进行逆转录定量聚合酶链反应和蛋白质印迹以分别评估mRNA和蛋白表达谱。结果表明,成功构建了稳定表达Smad7的Smad7-EGFP-BMSC。在用大鼠Smad7-EGFP-BMSC进行共同培养后,HSC的早期凋亡率显着增加(P <0.05)。培养基中的Smad7水平也显着增加(P <0.05),而TGF-(31,COL I,COL III,LN和HA的水平显着降低(P <0.05)。此外,mRNA和蛋白质Smad7和基质金属蛋白酶1的水平显着增加(P <0.05),而TGF-β1,α-SMA,SMAD2,SMAD3,TGF-β受体I,COL I,金属蛋白酶-1和COL III的组织抑制剂显着降低。本研究的结果表明,过表达SMAD7的大鼠BMSCs可以通过调节TGF-β1/ Smad信号通路来抑制HSC的纤维化。这提供了对未来肝纤维化治疗的新颖洞察力。

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