Bone marrow mesenchymal stem cells regulated hepatic stellate cells activation through LPS-TLR4 pathway
-
摘要: 目的研究人骨髓间充质干细胞(BMSC)是否可通过干预LPS-TLR4通路,调控肝星状细胞(HSC)LX2活化,阐明BMSC在肝纤维化形成中的作用。方法体外共培养BMSC、LX2,分为BMSC+LX2(LPS刺激)组、TLR4阻断剂+LX2(LPS刺激)组、LX2(LPS刺激)组、BMSC(LPS刺激)组、LX2(无LPS刺激)组,培养6、12、36、48 h;收集上清,ELISA检测IL-8及TGFβ表达,RT-PCR检测LX2的TLR4、Myd88及NF-κB的表达,Western Blot检测TGFβ、SMA、ColⅠ、MyD88、TLR4表达。免疫荧光检测NF-κB细胞内表达情况。结果 LPS可以刺激LX2活化,活化的LX2分泌IL-8及TGFβ增多,TGFβ、SMA、ColⅠ、MyD88、TLR4表达增加,NF-κB p65主要为核内表达。与BMSC共培养后,LPS导致的LX2活化减弱,LX2的TGF-β、SMA、ColⅠ、MyD88、TLR4的表达下降,NF-κB p65胞浆表达为主。结论 BMSC可以通过干预LPS-TLR4通路抑制LX2的活化。
-
关键词:
- 骨髓细胞 /
- 间质干细胞 /
- 肝细胞,星形细胞 /
- LPS-TLR4通路
Abstract: Objective To investigate whether bone marrow mesenchymal stem cells (BMSC) affect the hepatic stellate cells (LX2) through inhibiting LPS-TLR4 pathway, and to clarify the mechanism of LPS causing liver fibrosis by activating LX2.Methods Human BMSC and LX2 were isolated and cultured in vitro separately or co-cultured in transwell under different treatments in four groups, which were 2×105 BMSC and 2×105 LX2 (with 100μg/ml LPS stimulation) co-culture group, 2×105 BMSC and 2×105 LX2 (no LPS stimulation) co-culture group, 2×105 LX2 (with 100μg/ml LPS stimulation) group, 2×105 BMSC (with 100μg/ml LPS stimulation) group and 2×105 LX2 (no LPS stimulation) group.Supernatant of 6, 12, 36 and 48 hours after treatment was collected and detected for IL-8 and TGFβ expression by ELISA.The TLR4, Myd88 and NF-κB gene expression of LX2 were detected by RT-PCR.The SMA, TGFβ, TLR4, Myd88 and ColⅠ expression were detected by Western Blotting.NF-κB p65 expression in cell was observed by immunofluorescence.Results LPS can stimulate LX2 activation.Activated LX2 secreted more IL-8 and TGFβ than static LX2 respectively, P<0.05.Gene expression of α-SMA, TGFβ and ColⅠ were increased in activated LX2.NF-κB p65 was mainly expressed in nucleus of activated LX2.After co-culture with BMSC, LX2 activation by LPS was inhibited significantly as the SMA, TGFβ, TLR4, Myd88 and ColⅠ were reduced.NF-κB p65 was mainly expressed in cytoplasm.Conclusion BMSC can inhibit LX2 activation through LPS-TLR4 pathway.-
Key words:
- bone marrow cell /
- mesenchymal stem cells /
- hepatocytes /
- astrocytes
-
[1]Gaia S, Smedile A, Omede P, et al.Feasibility and safety ofG-CSF administration to induce bone marrow-derived cellsmobilization in patients with end stage liver disease[J].JHepatol, 2006, 45 (1) :13-19. [2]Terai S, Ishikawa T, Omori K, et al.Improved liver function inpatients with liver cirrhosis after autologous bone marrow cellinfusion therapy[J].Stem Cells, 2006, 24 (10) :2292-2298. [3]Gordon MY, Levicar N, Pai M, et al.Characterisation andclinical application of human CD34+stem/progenitor cellpopulations mobilized into the blood by granulocyte colony-stimulating factor[J].Stem Cells, 2006, 24 (7) :1822-1830. [4]RM.Baertschiger1, V Serre-Beinier1, P Morel, et al.FibrogenicPotential of Human Multipotent Mesenchymal Stromal Cells inInjured liver[J].PLoS One, 2009, 17 (8) :e6657. [5]Lin RS, Lee FY, Lee SD, et al.Endotoxemia in patientswith chronic liver diseases:relationship to severity of liverdiseases, presence of esophageal varices, and hyperdynamiccirculation[J].J Hepatol, 1995, 22 (2) :165-172. [6]Brun P, Castagliuolo I, Pinzani M, et al.Exposure to bacterialcell wall products triggers an inflammatory phenotype inhepatic stellate cells[J].Am J Physiol Gastrointest LiverPhysiol, 2005, 289 (3) :G571-578. [7]Seki E, De Minicis S, Osterreicher CH, et al.TLR4 enhancesTGF-βsignaling and hepatic fibrosis[J].Nat Med, 2007, 13 (11) :1324-1332. [8]Naugler WE, Sakurai T, Kim S, et al.Gender disparity in livercancer due to sex differences in MyD88-dependent IL-6production[J].Science, 2007, 317 (5834) :121-124. [9]Huang H, Shiffman ML, Friedman S, et al.A 7 gene signatureidentifies the risk of developing cirrhosis in patients withchronic hepatitis C[J].Hepatology, 2007, 46 (2) :297-306. [10]梁劲松, 张锡流, 梁健.IL-8和IL-10的表达在大鼠肝纤维化机制中的作用[J].现代检验医学杂志, 2006, 21 (4) :77-78. [11]Payne C, Samuel K, Pryde A, et al.The impact of bone marrowstem cells on liver fibrosis in critically determined by their routeof cell trafficking[J].Hepatology, 2007, 46 (3) :710A. [12] 高志良, 彭亮, 崇雨田, 等.骨髓间充质干细胞自体移植治疗慢性肝衰竭的疗效研究[J].现代消化及介入诊疗, 2007, 12 (Suppl) :23-27.
本文二维码
计量
- 文章访问数: 4133
- HTML全文浏览量: 23
- PDF下载量: 1581
- 被引次数: 0