首页> 外文期刊>Biochimica et Biophysica Acta. General Subjects >COMP-Ang1 inhibits apoptosis as well as improves the attenuated osteogenic differentiation of mesenchymal stem cells induced by advanced glycation end products
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COMP-Ang1 inhibits apoptosis as well as improves the attenuated osteogenic differentiation of mesenchymal stem cells induced by advanced glycation end products

机译:COMP-Ang1抑制凋亡,并改善晚期糖基化终产物诱导的间充质干细胞的成骨分化减弱

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Background In the present study, we have investigated the possibility that cartilage oligomeric matrix protein angiopoietin1 (COMP-Ang1), important factor in angiogenesis, osteogenesis and the survival of mesenchymal stem cells (MSCs) through the Ang1/Tie2 pathway has beneficial effects on osteogenic differentiated cells (ODCs) from MSCs treated by advanced glycation end products (AGE), which are pathological factors of diabetes. Methods Primary culture of MSCs was used. For comparison analysis of AGE and COMP-Ang1 effects, we performed cell viability assay with each treated variety concentration for 24 h. Apoptosis rate and Caspase-3 activity were measured by each ELISA assay. To make sure with Ang1/Tie2 pathway, we performed small interfering RNA transfected to MSCs. Real-time RT-PCR was performed to identify ODCs marker genes. Immunoblotting was used to evaluate the expression of Tie2, AKT, p38 and ERK. Results Our results clearly demonstrate that COMP-Ang1 upregulates the phosphorylation of AKT and p38 by activating the Ang1/Tie2 signaling pathway, indicating that COMP-Ang1 affects both AGE-induced apoptosis and the attenuated osteogenic differentiation of MSCs through the p38/MAPK and PI3K/AKT pathways. Conclusions COMP-Ang1 improves cell viability and differentiation function of ODCs against AGE via Ang/Tie2 signaling pathway. General significance Our results suggest the potential importance of COMP-Ang1 as a new therapy for impaired bone formation that is associated with diabetes and advanced age.
机译:背景技术在本研究中,我们研究了软骨寡聚基质蛋白血管生成素1(COMP-Ang1),血管生成,成骨和间充质干细胞(MSCs)通过Ang1 / Tie2途径存活的重要因素对成骨的有益作用的可能性。晚期糖基化终末产物(AGE)处理的MSC中的MSCs分化细胞(ODC),这是糖尿病的病理因素。方法采用MSCs原代培养。为了比较分析AGE和COMP-Ang1的作用,我们对每种处理的品种浓度进行了24小时的细胞活力分析。通过每个ELISA测定法测量细胞凋亡率和Caspase-3活性。为了确保Ang1 / Tie2途径,我们进行了小干扰RNA转染到MSCs。进行实时RT-PCR以鉴定ODCs标记基因。免疫印迹用于评估Tie2,AKT,p38和ERK的表达。结果我们的结果清楚地表明,COMP-Ang1通过激活Ang1 / Tie2信号通路上调AKT和p38的磷酸化,表明COMP-Ang1通过p38 / MAPK和PI3K同时影响AGE诱导的凋亡和MSC的成骨分化。 / AKT途径。结论COMP-Ang1可通过Ang / Tie2信号通路改善ODCs抗AGE的细胞活力和分化功能。一般意义我们的结果表明,COMP-Ang1作为治疗与糖尿病和高龄有关的骨形成受损的新疗法的潜在重要性。

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