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Differential proteome of bone marrow mesenchymal stem cells from osteoarthritis patients.

机译:骨关节炎患者骨髓间充质干细胞的差异蛋白质组。

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OBJECTIVE: Adult mesenchymal stem cells (MSCs) are multipotent cells whose primary reservoir is bone marrow (BM). Following situations of extensive tissue damage, MSCs are mobilized and migrate to the site of injury. Osteoarthritis (OA) is a condition that involves extensive cartilage and bone damage. To gain insight into the pathogenesis of OA, we have analyzed the differential BM-MSCs proteome of OA patients. METHODS: MSCs protein extracts were prepared from BM aspirates from six patients with OA and from six hip fracture subjects without OA, and analyzed by Two-dimensional gels, using the differential in-gel electrophoresis approach. Differentially expressed proteins were identified by mass spectrometry. In addition, the chemotactic responses of OA and control MSCs were assessed. RESULTS: The majority of proteins that changed at least 1.5-fold (P<0.05) belonged to the following three categories: metabolic enzymes (14 proteins, 36%), cytoskeleton/motility (12 proteins, 32%), and transporters (three proteins, 8%). In OA MSCs, a high percentage of metabolic enzymes (n=8, 57%) were up-regulated and most of the proteins related to cytoskeleton/motility (n=9, 75%) were down-regulated. There was a significant increase in the migration response of OA MSCs to platelet-derived growth factor-BB (chemotaxis index CI: 5.13+/-1.19 vs 3.35+/-0.42, P=0.043). CONCLUSIONS: In this study, we have described the differential proteome of BM-MSCs from OA patients together with an increased chemotactic response of these cells in the context of OA. These results could indicate an activation of OA BM-MSCs in response to chemotactic signals sent by the altered subchondral bone in an attempt to heal damaged tissue.
机译:目的:成体间充质干细胞(MSCs)是多能干细胞,其主要储库是骨髓(BM)。在广泛的组织损伤情况下,MSC被动员并迁移到受伤部位。骨关节炎(OA)是一种涉及广泛的软骨和骨骼损伤的疾病。为了深入了解OA的发病机理,我们分析了OA患者的差异性BM-MSCs蛋白质组。方法:从6例OA患者和6例无OA的髋部骨折患者的BM抽吸物中制备MSCs蛋白提取物,并使用差分凝胶电泳法进行二维凝胶分析。通过质谱鉴定差异表达的蛋白质。另外,评估了OA和对照MSC的趋化反应。结果:大多数变化至少1.5倍的蛋白质(P <0.05)属于以下三类:代谢酶(14种蛋白质,占36%),细胞骨架/运动(12种蛋白质,占32%)和转运蛋白(三种)蛋白质,8%)。在OA MSC中,高比例的代谢酶(n = 8,57%)被上调,而与细胞骨架/运动相关的大多数蛋白质(n = 9,75%)被下调。 OA MSCs对血小板衍生的生长因子-BB的迁移反应显着增加(趋化性指数CI:5.13 +/- 1.19 vs 3.35 +/- 0.42,P = 0.043)。结论:在这项研究中,我们描述了来自OA患者的BM-MSC的差异蛋白质组,以及在OA的情况下这些细胞的趋化反应增加。这些结果可能表明,OA BM-MSCs响应于软骨下骨改变后发出的趋化信号而激活,试图治愈受损的组织。

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