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Human mesenchymal stem cell co-culture modulates the immunological properties of human intervertebral disc tissue fragments in vitro

机译:人间充质干细胞共培养体外调控人椎间盘组织片段的免疫学特性

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The capacity of mesenchymal stem cells (MSCs) to differentiate into intervertebral disc (IVD)-like cells has been well described, but their ability to modulate the inflammatory processes in the IVD remains unclear. We found that tissue obtained by discectomy of degenerated and post-traumatic IVD contains significant amounts of IgG antibodies, a sign of lymphocyte infiltration. Further we investigated whether MSCs in vitro, which were characterized for their multilineage differentiation potential and may have immunomodulatory effects on IVD fragments. IVD fragments were co-cultured in contact with peripheral blood lymphocytes (PBLs) and MSCs, and as functional controls we used contact co-cultures of PBLs stimulated with pokeweed mitogen (2.5 μg/mL) and MSCs. The time course of lymphocyte proliferation (Alamar Blue), IgG (ELISA) and gene expression (RT-PCR) of anti-inflammatory cytokines (TGF-β1, IL-10) by MSCs and pro-inflammatory molecules (IL-1α, IL-1β and TNF-α) by the IVD fragments were analyzed. Depending on the response to the presence of MSCs, the IVD fragments (n = 13) were divided in two groups: responders (n = 9), where inflammation was inhibited by MSCs and non-responders (n = 4), where MSCs did not decrease inflammation. At 1 week in co-culture, MSCs reduced significantly the IgG production in the IVD responders group to 69% and PBLs proliferation to 57% of the control. MSCs expression of the anti-inflammatory TGF-β1 increased with time, while IL-10 was expressed only at day 1. IVD gene expression of TNF-α decreased constantly, whereas IL-1α and IL-1β expression increased. In conclusion, these data suggest that MSCs may modulate disc-specific inflammatory and pain status and aid regeneration of the host tissue.
机译:间充质干细胞(MSCs)分化为椎间盘(IVD)样细胞的能力已得到很好的描述,但它们调节IVD中炎症过程的能力仍不清楚。我们发现,通过椎间盘切除术获得的变性和创伤后IVD所获得的组织中含有大量的IgG抗体,这是淋巴细胞浸润的迹象。进一步,我们研究了是否以具有多向分化潜能为特征并且可能对IVD片段具有免疫调节作用的体外MSC。 IVD片段与外周血淋巴细胞(PBLs)和MSCs一起共培养,作为功能性对照,我们使用了由商陆有丝分裂原(2.5μg/ mL)和MSC刺激的PBLs的接触共培养。 MSCs和促炎分子(IL-1α,IL)的淋巴细胞增殖(Alamar Blue),IgG(ELISA)和抗炎细胞因子(TGF-β1,IL-10)的基因表达(RT-PCR)的时间过程用IVD片段分析-1β和TNF-α。根据对MSC存在的反应,将IVD片段(n = 13)分为两组:响应者(n = 9),其中炎症被MSC抑制;无响应者(n = 4),其中MSCs不减轻炎症。在共培养的第一个星期,MSCs使IVD应答组的IgG产量显着降低至对照组的69%,PBLs增殖降至对照组的57%。 MSCs抗炎TGF-β1的表达随时间增加,而IL-10仅在第1天表达。TNF-α的IVD基因表达持续减少,而IL-1α和IL-1β的表达增加。总之,这些数据表明,MSC可以调节椎间盘特异性炎症和疼痛状态,并有助于宿主组织的再生。

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