i3S - Instituto de Investigação e Inovação em Saúde, Porto, Portugal.
INEB - Instituto de Engenharia Biomédica, Porto, Portugal.
Front Immunol. 2019 Jul 3;10:1508. doi: 10.3389/fimmu.2019.01508. eCollection 2019.
Low back pain is a highly prevalent clinical problem and intervertebral disc (IVD) degeneration is now accepted as the major pathophysiological mechanism responsible for this condition. Accumulating evidence suggests that inflammation plays a crucial role in the progression of human IVD degeneration, with macrophages being pointed as the key immune cell players in this process since their infiltration in degenerated IVD samples has been extensively demonstrated. Since they are highly plastic, macrophages can play different roles depending on the microenvironmental cues. The study of inflammation associated with IVD degeneration has been somehow neglected and one of the reasons is related with lack of adequate models. To overcome this, we established and characterized a new model of IVD organ culture under pro-inflammatory conditions to further dissect the role of macrophages in IVD associated immune response. For that, human monocyte-derived macrophages were co-cultured either with bovine caudal IVD punches in the presence of the pro-inflammatory cytokine IL-1β, or IVD-conditioned medium (CM), to investigate how IVD-produced factors influence macrophage phenotype. After 72 h, metabolic activity, gene expression and cytokine profile of macrophages and IVD cells were measured. Our results show that macrophages and IVDs remain metabolically active in the presence of IL-1β, significantly upregulate CCR7 gene expression and increase production of IL-6 on macrophages. When treating macrophages with IL-1β-IVD-CM, CCR7 upregulation follows the same trend, while for IL-6 an opposite effect was observed. On the other hand, macrophages interfere with IVD ECM remodeling, decreasing MMP3 expression and downregulating aggrecan and collagen II gene expression in the presence of IL-1β. Overall, the co-culture model established in this study can be considered a suitable approach to address the cellular and molecular pathways that regulate macrophage-IVD crosstalk, suggesting that degenerated IVD tissue tends to polarize human macrophages toward a more pro-inflammatory profile, which seems to aggravate IVD degeneration. This model could be used to improve the knowledge of the mechanisms that link IVD degeneration and the immune response.
下背痛是一种高发的临床问题,目前认为椎间盘(IVD)退变是导致该疾病的主要病理生理机制。越来越多的证据表明,炎症在人类 IVD 退变的进展中起着关键作用,巨噬细胞作为这一过程中的关键免疫细胞,其在退变的 IVD 样本中的浸润已得到广泛证实。由于巨噬细胞具有高度可塑性,它们可以根据微环境线索发挥不同的作用。与 IVD 退变相关的炎症研究在某种程度上被忽视了,其中一个原因与缺乏合适的模型有关。为了克服这一问题,我们建立并表征了一种新的炎症条件下的 IVD 器官培养模型,以进一步剖析巨噬细胞在 IVD 相关免疫反应中的作用。为此,我们将人单核细胞来源的巨噬细胞与牛尾状 IVD 穿刺物共培养,在存在促炎细胞因子 IL-1β的情况下,或 IVD 条件培养基(CM),以研究 IVD 产生的因素如何影响巨噬细胞表型。72 小时后,测量巨噬细胞和 IVD 细胞的代谢活性、基因表达和细胞因子谱。我们的结果表明,在存在 IL-1β的情况下,巨噬细胞和 IVD 仍然保持代谢活性,CCR7 基因表达显著上调,并增加了巨噬细胞中 IL-6 的产生。当用 IL-1β-IVD-CM 处理巨噬细胞时,CCR7 的上调也遵循相同的趋势,而对于 IL-6,则观察到相反的效果。另一方面,巨噬细胞干扰 IVD ECM 重塑,在存在 IL-1β的情况下,降低 MMP3 表达,并下调聚集蛋白聚糖和胶原 II 的基因表达。总的来说,本研究建立的共培养模型可以被认为是一种合适的方法来解决调节巨噬细胞-IVD 相互作用的细胞和分子途径,表明退变的 IVD 组织倾向于使人类巨噬细胞向更具促炎表型极化,这似乎加剧了 IVD 退变。该模型可用于提高与 IVD 退变和免疫反应相关的机制的认识。
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