Poliklinik, Funktionsbereich & Hiller Forschungszentrum für Rheumatologie, University Hospital Duesseldorf, D-40225, Duesseldorf, Germany.
Wilhelm Sander-NeuroOncology Unit and Department of Neurology, University Hospital of Regensburg, D-93053, Regensburg, Germany.
Sci Rep. 2020 Jan 21;10(1):780. doi: 10.1038/s41598-020-57772-7.
Synovial fibroblasts (SF) were reported to produce B cell activating factor (BAFF) in response to stimulation with interferon-γ (IFN-γ) or tumor necrosis factor (TNF). However, the influence of these pro-inflammatory cytokines on other receptors/ligands of the TNF superfamily or associated cytokine receptors in SF has not been investigated yet. Here we show the differential regulation of BAFF (CD257), Fn14 (CD266), TACI (CD267), BAFF-R (CD268), BCMA (CD269), CD40 ligand (CD40L, CD154), IFN-γR (CD119), Leptin receptor (ObR, CD295), VCAM-1 (CD106) and membrane TGF-β in isolated SF and the impact of IFN-γ/TNF co-incubation on proliferation, IL-6 and IL-8 production. In addition, the impact of differentially stimulated SF on B cell survival in co-cultures was assessed. Surface cytokines and cytokine receptors were detected by flow cytometry. Soluble cytokine receptors and cytokines were quantified by ELISA. Proliferation was assessed by cell titer blue. Murine B cell survival in fibroblast/ B cell co-cultures was determined by annexin V/propidium iodide staining and flow cytometry. IFN-γ together with TNF synergistically and significantly increased the cell surface levels of BAFF, Fn14, TACI, BAFF-R, BCMA, CD40L, ObR and IFN-γR in rheumatoid arthritis SF after 72 h incubation. Soluble BAFF was only induced by IFN-γ and inhibited by TNF. Addition of TWEAK had no influence on proliferation or IL-8 production but decreased TNF-induced IL-6 production, whereas APRIL, BAFF and leptin did not modulate TNF or TNF/IFN-γ-induced proliferation or cytokine production. Proliferation was increased by TNF and further enhanced by the addition of IFN-γ. In co-culture experiments, SF stimulated with TNF/IFN but not TNF or IFN-γ alone increased shedding of VCAM-1 and expression of membrane TGFβ, which was associated with reduced survival of murine B cells. IFN-γ and TNF regulate the expression of TNF family member cytokines and associated receptors. Ligation of IFN-γR and Fn14 under pro-inflammatory conditions modulated IL-6/IL-8 production and proliferation. In B cell/SF co-cultures, the combination of TNF/IFN reduced B cell survival possibly via enhanced VCAM-1 shedding and/or increased TGF-β production. IFN-γ is necessary for the observed effects on B cell survival and SF cytokine production and emphasizes its anti-inflammatory role in rheumatoid arthritis.
滑膜成纤维细胞(SF)被报道在受到干扰素-γ(IFN-γ)或肿瘤坏死因子(TNF)的刺激后会产生 B 细胞激活因子(BAFF)。然而,这些促炎细胞因子对 SF 中其他 TNF 超家族受体/配体或相关细胞因子受体的影响尚未得到研究。在这里,我们展示了 BAFF(CD257)、Fn14(CD266)、TACI(CD267)、BAFF-R(CD268)、BCMA(CD269)、CD40 配体(CD40L,CD154)、IFN-γR(CD119)、瘦素受体(ObR,CD295)、VCAM-1(CD106)和膜 TGF-β在分离的 SF 中的差异调节,以及 IFN-γ/TNF 共孵育对增殖、IL-6 和 IL-8 产生的影响。此外,评估了差异刺激的 SF 对共培养中 B 细胞存活的影响。通过流式细胞术检测表面细胞因子和细胞因子受体。通过 ELISA 定量可溶性细胞因子受体和细胞因子。通过细胞滴定蓝评估增殖。通过 Annexin V/碘化丙啶染色和流式细胞术确定纤维母细胞/ B 细胞共培养中鼠 B 细胞的存活。IFN-γ 与 TNF 协同并显著增加类风湿关节炎 SF 中 BAFF、Fn14、TACI、BAFF-R、BCMA、CD40L、ObR 和 IFN-γR 的细胞表面水平,在孵育 72 小时后。可溶性 BAFF 仅由 IFN-γ诱导,由 TNF 抑制。添加 TWEAK 对增殖或 IL-8 产生没有影响,但降低了 TNF 诱导的 IL-6 产生,而 APRIL、BAFF 和瘦素没有调节 TNF 或 TNF/IFN-γ 诱导的增殖或细胞因子产生。TNF 促进增殖,并通过添加 IFN-γ进一步增强。在共培养实验中,与单独 TNF 或 IFN-γ 刺激相比,用 TNF/IFN 刺激的 SF 增加了 VCAM-1 的脱落和膜 TGFβ 的表达,这与鼠 B 细胞存活率降低有关。IFN-γ 和 TNF 调节 TNF 家族成员细胞因子和相关受体的表达。在促炎条件下,IFN-γR 和 Fn14 的配体结合调节了 IL-6/IL-8 产生和增殖。在 B 细胞/SF 共培养物中,TNF/IFN 的组合通过增强 VCAM-1 的脱落和/或增加 TGF-β 的产生,可能导致 B 细胞存活减少。IFN-γ 是观察到的对 B 细胞存活和 SF 细胞因子产生影响所必需的,强调了其在类风湿关节炎中的抗炎作用。
