Effect of Epstein-Barr virus on macrophage M2/M1 migration and EphA2 expression in adverse drug reactions.

Ran An, Dong-Jie Sun, Hao-Xue Lei, Ang-Ran He, Ying Tu, Jun-Ting Tang
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Abstract

This study aims to investigate the effect of Epstein-Barr virus (EBV) reactivation or EBV reactivation with dexamethasone (DXM) in patients with adverse drug reactions (ADRs) through evaluating the levels of monocyte, macrophage M2/M1, and cytokines, and investigating whether expression of EBV receptor EphA2 could specifically influence EBV activation in ADRs. We performed a prospective longitudinal study to analyze the monocytes, macrophages, M2/M1 ratio, and cytokines, including interleukin (IL)-4, IL-13, tumor necrosis factor (TNF)-α, interferon (IFN)-γ, IFN-β, C-X-C motif chemokine ligand (CXCL)9, and CXCL10, in patients with maculopapular exanthema (MPE) and Stevens-Johnson syndrome/toxic epidermal necrolysis (SJS/TEN), and control groups after disease onset. Skin biopsy samples from these patients were subjected to hematoxylin and eosin (H&E) staining to examine tissue architecture and inflammatory cell infiltration, as well as Epstein-Barr virus-encoded RNA (EBER) staining to detect the presence of EBV within the skin lesions. Peripheral blood mononuclear cells collected from these patients were co-cultured with EBV or EBV combined with DXM to assess the impact on monocytes, macrophages, the M2/M1 ratio, and the associated cytokine profile. Furthermore, we sought to identify which cytokines might be crucial in mediating the interaction between the M2/M1 ratio and EBV. EPhA2 expression was evaluated to determine its role in the reactivation of EBV and its correlation with increased viral load in MPE and SJS/TEN patients. Selective depletion of macrophages occurred during the acute stage of SJS/TEN, while a shift towards M2 macrophages was observed in MPE. Both IFN-β and CXCL9 levels were elevated in MPE and SJS/TEN. Additionally, our study demonstrated the presence of EBV in the skin lesions of SJS/TEN and MPE patients through H&E and EBER staining, confirming EBV's involvement in these conditions. Activation of EBV and EBV combined with DXM led to a shift from M1 to M2 macrophages, accompanied by increased levels of IL-4, IFN-γ, and CXCL9 in MPE and SJS/TEN, compared to healthy individuals. Specifically, EBV combined with DXM primarily drove IFN-γ and IL-4 expansions in MPE, while CXCL9 was predominantly elevated in SJS/TEN. The increased IL-4 levels were associated with the relative rise in EBV viral loads after EBV combined with DXM stimulation. Furthermore, EphA2 expression in monocytes was significantly higher in SJS/TEN and MPE patients compared to controls, with further increases on EBV stimulation. This elevation in EPhA2 correlated with increased EBV viral load, particularly in MPE and SJS/TEN patients. The gradual shift from M1 to M2 cell development observed during the clinical course of MPE and SJS/TEN is mediated by the predominance of EBV and EBV with DXM at the acute stage, leading to elevated IL-4, IFN-γ, and CXCL9 levels, which may exacerbate allergic reactions. The elevation in EPhA2 correlated with increased EBV viral load, particularly in MPE and SJS/TEN patients, suggesting that adverse drug reactions may induce EPhA2 expression, facilitating EBV replication and activation. EphA2 could thus serve as an indicator of EBV activation and a marker for assessing the risk of EBV in patients with adverse drug reactions.

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Epstein-Barr 病毒对药物不良反应中巨噬细胞 M2/M1 迁移和 EphA2 表达的影响。
本研究旨在通过评估药物不良反应(ADRs)患者的单核细胞、巨噬细胞 M2/M1 和细胞因子水平,研究 Epstein-Barr 病毒(EBV)再活化或 EBV 再活化与地塞米松(DXM)对药物不良反应(ADRs)患者的影响,并探讨 EBV 受体 EphA2 的表达是否会特别影响 ADRs 中 EBV 的活化。我们进行了一项前瞻性纵向研究,分析了单核细胞、巨噬细胞、M2/M1 比率和细胞因子,包括白细胞介素 (IL)-4、IL-13、肿瘤坏死因子 (TNF)-α、干扰素 (IFN)-γ、IFN-β、在斑丘疹性红斑(MPE)和史蒂文斯-约翰逊综合征/毒性表皮坏死症(SJS/TEN)患者以及对照组中,在发病后检测 C-X-C motif 趋化因子配体(CXCL)9 和 CXCL10。对这些患者的皮肤活检样本进行苏木精和伊红(H&E)染色,以检查组织结构和炎症细胞浸润情况,并进行爱泼斯坦-巴氏病毒编码 RNA(EBER)染色,以检测皮损中是否存在 EBV。从这些患者身上采集的外周血单核细胞与 EBV 或 EBV 与 DXM 共同培养,以评估对单核细胞、巨噬细胞、M2/M1 比率和相关细胞因子谱的影响。此外,我们还试图确定哪些细胞因子可能对介导 M2/M1 比率与 EBV 之间的相互作用至关重要。我们评估了 EPhA2 的表达,以确定它在 EBV 再激活中的作用及其与 MPE 和 SJS/TEN 患者病毒载量增加的相关性。在 SJS/TEN 的急性期,巨噬细胞发生了选择性耗竭,而在 MPE 中则观察到向 M2 巨噬细胞的转变。在 MPE 和 SJS/TEN 中,IFN-β 和 CXCL9 水平均升高。此外,我们的研究还通过 H&E 和 EBER 染色证明了 EBV 存在于 SJS/TEN 和 MPE 患者的皮肤病变中,从而证实了 EBV 与这些病症的关系。与健康人相比,在 MPE 和 SJS/TEN 中,EBV 和 EBV 联合 DXM 的激活导致巨噬细胞从 M1 向 M2 转移,同时 IL-4、IFN-γ 和 CXCL9 水平升高。具体来说,EBV与DXM结合主要促使IFN-γ和IL-4在MPE中扩张,而CXCL9则主要在SJS/TEN中升高。IL-4水平的升高与EBV联合DXM刺激后EBV病毒载量的相对升高有关。此外,与对照组相比,SJS/TEN 和 MPE 患者单核细胞中的 EphA2 表达明显升高,在 EBV 刺激下进一步升高。EPhA2 的升高与 EBV 病毒载量的增加有关,尤其是在 MPE 和 SJS/TEN 患者中。在 MPE 和 SJS/TEN 临床病程中观察到的从 M1 细胞逐渐向 M2 细胞发展的转变是由 EBV 和 EBV 与 DXM 在急性期的主要作用介导的,从而导致 IL-4、IFN-γ 和 CXCL9 水平升高,这可能会加剧过敏反应。EPhA2 的升高与 EBV 病毒载量的增加相关,尤其是在 MPE 和 SJS/TEN 患者中,这表明不良药物反应可能会诱导 EPhA2 的表达,从而促进 EBV 的复制和活化。因此,EphA2可作为EBV激活的指标和评估药物不良反应患者EBV风险的标志物。
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