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日本脑炎病毒感染调节原代星形胶质细胞和星形胶质细胞来源的细胞系中的促炎细胞因子/趋化因子谱。

Japanese encephalitis viral infection modulates proinflammatory cyto/chemokine profile in primary astrocyte and cell line of astrocytic origin.

机构信息

National Brain Research Centre, Manesar, Haryana, 122052, India.

出版信息

Metab Brain Dis. 2022 Jun;37(5):1487-1502. doi: 10.1007/s11011-022-00991-w. Epub 2022 Apr 29.

Abstract

Japanese Encephalitis Virus (JEV) is a neurotropic virus that invades Central Nervous System (CNS) and causes severe neuroinflammation. Given the abundance and the position of astrocytes in the CNS, we speculate that they might play a critical role in the process of neuroinflammation. Unfortunately, the role of astrocytes in JEV-mediated neuroinflammation has long been understated. In this study, we have attempted to assess the role of astrocyte-mediated neuroinflammation upon JEV infection. Mouse model of JEV infection, generated by intraperitoneal injection, showed severe reactive astrogliosis. To further address our hypothesis, we employed immortalized astrocytic cell line (in vitro) and primary astrocyte-enriched culture (ex vivo) as experimental models. JEV infection in the astrocytes induces proinflammatory cytokines like MCP1/CCL2 and IL6 in both ex vivo and in vitro cultures as observed from the cytometric bead array analysis. A significantly altered cytokine profile was observed using PCR analysis in in vitro and ex vivo models upon infection, with respect to control, validating our previous results. We also show that there exists a major inconsistency in the viral replication kinetics, wherein the cell line showed a robust rate of replication whereas the primary astrocyte-enriched culture showed negligibly low number of plaques, underlining the importance of the selection of appropriate experimental model system. In conclusion, we claim that astrocytes significantly contribute to JEV-mediated neuroinflammation, despite not being a CNS immune cell.

摘要

日本脑炎病毒(JEV)是一种神经嗜性病毒,可侵犯中枢神经系统(CNS)并引起严重的神经炎症。鉴于星形胶质细胞在 CNS 中的丰富度和位置,我们推测它们可能在神经炎症过程中发挥关键作用。不幸的是,星形胶质细胞在 JEV 介导的神经炎症中的作用长期以来被低估了。在这项研究中,我们试图评估星形胶质细胞介导的 JEV 感染后的神经炎症作用。通过腹腔注射建立的 JEV 感染小鼠模型显示出严重的反应性星形胶质增生。为了进一步验证我们的假设,我们使用永生化星形胶质细胞系(体外)和原代富含星形胶质细胞的培养物(离体)作为实验模型。如细胞因子珠阵列分析所示,JEV 感染星形胶质细胞会在体外和离体培养物中诱导促炎细胞因子,如 MCP1/CCL2 和 IL6。感染后,通过 PCR 分析在体外和离体模型中观察到细胞因子谱发生明显改变,与对照相比,验证了我们之前的结果。我们还表明,病毒复制动力学存在重大差异,其中细胞系显示出强大的复制率,而原代富含星形胶质细胞的培养物显示出可忽略不计的低数量蚀斑,这突出了选择适当的实验模型系统的重要性。总之,我们声称星形胶质细胞尽管不是 CNS 免疫细胞,但它们对 JEV 介导的神经炎症有显著贡献。

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