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New insights into type I interferon and the immunopathogenesis of persistent viral infections

机译:对I型干扰素和持续性病毒感染的免疫发病机制的新见解

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摘要

Most viruses generate potent T cell responses that rapidly control infection. However, certain viruses can subvert the immune response to establish persistent infections. The inability to clear virus induces an immunosuppressive program leading to the sustained expression of many immunoregulatory molecules that down-regulate T cell responses. Further, viral persistence is associated with multiple immune dysfunctions including lymphoid disorganization, defective antigen presentation, aberrant B cell responses and hypergammaglobulinemia. Although best known for its antiviral activity, recent data has highlighted the role of type I IFN (IFN-I) signaling as a central mediator of immunosuppression during viral persistence. It is also becoming increasingly apparent that many of the immune dysfunctions during persistent virus infection can be attributed directly or indirectly to the effects of chronic IFN-I signaling. This review explores the increasingly complex role of IFN-I in the regulation of immunity against persistently replicating virus infections and examines current and potential uses of IFN-I and blockade of IFN-I signaling to dampen chronic inflammation and activation in the clinic.
机译:大多数病毒会产生有效的T细胞反应,从而迅速控制感染。但是,某些病毒可以破坏免疫反应以建立持久性感染。无法清除病毒会诱导免疫抑制程序,导致许多下调T细胞反应的免疫调节分子持续表达。此外,病毒的持久性与多种免疫功能障碍有关,包括淋巴组织紊乱,抗原呈递缺陷,B细胞异常反应和高球蛋白血症。尽管最著名的是其抗病毒活性,但最近的数据突出了I型IFN(IFN-I)信号传导在病毒持续过程中作为免疫抑制的主要介质的作用。越来越明显的是,持续性病毒感染期间的许多免疫功能障碍可直接或间接地归因于慢性IFN-I信号传导的作用。这篇综述探讨了IFN-α在调节针对持续复制的病毒感染的免疫中日益复杂的作用,并探讨了IFN-I的当前和潜在用途以及对IFN-I信号传导的阻断,以减轻临床中的慢性炎症和活化。

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