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甲型流感病毒感染诱导的长期神经炎症及其对海马神经元形态和功能的影响。

Long-Term Neuroinflammation Induced by Influenza A Virus Infection and the Impact on Hippocampal Neuron Morphology and Function.

机构信息

Department of Cellular Neurobiology, Zoological Institute, TU Braunschweig, 38106 Braunschweig, Germany.

Helmholtz Centre for Infection Research, Neuroinflammation and Neurodegeneration Group, 38126 Braunschweig, Germany.

出版信息

J Neurosci. 2018 Mar 21;38(12):3060-3080. doi: 10.1523/JNEUROSCI.1740-17.2018. Epub 2018 Feb 27.

Abstract

Acute influenza infection has been reported to be associated with neurological symptoms. However, the long-term consequences of an infection with neurotropic and non-neurotropic influenza A virus (IAV) variants for the CNS remain elusive. We can show that spine loss in the hippocampus after infection with neurotropic H7N7 (rSC35M) and non-neurotropic H3N2 (maHK68) in female C57BL/6 mice persists well beyond the acute phase of the disease. Although spine number was significantly reduced at 30 d postinfection (dpi) with H7N7 or H3N2, full recovery could only be observed much later at 120 dpi. Infection with H1N1 virus, which was shown previously to affect spine number and hippocampus-dependent learning acutely, had no significant long-term effects. Spine loss was associated with an increase in the number of activated microglia, reduced long-term potentiation in the hippocampus, and impairment in spatial memory formation, indicating that IAV-associated inflammation induced functional and structural alterations in hippocampal networks. Transcriptome analyses revealed regulation of many inflammatory and neuron- and glia-specific genes in H3N2- and H7N7-infected mice at day 18 and in H7N7-infected mice at day 30 pi that related to the structural and functional alterations. Our data provide evidence that neuroinflammation induced by neurotropic H7N7 and infection of the lung with a non-neurotropic H3N2 IAV result in long-term impairments in the CNS. IAV infection in humans may therefore not only lead to short-term responses in infected organs, but may also trigger neuroinflammation and associated chronic alterations in the CNS. In the acute phase of influenza infection, neuroinflammation can lead to alterations in hippocampal neuronal morphology and cognitive deficits. The results of this study now also provide evidence that neuroinflammation induced by influenza A virus (IAV) infection can induce longer-lasting, virus-specific alterations in neuronal connectivity that are still detectable 1 month after infection and are associated with impairments in spatial memory formation. IAV infection in humans may therefore not only lead to short-term responses in infected organs, but may also trigger neuroinflammation and associated chronic alterations in the CNS.

摘要

急性流感感染已被报道与神经系统症状有关。然而,神经亲和性和非神经亲和性甲型流感病毒(IAV)变体感染中枢神经系统的长期后果仍不清楚。我们可以证明,在雌性 C57BL/6 小鼠中,感染神经亲和性 H7N7(rSC35M)和非神经亲和性 H3N2(maHK68)后,海马体中的脊柱损失在疾病的急性期之后仍然持续存在。尽管 H7N7 或 H3N2 感染后 30 天的脊柱数量显著减少,但只有在 120 天才能观察到完全恢复。先前已显示影响急性脊柱数量和海马依赖性学习的 H1N1 病毒没有明显的长期影响。脊柱损失与激活的小胶质细胞数量增加、海马体中的长时程增强减少以及空间记忆形成受损有关,表明 IAV 相关炎症诱导了海马体网络的功能和结构改变。转录组分析显示,在感染后第 18 天的 H3N2 和 H7N7 感染小鼠以及感染后第 30 天的 H7N7 感染小鼠中,许多炎症和神经元及神经胶质特异性基因的表达发生了调节,这些调节与结构和功能改变有关。我们的数据提供了证据,表明神经亲和性 H7N7 诱导的神经炎症和肺中非神经亲和性 H3N2 IAV 的感染导致中枢神经系统的长期损伤。因此,人类的 IAV 感染不仅会导致受感染器官的短期反应,还可能引发神经炎症和相关的中枢神经系统慢性改变。在流感感染的急性期,神经炎症可导致海马神经元形态的改变和认知缺陷。本研究的结果还提供了证据,表明流感病毒(IAV)感染诱导的神经炎症可导致神经元连接的更长时间、病毒特异性改变,这些改变在感染后 1 个月仍可检测到,并与空间记忆形成受损有关。因此,人类的 IAV 感染不仅会导致受感染器官的短期反应,还可能引发神经炎症和相关的中枢神经系统慢性改变。

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