Prolonged anesthesia induces neuroinflammation and complement-mediated microglial synaptic elimination involved in neurocognitive dysfunction and anxiety-like behaviors

Xu, Feng; Han, Linlin; Wang, Yafeng; Deng, Daling; Ding, Yuanyuan; Zhao, Shuai; Zhang, Qingtong; Ma, Lulin; Chen, Xiangdong

doi:10.1186/s12916-022-02705-6

Cited by 34 publications

(23 citation statements)

References 64 publications

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“…Second, the electrophysiology of synapses such as long-term potentiation/depression, EEG changes, or burst suppression was not measured. Previous studies have demonstrated that sevoflurane impaired synapse development and electrophysiological activity [ 23 , 61 – 64 ]. Last, we used intraperitoneal injection of ANX005 and NADNA to inhibit the expression of C1q and sialidase respectively, and we did not perform interventions at the gene and transcriptional levels.…”

Section: Discussionmentioning

confidence: 99%

“…C1q is the initiating protein in the complement cascade. A recent study showed that prolonged sevoflurane exposure increased C1q expression in the rat hippocampus, and deletion of C1q prevented microglial synaptic engulfment to alleviate cognitive dysfunction [ 23 ]. Several factors affect the binding of C1q to synapses, such as CD47, neuronal pentraxins, and sialic acids [ 24 ].…”

Section: Introductionmentioning

confidence: 99%

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Complement C1q-mediated microglial synaptic elimination by enhancing desialylation underlies sevoflurane-induced developmental neurotoxicity

Wang,

Liu,

Meng

et al. 2024

Cell Biosci

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Background Repeated neonatal sevoflurane exposures led to neurocognitive disorders in young mice. We aimed to assess the role of microglia and complement C1q in sevoflurane-induced neurotoxicity and explore the underlying mechanisms. Methods Neonatal mice were treated with sevoflurane on postnatal days 6, 8, and 10, and the Morris water maze was performed to assess cognitive functions. For mechanistic explorations, mice were treated with minocycline, C1q-antibody ANX005, and sialidase-inhibitor N-acetyl-2,3-dehydro-2-deoxyneuraminic acid (NADNA) before sevoflurane exposures. Western blotting, RT-qPCR, Golgi staining, 3D reconstruction and engulfment analysis, immunofluorescence, and microglial morphology analysis were performed. In vitro experiments were conducted in microglial cell line BV2 cells. Results Repeated neonatal sevoflurane exposures resulted in deficiencies in learning and cognition of young mice, accompanied by microglial activation and synapse loss. Sevoflurane enhanced microglia-mediated synapse elimination through C1q binding to synapses. Inhibition of microglial activation and phagocytosis with minocycline significantly reduced the loss of synapses. We further revealed the involvement of neuronal sialic acids in this process. The enhanced activity of sialidase by sevoflurane led to the loss of sialic acids, which facilitated C1q binding to synapses. Inhibition of C1q with ANX005 or inhibition of sialidase with NADNA significantly rescued microglia-mediated synapse loss and improved neurocognitive function. Sevoflurane enhanced the engulfment of BV2 cells, which was reversed by ANX005. Conclusions Our findings demonstrated that C1q-mediated microglial synaptic elimination by enhancing desialylation contributed to sevoflurane-induced developmental neurotoxicity. Inhibition of C1q or sialidase may be a potential therapeutic strategy for this neurotoxicity.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Complement C1q-mediated microglial synaptic elimination by enhancing desialylation underlies sevoflurane-induced developmental neurotoxicity

Wang,

Liu,

Meng

et al. 2024

Cell Biosci

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“…Drugs used for induction of general anesthesia, such as isoflurane, suppress LPS-induced expression of microglial pro-inflammatory cytokine IL-1β in mouse brains ( Tanaka et al, 2013 ). On the other hand, prolonged anesthesia using sevoflurane induces neuroinflammation by triggering the NF-κB pathway, activates microglia, and alters their morphology in the hippocampus of aged rats ( Xu et al, 2023 ). According to Brambrink et al (2012) , exposure to isoflurane for 5 h causes apoptosis of oligodendrocytes (estimated at 6.3% of the total oligodendrocyte population) in neonatal primate brains ( Brambrink et al, 2012 ).…”

Section: Factors Affecting Traumatic Brain Injury Outcome In Experimentsmentioning

confidence: 99%

Reactive gliosis in traumatic brain injury: a comprehensive review

Amlerova,

Chmelova,

Anderova

et al. 2024

Front. Cell. Neurosci.

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Traumatic brain injury (TBI) is one of the most common pathological conditions impacting the central nervous system (CNS). A neurological deficit associated with TBI results from a complex of pathogenetic mechanisms including glutamate excitotoxicity, inflammation, demyelination, programmed cell death, or the development of edema. The critical components contributing to CNS response, damage control, and regeneration after TBI are glial cells–in reaction to tissue damage, their activation, hypertrophy, and proliferation occur, followed by the formation of a glial scar. The glial scar creates a barrier in damaged tissue and helps protect the CNS in the acute phase post-injury. However, this process prevents complete tissue recovery in the late/chronic phase by producing permanent scarring, which significantly impacts brain function. Various glial cell types participate in the scar formation, but this process is mostly attributed to reactive astrocytes and microglia, which play important roles in several brain pathologies. Novel technologies including whole-genome transcriptomic and epigenomic analyses, and unbiased proteomics, show that both astrocytes and microglia represent groups of heterogenic cell subpopulations with different genomic and functional characteristics, that are responsible for their role in neurodegeneration, neuroprotection and regeneration. Depending on the representation of distinct glia subpopulations, the tissue damage as well as the regenerative processes or delayed neurodegeneration after TBI may thus differ in nearby or remote areas or in different brain structures. This review summarizes TBI as a complex process, where the resultant effect is severity-, region- and time-dependent and determined by the model of the CNS injury and the distance of the explored area from the lesion site. Here, we also discuss findings concerning intercellular signaling, long-term impacts of TBI and the possibilities of novel therapeutical approaches. We believe that a comprehensive study with an emphasis on glial cells, involved in tissue post-injury processes, may be helpful for further research of TBI and be the decisive factor when choosing a TBI model.

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“…Under physiological conditions, microglia play a crucial role in the process of synaptic pruning, which maintains the integrity of neural circuits. However, under pathological conditions, activated microglia can lead to excessive synaptic phagocytosis, resulting in the loss of synapses and consequent cognitive impairment [135] , [136] , [137] . In mice with chronic social defeat stress-induced depression, there is evidence of excessive synaptic pruning, which is attributed to microglia-dependent synaptic phagocytosis [138] .…”

Section: Immune Dysfunction In Depressive Disordermentioning

confidence: 99%

Intertwined associations between oxytocin, immune system and major depressive disorder

Jiang

Yang

Tian

et al. 2023

Biomedicine & Pharmacotherapy

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Prolonged anesthesia induces neuroinflammation and complement-mediated microglial synaptic elimination involved in neurocognitive dysfunction and anxiety-like behaviors

Cited by 34 publications

References 64 publications

Complement C1q-mediated microglial synaptic elimination by enhancing desialylation underlies sevoflurane-induced developmental neurotoxicity

Complement C1q-mediated microglial synaptic elimination by enhancing desialylation underlies sevoflurane-induced developmental neurotoxicity

Reactive gliosis in traumatic brain injury: a comprehensive review

Intertwined associations between oxytocin, immune system and major depressive disorder

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