Min Yi scite author profile

SUMMARY Microglia are an exquisitely tiled and self-contained population in the CNS that do not receive contributions from circulating monocytes in the periphery. While microglia are long-lived cells, the extent to which their cell bodies are fixed and the molecular mechanisms by which the microglial landscape is regulated have not been determined. Using chronic in vivo two-photon imaging to follow the microglial population in young adult mice, we document a daily rearrangement of the microglial landscape. Furthermore, we show that the microglial landscape can be modulated by severe seizures, acute injury, and sensory deprivation. Finally, we demonstrate a critical role for microglial P2Y12Rs in regulating the microglial landscape through cellular translocation independent of proliferation. These findings suggest that microglial patrol the CNS through both process motility and soma translocation.

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Chemogenetic manipulation of microglia inhibits neuroinflammation and neuropathic pain in mice

Liu

et al. 2021

Brain, Behavior, and Immunity

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Optogenetic activation of spinal microglia triggers chronic pain in mice

Liu

Umpierre

et al. 2021

PLoS Biol

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Spinal microglia are highly responsive to peripheral nerve injury and are known to be a key player in pain. However, there has not been any direct evidence showing that selective microglial activation in vivo is sufficient to induce chronic pain. Here, we used optogenetic approaches in microglia to address this question employing CX3CR1creER/+: R26LSL-ReaChR/+ transgenic mice, in which red-activated channelrhodopsin (ReaChR) is inducibly and specifically expressed in microglia. We found that activation of ReaChR by red light in spinal microglia evoked reliable inward currents and membrane depolarization. In vivo optogenetic activation of microglial ReaChR in the spinal cord triggered chronic pain hypersensitivity in both male and female mice. In addition, activation of microglial ReaChR up-regulated neuronal c-Fos expression and enhanced C-fiber responses. Mechanistically, ReaChR activation led to a reactive microglial phenotype with increased interleukin (IL)-1β production, which is likely mediated by inflammasome activation and calcium elevation. IL-1 receptor antagonist (IL-1ra) was able to reverse the pain hypersensitivity and neuronal hyperactivity induced by microglial ReaChR activation. Therefore, our work demonstrates that optogenetic activation of spinal microglia is sufficient to trigger chronic pain phenotypes by increasing neuronal activity via IL-1 signaling.

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Emergency Evacuation Simulation and Management Optimization in Urban Residential Communities

Chu

Wen

et al. 2019

Sustainability

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Timely and secure evacuation of residents in communities is of great importance during unexpected disasters or emergency events. This study proposes a framework of evacuation simulation for optimizing emergency management in urban residential communities. Compared to traditional methods, the advantage of our framework lies in three aspects: (1) The method highlights easy-crowded areas in both indoor and outdoor evacuations. (2) Family behaviors are considered and implemented in evacuations. (3) Detailed measures on management optimization are spatially mapped based on a multi-level analysis and the comparison of evacuation simulation results in different scenarios. A case study in Changhongfang residential community, Xuhui District, Shanghai, China, was conducted to demonstrate the method feasibility. Simulation results have exposed potential evacuation problems in the community. A series of detailed recommended measures have been generated. These measures can help to create better emergency management for the community.

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The voltage-gated proton channel Hv1 promotes microglia-astrocyte communication and neuropathic pain after peripheral nerve injury

Peng

Jeong

et al. 2021

Mol Brain

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Activation of spinal cord microglia contributes to the development of peripheral nerve injury-induced neuropathic pain. However, the molecular mechanisms underlying microglial function in neuropathic pain are not fully understood. We identified that the voltage-gated proton channel Hv1, which is functionally expressed in spinal microglia, was significantly increased after spinal nerve transection (SNT). Hv1 mediated voltage-gated proton currents in spinal microglia and mice lacking Hv1 (Hv1 KO) display attenuated pain hypersensitivities after SNT compared with wildtype (WT) mice. In addition, microglial production of reactive oxygen species (ROS) and subsequent astrocyte activation in the spinal cord was reduced in Hv1 KO mice after SNT. Cytokine screening and immunostaining further revealed that IFN-γ expression was compromised in spinal astrocytes in Hv1 KO mice. These results demonstrate that Hv1 proton channel contributes to microglial ROS production, astrocyte activation, IFN-γ upregulation, and subsequent pain hypersensitivities after SNT. This study suggests Hv1-dependent microglia-astrocyte communication in pain hypersensitivities and identifies Hv1 as a novel therapeutic target for alleviating neuropathic pain.

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Extracorporeal shockwave therapy enhances peripheral nerve remyelination and gait function in a crush model

et al. 2020

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Chromosomal aberration arises during somatic reprogramming to pluripotent stem cells

Liu

Zheng

et al. 2020

Cell Div

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Background Reprogramming somatic cells to induced pluripotent stem cells (iPSCs) has opened new therapeutic possibilities. However, karyotypic abnormalities detected in iPSCs compromised their utility, especially chromosomal aberrations found at early passages raised serious safety concerns. The mechanism underlying the chromosomal abnormality in early-passage iPSCs is not known. Methods Human dermal fibroblasts (HDFs) were stimulated with KMOS (KLF4, cMYC, OCT4 and SOX2) proteins to enhance their proliferative capacity and many vigorous clones were obtained. Clonal reprogramming was carried out by KMOS mRNAs transfection to confirm the ‘chromosomal mutagenicity’ of reprogramming process. Subculturing was performed to examine karyotypic stability of iPSCs after the re-establishment of stemness. And antioxidant N-acetyl-cysteine (NAC) was added to the culture medium for further confirmming the mutagenicity in the first few days of reprogramming. Results Chromosomal aberrations were found in a small percentage of newly induced iPS clones by reprogramming transcription factors. Clonal reprogramming ruled out the aberrant chromosomes inherited from rare karyotypically abnormal parental cell subpopulation. More importantly, the antioxidant NAC effectively reduced the occurrence of chromosomal aberrations at the early stage of reprogramming. Once iPS cell lines were established, they restored karyotypic stability in subsequent subculturing. Conclusions Our results provided the first line of evidence for the ‘chromosomal mutagenicity’ of reprogramming process.

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Min Yi

Astrocyte-microglia interaction drives evolving neuromyelitis optica lesion

P2Y12R-Dependent Translocation Mechanisms Gate the Changing Microglial Landscape

Chemogenetic manipulation of microglia inhibits neuroinflammation and neuropathic pain in mice

Optogenetic activation of spinal microglia triggers chronic pain in mice

Emergency Evacuation Simulation and Management Optimization in Urban Residential Communities

The voltage-gated proton channel Hv1 promotes microglia-astrocyte communication and neuropathic pain after peripheral nerve injury

Extracorporeal shockwave therapy enhances peripheral nerve remyelination and gait function in a crush model

Chromosomal aberration arises during somatic reprogramming to pluripotent stem cells

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