4.8 Article

Mapping microglia and astrocyte activation in vivo using diffusion MRI

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SCIENCE ADVANCES
卷 8, 期 21, 页码 -

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AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/sciadv.abq2923

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资金

  1. European Research Council through a Marie Sklodowska-Curie Individual Fellowship [749506]
  2. Spanish Agency of Research (AEI) [PGC2018-101055-B-I00]
  3. European Regional Development Fund (ERDF)
  4. Generalitat Valenciana [Prometeo/2019/015, SEJI/2019/038, CIDEGENT/2021/015]
  5. European Union [668863]
  6. Spanish State Research Agency through the Severo Ochoa Program for Centres of Excellence in RD [SEV-2017-0723]
  7. EPSRC [EP/M029778/1]
  8. Wolfson Foundation
  9. Wellcome Trust Investigator Award [096646/Z/11/Z]
  10. Wellcome Trust [096646/Z/11/Z, 104943/Z/14/Z]
  11. Marie Curie Actions (MSCA) [749506] Funding Source: Marie Curie Actions (MSCA)

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This study presents a noninvasive diffusion-weighted magnetic resonance imaging method to image changes in glia morphology. Using animal models, the researchers demonstrate that this method can quantify specific markers of glial cell activation and is sensitive to changes in morphology and proliferation. The study also proves the translational value of this approach in human experiments.
While glia are increasingly implicated in the pathophysiology of psychiatric and neurodegenerative disorders, available methods for imaging these cells in vivo involve either invasive procedures or positron emission tomography radiotracers, which afford low resolution and specificity. Here, we present a noninvasive diffusion-weighted magnetic resonance imaging (MRI) method to image changes in glia morphology. Using rat models of neuroinflammation, degeneration, and demyelination, we demonstrate that diffusion-weighted MRI carries a fingerprint of microglia and astrocyte activation and that specific signatures from each population can be quantified noninvasively. The method is sensitive to changes in glia morphology and proliferation, providing a quantitative account of neuroinflammation, regardless of the existence of a concomitant neuronal loss or demyelinating injury. We prove the translational value of the approach showing significant associations between MRI and histological microglia markers in humans. This framework holds the potential to transform basic and clinical research by clarifying the role of inflammation in health and disease.

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