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Merck
  • Longitudinal in vivo imaging of acute neuropathology in a monkey model of Ebola virus infection.

Longitudinal in vivo imaging of acute neuropathology in a monkey model of Ebola virus infection.

Nature communications (2021-05-19)
William Schreiber-Stainthorp, Jeffrey Solomon, Ji Hyun Lee, Marcelo Castro, Swati Shah, Neysha Martinez-Orengo, Rebecca Reeder, Dragan Maric, Robin Gross, Jing Qin, Katie R Hagen, Reed F Johnson, Dima A Hammoud
摘要

Ebola virus (EBOV) causes neurological symptoms yet its effects on the central nervous system (CNS) are not well-described. Here, we longitudinally assess the acute effects of EBOV on the brain, using quantitative MR-relaxometry, 18F-Fluorodeoxyglucose PET and immunohistochemistry in a monkey model. We report blood-brain barrier disruption, likely related to high cytokine levels and endothelial viral infection, with extravasation of fluid, Gadolinium-based contrast material and albumin into the extracellular space. Increased glucose metabolism is also present compared to the baseline, especially in the deep gray matter and brainstem. This regional hypermetabolism corresponds with mild neuroinflammation, sporadic neuronal infection and apoptosis, as well as increased GLUT3 expression, consistent with increased neuronal metabolic demands. Neuroimaging changes are associated with markers of disease progression including viral load and cytokine/chemokine levels. Our results provide insight into the pathophysiology of CNS involvement with EBOV and may help assess vaccine/treatment efficacy in real time.

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Sigma-Aldrich
抗-NeuN纯化抗体, from guinea pig, purified by affinity chromatography
Sigma-Aldrich
单克隆抗-白蛋白 小鼠抗, clone HSA-11, ascites fluid