Literature DB >> 19663686

Magnetic resonance imaging assessment of macrophage accumulation in mouse brain after experimental traumatic brain injury.

Lesley M Foley1, T Kevin Hitchens, Chien Ho, Keri L Janesko-Feldman, John A Melick, Hulya Bayir, Patrick M Kochanek.   

Abstract

Macrophages contribute to secondary damage and repair after central nervous system (CNS) injury. Micron-sized paramagnetic iron oxide (MPIO) particles can label macrophages in situ, facilitating three-dimensional (3D) mapping of macrophage accumulation following traumatic brain injury (TBI), via ex vivo magnetic resonance microscopy (MRM) and in vivo monitoring with magnetic resonance imaging (MRI). MPIO particles were injected intravenously (iv; 4.5 mg Fe/Kg) in male C57BL/6J mice (n = 21). A controlled cortical impact (CCI) was delivered to the left parietal cortex. Five protocols were used in naive and injured mice to assess feasibility, specificity, and optimal labeling time. In vivo imaging was carried out at 4.7 Tesla (T). Brains were then excised for 3D MRM at 11.7 T. Triple-label immunofluorescence (MPIO via Dragon Green, macrophages via F480, and nuclei via 4,6-diamidino-2-phenylindole [DAPI]) of brain sections confirmed MPIO particles within macrophages. MRM of naives showed an even distribution of a small number of MPIO-labeled macrophages in the brain. MRM at 48-72 h after CCI and MPIO injection revealed MPIO-labeled macrophages accumulated in the trauma region. When MPIO particles were injected 6 days before CCI, MRM 48 h after CCI also revealed labeled cells at the injury site. In vivo studies of macrophage accumulation by MRI suggest that this approach is feasible, but requires additional optimization. We conclude that MPIO labeling and ex vivo MRM mapping of macrophage accumulation for assessment of TBI is readily accomplished. This new technique could serve as an adjunct to conventional MR approaches by defining inflammatory mechanisms and therapeutic efficacy of anti-inflammatory agents in experimental TBI.

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Year:  2009        PMID: 19663686      PMCID: PMC2822809          DOI: 10.1089/neu.2008.0747

Source DB:  PubMed          Journal:  J Neurotrauma        ISSN: 0897-7151            Impact factor:   5.269


  47 in total

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Review 4.  Inflammatory response in acute traumatic brain injury: a double-edged sword.

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  21 in total

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2.  Labeling of Luciferase/eGFP-expressing bone marrow-derived stromal cells with fluorescent micron-sized iron oxide particles improves quantitative and qualitative multimodal imaging of cellular grafts in vivo.

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Journal:  Mol Imaging Biol       Date:  2011-12       Impact factor: 3.488

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4.  Advances in MRI-Based Detection of Cerebrovascular Changes after Experimental Traumatic Brain Injury.

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5.  Automated detection and characterization of SPIO-labeled cells and capsules using magnetic field perturbations.

Authors:  Parker H Mills; T Kevin Hitchens; Lesley M Foley; Thomas Link; Qing Ye; Clifford R Weiss; Joe D Thompson; Wesley D Gilson; Aravind Arepally; John A Melick; Patrick M Kochanek; Chien Ho; Jeff W M Bulte; Eric T Ahrens
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6.  Paths to Successful Translation of New Therapies for Severe Traumatic Brain Injury in the Golden Age of Traumatic Brain Injury Research: A Pittsburgh Vision.

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Review 7.  Quo vadis 2010? - carpe diem: challenges and opportunities in pediatric traumatic brain injury.

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8.  The evolution of traumatic brain injury in a rat focal contusion model.

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9.  Blood brain barrier is impermeable to solutes and permeable to water after experimental pediatric cardiac arrest.

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10.  Long-term in vivo imaging of viscoelastic properties of the mouse brain after controlled cortical impact.

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Journal:  J Neurotrauma       Date:  2013-08-01       Impact factor: 5.269

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