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首页> 外文期刊>The European Journal of Neuroscience >In vivo bioluminescence imaging of neurogenesis - the role of the blood brain barrier in an experimental model of Parkinson's disease
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In vivo bioluminescence imaging of neurogenesis - the role of the blood brain barrier in an experimental model of Parkinson's disease

机译:神经发生的体内生物发光成像 - 血脑屏障在帕金森病的实验模型中的作用

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Bioluminescence imaging in transgenic mice expressing firefly luciferase in Doublecortin + (Dcx) neuroblasts might serve as a powerful tool to study the role of neurogenesis in models of brain injury and neurodegeneration using non-invasive, longitudinal in vivo imaging. Therefore, we aimed to use BLI in B6(Cg)-Tyrc-2J/J Dcx-Luc (Doublecortin-Luciferase, Dcx-Luc) mice to investigate its suitability to assess neurogenesis in a unilateral injection model of Parkinson's disease. We further aimed to assess the blood brain barrier leakage associated with the intranigral 6-OHDA injection to evaluate its impact on substrate delivery and bioluminescence signal intensity. Two weeks after lesion, we observed an increase in bioluminescence signal in the ipsilateral hippocampal region in both, 6-OHDA and vehicle injected Dcx-Luc mice. At the same time, no corresponding increase in Dcx(+) neuroblast numbers could be observed in the dentate gyrus of C57Bl6 mice. Blood brain barrier leakage was observed in the hippocampal region and in the degenerating substantia nigra of C57Bl6 mice in vivo using T1 weighted Magnetic Resonance Imaging with Gadovist (R) and ex vivo using Evans Blue Fluorescence Reflectance Imaging and mouse Immunoglobulin G staining. Our data suggests a BLI signal dependency on blood brain barrier permeability, underlining a major pitfall of substrate/tracer dependent imaging in invasive disease models.
机译:在双峰素+(DCX)神经细胞中表达萤火虫荧光素酶的转基因小鼠的生物发光成像可以作为研究神经发生在脑损伤模型中的功能的强大工具,使用非侵入性,纵向体内成像。因此,我们的目标是在B6(CG)-TYRC-2J / J DCX-LUC(DOPBERRECORIN-LUCIFIRA酶,DCX-LUC)小鼠中使用BLI,以研究其适用性在帕金森病的单侧注射模型中评估神经发生。我们进一步旨在评估与肺中,血脑屏障渗漏与血糖6-OHDA注射相关,以评估其对基底递送和生物发光信号强度的影响。病变后两周,我们观察到6-OHDA和载体注射DCX-LUC小鼠的同侧海马区域中的生物发光信号增加。同时,在C57BL6小鼠的齿状回物中,不能观察到DCX(+)神经细胞数的相应增加。在海马区域中观察到血脑屏障泄漏,并使用evans蓝荧光反射成像和小鼠免疫球蛋白G染色,使用T1加权磁共振成像在体内的C57BL6小鼠的D57BL6小鼠的退化基质NIGRA。我们的数据表明BLI信号依赖性对血脑屏障渗透性的依赖性,下划线在侵袭性疾病模型中下划出基材/示踪剂依赖性成像的主要缺陷。

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