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Temporal window for detection of inflammatory disease using dynamic cell tracking with time-lapse MRI

机译:使用延时MRI动态细胞跟踪检测炎症性疾病的时间窗

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摘要

Time-lapse MRI was implemented for dynamic non-invasive cell tracking of individual slowly moving intravascular immune cells. Repetitive MRI acquisition enabled dynamic observation of iron oxide nanoparticle (ION) labelled cells. Simulations of MRI contrast indicated that only cells moving slower than 1 µm/s were detectable. Time-lapse MRI of the brain was performed after either IONs or ION-labelled monocytes were injected intravenously into naïve and experimental autoimmune encephalomyelitis (EAE) bearing mice at a presymptomatic or symptomatic stage. EAE mice showed a reduced number of slow moving, i.e. patrolling cells before and after onset of symptoms as compared to naïve controls. This observation is consistent with the notion of altered cell dynamics, i.e. higher velocities of immune cells rolling along the endothelium in the inflamed condition. Thus, time-lapse MRI enables for assessing immune cell dynamics non-invasively in deep tissue and may serve as a tool for detection or monitoring of an inflammatory response.
机译:延时MRI用于对缓慢移动的血管内免疫细胞进行动态无创细胞跟踪。重复进行MRI采集可动态观察氧化铁纳米颗粒(ION)标记的细胞。 MRI对比模拟表明,只有移动速度低于1μm/ s的细胞才能被检测到。将IONs或ION标记的单核细胞静脉注射到处于症状前或有症状阶段的幼稚和实验性自身免疫性脑脊髓炎(EAE)小鼠中后,对大脑进行延时MRI。与幼稚的对照组相比,EAE小鼠的症状发生前后,其移动缓慢,即巡逻细胞的数量减少。该观察结果与改变细胞动力学的想法是一致的,即在发炎状态下免疫细胞沿内皮滚动的更高速度。因此,延时MRI可以无创地评估深层组织中的免疫细胞动力学,并且可以用作检测或监测炎症反应的工具。

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