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Methods for detecting host genetic modifiers of tumor vascular function using dynamic near-infrared fluorescence imaging

机译:动态近红外荧光成像检测肿瘤血管功能宿主遗传修饰剂的方法

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摘要

Vascular supply is a critical component of the tumor microenvironment (TME) and is essential for tumor growth and metastasis, yet the endogenous genetic modifiers that impact vascular function in the TME are largely unknown. To identify the host TME modifiers of tumor vascular function, we combined a novel genetic mapping strategy [Consomic Xenograft Model] with near-infrared (NIR) fluorescence imaging and multiparametric analysis of pharmacokinetic modeling. To detect vascular flow, an intensified cooled camera based dynamic NIR imaging system with 785 nm laser diode based excitation was used to image the whole-body fluorescence emission of intravenously injected indocyanine green dye. Principal component analysis was used to extract the spatial segmentation information for the lungs, liver, and tumor regions-of-interest. Vascular function was then quantified by pK modeling of the imaging data, which revealed significantly altered tissue perfusion and vascular permeability that were caused by host genetic modifiers in the TME. Collectively, these data demonstrate that NIR fluorescent imaging can be used as a non-invasive means for characterizing host TME modifiers of vascular function that have been linked with tumor risk, progression, and response to therapy.
机译:血管供应是肿瘤微环境(TME)的关键组成部分,对于肿瘤的生长和转移至关重要,但是影响TME中血管功能的内源性遗传修饰因子尚不清楚。为了确定宿主的肿瘤血管功能的TME修饰剂,我们将一种新颖的遗传作图策略[Consomic Xenograft模型]与近红外(NIR)荧光成像和药代动力学模型的多参数分析相结合。为了检测血管血流,使用基于785激光二极管的激发的增强型基于冷却相机的动态NIR成像系统对静脉注射的吲哚菁绿色染料的全身荧光发射进行成像。主成分分析用于提取肺,肝和肿瘤感兴趣区域的空间分割信息。然后通过成像数据的pK建模对血管功能进行定量,结果显示TME中宿主基因修饰剂引起的组织灌注和血管通透性显着改变。总体而言,这些数据表明,NIR荧光成像可用作表征血管功能的宿主TME调节剂的非侵入性手段,这些调节剂与肿瘤风险,进展和对治疗的反应有关。

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