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In vivo characterization of tumor vasculature using iodine and gold nanoparticles and dual energy micro-CT

机译:碘和金纳米粒子和双能微CT在体内表征肿瘤血管

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Tumor blood volume and vascular permeability are well established indicators of tumor angiogenesis and important predictors in cancer diagnosis, planning and treatment. In this work, we establish a novel preclinical imaging protocol which allows quantitative measurement of both metrics simultaneously. First, gold nanoparticles are injected and allowed to extravasate into the tumor, and then liposomal iodine nanoparticles are injected. Combining a previously optimized dual energy micro-CT scan using high-flux polychromatic x-ray sources (energies: 40 kVp, 80 kVp) with a novel post-reconstruction spectral filtration scheme, we are able to decompose the results into 3D iodine and gold maps, allowing simultaneous measurement of extravasated gold and intravascular iodine concentrations. Using a digital resolution phantom, the mean limits of detectability (mean CNR = 5) for each element are determined to be 2.3 mg mL-1 (18 mM) for iodine and 1.0 mg mL-1 (5.1 mM) for gold, well within the observed in vivo concentrations of each element (I: 0-24 mg mL-1, Au: 0-9 mg mL-1) and a factor of 10 improvement over the limits without post-reconstruction spectral filtration. Using a calibration phantom, these limits are validated and an optimal sensitivity matrix for performing decomposition using our micro-CT system is derived. Finally, using a primary mouse model of soft-tissue sarcoma, we demonstrate the in vivo application of the protocol to measure fractional blood volume and vascular permeability over the course of five days of active tumor growth.
机译:肿瘤血容量和血管通透性是公认的肿瘤血管生成指标,并且是癌症诊断,计划和治疗中的重要预测指标。在这项工作中,我们建立了一种新颖的临床前成像协议,该协议允许同时对两个指标进行定量测量。首先,将金纳米颗粒注射并渗入肿瘤,然后注射脂质体碘纳米颗粒。将先前优化的使用高通量多色x射线源(能量:40 kVp,80 kVp)的双能量微CT扫描与新颖的重建后光谱过滤方案相结合,我们能够将结果分解为3D碘和金地图,可以同时测量渗出的金和血管内碘的浓度。使用数字分辨率幻象,每个元素的可检测性平均限值(平均CNR = 5)确定为碘为2.3 mg mL-1(18 mM),金为1.0 mg mL-1(5.1 mM),在观察到的每种元素的体内浓度(I:0-24 mg mL-1,Au:0-9 mg mL-1),并且在没有重建后光谱过滤的情况下,比限值提高了10倍。使用校准模型,可以验证这些限制,并得出使用我们的微型CT系统进行分解的最佳灵敏度矩阵。最后,使用软组织肉瘤的原代小鼠模型,我们证明了该方案的体内应用,可在活动性肿瘤生长的五天过程中测量分数的血容量和血管通透性。

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