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A multimodality imaging model to track viable breast cancer cells from single arrest to metastasis in the mouse brain

机译:一种多模态成像模型可追踪活泼性乳腺癌细胞从单次逮捕到小鼠脑转移

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摘要

Cellular MRI involves sensitive visualization of iron-labeled cells in vivo but cannot differentiate between dead and viable cells. Bioluminescence imaging (BLI) measures cellular viability, and thus we explored combining these tools to provide a more holistic view of metastatic cancer cell fate in mice. Human breast carcinoma cells stably expressing Firefly luciferase were loaded with iron particles, injected into the left ventricle, and BLI and MRI were performed on days 0, 8, 21 and 28. The number of brain MR signal voids (i.e., iron-loaded cells) on day 0 significantly correlated with BLI signal. Both BLI and MRI signals decreased from day 0 to day 8, indicating a loss of viable cells rather than a loss of iron label. Total brain MR tumour volume on day 28 also correlated with BLI signal. Overall, BLI complemented our sensitive cellular MRI technologies well, allowing us for the first time to screen animals for successful injections, and, in addition to MR measures of cell arrest and tumor burden, provided longitudinal measures of cancer cell viability in individual animals. We predict this novel multimodality molecular imaging framework will be useful for evaluating the efficacy of emerging anti-cancer drugs at different stages of the metastatic cascade.
机译:细胞核磁共振成像涉及体内铁标记细胞的灵敏可视化,但不能区分死细胞和活细胞。生物发光成像(BLI)可以测量细胞活力,因此我们探索了将这些工具结合使用的方法,可以更全面地了解小鼠转移性癌细胞的命运。将稳定表达萤火虫荧光素酶的人乳腺癌细胞加载铁颗粒,注入左心室,并在第0、8、21和28天进行BLI和MRI。脑MR信号空洞的数量(即,加载铁的细胞)在第0天与BLI信号显着相关。从第0天到第8天,BLI和MRI信号均下降,表明有活力的细胞丢失而不是铁标记丢失。第28天的总脑MR肿瘤体积也与BLI信号相关。总体而言,BLI很好地补充了我们敏感的细胞核磁共振成像技术,使我们首次能够筛选动物进行成功注射,并且除了可以对细胞停滞和肿瘤负荷进行MR测量外,还可以纵向测量单个动物中癌细胞的生存能力。我们预测这种新颖的多峰态分子成像框架将可用于评估转移级联反应不同阶段出现的抗癌药物的疗效。

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