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High accuracy of mesoscopic epi-fluorescence tomography for non-invasive quantitative volume determination of fluorescent protein-expressing tumours in mice

机译:高精度的介观落射荧光层析成像技术可无损定量测定小鼠中表达荧光蛋白的肿瘤

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Objectives To compare mesoscopic epi-fluorescence tomography (MEFT) and EPRI-illumination reflectance imaging (EPRI) for quantitative tumour size assessment in mice. Methods Tumour xenografts of green/red fluorescent protein (GFP/RFP)-expressing colon cancer cells were measured using MEFT, EPRI, ultrasound (US) and micro computed tomography (μCT) at day 14 post-injection (n06). Results from MEFT and EPRI were correlated with each other and with US and μCT (reference methods). Tumour volumes were measured ex vivo by GFP and RFP fluorescence imaging on cryoslices and compared with the in vivo measurements. Results High correlation and congruency were observed between MEFT, US and μCT (MEFT/US: GFP: r200.96; RFP: r200.97, both P<0.05; MEFT/μCT: GFP: r200.93; RFP: r200.90; both P<0.05). Additionally, in vivo MEFT data were highly correlated and congruent with ex vivo cryoslice imaging results (GFP: r200.96; RFP: r200.99; both P<0.05). In comparison, EPRI significantly overestimated tumour volumes (P<0.05), although there was a significant correlation with US and μCT (EPRI/US: GFP: r200.95; RFP: r200.94; both P<0.05; EPRI/μCT GFP: r200.86; RFP: r200.86; both P<0.05). Conclusions Fluorescence distribution reconstruction using MEFT affords highly accurate three-dimensional (3D) tumour volume data showing superior accuracy compared to EPRI. Thus, MEFT is a very suitable technique for quantitatively assessing fluorescence distribution in superficial tumours at high spatial resolution. Key Points ? Mesoscopic epi-fluorescence tomography (MEFT) is an important new molecular imaging technique. ? MEFT allows accurate size determination of superficial tumours with high resolution. ? MEFT is a suitable technique for longitudinal assessment of tumour growth. ? MEFT allows 3D reconstruction and quantification of fluorescence distributions.
机译:目的比较介观落射荧光层析成像(MEFT)和EPRI-照明反射成像(EPRI)在小鼠中定量肿瘤大小的评估。方法在注射后第14天(n06),使用MEFT,EPRI,超声(US)和微型计算机断层扫描(μCT)检测表达绿色/红色荧光蛋白(GFP / RFP)的结肠癌细胞的异种移植。 MEFT和EPRI的结果相互关联,并与US和μCT(参考方法)相关。通过冷冻切片上的GFP和RFP荧光成像离体测量肿瘤体积,并与体内测量结果进行比较。结果MEFT,US和μCT之间具有高度相关性和一致性(MEFT / US:GFP:r200.96; RFP:r200.97,均P <0.05; MEFT /μCT:GFP:r200.93; RFP:r200.90 ;均P <0.05)。另外,体内MEFT数据与离体冷冻切片成像结果高度相关且一致(GFP:r200.96; RFP:r200.99;两者P <0.05)。相比之下,EPRI显着高估了肿瘤体积(P <0.05),尽管与US和μCT有显着相关性(EPRI / US:GFP:r200.95; RFP:r200.94;两者均P <0.05; EPRI /μCTGFP :r200.86; RFP:r200.86;均P <0.05)。结论使用MEFT进行荧光分布重建可提供高度精确的三维(3D)肿瘤体积数据,与EPRI相比,其准确性更高。因此,MEFT是一种非常适合用于以高空间分辨率定量评估浅表肿瘤中荧光分布的技术。关键点 ?介观落射荧光层析成像(MEFT)是一种重要的新分子成像技术。 ? MEFT可以高分辨率准确确定浅表肿瘤的大小。 ? MEFT是用于纵向评估肿瘤生长的合适技术。 ? MEFT允许3D重建和荧光分布的量化。

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