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首页> 外文期刊>International Journal of Cancer =: Journal International du Cancer >Fluorescence‐ and multispectral optoacoustic imaging for an optimized detection of deeply located tumors in an orthotopic mouse model of pancreatic carcinoma
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Fluorescence‐ and multispectral optoacoustic imaging for an optimized detection of deeply located tumors in an orthotopic mouse model of pancreatic carcinoma

机译:荧光和多光谱光声成像,用于胰腺癌原位小鼠模型中深受肿瘤的优化检测

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A crucial point for the management of pancreatic ductal adenocarcinoma (PDAC) is the decrease of R1 resections. Our aim was to evaluate the combination of multispectral optoacoustic tomography (MSOT) with fluorescence guided surgery (FGS) for diagnosis and perioperative detection of tumor nodules and resection margins in a xenotransplant mouse model of human pancreatic cancer. The peptide cRGD, conjugated with the near infrared fluorescent (NIRF) dye IRDye800CW and with a trans ‐cyclooctene (TCO) tag for future click chemistry (cRGD‐800CW‐TCO), was applied to PDAC bearing immunodeficient nude mice; 27 days after orthotopic transplantation of human AsPC‐1 cells into the head of the pancreas, mice were injected with cRGD‐800CW‐TCO and imaged with fluorescence‐ and optoacoustic devices before and 2, 6 and 24 hr after injection, before they were sacrificed and dissected with a guidance of FGS imaging system. Fluorescence imaging of cRGD‐800CW‐TCO allowed detection of the tumor area but without information about the depth, whereas MSOT allowed high resolution 3 D identification of the tumor area, in particular of small tumor nodules. Highly sensitive delineation of tumor burden was achieved during FGS in all mice. Imaging of whole‐mouse cryosections, histopathological analysis and NIRF microscopy confirmed the localization of cRGD‐800CW‐TCO within the tumor tissue. In principle, all imaging modalities applied here were able to detect PDAC in vivo . However, the combination of MSOT and FGS provided detailed spatial information of the signal and achieved a complete overview of the distribution and localization of cRGD‐800CW‐TCO within the tumor before and during surgical intervention.
机译:胰腺导管腺癌(PDAC)管理的关键点是R1切除的降低。我们的目的是评估多光谱光声断层摄影(MSOT)与荧光引导手术(FGS)的组合,用于诊断和围手术期检测人胰腺癌的异种植物小鼠模型中的肿瘤结节和切除乳头。将肽CRGD与近红外荧光(NIRF)染料IRDYE800CW和反式环偶联(TCO)标签缀合,用于将来咔哒化化学(CRGD-800CW-TCO)应用于PDAC轴承免疫缺陷裸鼠;在原位移植到胰腺头部后27天后,用CRGD-800CW-TCO注射小鼠并用荧光 - 和光声器件进行成像,然后注射后2,6和24小时,在处死之前并解剖FGS成像系统的指导。 CRGD-800CW-TCO的荧光成像允许检测肿瘤区域但没有关于深度的信息,而MSOT允许高分辨率3d鉴定肿瘤区域,特别是小肿瘤结节。在所有小鼠的FGS期间,在FGS期间实现了高度敏感的肿瘤负担。全小鼠冷冻乳糖的成像,组织病理学分析和NIRF显微镜证实CRGD-800CW-TCO的定位在肿瘤组织内。原则上,这里应用的所有成像模式都能够在体内检测PDAC。然而,MSOT和FGS的组合提供了该信号的详细空间信息,并在手术干预之前和期间达到了CRGD-800CW-TCO的分布和定位的完整概述。

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