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本文引用的文献

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Determination of optimal rhodamine fluorophore for in vivo optical imaging.用于体内光学成像的最佳罗丹明荧光团的测定。
Bioconjug Chem. 2008 Aug;19(8):1735-42. doi: 10.1021/bc800140c. Epub 2008 Jul 9.
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Imaging in the era of molecular oncology.分子肿瘤学时代的影像学
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In vivo molecular imaging to diagnose and subtype tumors through receptor-targeted optically labeled monoclonal antibodies.通过受体靶向光学标记单克隆抗体进行体内分子成像以诊断肿瘤并对其进行亚型分类。
Neoplasia. 2007 Dec;9(12):1021-9. doi: 10.1593/neo.07787.
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D-galactose receptor-targeted in vivo spectral fluorescence imaging of peritoneal metastasis using galactosamin-conjugated serum albumin-rhodamine green.使用半乳糖胺偶联血清白蛋白-罗丹明绿对腹膜转移进行D-半乳糖受体靶向的体内光谱荧光成像。
J Biomed Opt. 2007 Sep-Oct;12(5):051501. doi: 10.1117/1.2779351.
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Targeted optical fluorescence imaging of human ovarian adenocarcinoma using a galactosyl serum albumin-conjugated fluorophore.使用半乳糖基血清白蛋白偶联荧光团对人卵巢腺癌进行靶向光学荧光成像。
Cancer Sci. 2007 Nov;98(11):1727-33. doi: 10.1111/j.1349-7006.2007.00602.x. Epub 2007 Sep 2.
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Whole-body subcellular multicolor imaging of tumor-host interaction and drug response in real time.肿瘤-宿主相互作用及药物反应的全身亚细胞多色实时成像
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Spectral fluorescence molecular imaging of lung metastases targeting HER2/neu.靶向HER2/neu的肺转移灶的光谱荧光分子成像
Clin Cancer Res. 2007 May 15;13(10):2936-45. doi: 10.1158/1078-0432.CCR-06-2240.
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A target cell-specific activatable fluorescence probe for in vivo molecular imaging of cancer based on a self-quenched avidin-rhodamine conjugate.一种基于自猝灭抗生物素蛋白-罗丹明共轭物的用于癌症体内分子成像的靶细胞特异性可激活荧光探针。
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Image-guided oncologic surgery using invisible light: completed pre-clinical development for sentinel lymph node mapping.使用不可见光的图像引导肿瘤手术:前哨淋巴结 mapping 的临床前开发已完成。
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弥漫性腹膜卵巢癌模型中的多靶点多色体内光学成像

Multi-targeted multi-color in vivo optical imaging in a model of disseminated peritoneal ovarian cancer.

作者信息

Kosaka Nobuyuki, Ogawa Mikako, Longmire Michelle R, Choyke Peter L, Kobayashi Hisataka

机构信息

National Institutes of Health, National Cancer Institute, Center for Cancer Research, Molecular Imaging Program, 10 Center Drive, Bethesda, Maryland 20892-1088, USA.

出版信息

J Biomed Opt. 2009 Jan-Feb;14(1):014023. doi: 10.1117/1.3083449.

DOI:10.1117/1.3083449
PMID:19256711
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2788995/
Abstract

Commonly used in flow cytometry, multiplexed optical probes can diagnose multiple types of cell surface marker, potentially leading to improved diagnosis accuracy in vivo. Herein, we demonstrate the targeting of two different tumor markers in models of disseminated ovarian cancer. Two ovarian cancer cell lines (SKOV3 and SHIN3) were employed; both overexpress D-galactose receptor (D-galR), but only SKOV3 overexpresses HER2/neu. Additionally, fusion tumors composed of SKOV3 and SHIN3/RFP were evaluated. Both galactosyl serum albumin-rhodamine green (GSA-RhodG), which binds D-galR, and trastuzumab-Alexa680, which binds HER2/neu, were administered to tumor-bearing mice for in vivo fluorescence imaging and in situ fluorescence microscopy. In vivo fluorescence imaging depicted 64 of 69 SKOV3 tumors (94.2%) based on their dual spectra corresponding to both RhodG and Alexa680, while all 71 SHIN3 tumors (100%) were detected based on their single spectrum corresponding only to RhodG. All 59 SHIN3 and 36 SKOV3 tumors were correctly diagnosed with in situ microscopy. Additionally, in the mixed tumor model, all tumors could be depicted using the RhodG spectrum, but only SKOV3 components also showed the Alexa680 spectrum. In conclusion, multitargeted multicolor optical imaging enabled specific in vivo diagnosis of tumors expressing distinct patterns of receptors, leading to improved diagnostic accuracy.

摘要

多重光学探针常用于流式细胞术,可诊断多种类型的细胞表面标志物,有可能提高体内诊断的准确性。在此,我们在播散性卵巢癌模型中展示了对两种不同肿瘤标志物的靶向作用。使用了两种卵巢癌细胞系(SKOV3和SHIN3);两者均过度表达D-半乳糖受体(D-galR),但只有SKOV3过度表达HER2/neu。此外,还评估了由SKOV3和SHIN3/RFP组成的融合肿瘤。将与D-galR结合的半乳糖基血清白蛋白-罗丹明绿(GSA-RhodG)和与HER2/neu结合的曲妥珠单抗-Alexa680给予荷瘤小鼠,用于体内荧光成像和原位荧光显微镜检查。体内荧光成像根据对应于RhodG和Alexa680的双光谱描绘了69个SKOV3肿瘤中的64个(94.2%),而所有71个SHIN3肿瘤(100%)根据仅对应于RhodG的单光谱被检测到。通过原位显微镜检查正确诊断了所有59个SHIN3肿瘤和36个SKOV3肿瘤。此外,在混合肿瘤模型中,所有肿瘤都可以使用RhodG光谱描绘,但只有SKOV3成分也显示出Alexa680光谱。总之,多靶点多色光学成像能够对表达不同受体模式的肿瘤进行特异性体内诊断,从而提高诊断准确性。