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使用叶酸受体靶向的近红外荧光染料共轭物增强肿瘤检测。

Enhanced tumor detection using a folate receptor-targeted near-infrared fluorochrome conjugate.

作者信息

Moon Woo Kyung, Lin Yuhui, O'Loughlin Terence, Tang Yi, Kim Dong-Eog, Weissleder Ralph, Tung Ching-Hsuan

机构信息

Center for Molecular Imaging Research,Massachusetts General Hospital, Harvard Medical School, Charlestown, Massachusetts 02129, USA.

出版信息

Bioconjug Chem. 2003 May-Jun;14(3):539-45. doi: 10.1021/bc0340114.

DOI:10.1021/bc0340114
PMID:12757377
Abstract

Fluorescence optical imaging technologies are currently being developed to image specific molecular targets in vivo. Detection technologies range from those providing microscopic detail to whole body imaging systems with potential clinical use. A number of target-specific near-infrared imaging probes have recently been developed to image receptors, antigens, and enzymes. The goal of the current study was to evaluate a new near-infrared (NIR) folate receptor (FR)-targeted imaging probe for its ability to improve detection of FR-positive cancers. We hypothesized that modification of folate would retain receptor affinity in vivo, despite the bulkier NIR fluorochrome, NIR2 (em = 682 nm). Cellular uptake of the NIR conjugates was significantly higher in FR-positive nasopharyngeal epidermoid carcinoma, KB cells, compared to FR-negative human fibrosarcoma, HT1080 cells. When tumors were implanted in vivo, equal-sized KB tumors showed a 2.4-fold higher signal intensity compared to HT1080 tumors (24 h). The maximum signal-to-background ratio (3-fold) was observed at 24 h in KB tumor. Injection of the unmodified NIR2 fluorochrome did not result in persistent contrast increases under similar conditions. Furthermore, tumor enhancement with the NIR2-folate probe persisted over 48 h and was inhibitable in vivo by administration of unlabeled folate. These results indicate that folate-modified NIR fluorochrome conjugate can be used for improved detection of FR-positive tumors.

摘要

荧光光学成像技术目前正在开发中,用于体内特定分子靶点的成像。检测技术涵盖了从提供微观细节的技术到具有潜在临床应用价值的全身成像系统。最近已开发出许多针对特定靶点的近红外成像探针,用于受体、抗原和酶的成像。本研究的目的是评估一种新型近红外(NIR)叶酸受体(FR)靶向成像探针改善FR阳性癌症检测的能力。我们假设,尽管近红外荧光染料NIR2(发射波长=682nm)体积较大,但叶酸的修饰仍能在体内保持受体亲和力。与FR阴性的人纤维肉瘤HT1080细胞相比,FR阳性的鼻咽表皮样癌KB细胞对NIR偶联物的细胞摄取显著更高。当肿瘤植入体内时,大小相同的KB肿瘤在24小时时的信号强度比HT1080肿瘤高2.4倍。在KB肿瘤中,24小时时观察到最大信号背景比(3倍)。在类似条件下,注射未修饰的NIR2荧光染料不会导致持续的对比度增加。此外,NIR2-叶酸探针的肿瘤增强持续超过48小时,并且在体内可通过给予未标记的叶酸来抑制。这些结果表明,叶酸修饰的近红外荧光染料偶联物可用于改善FR阳性肿瘤的检测。

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