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Invivo fluorescence imaging for cancer diagnosis using receptor-targeted epidermal growth factor-based nanoprobe

机译:使用基于受体的表皮生长因子为基础的纳米探针的体内荧光成像诊断癌症

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Receptor-targeted imaging is emerging as a promising strategy for diagnosis of human cancer. Herein, we developed an epidermal growth factor-based nanoprobe (EGF-NP) for invivo optical imaging of epidermal growth factor receptor (EGFR), an important target for cancer imaging. The self-quenched EGF-NP is fabricated by sequentially conjugating a near-infrared (NIR) fluorophore (Cy5.5) and a quencher (BHQ-3) to EGF, a low-molecular weight polypeptide (6.2kDa), compared to EGFR antibody (150kDa). The self-quenched EGF-NP presented great specificity to EGFR, and rapidly internalized into the cells, as monitored by time-lapse imaging. Importantly, the self-quenched EGF-NP boosted strong fluorescence signals upon EGFR-targeted uptake into EGFR-expressing cells, followed by lysosomal degradation, as confirmed by lysosomal marker cell imaging. Consistent with cellular results, intravenous injection of EGF-NP into tumor-bearing mice induced strong NIR fluorescence intensity in the target tumor tissue with high specificity against EGFR-expressing cancer cells. Signal accumulation of EGF-NP in tumor was much faster than that of EGFR monoclonal antibody (Cetuximab)-Cy5.5 conjugates due to the rapid clearance from the body and tissue permeability of low-molecular weight EGF. This self-quenched, EGF-based imaging probe can be applied for diagnosis of various cancers.
机译:受体靶向成像正在成为诊断人类癌症的有前途的策略。本文中,我们开发了一种基于表皮生长因子的纳米探针(EGF-NP),用于对表皮生长因子受体(EGFR)进行体内光学成像,这是癌症成像的重要目标。通过将近红外(NIR)荧光团(Cy5.5)和猝灭剂(BHQ-3)与EGFR相比低分子量多肽(6.2kDa)依次缀合来制备自淬灭EGF-NP抗体(150kDa)。通过延时成像监测,自淬灭的EGF-NP对EGFR表现出极大的特异性,并迅速内化到细胞中。重要的是,如通过溶酶体标记细胞成像所证实的,当EGFR靶向摄取进入EGFR表达细胞后,自淬灭的EGF-NP增强了强荧光信号。与细胞结果一致,向荷瘤小鼠静脉内注射EGF-NP在靶肿瘤组织中诱导了强烈的NIR荧光强度,对表达EGFR的癌细胞具有高度特异性。 EGF-NP在肿瘤中的信号蓄积比EGFR单克隆抗体(Cetuximab)-Cy5.5缀合物快得多,这是由于低分子量EGF从体内的快速清除和组织通透性所致。这种基于EGF的自淬灭成像探针可用于诊断各种癌症。

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