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Molecular Scaffolds as Double-Targeting Agents For the Diagnosis and Treatment of Neuroblastoma

机译:作为双靶向剂的分子支架,用于诊断和治疗神经母细胞瘤

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摘要

The selective delivery of therapeutic and imaging agents to tumoral cells has been postulated as one of the most important challenges in the nanomedicine field. Meta-iodobenzilguanidine (MIBG) is widely used for the diagnosis of neuroblastoma (NB) due to its strong affinity for the norepinephrine transporter (NET), usually overexpressed on the membrane of malignant cells. Herein, a family of novel Y-shaped scaffolds has been synthesized, which have structural analogues of MIBG covalently attached at each end of the Y-structure. The cellular uptake capacity of these double-targeting ligands has been evaluated in vitro and in vivo, yielding one specific Y-shaped structure that is able to be engulfed by the malignant cells, and accumulates in the tumoral tissue, at significantly higher levels than the structure containing only one single targeting agent. This Y-shaped ligand can provide a powerful tool for the current treatment and diagnosis of this disease.
机译:治疗剂和成像剂对肿瘤细胞的选择性递送已被假定为纳米美床领域中最重要的挑战之一。 Meta-Iodobenzilguanidine(MIBG)广泛用于诊断神经母细胞瘤(NB)由于其对去甲肾上腺素转运蛋白转运蛋白(净)的强亲和力,通常在恶性细胞膜上过表达。 在此,已经合成了一种新型Y形支架的家族,其具有在Y结构的每个端部共价连接的MIBG的结构类似物。 已经在体外和体内评估了这些双靶向配体的细胞摄取能力,得到一种能够被恶性细胞吞噬的一种特异性Y形结构,并在肿瘤组织中积聚,比水平明显高于 仅含有一个靶向剂的结构。 这种Y形配体可以为目前的治疗和诊断提供强大的工具。

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