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ICF01012新型喹喔啉衍生物作为黑色素瘤靶向探针的合成及生物学评价

Synthesis and Biological Evaluation of New Quinoxaline Derivatives of ICF01012 as Melanoma-Targeting Probes.

作者信息

El Aissi Radhia, Liu Jianrong, Besse Sophie, Canitrot Damien, Chavignon Olivier, Chezal Jean-Michel, Miot-Noirault Elisabeth, Moreau Emmanuel

机构信息

INSERM-Université d'Auvergne , UMR 990, IMTV, BP 184, F-63005 Clermont-Ferrand Cedex, France ; Clermont Université , Université d'Auvergne, Imagerie Moléculaire et Thérapie Vectorisée, BP 10448, F-63005 Clermont-Ferrand Cedex, France.

出版信息

ACS Med Chem Lett. 2014 Feb 20;5(5):468-73. doi: 10.1021/ml400468x. eCollection 2014 May 8.

Abstract

The aim of this study was the synthesis and pharmacokinetic selection of a best melanin-targeting ligand for addressing anticancer agents to pigmented melanoma. Seven quinoxaline carboxamide derivatives were synthesized and radiolabeled with iodine-125. Biodistribution studies of compounds [ (125) I]1a-g performed in melanoma-bearing mice tumor showed significant tumor uptake (range 2.43-5.68%ID/g) within 1 h after i.v. injection. Fast clearance of the radioactivity from the nontarget organs mainly via the urinary system gave high tumor-to-blood and tumor-to-muscle ratios. Given its favorable clearance and high tumor-melanoma uptake at 72 h, amide 1d was the most promising melanoma-targeting ligand in this series. Compound 1d will be used as building block for the design of new melanoma-selective drug delivery systems.

摘要

本研究的目的是合成并进行药代动力学筛选,以找到一种最佳的黑色素靶向配体,用于将抗癌药物递送至色素性黑色素瘤。合成了七种喹喔啉甲酰胺衍生物并用碘 - 125进行放射性标记。在荷黑色素瘤小鼠肿瘤中对化合物[(125)I]1a - g进行的生物分布研究表明,静脉注射后1小时内肿瘤摄取显著(范围为2.43 - 5.68%ID/g)。放射性主要通过泌尿系统从非靶器官快速清除,从而产生高的肿瘤与血液以及肿瘤与肌肉的比率。鉴于其在72小时时具有良好的清除率和高的肿瘤 - 黑色素瘤摄取率,酰胺1d是该系列中最有前景的黑色素靶向配体。化合物1d将用作设计新型黑色素瘤选择性药物递送系统的基础材料。

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