R&D Department, Philochem AG, CH-8112 Otelfingen, Switzerland.
Department of Physics, University of Cagliari, Cagliari I-09042, Monserrato, Italy.
J Med Chem. 2024 Aug 8;67(15):13392-13408. doi: 10.1021/acs.jmedchem.4c01295. Epub 2024 Jul 30.
Fibroblast activation protein (FAP) is a protein biomarker widely expressed in most solid human malignancies of epithelial origin. In recent years, a number of FAP-targeted small organic radioligands, including OncoFAP, have been utilized in the clinic for the detection and diagnosis of cancer. Despite their selective accumulation, conventional FAP ligands present a relatively short half-life in tumors, corresponding to a few hours after systemic administration. In order to maximize their efficacy, FAP-targeted radioligand therapeutics must possess prolonged tumor retention, thus irradiating tumor cells for days. In this work, we describe the development of compact OncoFAP multimers with improved FAP affinity (low picomolar ICs), aimed at increasing tumor-residence time for therapeutic applications. An analysis of the interaction of the multimers with FAP revealed a wide and deep pocket and six additional secondary binding sites. TriOncoFAP-DOTAGA emerged for its favorable profile and superior biodistribution performance in tumor-bearing mice.
成纤维细胞激活蛋白(FAP)是一种在大多数上皮来源的实体人类恶性肿瘤中广泛表达的蛋白生物标志物。近年来,许多 FAP 靶向的小分子放射性配体,包括 OncoFAP,已被用于临床癌症的检测和诊断。尽管它们具有选择性的积累,但传统的 FAP 配体在肿瘤中的半衰期相对较短,在全身给药后几个小时内。为了最大限度地提高它们的疗效,FAP 靶向放射性配体疗法必须具有延长的肿瘤保留时间,从而对肿瘤细胞进行数天的照射。在这项工作中,我们描述了具有改进的 FAP 亲和力(低皮摩尔 ICs)的紧凑型 OncoFAP 多聚体的开发,旨在增加肿瘤的滞留时间以用于治疗应用。对多聚体与 FAP 的相互作用进行了分析,揭示了一个广泛而深的口袋和六个额外的二级结合位点。TriOncoFAP-DOTAGA 因其有利的特性和在荷瘤小鼠中的优越的生物分布性能而脱颖而出。
