Division of Diagnostic Oncology, The Netherlands Cancer Institute Antoni van Leeuwenhoek Hospital, 1066 CX Amsterdam, The Netherlands.
Mol Pharm. 2011 Dec 5;8(6):2444-53. doi: 10.1021/mp200401p. Epub 2011 Nov 15.
The chemokine receptor 4 (CXCR4), which is overexpressed in many types of cancer, is an emerging target in the field of molecular imaging and therapeutics. The CXCR4 binding of several peptides, including the cyclic Ac-TZ14011, has already been validated. In this study mono-, di- and tetrameric Ac-TZ14011-containing dendrimers were prepared and functionalized with a multimodal (hybrid) label, consisting of a Cy5.5-like fluorophore and a DTPA chelate. Confocal microscopy revealed that all three dendrimers were membrane bound at 4 °C, consistent with CXCR4 binding in vitro. The unlabeled dimer and tetramer had a somewhat lower affinity for CXCR4 than the unlabeled monomer. However, when labeled with the multimodal label the CXCR4 affinity of the dimer and tetramer was considerably higher compared to that of the labeled monomer. On top of that, biodistribution studies revealed that the additional peptides in the dimer and tetramer reduced nonspecific muscle uptake. Thus, multimerization of the cyclic Ac-TZ14011 peptide reduces the negative influence of the multimodal label on the receptor affinity and the biodistribution.
趋化因子受体 4(CXCR4)在许多类型的癌症中过表达,是分子成像和治疗领域的一个新兴靶点。已经验证了几种包括环 Ac-TZ14011 的肽与 CXCR4 的结合。在这项研究中,制备了含有单、二聚体和四聚体 Ac-TZ14011 的树枝状聚合物,并与一种多模态(杂合)标记物功能化,该标记物由一个 Cy5.5 样荧光团和一个 DTPA 螯合物组成。共焦显微镜显示,所有三种树枝状聚合物在 4°C 时都与细胞膜结合,与体外的 CXCR4 结合一致。未标记的二聚体和四聚体对 CXCR4 的亲和力比未标记的单体略低。然而,当用多模态标记物标记时,二聚体和四聚体与标记单体相比,对 CXCR4 的亲和力要高得多。除此之外,生物分布研究表明,二聚体和四聚体中的额外肽减少了非特异性肌肉摄取。因此,环 Ac-TZ14011 肽的多聚化降低了多模态标记物对受体亲和力和生物分布的负面影响。
