Synthesis, characterization and biological evaluation of In(III) complexes anchored by DOTA-like chelators bearing a quinazoline moiety

被引:17
|
作者
Garcia, Raquel [1 ]
Kubicek, Vojtech [2 ]
Drahos, Bohuslav [2 ]
Gano, Lurdes [1 ]
Santos, Isabel C. [1 ]
Campello, Paula [1 ]
Paulo, Antonio [1 ]
Toth, Eva [2 ]
Santos, Isabel [1 ]
机构
[1] Inst Tecnol & Nucl, Unidade Ciencias Quim & Radiofarmaceut, P-2686953 Sacavem, Portugal
[2] CNRS, Ctr Biophys Mol, F-45071 Orleans 2, France
关键词
GROWTH-FACTOR RECEPTOR; STRUCTURAL-CHARACTERIZATION; EGFR INHIBITORS; BIOMARKER; CANCER; AGENTS; DERIVATIVES; TC-99M; TARGET; MUTANT;
D O I
10.1039/c004797j
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Following previous studies with a DOTA-like bifunctional chelator (H(3)L1) containing an ethylenic linker between the macrocycle backbone and a quinazoline pharmacophore, we synthesized and fully characterized a congener rnacrocyclic ligand (H(3)L2) having a longer, five-carbon spacer for the linkage of the quinazoline moiety. Both H(3)L1 and H(3)L2 were used to prepare indium(III) complexes aiming at their evaluation as radioactive probes for in vivo targeting of EGFR-TK. The protonation constants (log K-Hi) of H(3)L2 were determined by potentiometry and UV-Vis spectrophotometry and the values found are 12.18, 9.74, 4.99, 3.91 and 2.53. The stability and protonation constants of InL (L = L1, L2) were also obtained from a combined potentiometry and UV-VIS spectrophotometry study. The reaction of InCl3 with H(3)L1 and H(3)L2 led to the formation of the well-defined complexes InL1 and InL2, containing In(III) ions coordinated by a seven (N-4,O-3) donor atom set. These new complexes were fully characterized by spectroscopic methods (IR, NMR, ESI-MS), HPLC and by X-ray diffraction analysis in the case of InL1. The radioactive congener (III)InL2 was prepared from the reaction of In-III-chloride with H(3)L2, in high yield and high radiochemical purity. (III)InL2 is a neutral complex that presents a hydrophilic character and exhibits a high in vitro and in vivo stability. H(3)L2 and InL2 do not inhibit the cell growth of A431 cervical carcinoma cells. In this EGFR-expressing cell line, (III)InL2 has shown very low cell internalization. These findings indicate that these DOTA-like chelators are not the best suited bifunctional ligands to obtain In(III) complexes with adequate biological properties for targeting the EGFR-TK.
引用
收藏
页码:571 / 580
页数:10
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