Design, synthesis and evaluation of 18F-labeled bradykinin B1 receptor-targeting small molecules for PET imaging

被引:6
|
作者
Zhang, Zhengxing [1 ]
Kuo, Hsiou-Ting [1 ]
Lau, Joseph [1 ]
Jenni, Silvia [1 ]
Zhang, Chengcheng [1 ]
Zeisler, Jutta [1 ]
Benard, Francois [1 ,2 ]
Lin, Kuo-Shyan [1 ,2 ]
机构
[1] BC Canc Agcy, Dept Mol Oncol, 675 West 10th Ave, Vancouver, BC V5Z 1L3, Canada
[2] Univ British Columbia, Dept Radiol, 950 West 10th Ave, Vancouver, BC V5Z 4E3, Canada
基金
加拿大健康研究院;
关键词
Bradykinin B1 receptor; Antagonist; Fluorine-18; Molecular imaging; Positron emission tomography; POSITRON-EMISSION-TOMOGRAPHY; F-18-TRIFLUOROBORATE DERIVATIVES; NOREPINEPHRINE TRANSPORTER; ENANTIOMERIC RESOLUTION; KININ RECEPTORS; CELL MASS; ANTAGONISTS; CANCER; BIODISTRIBUTION; ANALOGS;
D O I
10.1016/j.bmcl.2016.06.066
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Two fluorine-18 (F-18) labeled bradykinin B1 receptor (B1R)-targeting small molecules, F-18-Z02035 and F-18-Z02165, were synthesized and evaluated for imaging with positron emission tomography (PET). Z02035 and Z02165 were derived from potent antagonists, and showed high binding affinity (0.93 +/- 0.44 and 2.80 +/- 0.50 nM, respectively) to B1R. F-18-Z02035 and F-18-Z02165 were prepared by coupling 2-[F-18] fluoroethyl tosylate with their respective precursors, and were obtained in 10 +/- 5 (n = 4) and 22 +/- 14% (n = 3), respectively, decay-corrected radiochemical yield with >99% radiochemical purity. F-18-Z02035 and F-18- Z02165 exhibited moderate lipophilicity (LogD(7.4) = 1.10 and 0.59, respectively), and were stable in mouse plasma. PET imaging and biodistribution studies in mice showed that both tracers enabled visualization of the B1R-positive HEK293T::hB1R tumor xenografts with better contrast than control B1R-negative HEK293T tumors. Our data indicate that small molecule antagonists can be used as pharmacophores for the design of B1R-targeting PET tracers. (C) 2016 Elsevier Ltd. All rights reserved.
引用
收藏
页码:4095 / 4100
页数:6
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