64Cu-Labeled Somatostatin Analogues Conjugated with Cross-Bridged Phosphonate-Based Chelators via Strain-Promoted Click Chemistry for PET Imaging: In silico through in Vivo Studies

被引:33
作者
Cai, Zhengxin [1 ]
Ouyang, Qin [2 ]
Zeng, Dexing [1 ]
Nguyen, Kim N. [6 ]
Modi, Jalpa [1 ]
Wang, Lirong [2 ]
White, Alexander G. [1 ]
Rogers, Buck E. [6 ]
Xie, Xiang-Qun [2 ,3 ]
Anderson, Carolyn J. [1 ,4 ,5 ]
机构
[1] Univ Pittsburgh, Dept Radiol, Computat Chem Genom Screening Ctr, Sch Pharm, Pittsburgh, PA 15219 USA
[2] Univ Pittsburgh, Dept Pharmaceut Sci, Computat Chem Genom Screening Ctr, Sch Pharm, Pittsburgh, PA 15219 USA
[3] Univ Pittsburgh, Drug Discovery Inst, Pittsburgh, PA 15219 USA
[4] Univ Pittsburgh, Dept Pharmacol & Chem Biol, Pittsburgh, PA 15219 USA
[5] Univ Pittsburgh, Dept Bioengn, Pittsburgh, PA 15219 USA
[6] Washington Univ, Dept Radiat Oncol, St Louis, MO 63130 USA
关键词
COPPER-FREE; BIOLOGICAL EVALUATION; CU-64; NANOPARTICLES; SELECTIVITY; INHIBITION; ANTAGONIST; EXPRESSION; RECEPTORS; CARCINOMA;
D O I
10.1021/jm500416f
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Somatostatin receptor subtype 2 (sstr2) is a G-protein-coupled receptor (GPCR) that is overexpressed in neuroendocrine tumors. The homology model of sstr2 was built and was used to aid the design of new somatostatin analogues modified with phosphonate-containing cross-bridged chelators for evaluation of using them as PET imaging radiopharmaceuticals. The new generation chelators were conjugated to Tyr(3)-octreotate (Y3-TATE) through bioorthogonal, strain-promoted alkyne azide cycloaddition (SPAAC) to form CB-TE1A1P-DBCO-Y3-TATE (AP) and CB-TE1K1P-PEG4-DBCO-Y3-TATE (KP) in improved yields compared to standard direct conjugation methods of amide bond formation. Consistent with docking studies, the clicked bioconjugates showed high binding affinities to sstr2, with K-d values ranging from 0.6 to 2.3 nM. Selected isomers of the clicked products were used in biodistribution and PET/CT imaging. Introduction of the bulky dibenzocyclooctyne group in AP decreased clearance rates from circulation. However, the additional carboxylate group and PEG linker from the KP conjugate significantly improved labeling conditions and in vivo stability of the copper complex and ameliorated the slower pharmacokinetics of the clicked somatostatin analogues.
引用
收藏
页码:6019 / 6029
页数:11
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