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制备具有不同亲脂性的四齿/单齿配位的99mTc(III)配合物以及适配188Re类似物的新方法。

Novel procedures for preparing 99mTc(III) complexes with tetradentate/monodentate coordination of varying lipophilicity and adaptation to 188Re analogues.

作者信息

Seifert S, Künstler J-U, Schiller E, Pietzsch H-J, Pawelke B, Bergmann R, Spies H

机构信息

Forschungszentrum Rossendorf, Institut für Bioanorganische und Radiopharmazeutische Chemie, PF 510 119, D-01314 Dresden, Germany.

出版信息

Bioconjug Chem. 2004 Jul-Aug;15(4):856-63. doi: 10.1021/bc0300798.

Abstract

Improved methods are presented for the preparation of 99mTc and 188Re mixed-ligand complexes with tetradentate and monodentate ligands of the general formula [MIII(Lm)(Ln)] (M = Tc, Re; Lm = NS3 or NS3COOH; Ln = isocyanide or phosphine). To avoid the undesired formation of reduced-hydrolyzed species of both metals, the preparation of complexes is performed in a two-step procedure. At first the Tc(III)- or Re(III)-EDTA complex is formed which reacts in a second step with the tripodal ligand 2,2',2' '-nitrilotris(ethanethiol) (NS3) or its carboxyl derivative NS3COOH (a) and the monodentate phosphine ligands (triphenylphosphine L1, dimethylphenylphosphine L2) or isocyanides (tert-butyl isonitrile L3, methoxyisobutyl isonitrile L4, 4-isocyanomethylbenzoic acid-L-arginine L5, 4-isocyanomethylbenzoic acid-L-arginyl-L-arginine L6, 4-isocyanomethylbenzoic acid-neurotensin(8-13) L7) to the so-called '4+1' complex. Copper(I) isocyanide complexes are used for preparing the '4+1' complexes. That facilitates storage stability and allows kit formulations, and, moreover, enables the formation of 188Re complexes in acidic solution. Only micromolar amounts of the monodentate ligand are needed, and that results in high specific activity labeling of interesting molecules. The lipophilicity of complexes can be controlled by introducing a carboxyl group into the tetradentate ligand and/or derivatization of the monodentate ligands. Furthermore, the carboxyl group enables the conjugation of biomolecules. As an example, the neurotensin derivative CN-NT(8-13) was prepared and labeled with 99mTc according to the '4+1' approach, and its behavior in vivo was studied.

摘要

本文介绍了制备通式为[MIII(Lm)(Ln)](M = Tc、Re;Lm = NS3或NS3COOH;Ln = 异腈或膦)的99mTc和188Re混合配体配合物的改进方法。为避免两种金属形成不需要的还原水解产物,配合物的制备采用两步法。首先形成Tc(III)-或Re(III)-EDTA配合物,其在第二步中与三脚架配体2,2',2''-次氮基三(乙硫醇)(NS3)或其羧基衍生物NS3COOH(a)以及单齿膦配体(三苯基膦L1、二甲基苯基膦L2)或异腈(叔丁基异腈L3、甲氧基异丁基异腈L4、4-异氰基甲基苯甲酸-L-精氨酸L5、4-异氰基甲基苯甲酸-L-精氨酰-L-精氨酸L6、4-异氰基甲基苯甲酸-神经降压素(8 - 13) L7)反应生成所谓的“4 + 1”配合物。铜(I)异腈配合物用于制备“4 + 1”配合物。这有利于储存稳定性并允许试剂盒配方,而且能够在酸性溶液中形成188Re配合物。仅需要微摩尔量的单齿配体,这导致对感兴趣分子的高比活度标记。通过将羧基引入四齿配体和/或单齿配体的衍生化可以控制配合物的亲脂性。此外,羧基能够实现生物分子的缀合。例如,制备了神经降压素衍生物CN-NT(8 - 13)并根据“4 + 1”方法用99mTc进行标记,并研究了其体内行为。

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