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Peptidyl Molecular Imaging Contrast Agents Using a New Solid Phase Peptide Synthesis Approach

机译:使用新型固相肽合成方法的肽基分子成像造影剂

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摘要

A versatile method is disclosed for solid phase peptide synthesis (SPPS) of molecular imaging contrast agents. A DO3A moiety was derivatized to introduce a CBZ-protected amino group and then coupled to a polymeric support. CBZ cleavage with Et2AlCl/thioanisole was optimized for SPPS. Amino acids were then coupled to the aminoDOTA loaded resin using conventional step-wise Fmoc SPPS to create a product with DOTA coupled to the C-terminus of the peptide. In a second study, the DO3A moiety was coupled to a glycine-loaded polymeric support, and amino acids were then coupled to the amino-DOTA-peptide loaded resin using SPPS, to incorporate DOTA within the peptide sequence. The peptide-(Tm3+-DOTA) amide showed a PARAmagnetic Chemical Exchange Saturation Transfer (PARACEST) effect, which demonstrated the utility of this contrast agent for molecular imaging. These results demonstrate the advantages of exploiting SPPS methodologies through the development of unique DOTA derivatives to create peptide-based molecular imaging contrast agents.
机译:公开了一种用于分子成像造影剂的固相肽合成(SPPS)的通用方法。将DO3A部分衍生化以引入CBZ保护的氨基,然后偶联到聚合物载体上。用Et2AlCl /硫代苯甲醚裂解CBZ已针对SPPS进行了优化。然后使用常规的逐步Fmoc SPPS将氨基酸偶联至负载有氨基DOTA的树脂,以生成具有DOTA偶联至肽C端的产物。在第二项研究中,DO3A部分与甘氨酸负载的聚合物支持物偶联,然后使用SPPS将氨基酸与氨基DOTA肽负载的树脂偶联,以将DOTA掺入肽序列中。肽-(Tm 3 + -DOTA)酰胺表现出PARA磁性化学交换饱和转移(PARACEST)效应,证明该造影剂可用于分子成像。这些结果证明了通过开发独特的DOTA衍生物来开发基于肽的分子成像造影剂来开发SPPS方法的优势。

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