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Synthesis and Biological Evaluation of Substrate-Based Imaging Agents for the Prostate-Specific Membrane Antigen

机译:前列腺特异性膜抗原的基于底物的成像剂的合成和生物学评估

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摘要

Prostate-specific membrane antigen (PSMA) is an attractive target for the imaging of prostate Cancer (PCa) due to the elevated expression on the surface of prostate tumor cells. Most PSMA-targeted low molecular weight imaging agents are inhibitors of PSMA. We have synthesized a series of substrate-based PSMA-targeted imaging agents by mimicking poly-γ-glutamyl folic acid, an endogenous substrate of PSMA. In vitro the γ-linked polyglutamate conjugates proved to be better substrates than the corresponding α-linked glutamates. However, in vivo imaging studies of γ-ray-emitting and γ-linked glutamates did not demonstrate selective uptake in PSMA-pos-itive over PSMA-negative tumors. Subsequent chromatographic studies and in silico molecular dynamics simulations indicated that hydrolysis of the substrates is slow and access to the enzymatic active site is limited. These results inform the design of future substrate-based imaging agents for PSMA.
机译:前列腺特异性膜抗原(PSMA)由于在前列腺肿瘤细胞表面的表达升高而成为前列腺癌(PCa)成像的有吸引力的靶标。大多数靶向PSMA的低分子量成像剂都是PSMA抑制剂。我们已经通过模仿聚-γ-谷氨酰叶酸(PSMA的内源性底物)合成了一系列基于底物的PSMA靶向成像剂。在体外,γ-连接的聚谷氨酸缀合物被证明是比相应的α-连接的谷氨酸盐更好的底物。但是,体内对γ射线发射和γ-连接的谷氨酸的成像研究并未显示出PSMA阳性肿瘤对PSMA阴性肿瘤有选择性摄取。随后的色谱研究和计算机分子动力学模拟表明,底物的水解缓慢,并且限制了对酶活性位点的访问。这些结果为未来基于PSMA的基于基质的成像剂的设计提供了依据。

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