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肿瘤与血管生成中氨肽酶 N 的分子影像学研究

Molecular Imaging of Aminopeptidase N in Cancer and Angiogenesis.

机构信息

Department of Chemistry and Biochemistry, University of Notre Dame, 236 Nieuwland Science Hall, Notre Dame, IN 46556, USA.

出版信息

Contrast Media Mol Imaging. 2018 Jun 25;2018:5315172. doi: 10.1155/2018/5315172. eCollection 2018.

Abstract

This review focuses on recent advances in the molecular imaging of aminopeptidase N (APN, also known as CD13), a zinc metalloenzyme that cleaves -terminal neutral amino acids. It is overexpressed in multiple cancer types and also on the surface of vasculature undergoing angiogenesis, making it a promising target for molecular imaging and targeted therapy. Molecular imaging probes for APN are divided into two large subgroups: reactive and nonreactive. The structures of the reactive probes (substrates) contain a reporter group that is cleaved and released by the APN enzyme. The nonreactive probes are not cleaved by the enzyme and contain an antibody, peptide, or nonpeptide for targeting the enzyme exterior or active site. Multivalent homotopic probes utilize multiple copies of the same targeting unit, whereas multivalent heterotopic molecular probes are equipped with different targeting units for different receptors. Several recent preclinical cancer imaging studies have shown that multivalent APN probes exhibit enhanced tumor specificity and accumulation compared to monovalent analogues. The few studies that have evaluated APN-specific probes for imaging angiogenesis have focused on cardiac regeneration. These promising results suggest that APN imaging can be expanded to detect and monitor other diseases that are associated with angiogenesis.

摘要

这篇综述重点介绍了天冬氨酰蛋白酶 N(APN,也称为 CD13)的分子成像的最新进展,APN 是一种锌金属酶,可切割 -末端中性氨基酸。它在多种癌症类型中过度表达,也存在于血管生成过程中的血管表面,使其成为分子成像和靶向治疗的有前途的靶标。APN 的分子成像探针分为两大类:反应性和非反应性。反应性探针(底物)的结构包含一个报告基团,该基团被 APN 酶切割并释放。非反应性探针不会被酶切割,并且包含抗体、肽或非肽,用于靶向酶的外部或活性部位。多价同型探针利用相同靶向单元的多个副本,而多价异型分子探针则配备有用于不同受体的不同靶向单元。最近的几项临床前癌症成像研究表明,与单价类似物相比,多价 APN 探针表现出增强的肿瘤特异性和积累。少数评估用于血管生成成像的 APN 特异性探针的研究集中在心脏再生上。这些有希望的结果表明,APN 成像可以扩展到检测和监测与血管生成相关的其他疾病。

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