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TSPO PET 配体在神经炎症成像中的发展的基本原理和最新进展。

Essential Principles and Recent Progress in the Development of TSPO PET Ligands for Neuroinflammation Imaging.

机构信息

Department of Pharmacy, University of Salerno, 84084 Fisciano (SA), Italy.

Department of Pharmacy, University of Pisa, 56126, Pisa, Italy.

出版信息

Curr Med Chem. 2022 Aug 6;29(28):4862-4890. doi: 10.2174/0929867329666220329204054.

Abstract

The translocator protein 18kDa (TSPO) is expressed in the outer mitochondrial membrane and is implicated in several functions, including cholesterol transport and steroidogenesis. Under normal physiological conditions, TSPO is present in very low concentrations in the human brain but is markedly upregulated in response to brain injury and inflammation. This upregulation is strongly associated with activated microglia. Therefore, TSPO is particularly suited for assessing active gliosis associated with brain lesions following injury or disease. For over three decades, TSPO has been studied as a biomarker. Numerous radioligands for positron emission tomography (PET) that target TSPO have been developed for imaging inflammatory progression in the brain. Although [C]PK11195, the prototypical first-generation PET radioligand, is still widely used for in vivo studies, mainly now as its single more potent R-enantiomer, it has severe limitations, including low sensitivity and poor amenability to quantification. Second-generation radioligands are characterized by higher TSPO specific signals but suffer from other drawbacks, such as sensitivity to the TSPO single nucleotide polymorphism (SNP) rs6971. Therefore, their applications in human studies have the burden of needing to genotype subjects. Consequently, recent efforts are focused on developing improved radioligands that combine the optimal features of the second generation with the ability to overcome the differences in binding affinities across the population. This review presents essential principles in the design and development of TSPO PET ligands and discusses prominent examples among the main chemotypes.

摘要

转位蛋白 18kDa(TSPO)表达在外膜线粒体中,与多种功能相关,包括胆固醇转运和类固醇生成。在正常生理条件下,TSPO 在人脑中的含量非常低,但在脑损伤和炎症时会显著上调。这种上调与激活的小胶质细胞强烈相关。因此,TSPO 特别适合评估损伤或疾病后与脑损伤相关的活跃神经胶质增生。三十多年来,TSPO 一直被作为生物标志物进行研究。已经开发出许多针对 TSPO 的正电子发射断层扫描(PET)放射性配体,用于成像大脑中的炎症进展。尽管 [C]PK11195(第一代 PET 放射性配体的原型)仍广泛用于体内研究,主要是其单一的更有效 R-对映体,但它具有严重的局限性,包括灵敏度低和定量能力差。第二代放射性配体的特点是具有更高的 TSPO 特异性信号,但存在其他缺点,例如对 TSPO 单核苷酸多态性(SNP)rs6971 的敏感性。因此,它们在人类研究中的应用需要对受试者进行基因分型。因此,最近的努力集中在开发能够结合第二代最佳特性并克服人群中结合亲和力差异的改良放射性配体上。本文介绍了 TSPO PET 配体设计和开发的基本原则,并讨论了主要化学类型中的突出实例。

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