Imaging the Activity of Efflux Transporters at the Blood–Brain Barrier in Neurologic Diseases: Radiotracer Selection Criteria

Nicolas Tournier, Oliver Langer
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Abstract

Efflux transporters of the adenosine triphosphate–binding cassette (ABC) superfamily, such as P-glycoprotein (P-gp/ABCB1) and breast cancer resistance protein (BCRP/ABCG2), are highly expressed at the blood–brain barrier (BBB), where they contribute to maintaining brain homeostasis. P-gp may serve as an imaging biomarker to assess the contribution of BBB functionality rather than integrity to the onset or progression of various neurologic diseases. Considerable efforts have been made to develop radiolabeled P-gp substrates to assess cerebral P-gp activity with PET. However, initially developed radiotracers have limited clinical utility as they lack sensitivity to detect moderate, physiologically relevant changes in cerebral P-gp activity. Learning from this molecular imaging area has called for specific criteria, different from those classically used for other central nervous system targets, for developing and selecting suitable PET tracers to study ABC transporter activity at the BBB in different neurologic diseases.

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神经系统疾病的血脑屏障外排转运蛋白活性成像:放射性示踪剂选择标准
三磷酸腺苷结合盒(ABC)超家族的外排转运蛋白,如p -糖蛋白(P-gp/ABCB1)和乳腺癌抵抗蛋白(BCRP/ABCG2),在血脑屏障(BBB)高度表达,在那里它们有助于维持大脑稳态。P-gp可以作为一种成像生物标志物来评估血脑屏障的功能,而不是完整性对各种神经疾病的发生或进展的贡献。大量的努力已经被用于开发放射性标记的P-gp底物,以PET评估脑P-gp活性。然而,最初开发的放射性示踪剂的临床应用有限,因为它们缺乏检测大脑P-gp活性中度生理相关变化的敏感性。从这一分子成像领域的学习需要特定的标准,不同于传统上用于其他中枢神经系统靶点的标准,以开发和选择合适的PET示踪剂来研究不同神经系统疾病中血脑屏障处ABC转运蛋白的活性。
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