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首页> 外文期刊>Journal of Labelled Compounds and Radiopharmaceuticals >The development of PET radioligands for imaging the translocator protein (18 kDa): What have we learned?
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The development of PET radioligands for imaging the translocator protein (18 kDa): What have we learned?

机译:宠物放射性配偶的开发用于成像译者蛋白(18 kDa):我们学到了什么?

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摘要

The translocator protein (TSPO; 18 kDa), formerly known as the peripheral benzodiazepine receptor (PBR), is minimally expressed in the healthy brain. On the other hand, increased levels of TSPO have been noted in brain disorders for which an immune response is elicited. This increase in TSPO expression has been reported to coincide with the process of microglial activation making the measurement of TSPO density a useful indicator of active brain disease. To this end several new classes of TSPO positron emission tomography radioligands have been developed and evaluated. However, the incomplete pharmacological characterization of the TSPO and its ligands as well as differences in pathophysiology, pharmacology and molecular nature across species and tissue types means that caution must be exercised when comparing data obtained with various TSPO radioligands. A re-evaluation of our interpretation of imaging data, which better correlates with our current understanding of TSPO pharmacology in disease, requires consideration.
机译:以前称为外周苯二氮卓受体(PBR)以前称为外周苯二氮卓受体(PBR)的译者蛋白质(Tspo; 18 kda)在健康的脑中表达。另一方面,已在引起免疫应答的脑疾病中,注意到TSPO水平增加。据报道,TSPO表达的这种增加与微胶质激活的过程一致,使得测量TSPO密度是活性脑疾病的有用指标。为此,已经开发并评估了几个新的TSPO正电子发射断层摄影射线植树积射线。然而,TSPO及其配体的不完全药理表征以及物种和组织类型的病理生理学,药理和分子性质的差异是指在比较用各种TSPO放射性配体获得的数据时必须注意。重新评估我们对成像数据的解释,与我们目前对疾病中TSPO药理学的理解更好地相关,需要考虑。

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