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18FGE-180 PET Detects Reduced Microglia Activation After LM11A-31 Therapy in a Mouse Model of Alzheimers Disease

机译:18F GE-180 PET在阿尔茨海默氏病小鼠模型中检测到LM11A-31治疗后小胶质细胞活化降低

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摘要

Microglial activation is a key pathological feature of Alzheimer's disease (AD). PET imaging of translocator protein 18 kDa (TSPO) is a strategy to detect microglial activation in vivo. Here we assessed flutriciclamide ([18F]GE-180), a new second-generation TSPO-PET radiotracer, for its ability to monitor response to LM11A-31, a novel AD therapeutic in clinical trials. AD mice displaying pathology were treated orally with LM11A-31 for 3 months. Subsequent [18F]GE-180-PET imaging revealed significantly lower signal in cortex and hippocampus of LM11A-31-treated AD mice compared to those treated with vehicle, corresponding with decreased levels of TSPO immunostaining and microglial Iba1 immunostaining. In addition to detecting decreased microglial activation following LM11A-31 treatment, [18F]GE-180 identified activated microglia in AD mice with greater sensitivity than another second-generation TSPO radiotracer, [18F]PBR06. Together, these data demonstrate the promise of [18F]GE-180 as a potentially sensitive tool for tracking neuroinflammation in AD mice and for monitoring therapeutic modulation of microglial activation.
机译:小胶质细胞激活是阿尔茨海默氏病(AD)的关键病理特征。定位蛋白18 kDa(TSPO)的PET成像是一种在体内检测小胶质细胞活化的策略。在这里,我们评估了氟尿酰胺([ 18 F] GE-180),它是新型的第二代TSPO-PET放射性示踪剂,具有监测对LM11A-31(一种临床试验中的新型AD疗法)的反应的能力。将显示病理的AD小鼠用LM11A-31口服治疗3个月。随后的[ 18 F] GE-180-PET成像显示,与用媒介物治疗的小鼠相比,LM11A-31治疗的AD小鼠的皮质和海马信号明显降低,与TSPO免疫染色和小胶质细胞水平降低有关Iba1免疫染色。除了检测到LM11A-31治疗后小胶质细胞活化减少外,[ 18 F] GE-180还比其他第二代TSPO放射性示踪剂[ 18 < / sup> F] PBR06。这些数据一起证明了[ 18 F] GE-180有望成为跟踪AD小鼠神经炎症和监测小胶质细胞活化的治疗性调节的潜在敏感工具。

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