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Functional Effects of AAV2-GDNF on the Dopaminergic Nigrostriatal Pathway in Parkinsonian Rhesus Monkeys

机译:AAV2-GDNF对帕金森氏猕猴的多巴胺能黑质纹状体途径的功能作用

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摘要

We investigated the safety and neuroregenerative potential of an adeno-associated virus (AAV2) containing human glial cell line-derived neurotrophic factor (GDNF) in an MPTP primate model of Parkinson's disease. Dopaminergic function was evaluated by positron emission tomography with 6-[18F]fluoro-l-m-tyrosine (FMT) before and after AAV2-GDNF or phosphate-buffered saline infusion bilaterally into the putamen. FMT uptake was significantly increased bilaterally in the putamen of AAV2-GDNF but not phosphate-buffered saline-treated animals 6 months after infusion, indicating increased dopaminergic activity in the nigrostriatal pathways. AAV2-GDNF-treated animals also showed clinical improvement without adverse effects. These findings are consistent with our previous report in aged nonhuman primates that showed evidence of enhanced use of striatal dopamine and dopaminergic nigrostriatal innervation. Clinical improvement and evidence of functional recovery in the nigrostriatal pathway, and the absence of adverse effects, support the safety of this approach for the delivery of GDNF over a 6-month period.
机译:我们在帕金森氏病的MPTP灵长类动物模型中研究了包含人胶质细胞系衍生的神经营养因子(GDNF)的腺相关病毒(AAV2)的安全性和神经再生潜力。在AAV2-GDNF或双侧磷酸盐缓冲液注入核壳之前和之后,用6-[ 18 F]氟-1-m-酪氨酸(FMT)进行正电子发射断层扫描,评估多巴胺能功能。输注后6个月,AAV2-GDNF的壳核中FMT的摄取显着增加,但磷酸盐缓冲液处理的动物的FMT摄取没有明显增加,这表明黑质纹状体途径中的多巴胺能活性增加。 AAV2-GDNF处理的动物也显示出临床改善,而没有不良影响。这些发现与我们先前关于老年非人类灵长类动物的报告一致,后者显示出增加使用纹状体多巴胺和多巴胺能黑质纹状体神经支配的证据。临床改善和黑质纹状体途径功能恢复的证据以及没有不良反应,支持了该方法在6个月内递送GDNF的安全性。

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