Araki T, Tanji H, Fujihara K, Kato H, Itoyama Y
Department of Neurology, Tohoku University School of Medicine, Sendai, Japan.
Metab Brain Dis. 1999 Mar;14(1):21-31. doi: 10.1023/a:1020605429535.
Receptor autoradiographic technique was studied to investigate sequential changes in FK-506 binding proteins, nitric oxide synthase and dopamine uptake sites in the brain 1 week to 8 weeks after unilateral 6-hydroxydopamine injection of the medial forebrain bundle in rats. [3H]FK-506, [3H]L-N(G)-nitro-arginine and [3H]mazindol were used to label FK-506 binding proteins (immunophilin), nitric oxide synthase and dopamine uptake sites, respectively. [3H]FK-506 binding showed about 13-25% increase in the ipsilateral striatum from 2 to 8 weeks after degeneration of nigrostriatal pathway. However, no significant change in [3H]FK-506 binding was observed in the ipsilateral substantia nigra during the postlesion periods. In the contralateral side, [3H]FK-506 binding also showed about 13-25% increase in the striatum from 2 to 8 weeks postlesion. The substantia nigra showed a 21% increase in [3H]FK-506 binding only 2 weeks after the lesioning. On the other hand, [3H]L-N(G)-nitro-arginine binding showed about 21-31% increase in the parietal cortex and striatum 1 week or 2 weeks postlesion. In the contralateral side, a 21% increase in [3H]L-N(G)-nitro-arginine binding was found in the dorsolateral striatum only 1 week postlesion. In contrast, degeneration of nigrostriatal pathway caused a conspicuous loss of [3H]mazindol binding in the ipsilateral striatum (87-96%), substantia nigra (36-73%) and ventral tegmental area (91-100%) during the postlesion periods. In the contralateral side, no significant changes in [3H]mazindol binding were observed in these areas up to 8 weeks after the postlesion. The present study demonstrates that unilateral injection of 6-hydroxydopamine into the medial forebrain bundle of rats can cause a significant increase in [3H]FK-506 and [3H]L-N(G)-nitro-arginine bindings in the brains. In contrast, a marked reduction in [3H]mazindol binding is observed in the brains after the lesioning, indicating severe damage to nigrostriatal dopaminergic pathway. These results suggest that immunophilin and nitric oxide synthase may play some role in the pathogenesis of neurodegenerative disorders such as Parkinson's disease.
采用受体放射自显影技术,研究大鼠单侧内侧前脑束注射6-羟基多巴胺后1周8周,脑内FK-506结合蛋白、一氧化氮合酶和多巴胺摄取位点的动态变化。分别用[3H]FK-506、[3H]L-N(G)-硝基精氨酸和[3H]吗茚酮标记FK-506结合蛋白(亲免素)、一氧化氮合酶和多巴胺摄取位点。黑质纹状体通路退变后2周8周,同侧纹状体[3H]FK-506结合增加约13%25%。然而,损伤后同侧黑质[3H]FK-506结合未见明显变化。在对侧,损伤后2周8周,纹状体[3H]FK-506结合也增加约13%25%。损伤后仅2周,黑质[3H]FK-506结合增加21%。另一方面,损伤后1周或2周,顶叶皮质和纹状体[3H]L-N(G)-硝基精氨酸结合增加约21%31%。在对侧,损伤后仅1周,背外侧纹状体[3H]L-N(G)-硝基精氨酸结合增加21%。相反,损伤后同侧纹状体(87%96%)、黑质(36%73%)和腹侧被盖区(91%~100%)[3H]吗茚酮结合显著减少。在对侧,损伤后8周内这些区域[3H]吗茚酮结合未见明显变化。本研究表明,大鼠单侧内侧前脑束注射6-羟基多巴胺可使脑内[3H]FK-506和[3H]L-N(G)-硝基精氨酸结合显著增加。相反,损伤后脑内[3H]吗茚酮结合明显减少,提示黑质纹状体多巴胺能通路严重受损。这些结果提示,亲免素和一氧化氮合酶可能在帕金森病等神经退行性疾病的发病机制中发挥一定作用。
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