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首页> 美国卫生研究院文献>Frontiers in Neuroanatomy >Life-time expression of the proteins peroxiredoxin beta-synuclein PARK7/DJ-1 and stathmin in the primary visual and primary somatosensory cortices in rats
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Life-time expression of the proteins peroxiredoxin beta-synuclein PARK7/DJ-1 and stathmin in the primary visual and primary somatosensory cortices in rats

机译:大鼠过氧化物酶β-突触核蛋白PARK7 / DJ-1和stathmin在大鼠原代视觉和原代体感皮质中的终生表达

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Four distinct proteins are regulated in the aging neuroretina and may be regulated in the cerebral cortex, too: peroxiredoxin, beta-synuclein, PARK[Parkinson disease(autosomal recessive, early onset)]7/DJ-1, and Stathmin. Thus, we performed a comparative analysis of these proteins in the the primary somatosensory cortex (S1) and primary visual cortex (V1) in rats, in order to detect putative common development-, maturation- and age-related changes. The expressions of peroxiredoxin, beta-synuclein, PARK[Parkinson disease (autosomal recessive, early onset)]7/DJ-1, and Stathmin were compared in the newborn, juvenile, adult, and aged S1 and V1. Western blot (WB), quantitative reverse-transcription polymerase chain reaction (qRT-PCR), and immunohistochemistry (IHC) analyses were employed to determine whether the changes identified by proteomics were verifiable at the cellular and molecular levels. All of the proteins were detected in both of the investigated cortical areas. Changes in the expressions of the four proteins were found throughout the life-time of the rats. Peroxiredoxin expression remained unchanged over life-time. Beta-Synuclein expression was massively increased up to the adult stage of life in both the S1 and V1. PARK[Parkinson disease (autosomal recessive, early onset)]7/DJ-1 exhibited a massive up-regulation in both the S1 and V1 at all ages. Stathmin expression was massively down regulated after the neonatal period in both the S1 and V1. The detected protein alterations were analogous to their retinal profiles. This study is the first to provide evidence that peroxiredoxin, beta-synuclein, PARK[Parkinson disease (autosomal recessive, early onset)]7/DJ-1, and Stathmin are associated with postnatal maturation and aging in both the S1 and V1 of rats. These changes may indicate their involvement in key functional pathways and may account for the onset or progression of age-related pathologies.
机译:四种不同的蛋白质在衰老的神经视网膜中受到调节,并且在大脑皮层中也可能受到调节:过氧化物酶,β-突触核蛋白,PARK [帕金森病(常染色体隐性遗传,早发)] 7 / DJ-1和Stathmin。因此,我们对大鼠初级体感皮层(S1)和初级视觉皮层(V1)中的这些蛋白质进行了比较分析,以检测推测的共同发育,成熟和年龄相关的变化。比较了新生儿,少年,成人和S1和V1年龄段的过氧化物酶,β-突触核蛋白,PARK [帕金森病(常染色体隐性遗传,早期发作)] 7 / DJ-1和Stathmin的表达。使用蛋白质印迹(WB),定量逆转录聚合酶链反应(qRT-PCR)和免疫组化(IHC)分析来确定蛋白质组学鉴定的变化在细胞和分子水平上是否可验证。在研究的两个皮层区域均检测到所有蛋白质。在大鼠的整个生命周期中发现了这四种蛋白表达的变化。在整个生命周期中,Peroxiredoxin表达保持不变。在S1和V1中,β-突触核蛋白的表达一直大量增加直至成年阶段。 PARK [帕金森病(常染色体隐性遗传,早期发作)] 7 / DJ-1在所有年龄段的S1和V1均表现出大量上调。 S1和V1的新生儿期后,stathmin的表达被大幅下调。检测到的蛋白质改变类似于它们的视网膜特征。这项研究首次提供证据,证明过氧化物酶,β-突触核蛋白,PARK [帕金森病(常染色体隐性遗传,早期发作)] 7 / DJ-1和Stathmin与大鼠S1和V1的出生后成熟和衰老相关。这些变化可能表明它们参与了关键的功能途径,并可能解释了与年龄有关的病理的发作或进展。

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