首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Activating transcription factor 2 expression in the adult human brain: association with both neurodegeneration and neurogenesis.
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Activating transcription factor 2 expression in the adult human brain: association with both neurodegeneration and neurogenesis.

机译:在成年人的大脑中激活转录因子2的表达:与神经退行性变和神经发生有关。

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摘要

Activating transcription factor 2 (ATF2) is a member of the activator protein-1 family of transcription factors, which includes c-Jun and c-Fos. ATF2 is highly expressed in the mammalian brain although little is known about its function in nerve cells. Knockout mouse studies show that this transcription factor plays a role in neuronal migration during development but over-expression of ATF2 in neuronal-like cell culture promotes nerve cell death. Using immunohistochemical techniques we demonstrate ATF2 expression in the normal human brain is neuronal, is found throughout the cerebral cortex and is particularly high in the granule cells of the hippocampus, in the brain stem, in the pigmented cells of the substantia nigra and locus coeruleus, and in the granule and molecular cell layers of the cerebellum. In contrast to normal cases, ATF2 expression is down-regulated in the hippocampus, substantia nigra pars compacta and caudate nucleus of the neurological diseases Alzheimer's, Parkinson's and Huntington's, respectively. Paradoxically, an increase in ATF2 expression was found in the subependymal layer of Huntington's disease cases, compared with normal brains; a region reported to contain increased numbers of proliferating progenitor cells in Huntington's disease. We propose ATF2 plays a role in neuronal viability in the normal brain, which is compromised in susceptible regions of neurological diseases leading to its down-regulation. In contrast, the increased expression of ATF2 in the subependymal layer of Huntington's disease suggests a role for ATF2 in some aspect of neurogenesis in the diseased brain.
机译:激活转录因子2(ATF2)是转录因子激活蛋白1家族的成员,该家族包括c-Jun和c-Fos。 ATF2在哺乳动物脑中高表达,尽管对其在神经细胞中的功能知之甚少。敲除小鼠研究表明,该转录因子在发育过程中在神经元迁移中起作用,但在神经元样细胞培养物中ATF2的过表达促进神经细胞死亡。使用免疫组化技术,我们证明ATF2在正常人脑中是神经元表达,遍布整个大脑皮层,在海马的颗粒细胞,脑干,黑质和色素蓝斑的色素细胞中特别高,在小脑的颗粒和分子细胞层中与正常情况相反,在神经疾病阿尔茨海默氏症,帕金森氏症和亨廷顿氏症的海马,黑质致密部和尾状核中,ATF2表达分别下调。矛盾的是,与正常大脑相比,在亨廷顿氏病病例的室管膜下层中发现了ATF2表达的增加。据报道,该区域在亨廷顿舞蹈病中的增殖祖细胞数量增加。我们建议ATF2在正常大脑的神经元生存能力中起作用,这在神经系统疾病的易感区域受到损害,导致其下调。相反,亨廷顿氏病的室管膜下层中ATF2的表达增加表明ATF2在患病的神经发生的某些方面起作用。

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