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对老年、帕金森病和阿尔茨海默病患者大脑特定区域的异铁蛋白进行定量分析。

A quantitative analysis of isoferritins in select regions of aged, parkinsonian, and Alzheimer's diseased brains.

作者信息

Connor J R, Snyder B S, Arosio P, Loeffler D A, LeWitt P

机构信息

George M. Leader Family Laboratory for Alzheimer's Disease Research, Department of Neuroscience and Anatomy, Pennsylvania State University, M.S. Hershey Medical Center, Hershey 17033, USA.

出版信息

J Neurochem. 1995 Aug;65(2):717-24. doi: 10.1046/j.1471-4159.1995.65020717.x.

DOI:10.1046/j.1471-4159.1995.65020717.x
PMID:7616228
Abstract

The brain requires a ready supply of iron for normal neurological function, but free iron is toxic. Consequently, iron bioavailability must be stringently regulated. Recent evidence has suggested that the brain iron regulatory system is dysfunctional in neurological disorders such as Alzheimer's and Parkinson's diseases (AD and PD, respectively). A key component of the iron regulatory system in the brain is ferritin. Ferritin consists of 24 subunits, which are distinguished as either a heavy-chain (H) or light-chain (L) isoform. These peptide subunits are genetically and functionally distinct. Thus, the ability to investigate separately the types of ferritin in brain should provide insight into iron management at both the cellular and the molecular level. In this study, the ratio of isoferritins was determined in select regions of adult elderly AD and PD human brains. The H-rich ferritin was more abundant in the young brain, except in the globus pallidus where the ratio of H/L ferritin was 1:1. The balance of H/L isoferritins was influenced by age, brain region, and disease state. With normal aging, both H and L ferritin increased; however, the age-associated increase in isoferritins generally failed to occur in AD and PD brain tissue. The imbalance in H/L isoferritins was disease and region specific. For example, in frontal cortex, there was a dramatic (fivefold) increase in the ratio of H/L ferritin in AD brains but not in PD brains. In PD, caudate and putamen H/L ratios were higher than in AD and the elderly control group.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

大脑正常神经功能需要充足的铁供应,但游离铁具有毒性。因此,铁的生物利用率必须受到严格调控。最近有证据表明,在阿尔茨海默病和帕金森病(分别为AD和PD)等神经疾病中,大脑铁调节系统功能失调。大脑中铁调节系统的一个关键组成部分是铁蛋白。铁蛋白由24个亚基组成,可分为重链(H)或轻链(L)亚型。这些肽亚基在基因和功能上是不同的。因此,分别研究大脑中铁蛋白类型的能力应能在细胞和分子水平上深入了解铁的管理情况。在本研究中,测定了成年老年AD和PD患者大脑特定区域的异铁蛋白比例。富含H的铁蛋白在年轻大脑中更为丰富,但苍白球除外,其H/L铁蛋白比例为1:1。H/L异铁蛋白的平衡受年龄、脑区和疾病状态的影响。随着正常衰老,H和L铁蛋白均增加;然而,在AD和PD脑组织中,异铁蛋白通常未出现与年龄相关的增加。H/L异铁蛋白的失衡具有疾病和区域特异性。例如,在额叶皮质,AD大脑中H/L铁蛋白比例急剧增加(五倍),而PD大脑中则没有。在PD中,尾状核和壳核的H/L比例高于AD和老年对照组。(摘要截选至250字)

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