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载脂蛋白 E 在人额皮质和海马中形成二聚体。

Apolipoprotein-E forms dimers in human frontal cortex and hippocampus.

机构信息

Prince of Wales Medical Research Institute, Randwick NSW 2031, Australia.

出版信息

BMC Neurosci. 2010 Feb 20;11:23. doi: 10.1186/1471-2202-11-23.

Abstract

BACKGROUND

Apolipoprotein-E (apoE) plays important roles in neurobiology and the apoE4 isoform increases risk for Alzheimer's disease (AD). ApoE3 and apoE2 are known to form disulphide-linked dimers in plasma and cerebrospinal fluid whereas apoE4 cannot form these dimers as it lacks a cysteine residue. Previous in vitro research indicates dimerisation of apoE3 has a significant impact on its functions related to cholesterol homeostasis and amyloid-beta peptide degradation. The possible occurrence of apoE dimers in cortical tissues has not been examined and was therefore assessed. Human frontal cortex and hippocampus from control and AD post-mortem samples were homogenised and analysed for apoE by western blotting under both reducing and non-reducing conditions.

RESULTS

In apoE3 homozygous samples, approximately 12% of apoE was present as a homodimer and approximately 2% was detected as a 43 kDa heterodimer. The level of dimerisation was not significantly different when control and AD samples were compared. As expected, these dimerised forms of apoE were not detected in apoE4 homozygous samples but were detected in apoE3/4 heterozygotes at a level approximately 60% lower than seen in the apoE3 homozygous samples. Similar apoE3 dimers were also detected in lysates of SK-N-SH neuroblastoma cells and in freshly prepared rabbit brain homogenates. The addition of the thiol trapping agent, iodoacetamide, to block reactive thiols during both human and rabbit brain sample homogenisation and processing did not reduce the amount of apoE homodimer recovered. These data indicate that the apoE dimers we detected in the human brain are not likely to be post-mortem artefacts.

CONCLUSION

The identification of disulphide-linked apoE dimers in human cortical and hippocampal tissues represents a distinct structural difference between the apoE3 and apoE4 isoforms that may have functional consequences.

摘要

背景

载脂蛋白-E(apoE)在神经生物学中发挥着重要作用,apoE4 同工型增加了阿尔茨海默病(AD)的风险。已知 apoE3 和 apoE2 在血浆和脑脊液中形成二硫键连接的二聚体,而 apoE4 由于缺乏半胱氨酸残基而不能形成这些二聚体。先前的体外研究表明,apoE3 的二聚化对其与胆固醇稳态和淀粉样β肽降解相关的功能有重大影响。尚未检查皮质组织中 apoE 二聚体的可能发生情况,因此对此进行了评估。将来自对照和 AD 死后样本的人额皮质和海马组织匀浆,并在还原和非还原条件下通过 Western blot 分析 apoE。

结果

在 apoE3 纯合子样本中,约 12%的 apoE 以同源二聚体形式存在,约 2%以 43 kDa 异源二聚体形式检测到。当对照和 AD 样本进行比较时,二聚化水平没有显着差异。如预期的那样,apoE4 纯合子样本中未检测到这些二聚化形式的 apoE,但在 apoE3/4 杂合子中以比 apoE3 纯合子样本低约 60%的水平检测到。在 SK-N-SH 神经母细胞瘤细胞的裂解物和新鲜制备的兔脑匀浆中也检测到类似的 apoE3 二聚体。在人脑和兔脑样本匀浆和处理过程中加入硫醇捕获剂碘乙酰胺以阻断反应性硫醇,不会减少回收的 apoE 同源二聚体的量。这些数据表明,我们在人脑检测到的 apoE 二聚体不太可能是死后的人为假象。

结论

在人皮质和海马组织中二硫键连接的 apoE 二聚体的鉴定代表了 apoE3 和 apoE4 同工型之间的明显结构差异,可能具有功能后果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5656/2837047/0c6c53162d70/1471-2202-11-23-2.jpg

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