载脂蛋白E的凝血酶切割片段表现出异构体特异性神经毒性。

A thrombin cleavage fragment of apolipoprotein E exhibits isoform-specific neurotoxicity.

作者信息

Marques M A, Tolar M, Harmony J A, Crutcher K A

机构信息

Department of Neurosurgery, University of Cincinnati Medical Center, OH 45267, USA.

出版信息

Neuroreport. 1996 Nov 4;7(15-17):2529-32. doi: 10.1097/00001756-199611040-00025.

DOI:10.1097/00001756-199611040-00025

PMID:8981417

Abstract

A 22 kDa fragment of apoE containing a putative cytotoxi domain was identified in postmortem human brain tissue and fresh CSF. This fragment is apparently equivalent to the major apoE thrombin cleavage product. In vitro toxicity assays demonstrate that the corresponding fragment derived from recombinantly expressed human apoE is toxic to primary neurons in culture and that the E4-derived fragment is significantly more toxic than the fragment derived from the E3 isoform. These results suggest that proteolytic fragments of apoE may play a direct role in the pathology associated with AD and other diseases in which apoE has been implicated.

摘要

在人类尸检脑组织和新鲜脑脊液中鉴定出一种载脂蛋白E（apoE）的22 kDa片段，其含有一个假定的细胞毒性结构域。该片段显然等同于主要的apoE凝血酶裂解产物。体外毒性试验表明，重组表达的人类apoE衍生的相应片段对培养中的原代神经元有毒性，并且E4衍生片段的毒性明显高于E3异构体衍生的片段。这些结果表明，apoE的蛋白水解片段可能在与阿尔茨海默病（AD）及其他与apoE相关疾病的病理学中起直接作用。

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载脂蛋白E的凝血酶切割片段表现出异构体特异性神经毒性。

A thrombin cleavage fragment of apolipoprotein E exhibits isoform-specific neurotoxicity.

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