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来自正常和朊病毒感染人类大脑的小窝蛋白-1的理化性质表征。

Characterization of physiochemical properties of caveolin-1 from normal and prion-infected human brains.

作者信息

Xiao Xiangzhu, Shen Pingping, Wang Zerui, Dang Johnny, Adornato Alise, Zou Lewis S, Dong Zhiqian, Yuan Jue, Feng Jiachun, Cui Li, Zou Wen-Quan

机构信息

Department of Pathology, Case Western Reserve University, Cleveland, OH, USA.

Institute of Neuroscience Center and Neurology Department, The First Hospital of Jilin University, Changchun, Jilin, China.

出版信息

Oncotarget. 2017 Jul 21;8(33):53888-53898. doi: 10.18632/oncotarget.19431. eCollection 2017 Aug 15.

Abstract

Caveolin-1 is a major component protein of the caveolae-a type of flask shaped, 50-100 nm, nonclathrin-coated, microdomain present in the plasma membrane of most mammalian cells. Caveolin-1 functions as a scaffolding protein to organize and concentrate signaling molecules within the caveolae, which may be associated with its unique physicochemical properties including oligomerization, acquisition of detergent insolubility, and association with cholesterol. Here we demonstrate that caveolin-1 is detected in all brain areas examined and recovered in both detergent-soluble and -insoluble fractions. Surprisingly, the recovered molecules from the two different fractions share a similar molecular size ranging from 200 to 2,000 kDa, indicated by gel filtration. Furthermore, both soluble and insoluble caveolin-1 molecules generate a proteinase K (PK)-resistant C-terminal core fragment upon the PK-treatment, by removing ˜36 amino acids from the N-terminus of the protein. Although it recognizes caveolin-1 from A431 cell lysate, an antibody against the C-terminus of caveolin-1 fails to detect the brain protein by Western blotting, suggesting that the epitope in the brain caveolin-1 is concealed. No significant differences in the physicochemical properties of caveolin-1 between uninfected and prion-infected brains are observed.

摘要

小窝蛋白-1是小窝的主要组成蛋白,小窝是一种烧瓶状、50-100纳米、无网格蛋白包被的微区,存在于大多数哺乳动物细胞的质膜中。小窝蛋白-1作为一种支架蛋白,在小窝内组织和浓缩信号分子,这可能与其独特的物理化学性质有关,包括寡聚化、获得去污剂不溶性以及与胆固醇结合。在这里,我们证明在所有检测的脑区中都能检测到小窝蛋白-1,并且在去污剂可溶性和不溶性组分中都能回收。令人惊讶的是,通过凝胶过滤显示,从这两种不同组分中回收的分子具有相似的分子大小,范围从200到2000 kDa。此外,可溶性和不溶性小窝蛋白-1分子在蛋白酶K(PK)处理后,通过从蛋白质的N端去除约36个氨基酸,产生一个抗蛋白酶K的C端核心片段。尽管一种针对小窝蛋白-1 C端的抗体能够识别A431细胞裂解物中的小窝蛋白-1,但通过蛋白质印迹法未能检测到脑蛋白中的小窝蛋白-1,这表明脑小窝蛋白-1中的表位被隐藏。在未感染和朊病毒感染的脑之间,未观察到小窝蛋白-1的物理化学性质有显著差异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/adf1/5589549/a9b11a146d99/oncotarget-08-53888-g001.jpg

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