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三种重复形式的 tau 蛋白抑制了四种重复 tau 丝的组装。

Three repeat isoforms of tau inhibit assembly of four repeat tau filaments.

机构信息

Department of Neuroscience, Mayo Clinic College of Medicine, Jacksonville, Florida, USA.

出版信息

PLoS One. 2010 May 25;5(5):e10810. doi: 10.1371/journal.pone.0010810.

Abstract

Tauopathies are defined by assembly of the microtubule associated protein tau into filamentous tangles and classified by the predominant tau isoform within these aggregates. The major isoforms are determined by alternative mRNA splicing of exon 10 generating tau with three (3R) or four (4R) approximately 32 amino acid imperfect repeats in the microtubule binding domain. In normal adult brains there is an approximately equimolar ratio of 3R and 4R tau which is altered by several disease-causing mutations in the tau gene. We hypothesized that when 4R and 3R tau isoforms are not at equimolar ratios aggregation is favored. Here we provide evidence for the first time that the combination of 3R and 4R tau isoforms results in less in vitro heparin induced polymerization than with 4R preparations alone. This effect was independent of reducing conditions and the presence of alternatively spliced exons 2 and 3 N-terminal inserts. The addition of even small amounts of 3R to 4R tau assembly reactions significantly decreased 4R assembly. Together these findings suggest that co-expression of 3R and 4R tau isoforms reduce tau filament assembly and that 3R tau isoforms inhibit 4R tau assembly. Expression of equimolar amounts of 3R and 4R tau in adult humans may be necessary to maintain proper neuronal microtubule dynamics and to prevent abnormal tau filament assembly. Importantly, these findings indicate that disruption of the normal equimolar 3R to 4R ratio may be sufficient to drive tau aggregation and that restoration of the tau isoform balance may have important therapeutic implications in tauopathies.

摘要

tau 病是以微管相关蛋白 tau 组装成纤维缠结为特征,并根据这些聚集体中主要的 tau 同工型进行分类。主要同工型是通过外显子 10 的选择性 mRNA 剪接产生的,在微管结合域中产生具有三个(3R)或四个(4R)大约 32 个氨基酸不完全重复的 tau。在正常成人脑中,3R 和 4R tau 的比例约为等摩尔,这一比例因 tau 基因中的几种致病突变而改变。我们假设,当 4R 和 3R tau 同工型的比例不是等摩尔时,聚集就会被优先。在这里,我们首次提供了证据表明,3R 和 4R tau 同工型的组合导致体外肝素诱导聚合的程度低于单独使用 4R 制剂。这种效应独立于还原条件以及选择性剪接的外显子 2 和 3 N 端插入的存在。即使向 4R tau 组装反应中添加少量的 3R,也会显著降低 4R 的组装。这些发现表明,3R 和 4R tau 同工型的共表达减少了 tau 纤维的组装,并且 3R tau 同工型抑制了 4R tau 的组装。在成年人体内表达等量的 3R 和 4R tau 可能是维持适当的神经元微管动力学和防止异常 tau 纤维组装所必需的。重要的是,这些发现表明,破坏正常的 3R 与 4R 比例可能足以驱动 tau 聚集,并且恢复 tau 同工型平衡可能对 tau 病具有重要的治疗意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b6e7/2876030/f9ee59c22699/pone.0010810.g001.jpg

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