首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >In situ structural studies of tripeptidyl peptidase II (TPPII) reveal spatial association with proteasomes
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In situ structural studies of tripeptidyl peptidase II (TPPII) reveal spatial association with proteasomes

机译:三肽基肽酶II(TPPII)的原位结构研究揭示了与蛋白酶体的空间关联

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摘要

Tripeptidyl peptidase II (TPPII) is a eukaryotic protease acting downstream of the 26S proteasome; it removes tripeptides from the degradation products released by the proteasome. Structural studies in vitro have revealed the basic architecture of TPPII, a two-stranded linear polymer that assembles to form a spindle-shaped complex of ∼6 MDa. Dependent on protein concentration, TPPII has a distinct tendency for polymorphism. Therefore, its structure in vivo has remained unclear. To resolve this issue, we have scrutinized cryo-electron tomograms of rat hippocampal neurons for the occurrence and spatial distribution of TPPII by template matching. The quality of the tomograms recorded with the Volta phase plate enabled a detailed structural analysis of TPPII despite its low abundance. Two different assembly states (36-mers and 32-mers) coexist as well as occasional extended forms with longer strands. A distance analysis of the relative locations of TPPII and 26S proteasomes confirmed the visual impression that these two complexes spatially associate in agreement with TPPII’s role in postproteasomal degradation.
机译:三肽基肽酶II(TPPII)是作用于26S蛋白酶体下游的真核蛋白酶。它从蛋白酶体释放的降解产物中除去三肽。体外结构研究揭示了TPPII的基本结构,TPPII是一种两链线性聚合物,可组装形成约6 MDa的纺锤形复合物。根据蛋白质浓度,TPPII具有明显的多态性趋势。因此,其体内结构仍不清楚。为解决此问题,我们通过模板匹配仔细检查了大鼠海马神经元的冷冻电子断层图,以了解TPPII的发生和空间分布。尽管Volta相板的丰度较低,但其层析图像的质量仍可对TPPII进行详细的结构分析。两种不同的组装状态(36聚体和32聚体)共存,偶尔也有较长链的延伸形式。对TPPII和26S蛋白酶体相对位置的距离分析证实了视觉印象,即这两种复合物在空间上与TPPII在蛋白酶体降解中的作用相一致。

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