+検索条件
-Structure paper
タイトル | Mechanism of autocatalytic activation during proteasome assembly. |
---|---|
ジャーナル・号・ページ | Nat Struct Mol Biol, Year 2024 |
掲載日 | 2024年4月10日 |
著者 | Benjamin Velez / Richard M Walsh / Shaun Rawson / Aida Razi / Lea Adams / Erignacio Fermin Perez / Fenglong Jiao / Marie Blickling / Tamayanthi Rajakumar / Darlene Fung / Lan Huang / John Hanna / |
PubMed 要旨 | Many large molecular machines are too elaborate to assemble spontaneously and are built through ordered pathways orchestrated by dedicated chaperones. During assembly of the core particle (CP) of the ...Many large molecular machines are too elaborate to assemble spontaneously and are built through ordered pathways orchestrated by dedicated chaperones. During assembly of the core particle (CP) of the proteasome, where protein degradation occurs, its six active sites are simultaneously activated via cleavage of N-terminal propeptides. Such activation is autocatalytic and coupled to fusion of two half-CP intermediates, which protects cells by preventing activation until enclosure of the active sites within the CP interior. Here we uncover key mechanistic aspects of autocatalytic activation, which proceeds through alignment of the β5 and β2 catalytic triad residues, respectively, with these triads being misaligned before fusion. This mechanism contrasts with most other zymogens, in which catalytic centers are preformed. Our data also clarify the mechanism by which individual subunits can be added in a precise, temporally ordered manner. This work informs two decades-old mysteries in the proteasome field, with broader implications for protease biology and multisubunit complex assembly. |
リンク | Nat Struct Mol Biol / PubMed:38600323 |
手法 | EM (単粒子) |
解像度 | 2.16 - 2.8 Å |
構造データ | EMDB-41963, PDB-8u6y: EMDB-41993, PDB-8u7u: |
由来 |
|
キーワード | HYDROLASE (加水分解酵素) / Proteasome (プロテアソーム) / core particle (ヌクレオソーム) |