The Structure of the 26S Proteasome Subunit Rpn2 Reveals Its PC Repeat Domain as a Closed Toroid of Two Concentric ¦Á-Helical Rings

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• 作者：Jun He¹ ; ³ ; Kiran Kulkarni¹ ; ³ ; Paula  ; C.A. da  ; Fonseca¹ ; Dasha Krutauz² ; Michael  ; H. Glickman² ; David Barford¹ ; ^{david.barford@icr.ac.uk} ; Edward  ; P. Morris¹ ; ^{edward.morris@icr.ac.uk}
• 刊名：Structure
• 出版年：2012
• 出版时间：7 March, 2012
• 年：2012
• 卷：20
• 期：3
• 页码：513-521
• 全文大小：1965 K

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Summary

The 26S proteasome proteolyses ubiquitylated proteins and is assembled from a 20S proteolytic core and two 19S regulatory particles (19S-RP). The 19S-RP scaffolding subunits Rpn1 and Rpn2 function to engage ubiquitin receptors. Rpn1 and Rpn2 are characterized by eleven tandem copies of a 35-40 amino acid repeat motif termed the proteasome/cyclosome (PC) repeat. Here, we reveal that the eleven PC repeats of Rpn2 form a closed toroidal structure incorporating two concentric rings of?¦Á helices encircling two axial ¦Á helices. A rod-like N-terminal domain consisting of 17 stacked ¦Á helices and a globular C-terminal domain emerge from one face of the toroid. Rpn13, an ubiquitin receptor, binds to the C-terminal 20 residues of Rpn2. Rpn1 adopts a similar conformation to Rpn2 but differs in the orientation of its rod-like N-terminal domain. These findings have implications for understanding how 19S-RPs recognize, unfold, and deliver ubiquitylated substrates to the 20S core.