Literature DB >> 31767681

Structure of spastin bound to a glutamate-rich peptide implies a hand-over-hand mechanism of substrate translocation.

Han Han1, Heidi L Schubert1, John McCullough1, Nicole Monroe1, Michael D Purdy2, Mark Yeager2,3,4,5, Wesley I Sundquist6, Christopher P Hill7.   

Abstract

Many members of the AAA+ ATPase family function as hexamers that unfold their protein substrates. These AAA unfoldases include spastin, which plays a critical role in the architecture of eukaryotic cells by driving the remodeling and severing of microtubules, which are cytoskeletal polymers of tubulin subunits. Here, we demonstrate that a human spastin binds weakly to unmodified peptides from the C-terminal segment of human tubulin α1A/B. A peptide comprising alternating glutamate and tyrosine residues binds more tightly, which is consistent with the known importance of glutamylation for spastin microtubule severing activity. A cryo-EM structure of the spastin-peptide complex at 4.2 Å resolution revealed an asymmetric hexamer in which five spastin subunits adopt a helical, spiral staircase configuration that binds the peptide within the central pore, whereas the sixth subunit of the hexamer is displaced from the peptide/substrate, as if transitioning from one end of the helix to the other. This configuration differs from a recently published structure of spastin from Drosophila melanogaster, which forms a six-subunit spiral without a transitioning subunit. Our structure resembles other recently reported AAA unfoldases, including the meiotic clade relative Vps4, and supports a model in which spastin utilizes a hand-over-hand mechanism of tubulin translocation and microtubule remodeling.
© 2020 Han et al.

Entities:  

Keywords:  ATPases associated with diverse cellular activities (AAA); cryo-electron microscopy; microtubule severing mechanism; molecular machine; peptide interaction; protein structure; structure-function

Mesh:

Substances:

Year:  2019        PMID: 31767681      PMCID: PMC6956536          DOI: 10.1074/jbc.AC119.009890

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


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5.  Structural basis of protein translocation by the Vps4-Vta1 AAA ATPase.

Authors:  Nicole Monroe; Han Han; Peter S Shen; Wesley I Sundquist; Christopher P Hill
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6.  Cryo-EM structures and dynamics of substrate-engaged human 26S proteasome.

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