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Get Free AccessHelical membrane proteins constitute roughly a quarter of all proteomes and perform diverse biological functions. To avoid aggregation, they undergo cotranslational membrane insertion and are typically assumed to attain stable transmembrane topologies immediately upon insertion. To what extent post-translational changes in topology are possible in-vivo and how they may affect biogenesis is incompletely understood. Here, we show that monomeric forms of Small Multidrug Resistance (SMR) proteins display topological dynamics, where the N-terminal transmembrane helix equilibrates between membrane-inserted and non-inserted states. We characterize the kinetics of the process and show how the composition of the helix regulates the topological dynamics. We further show that topological dynamics is a property of the unassembled monomeric protein, as the N-terminal helix becomes fixed in a transmembrane disposition upon dimerization. Membrane protein topology can thus remain dynamic long after cotranslational membrane insertion, and can be regulated by later assembly processes.
Maximilian Seurig, Moira Ek, Gunnar Von Heijne, Nir Fluman (2019). Dynamic membrane topology in an unassembled membrane protein. bioRxiv (Cold Spring Harbor Laboratory), DOI: 10.1101/548537.
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Type
Preprint
Year
2019
Authors
4
Datasets
0
Total Files
0
Language
English
Journal
bioRxiv (Cold Spring Harbor Laboratory)
DOI
10.1101/548537
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