Arrestin-1 engineering facilitates complex stabilization with native rhodopsin

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作者
Raphael S. Haider
Florian Wilhelm
Aurélien Rizk
Eshita Mutt
Xavier Deupi
Christian Peterhans
Jonas Mühle
Philipp Berger
Gebhard F. X. Schertler
Jörg Standfuss
Martin K. Ostermaier
机构
[1] InterAx Biotech AG,
[2] PARK InnovAARE,undefined
[3] Laboratory of Biomolecular Research,undefined
[4] Paul Scherrer Institute,undefined
[5] Institute of Molecular Cell Biology,undefined
[6] ETH Zurich,undefined
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摘要
Arrestin-1 desensitizes the activated and phosphorylated photoreceptor rhodopsin by forming transient rhodopsin−arrestin-1 complexes that eventually decay to opsin, retinal and arrestin-1. Via a multi-dimensional screening setup, we identified and combined arrestin-1 mutants that form lasting complexes with light-activated and phosphorylated rhodopsin in harsh conditions, such as high ionic salt concentration. Two quadruple mutants, D303A + T304A + E341A + F375A and R171A + T304A + E341A + F375A share similar heterologous expression and thermo-stability levels with wild type (WT) arrestin-1, but are able to stabilize complexes with rhodopsin with more than seven times higher half-maximal inhibitory concentration (IC50) values for NaCl compared to the WT arrestin-1 protein. These quadruple mutants are also characterized by higher binding affinities to phosphorylated rhodopsin, light-activated rhodopsin and phosphorylated opsin, as compared with WT arrestin-1. Furthermore, the assessed arrestin-1 mutants are still specifically associating with phosphorylated or light-activated receptor states only, while binding to the inactive ground state of the receptor is not significantly altered. Additionally, we propose a novel functionality for R171 in stabilizing the inactive arrestin-1 conformation as well as the rhodopsin–arrestin-1 complex. The achieved stabilization of the active rhodopsin–arrestin-1 complex might be of great interest for future structure determination, antibody development studies as well as drug-screening efforts targeting G protein-coupled receptors (GPCRs).
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