A live cell assay of GPCR coupling allows identification of optogenetic tools for controlling Go and Gi signaling

A live cell assay of GPCR coupling allows identification of optogenetic tools for controlling Go and Gi signaling

Abstract Background Animal opsins are light-sensitive G-protein-coupled receptors (GPCRs) that enable optogenetic control over the major heterotrimeric G-protein signaling pathways in animal cells. As such, opsins have potential applications in both biomedical research and therapy. Selecting the ops...

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Main Authors: Edward R. Ballister, Jessica Rodgers, Franck Martial, Robert J. Lucas
Format: Article
Language:English
Published: BMC 2018-01-01
Series:BMC Biology
Subjects:
Optogenetics
Opsin
GPCR
GalphaO
Retinal degeneration
Gene therapy
Online Access:http://link.springer.com/article/10.1186/s12915-017-0475-2
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spelling doaj-6e01465ae3e94446a2655711330227302020-11-25T00:30:25ZengBMCBMC Biology1741-70072018-01-0116111610.1186/s12915-017-0475-2A live cell assay of GPCR coupling allows identification of optogenetic tools for controlling Go and Gi signalingEdward R. Ballister0Jessica Rodgers1Franck Martial2Robert J. Lucas3University of ManchesterUniversity of ManchesterUniversity of ManchesterUniversity of ManchesterAbstract Background Animal opsins are light-sensitive G-protein-coupled receptors (GPCRs) that enable optogenetic control over the major heterotrimeric G-protein signaling pathways in animal cells. As such, opsins have potential applications in both biomedical research and therapy. Selecting the opsin with the best balance of activity and selectivity for a given application requires knowing their ability to couple to a full range of relevant Gα subunits. We present the GsX assay, a set of tools based on chimeric Gs subunits that transduce coupling of opsins to diverse G proteins into increases in cAMP levels,  measured with a real-time reporter in living cells. We use this assay to compare coupling to Gi/o/t across a panel of natural and chimeric opsins selected for potential application in gene therapy for retinal degeneration. Results Of the opsins tested, wild-type human rod opsin had the highest activity for chimeric Gs proxies for Gi and Gt (Gsi and Gst) and was matched in Go proxy (Gso) activity only by a human rod opsin/scallop opsin chimera. Rod opsin drove roughly equivalent responses via Gsi, Gso, and Gst, while cone opsins showed much lower activities with Gso than Gsi or Gst, and a human rod opsin/amphioxus opsin chimera demonstrated higher activity with Gso than with Gsi or Gst. We failed to detect activity for opsin chimeras bearing three intracellular fragments of mGluR6, and observed unexpectedly complex response profiles for scallop and amphioxus opsins thought to be specialized for Go. Conclusions These results identify rod opsin as the most potent non-selective Gi/o/t-coupled opsin, long-wave sensitive cone opsin as the best for selectively activating Gi/t over Go, and a rod opsin/amphioxus opsin chimera as the best choice for selectively activating Go over Gi/t.http://link.springer.com/article/10.1186/s12915-017-0475-2OptogeneticsOpsinGPCRGalphaORetinal degenerationGene therapy
collection DOAJ
language English
format Article
sources DOAJ
author Edward R. Ballister
Jessica Rodgers
Franck Martial
Robert J. Lucas
spellingShingle Edward R. Ballister
Jessica Rodgers
Franck Martial
Robert J. Lucas
A live cell assay of GPCR coupling allows identification of optogenetic tools for controlling Go and Gi signaling
BMC Biology
Optogenetics
Opsin
GPCR
GalphaO
Retinal degeneration
Gene therapy
author_facet Edward R. Ballister
Jessica Rodgers
Franck Martial
Robert J. Lucas
author_sort Edward R. Ballister
title A live cell assay of GPCR coupling allows identification of optogenetic tools for controlling Go and Gi signaling
title_short A live cell assay of GPCR coupling allows identification of optogenetic tools for controlling Go and Gi signaling
title_full A live cell assay of GPCR coupling allows identification of optogenetic tools for controlling Go and Gi signaling
title_fullStr A live cell assay of GPCR coupling allows identification of optogenetic tools for controlling Go and Gi signaling
title_full_unstemmed A live cell assay of GPCR coupling allows identification of optogenetic tools for controlling Go and Gi signaling
title_sort live cell assay of gpcr coupling allows identification of optogenetic tools for controlling go and gi signaling
publisher BMC
series BMC Biology
issn 1741-7007
publishDate 2018-01-01
description Abstract Background Animal opsins are light-sensitive G-protein-coupled receptors (GPCRs) that enable optogenetic control over the major heterotrimeric G-protein signaling pathways in animal cells. As such, opsins have potential applications in both biomedical research and therapy. Selecting the opsin with the best balance of activity and selectivity for a given application requires knowing their ability to couple to a full range of relevant Gα subunits. We present the GsX assay, a set of tools based on chimeric Gs subunits that transduce coupling of opsins to diverse G proteins into increases in cAMP levels,  measured with a real-time reporter in living cells. We use this assay to compare coupling to Gi/o/t across a panel of natural and chimeric opsins selected for potential application in gene therapy for retinal degeneration. Results Of the opsins tested, wild-type human rod opsin had the highest activity for chimeric Gs proxies for Gi and Gt (Gsi and Gst) and was matched in Go proxy (Gso) activity only by a human rod opsin/scallop opsin chimera. Rod opsin drove roughly equivalent responses via Gsi, Gso, and Gst, while cone opsins showed much lower activities with Gso than Gsi or Gst, and a human rod opsin/amphioxus opsin chimera demonstrated higher activity with Gso than with Gsi or Gst. We failed to detect activity for opsin chimeras bearing three intracellular fragments of mGluR6, and observed unexpectedly complex response profiles for scallop and amphioxus opsins thought to be specialized for Go. Conclusions These results identify rod opsin as the most potent non-selective Gi/o/t-coupled opsin, long-wave sensitive cone opsin as the best for selectively activating Gi/t over Go, and a rod opsin/amphioxus opsin chimera as the best choice for selectively activating Go over Gi/t.
topic Optogenetics
Opsin
GPCR
GalphaO
Retinal degeneration
Gene therapy
url http://link.springer.com/article/10.1186/s12915-017-0475-2
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