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Super-resolution microscopy compatible fluorescent probes reveal endogenous glucagon-like peptide-1 receptor distribution and dynamics

Authors :
Shugo Sasaki
Julia Ast
Daniela Nasteska
Fiona B. Ashford
Andrea Bacon
Zania Stamataki
Tom Podewin
Alejandra Tomas
Nicholas H. F. Fine
David J. Hodson
Giuseppe D'Agostino
Maria Lucey
Elisa D’Este
Christopher A. Reissaus
Amelia K. Linnemann
Stefan Trapp
Zsombor Koszegi
Johannes Broichhagen
Ben Jones
Kai Johnsson
Daniel I. Brierley
Francis C. Lynn
Benoit Hastoy
Anastasia Arvaniti
Frank Reimann
Davide Calebiro
Ast, Julia [0000-0002-0039-4762]
Fine, Nicholas H F [0000-0003-2343-8534]
Nasteska, Daniela [0000-0002-8996-5102]
Stamataki, Zania [0000-0003-3823-4497]
Sasaki, Shugo [0000-0002-3696-7809]
Brierley, Daniel I [0000-0002-4360-2648]
Hastoy, Benoit [0000-0003-1244-7857]
D'Agostino, Giuseppe [0000-0002-3502-4251]
Reimann, Frank [0000-0001-9399-6377]
Lynn, Francis C [0000-0001-9318-1063]
Linnemann, Amelia K [0000-0001-7356-4876]
Calebiro, Davide [0000-0002-3811-1553]
Trapp, Stefan [0000-0003-0665-4948]
Johnsson, Kai [0000-0002-8002-1981]
Podewin, Tom [0000-0002-1632-5104]
Broichhagen, Johannes [0000-0003-3084-6595]
Hodson, David J [0000-0002-8641-8568]
Apollo - University of Cambridge Repository
Medical Research Council (MRC)
Fine, Nicholas H. F. [0000-0003-2343-8534]
Brierley, Daniel I. [0000-0002-4360-2648]
D’Agostino, Giuseppe [0000-0002-3502-4251]
Lynn, Francis C. [0000-0001-9318-1063]
Linnemann, Amelia K. [0000-0001-7356-4876]
Hodson, David J. [0000-0002-8641-8568]
Fine, Nicholas HF [0000-0003-2343-8534]
Source :
Nature Communications, Vol 11, Iss 1, Pp 1-18 (2020), Nature Communications, Ast, J, Arvaniti, A, Fine, N H F, Nasteska, D, Ashford, F B, Stamataki, Z, Koszegi, Z, Bacon, A, Jones, B J, Lucey, M A, Sasaki, S, Brierley, D I, Hastoy, B, Tomas, A, D'Agostino, G, Reimann, F, Lynn, F C, Reissaus, C A, Linnemann, A K, D'Este, E, Calebiro, D, Trapp, S, Johnsson, K, Podewin, T, Broichhagen, J & Hodson, D J 2020, ' Super-resolution microscopy compatible fluorescent probes reveal endogenous glucagon-like peptide-1 receptor distribution and dynamics ', Nature Communications, vol. 11, no. 1, 467, pp. 467 . https://doi.org/10.1038/s41467-020-14309-w
Publication Year :
2020
Publisher :
Nature Publishing Group, 2020.

Abstract

The glucagon-like peptide-1 receptor (GLP1R) is a class B G protein-coupled receptor (GPCR) involved in metabolism. Presently, its visualization is limited to genetic manipulation, antibody detection or the use of probes that stimulate receptor activation. Herein, we present LUXendin645, a far-red fluorescent GLP1R antagonistic peptide label. LUXendin645 produces intense and specific membrane labeling throughout live and fixed tissue. GLP1R signaling can additionally be evoked when the receptor is allosterically modulated in the presence of LUXendin645. Using LUXendin645 and LUXendin651, we describe islet, brain and hESC-derived β-like cell GLP1R expression patterns, reveal higher-order GLP1R organization including membrane nanodomains, and track single receptor subpopulations. We furthermore show that the LUXendin backbone can be optimized for intravital two-photon imaging by installing a red fluorophore. Thus, our super-resolution compatible labeling probes allow visualization of endogenous GLP1R, and provide insight into class B GPCR distribution and dynamics both in vitro and in vivo.<br />Glucagon-like peptide-1 receptor is an important regulator of appetite and glucose homeostasis. Here the authors describe super-resolution microscopy and in vivo imaging compatible fluorescent probes, which reveal endogenous glucagon-like peptide-1 receptor distribution and dynamics in islets and brain.

Details

Language :
English
ISSN :
20411723
Volume :
11
Issue :
1
Database :
OpenAIRE
Journal :
Nature Communications
Accession number :
edsair.doi.dedup.....c39bcef7b82d9b4f5c53076b4bcbaa9a
Full Text :
https://doi.org/10.1038/s41467-020-14309-w