Tripartite split-GFP assay to identify selective intracellular nanobody that suppresses GTPase RHOA subfamily downstream signaling

Strategies based on intracellular expression of artificial binding domains present several advantages over manipulating nucleic acid expression or the use of small molecule inhibitors. Intracellularly-functional nanobodies can be considered as promising macrodrugs to study key signaling pathways by...

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Autores principales: Keller, Laura, Tardy, Claudine, Ligat, Laetitia, Le Pennec, Soazig, Bery, Nicolas, Koraïchi, Faten, Chinestra, Patrick, David, Mélissa, Gence, Rémi, Favre, Gilles, Cabantous, Stéphanie, Olichon, Aurélien
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9433928/
https://www.ncbi.nlm.nih.gov/pubmed/36059552
http://dx.doi.org/10.3389/fimmu.2022.980539
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author Keller, Laura
Tardy, Claudine
Ligat, Laetitia
Le Pennec, Soazig
Bery, Nicolas
Koraïchi, Faten
Chinestra, Patrick
David, Mélissa
Gence, Rémi
Favre, Gilles
Cabantous, Stéphanie
Olichon, Aurélien
author_facet Keller, Laura
Tardy, Claudine
Ligat, Laetitia
Le Pennec, Soazig
Bery, Nicolas
Koraïchi, Faten
Chinestra, Patrick
David, Mélissa
Gence, Rémi
Favre, Gilles
Cabantous, Stéphanie
Olichon, Aurélien
author_sort Keller, Laura
collection PubMed
description Strategies based on intracellular expression of artificial binding domains present several advantages over manipulating nucleic acid expression or the use of small molecule inhibitors. Intracellularly-functional nanobodies can be considered as promising macrodrugs to study key signaling pathways by interfering with protein-protein interactions. With the aim of studying the RAS-related small GTPase RHOA family, we previously isolated, from a synthetic phage display library, nanobodies selective towards the GTP-bound conformation of RHOA subfamily proteins that lack selectivity between the highly conserved RHOA-like and RAC subfamilies of GTPases. To identify RHOA/ROCK pathway inhibitory intracellular nanobodies, we implemented a stringent, subtractive phage display selection towards RHOA-GTP followed by a phenotypic screen based on F-actin fiber loss. Intracellular interaction and intracellular selectivity between RHOA and RAC1 proteins was demonstrated by adapting the sensitive intracellular protein-protein interaction reporter based on the tripartite split-GFP method. This strategy led us to identify a functional intracellular nanobody, hereafter named RH28, that does not cross-react with the close RAC subfamily and blocks/disrupts the RHOA/ROCK signaling pathway in several cell lines without further engineering or functionalization. We confirmed these results by showing, using SPR assays, the high specificity of the RH28 nanobody towards the GTP-bound conformation of RHOA subfamily GTPases. In the metastatic melanoma cell line WM266-4, RH28 expression triggered an elongated cellular phenotype associated with a loss of cellular contraction properties, demonstrating the efficient intracellular blocking of RHOA/B/C proteins downstream interactions without the need of manipulating endogenous gene expression. This work paves the way for future therapeutic strategies based on protein-protein interaction disruption with intracellular antibodies.
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spelling pubmed-94339282022-09-02 Tripartite split-GFP assay to identify selective intracellular nanobody that suppresses GTPase RHOA subfamily downstream signaling Keller, Laura Tardy, Claudine Ligat, Laetitia Le Pennec, Soazig Bery, Nicolas Koraïchi, Faten Chinestra, Patrick David, Mélissa Gence, Rémi Favre, Gilles Cabantous, Stéphanie Olichon, Aurélien Front Immunol Immunology Strategies based on intracellular expression of artificial binding domains present several advantages over manipulating nucleic acid expression or the use of small molecule inhibitors. Intracellularly-functional nanobodies can be considered as promising macrodrugs to study key signaling pathways by interfering with protein-protein interactions. With the aim of studying the RAS-related small GTPase RHOA family, we previously isolated, from a synthetic phage display library, nanobodies selective towards the GTP-bound conformation of RHOA subfamily proteins that lack selectivity between the highly conserved RHOA-like and RAC subfamilies of GTPases. To identify RHOA/ROCK pathway inhibitory intracellular nanobodies, we implemented a stringent, subtractive phage display selection towards RHOA-GTP followed by a phenotypic screen based on F-actin fiber loss. Intracellular interaction and intracellular selectivity between RHOA and RAC1 proteins was demonstrated by adapting the sensitive intracellular protein-protein interaction reporter based on the tripartite split-GFP method. This strategy led us to identify a functional intracellular nanobody, hereafter named RH28, that does not cross-react with the close RAC subfamily and blocks/disrupts the RHOA/ROCK signaling pathway in several cell lines without further engineering or functionalization. We confirmed these results by showing, using SPR assays, the high specificity of the RH28 nanobody towards the GTP-bound conformation of RHOA subfamily GTPases. In the metastatic melanoma cell line WM266-4, RH28 expression triggered an elongated cellular phenotype associated with a loss of cellular contraction properties, demonstrating the efficient intracellular blocking of RHOA/B/C proteins downstream interactions without the need of manipulating endogenous gene expression. This work paves the way for future therapeutic strategies based on protein-protein interaction disruption with intracellular antibodies. Frontiers Media S.A. 2022-08-18 /pmc/articles/PMC9433928/ /pubmed/36059552 http://dx.doi.org/10.3389/fimmu.2022.980539 Text en Copyright © 2022 Keller, Tardy, Ligat, Le Pennec, Bery, Koraïchi, Chinestra, David, Gence, Favre, Cabantous and Olichon https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Keller, Laura
Tardy, Claudine
Ligat, Laetitia
Le Pennec, Soazig
Bery, Nicolas
Koraïchi, Faten
Chinestra, Patrick
David, Mélissa
Gence, Rémi
Favre, Gilles
Cabantous, Stéphanie
Olichon, Aurélien
Tripartite split-GFP assay to identify selective intracellular nanobody that suppresses GTPase RHOA subfamily downstream signaling
title Tripartite split-GFP assay to identify selective intracellular nanobody that suppresses GTPase RHOA subfamily downstream signaling
title_full Tripartite split-GFP assay to identify selective intracellular nanobody that suppresses GTPase RHOA subfamily downstream signaling
title_fullStr Tripartite split-GFP assay to identify selective intracellular nanobody that suppresses GTPase RHOA subfamily downstream signaling
title_full_unstemmed Tripartite split-GFP assay to identify selective intracellular nanobody that suppresses GTPase RHOA subfamily downstream signaling
title_short Tripartite split-GFP assay to identify selective intracellular nanobody that suppresses GTPase RHOA subfamily downstream signaling
title_sort tripartite split-gfp assay to identify selective intracellular nanobody that suppresses gtpase rhoa subfamily downstream signaling
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9433928/
https://www.ncbi.nlm.nih.gov/pubmed/36059552
http://dx.doi.org/10.3389/fimmu.2022.980539
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