Calcineurin A versus NS5A-TP2/HD Domain Containing 2: A Case Study of Site-directed Low-frequency Random Mutagenesis for Dissecting Target Specificity of Peptide Aptamers

We previously identified a peptide aptamer (named R5G42) via functional selection for its capacity to slow cell proliferation. A yeast two-hybrid screen of human cDNA libraries, using R5G42 as “bait,” allowed the identification of two binding proteins with very different functions: calcineurin A (Cn...

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Autores principales: Dibenedetto, Silvia, Cluet, David, Stebe, Pierre-Nicolas, Baumle, Véronique, Léault, Jérémie, Terreux, Raphaël, Bickle, Marc, Chassey, Benoit D. E., Mikaelian, Ivan, Colas, Pierre, Spichty, Martin, Zoli, Michele, Rudkin, Brian B.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The American Society for Biochemistry and Molecular Biology 2013
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3708177/
https://www.ncbi.nlm.nih.gov/pubmed/23579184
http://dx.doi.org/10.1074/mcp.M112.024612
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author Dibenedetto, Silvia
Cluet, David
Stebe, Pierre-Nicolas
Baumle, Véronique
Léault, Jérémie
Terreux, Raphaël
Bickle, Marc
Chassey, Benoit D. E.
Mikaelian, Ivan
Colas, Pierre
Spichty, Martin
Zoli, Michele
Rudkin, Brian B.
author_facet Dibenedetto, Silvia
Cluet, David
Stebe, Pierre-Nicolas
Baumle, Véronique
Léault, Jérémie
Terreux, Raphaël
Bickle, Marc
Chassey, Benoit D. E.
Mikaelian, Ivan
Colas, Pierre
Spichty, Martin
Zoli, Michele
Rudkin, Brian B.
author_sort Dibenedetto, Silvia
collection PubMed
description We previously identified a peptide aptamer (named R5G42) via functional selection for its capacity to slow cell proliferation. A yeast two-hybrid screen of human cDNA libraries, using R5G42 as “bait,” allowed the identification of two binding proteins with very different functions: calcineurin A (CnA) (PP2B/PPP3CA), a protein phosphatase well characterized for its role in the immune response, and NS5A-TP2/HD domain containing 2, a much less studied protein induced subsequent to hepatitis C virus non-structural protein 5A expression in HepG2 hepatocellular carcinoma cells, with no known activity. Our objective in the present study was to dissect the dual target specificity of R5G42 in order to have tools with which to better characterize the actions of the peptide aptamers toward their individual targets. This was achieved through the selection of random mutants of the variable loop, derived from R5G42, evaluating their specificity toward CnA and NS5A-TP2 and analyzing their sequence. An interdisciplinary approach involving biomolecular computer simulations with integration of the sequence data and yeast two-hybrid binding phenotypes of these mutants yielded two structurally distinct conformers affording the potential molecular basis of the binding diversity of R5G42. Evaluation of the biological impact of CnA- versus NS5A-TP2-specific peptide aptamers indicated that although both contributed to the anti-proliferative effect of R5G42, CnA-binding was essential to stimulate the nuclear translocation of nuclear factor of activated T cells, indicative of the activation of endogenous CnA. By dissecting the target specificity of R5G42, we have generated novel tools with which to study each target individually. Apta-C8 is capable of directly activating CnA independent of binding to NS5A-TP2 and will be an important tool in studying the role of CnA activation in the regulation of different signaling pathways, whereas Apta-E1 will allow dissection of the function of NS5A-TP2, serving as an example of the usefulness of peptide aptamer technology for investigating signaling pathways.
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spelling pubmed-37081772013-07-19 Calcineurin A versus NS5A-TP2/HD Domain Containing 2: A Case Study of Site-directed Low-frequency Random Mutagenesis for Dissecting Target Specificity of Peptide Aptamers Dibenedetto, Silvia Cluet, David Stebe, Pierre-Nicolas Baumle, Véronique Léault, Jérémie Terreux, Raphaël Bickle, Marc Chassey, Benoit D. E. Mikaelian, Ivan Colas, Pierre Spichty, Martin Zoli, Michele Rudkin, Brian B. Mol Cell Proteomics Research We previously identified a peptide aptamer (named R5G42) via functional selection for its capacity to slow cell proliferation. A yeast two-hybrid screen of human cDNA libraries, using R5G42 as “bait,” allowed the identification of two binding proteins with very different functions: calcineurin A (CnA) (PP2B/PPP3CA), a protein phosphatase well characterized for its role in the immune response, and NS5A-TP2/HD domain containing 2, a much less studied protein induced subsequent to hepatitis C virus non-structural protein 5A expression in HepG2 hepatocellular carcinoma cells, with no known activity. Our objective in the present study was to dissect the dual target specificity of R5G42 in order to have tools with which to better characterize the actions of the peptide aptamers toward their individual targets. This was achieved through the selection of random mutants of the variable loop, derived from R5G42, evaluating their specificity toward CnA and NS5A-TP2 and analyzing their sequence. An interdisciplinary approach involving biomolecular computer simulations with integration of the sequence data and yeast two-hybrid binding phenotypes of these mutants yielded two structurally distinct conformers affording the potential molecular basis of the binding diversity of R5G42. Evaluation of the biological impact of CnA- versus NS5A-TP2-specific peptide aptamers indicated that although both contributed to the anti-proliferative effect of R5G42, CnA-binding was essential to stimulate the nuclear translocation of nuclear factor of activated T cells, indicative of the activation of endogenous CnA. By dissecting the target specificity of R5G42, we have generated novel tools with which to study each target individually. Apta-C8 is capable of directly activating CnA independent of binding to NS5A-TP2 and will be an important tool in studying the role of CnA activation in the regulation of different signaling pathways, whereas Apta-E1 will allow dissection of the function of NS5A-TP2, serving as an example of the usefulness of peptide aptamer technology for investigating signaling pathways. The American Society for Biochemistry and Molecular Biology 2013-07 2013-04-10 /pmc/articles/PMC3708177/ /pubmed/23579184 http://dx.doi.org/10.1074/mcp.M112.024612 Text en © 2013 by The American Society for Biochemistry and Molecular Biology, Inc. Author's Choice—Final version full access. Creative Commons Attribution Unported License (http://creativecommons.org/licenses/by/3.0/) applies to Author Choice Articles
spellingShingle Research
Dibenedetto, Silvia
Cluet, David
Stebe, Pierre-Nicolas
Baumle, Véronique
Léault, Jérémie
Terreux, Raphaël
Bickle, Marc
Chassey, Benoit D. E.
Mikaelian, Ivan
Colas, Pierre
Spichty, Martin
Zoli, Michele
Rudkin, Brian B.
Calcineurin A versus NS5A-TP2/HD Domain Containing 2: A Case Study of Site-directed Low-frequency Random Mutagenesis for Dissecting Target Specificity of Peptide Aptamers
title Calcineurin A versus NS5A-TP2/HD Domain Containing 2: A Case Study of Site-directed Low-frequency Random Mutagenesis for Dissecting Target Specificity of Peptide Aptamers
title_full Calcineurin A versus NS5A-TP2/HD Domain Containing 2: A Case Study of Site-directed Low-frequency Random Mutagenesis for Dissecting Target Specificity of Peptide Aptamers
title_fullStr Calcineurin A versus NS5A-TP2/HD Domain Containing 2: A Case Study of Site-directed Low-frequency Random Mutagenesis for Dissecting Target Specificity of Peptide Aptamers
title_full_unstemmed Calcineurin A versus NS5A-TP2/HD Domain Containing 2: A Case Study of Site-directed Low-frequency Random Mutagenesis for Dissecting Target Specificity of Peptide Aptamers
title_short Calcineurin A versus NS5A-TP2/HD Domain Containing 2: A Case Study of Site-directed Low-frequency Random Mutagenesis for Dissecting Target Specificity of Peptide Aptamers
title_sort calcineurin a versus ns5a-tp2/hd domain containing 2: a case study of site-directed low-frequency random mutagenesis for dissecting target specificity of peptide aptamers
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3708177/
https://www.ncbi.nlm.nih.gov/pubmed/23579184
http://dx.doi.org/10.1074/mcp.M112.024612
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