In Vivo Human Single‐Chain Fragment Variable Phage Display‐Assisted Identification of Galectin‐3 as a New Biomarker of Atherosclerosis

BACKGROUND: Atherosclerosis is a complex pathology in which dysfunctional endothelium, activated leucocytes, macrophages, and lipid‐laden foam cells are implicated, and in which plaque disruption is driven by many putative actors. This study aimed to identify accurate targetable biomarkers using new...

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Autores principales: Hemadou, Audrey, Fontayne, Alexandre, Laroche‐Traineau, Jeanny, Ottones, Florence, Mondon, Philippe, Claverol, Stéphane, Ducasse, Éric, Sanchez, Stéphane, Mohamad, Sarah, Lorenzato, Cyril, Duonor‐Cerutti, Martine, Clofent‐Sanchez, Gisèle, Jacobin‐Valat, Marie‐Josée
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2021
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8649142/
https://www.ncbi.nlm.nih.gov/pubmed/34569248
http://dx.doi.org/10.1161/JAHA.120.016287
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author Hemadou, Audrey
Fontayne, Alexandre
Laroche‐Traineau, Jeanny
Ottones, Florence
Mondon, Philippe
Claverol, Stéphane
Ducasse, Éric
Sanchez, Stéphane
Mohamad, Sarah
Lorenzato, Cyril
Duonor‐Cerutti, Martine
Clofent‐Sanchez, Gisèle
Jacobin‐Valat, Marie‐Josée
author_facet Hemadou, Audrey
Fontayne, Alexandre
Laroche‐Traineau, Jeanny
Ottones, Florence
Mondon, Philippe
Claverol, Stéphane
Ducasse, Éric
Sanchez, Stéphane
Mohamad, Sarah
Lorenzato, Cyril
Duonor‐Cerutti, Martine
Clofent‐Sanchez, Gisèle
Jacobin‐Valat, Marie‐Josée
author_sort Hemadou, Audrey
collection PubMed
description BACKGROUND: Atherosclerosis is a complex pathology in which dysfunctional endothelium, activated leucocytes, macrophages, and lipid‐laden foam cells are implicated, and in which plaque disruption is driven by many putative actors. This study aimed to identify accurate targetable biomarkers using new in vivo approaches to propose tools for improved diagnosis and treatment. METHODS AND RESULTS: Human scFv (single‐chain fragment variable) selected by in vivo phage display in a rabbit model of atherosclerosis was reformatted as scFv fused to the scFv‐Fc (single‐chain fragment variable fused to the crystallizable fragment of immunoglobulin G format) antibodies. Their reactivity was tested using flow cytometry and immunoassays, and aorta sections from animal models and human carotid and coronary artery specimens. A pool of atherosclerotic proteins from human endarterectomies was co‐immunoprecipitated with the selected scFv‐Fc followed by mass spectrometry for target identification. Near‐infrared fluorescence imaging was performed in Apoe (−/−) mice after injection of an Alexa Fluor 647–labeled scFv‐Fc‐2c antibody produced in a baculovirus system with 2 additional cysteine residues (ie, 2c) for future coupling to nano‐objects for theranostic applications. One scFv‐Fc clone (P3) displayed the highest cross‐reactivity against atherosclerotic lesion sections (rabbit, mouse, and human) and was chosen for translational development. Mass spectrometry identified galectin‐3, a β‐galactoside‐binding lectin, as the leader target. ELISA and immunofluorescence assays with a commercial anti‐galectin‐3 antibody confirmed this specificity. P3 scFv‐Fc‐2c specifically targeted atherosclerotic plaques in the Apoe (−/−) mouse model. CONCLUSIONS: These results provide evidence that the P3 antibody holds great promise for molecular imaging of atherosclerosis and other inflammatory pathologies involving macrophages. Recently, galectin‐3 was proposed as a high‐value biomarker for the assessment of coronary and carotid atherosclerosis.
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spelling pubmed-86491422022-03-21 In Vivo Human Single‐Chain Fragment Variable Phage Display‐Assisted Identification of Galectin‐3 as a New Biomarker of Atherosclerosis Hemadou, Audrey Fontayne, Alexandre Laroche‐Traineau, Jeanny Ottones, Florence Mondon, Philippe Claverol, Stéphane Ducasse, Éric Sanchez, Stéphane Mohamad, Sarah Lorenzato, Cyril Duonor‐Cerutti, Martine Clofent‐Sanchez, Gisèle Jacobin‐Valat, Marie‐Josée J Am Heart Assoc Original Research BACKGROUND: Atherosclerosis is a complex pathology in which dysfunctional endothelium, activated leucocytes, macrophages, and lipid‐laden foam cells are implicated, and in which plaque disruption is driven by many putative actors. This study aimed to identify accurate targetable biomarkers using new in vivo approaches to propose tools for improved diagnosis and treatment. METHODS AND RESULTS: Human scFv (single‐chain fragment variable) selected by in vivo phage display in a rabbit model of atherosclerosis was reformatted as scFv fused to the scFv‐Fc (single‐chain fragment variable fused to the crystallizable fragment of immunoglobulin G format) antibodies. Their reactivity was tested using flow cytometry and immunoassays, and aorta sections from animal models and human carotid and coronary artery specimens. A pool of atherosclerotic proteins from human endarterectomies was co‐immunoprecipitated with the selected scFv‐Fc followed by mass spectrometry for target identification. Near‐infrared fluorescence imaging was performed in Apoe (−/−) mice after injection of an Alexa Fluor 647–labeled scFv‐Fc‐2c antibody produced in a baculovirus system with 2 additional cysteine residues (ie, 2c) for future coupling to nano‐objects for theranostic applications. One scFv‐Fc clone (P3) displayed the highest cross‐reactivity against atherosclerotic lesion sections (rabbit, mouse, and human) and was chosen for translational development. Mass spectrometry identified galectin‐3, a β‐galactoside‐binding lectin, as the leader target. ELISA and immunofluorescence assays with a commercial anti‐galectin‐3 antibody confirmed this specificity. P3 scFv‐Fc‐2c specifically targeted atherosclerotic plaques in the Apoe (−/−) mouse model. CONCLUSIONS: These results provide evidence that the P3 antibody holds great promise for molecular imaging of atherosclerosis and other inflammatory pathologies involving macrophages. Recently, galectin‐3 was proposed as a high‐value biomarker for the assessment of coronary and carotid atherosclerosis. John Wiley and Sons Inc. 2021-09-25 /pmc/articles/PMC8649142/ /pubmed/34569248 http://dx.doi.org/10.1161/JAHA.120.016287 Text en © 2021 The Authors and LFB Biotechnologies. Published on behalf of the American Heart Association, Inc., by Wiley. https://creativecommons.org/licenses/by-nc/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by-nc/4.0/ (https://creativecommons.org/licenses/by-nc/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited and is not used for commercial purposes.
spellingShingle Original Research
Hemadou, Audrey
Fontayne, Alexandre
Laroche‐Traineau, Jeanny
Ottones, Florence
Mondon, Philippe
Claverol, Stéphane
Ducasse, Éric
Sanchez, Stéphane
Mohamad, Sarah
Lorenzato, Cyril
Duonor‐Cerutti, Martine
Clofent‐Sanchez, Gisèle
Jacobin‐Valat, Marie‐Josée
In Vivo Human Single‐Chain Fragment Variable Phage Display‐Assisted Identification of Galectin‐3 as a New Biomarker of Atherosclerosis
title In Vivo Human Single‐Chain Fragment Variable Phage Display‐Assisted Identification of Galectin‐3 as a New Biomarker of Atherosclerosis
title_full In Vivo Human Single‐Chain Fragment Variable Phage Display‐Assisted Identification of Galectin‐3 as a New Biomarker of Atherosclerosis
title_fullStr In Vivo Human Single‐Chain Fragment Variable Phage Display‐Assisted Identification of Galectin‐3 as a New Biomarker of Atherosclerosis
title_full_unstemmed In Vivo Human Single‐Chain Fragment Variable Phage Display‐Assisted Identification of Galectin‐3 as a New Biomarker of Atherosclerosis
title_short In Vivo Human Single‐Chain Fragment Variable Phage Display‐Assisted Identification of Galectin‐3 as a New Biomarker of Atherosclerosis
title_sort in vivo human single‐chain fragment variable phage display‐assisted identification of galectin‐3 as a new biomarker of atherosclerosis
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8649142/
https://www.ncbi.nlm.nih.gov/pubmed/34569248
http://dx.doi.org/10.1161/JAHA.120.016287
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