A Multipronged Unbiased Strategy Guides the Development of an Anti-EGFR/EPHA2–Bispecific Antibody for Combination Cancer Therapy

PURPOSE: Accumulating analyses of pro-oncogenic molecular mechanisms triggered a rapid development of targeted cancer therapies. Although many of these treatments produce impressive initial responses, eventual resistance onset is practically unavoidable. One of the main approaches for preventing thi...

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Autores principales: El Zawily, Amr, Vizeacoumar, Frederick S., Dahiya, Renuka, Banerjee, Sara L., Bhanumathy, Kalpana K., Elhasasna, Hussain, Hanover, Glinton, Sharpe, Jessica C., Sanchez, Malkon G., Greidanus, Paul, Stacey, R. Greg, Moon, Kyung-Mee, Alexandrov, Ilya, Himanen, Juha P., Nikolov, Dimitar B., Fonge, Humphrey, White, Aaron P., Foster, Leonard J., Wang, Bingcheng, Toosi, Behzad M., Bisson, Nicolas, Mirzabekov, Tajib A., Vizeacoumar, Franco J., Freywald, Andrew
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Association for Cancer Research 2023
Materias:
Translational Cancer Mechanisms and Therapy
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10345963/
https://www.ncbi.nlm.nih.gov/pubmed/36976175
http://dx.doi.org/10.1158/1078-0432.CCR-22-2535
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author El Zawily, Amr
Vizeacoumar, Frederick S.
Dahiya, Renuka
Banerjee, Sara L.
Bhanumathy, Kalpana K.
Elhasasna, Hussain
Hanover, Glinton
Sharpe, Jessica C.
Sanchez, Malkon G.
Greidanus, Paul
Stacey, R. Greg
Moon, Kyung-Mee
Alexandrov, Ilya
Himanen, Juha P.
Nikolov, Dimitar B.
Fonge, Humphrey
White, Aaron P.
Foster, Leonard J.
Wang, Bingcheng
Toosi, Behzad M.
Bisson, Nicolas
Mirzabekov, Tajib A.
Vizeacoumar, Franco J.
Freywald, Andrew
author_facet El Zawily, Amr
Vizeacoumar, Frederick S.
Dahiya, Renuka
Banerjee, Sara L.
Bhanumathy, Kalpana K.
Elhasasna, Hussain
Hanover, Glinton
Sharpe, Jessica C.
Sanchez, Malkon G.
Greidanus, Paul
Stacey, R. Greg
Moon, Kyung-Mee
Alexandrov, Ilya
Himanen, Juha P.
Nikolov, Dimitar B.
Fonge, Humphrey
White, Aaron P.
Foster, Leonard J.
Wang, Bingcheng
Toosi, Behzad M.
Bisson, Nicolas
Mirzabekov, Tajib A.
Vizeacoumar, Franco J.
Freywald, Andrew
author_sort El Zawily, Amr
collection PubMed
description PURPOSE: Accumulating analyses of pro-oncogenic molecular mechanisms triggered a rapid development of targeted cancer therapies. Although many of these treatments produce impressive initial responses, eventual resistance onset is practically unavoidable. One of the main approaches for preventing this refractory condition relies on the implementation of combination therapies. This includes dual-specificity reagents that affect both of their targets with a high level of selectivity. Unfortunately, selection of target combinations for these treatments is often confounded by limitations in our understanding of tumor biology. Here, we describe and validate a multipronged unbiased strategy for predicting optimal co-targets for bispecific therapeutics. EXPERIMENTAL DESIGN: Our strategy integrates ex vivo genome-wide loss-of-function screening, BioID interactome profiling, and gene expression analysis of patient data to identify the best fit co-targets. Final validation of selected target combinations is done in tumorsphere cultures and xenograft models. RESULTS: Integration of our experimental approaches unambiguously pointed toward EGFR and EPHA2 tyrosine kinase receptors as molecules of choice for co-targeting in multiple tumor types. Following this lead, we generated a human bispecific anti-EGFR/EPHA2 antibody that, as predicted, very effectively suppresses tumor growth compared with its prototype anti-EGFR therapeutic antibody, cetuximab. CONCLUSIONS: Our work not only presents a new bispecific antibody with a high potential for being developed into clinically relevant biologics, but more importantly, successfully validates a novel unbiased strategy for selecting biologically optimal target combinations. This is of a significant translational relevance, as such multifaceted unbiased approaches are likely to augment the development of effective combination therapies for cancer treatment. See related commentary by Kumar, p. 2570
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spelling pubmed-103459632023-07-15 A Multipronged Unbiased Strategy Guides the Development of an Anti-EGFR/EPHA2–Bispecific Antibody for Combination Cancer Therapy El Zawily, Amr Vizeacoumar, Frederick S. Dahiya, Renuka Banerjee, Sara L. Bhanumathy, Kalpana K. Elhasasna, Hussain Hanover, Glinton Sharpe, Jessica C. Sanchez, Malkon G. Greidanus, Paul Stacey, R. Greg Moon, Kyung-Mee Alexandrov, Ilya Himanen, Juha P. Nikolov, Dimitar B. Fonge, Humphrey White, Aaron P. Foster, Leonard J. Wang, Bingcheng Toosi, Behzad M. Bisson, Nicolas Mirzabekov, Tajib A. Vizeacoumar, Franco J. Freywald, Andrew Clin Cancer Res Translational Cancer Mechanisms and Therapy PURPOSE: Accumulating analyses of pro-oncogenic molecular mechanisms triggered a rapid development of targeted cancer therapies. Although many of these treatments produce impressive initial responses, eventual resistance onset is practically unavoidable. One of the main approaches for preventing this refractory condition relies on the implementation of combination therapies. This includes dual-specificity reagents that affect both of their targets with a high level of selectivity. Unfortunately, selection of target combinations for these treatments is often confounded by limitations in our understanding of tumor biology. Here, we describe and validate a multipronged unbiased strategy for predicting optimal co-targets for bispecific therapeutics. EXPERIMENTAL DESIGN: Our strategy integrates ex vivo genome-wide loss-of-function screening, BioID interactome profiling, and gene expression analysis of patient data to identify the best fit co-targets. Final validation of selected target combinations is done in tumorsphere cultures and xenograft models. RESULTS: Integration of our experimental approaches unambiguously pointed toward EGFR and EPHA2 tyrosine kinase receptors as molecules of choice for co-targeting in multiple tumor types. Following this lead, we generated a human bispecific anti-EGFR/EPHA2 antibody that, as predicted, very effectively suppresses tumor growth compared with its prototype anti-EGFR therapeutic antibody, cetuximab. CONCLUSIONS: Our work not only presents a new bispecific antibody with a high potential for being developed into clinically relevant biologics, but more importantly, successfully validates a novel unbiased strategy for selecting biologically optimal target combinations. This is of a significant translational relevance, as such multifaceted unbiased approaches are likely to augment the development of effective combination therapies for cancer treatment. See related commentary by Kumar, p. 2570 American Association for Cancer Research 2023-07-14 2023-03-28 /pmc/articles/PMC10345963/ /pubmed/36976175 http://dx.doi.org/10.1158/1078-0432.CCR-22-2535 Text en ©2023 The Authors; Published by the American Association for Cancer Research https://creativecommons.org/licenses/by-nc-nd/4.0/This open access article is distributed under the Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0) license.
spellingShingle Translational Cancer Mechanisms and Therapy
El Zawily, Amr
Vizeacoumar, Frederick S.
Dahiya, Renuka
Banerjee, Sara L.
Bhanumathy, Kalpana K.
Elhasasna, Hussain
Hanover, Glinton
Sharpe, Jessica C.
Sanchez, Malkon G.
Greidanus, Paul
Stacey, R. Greg
Moon, Kyung-Mee
Alexandrov, Ilya
Himanen, Juha P.
Nikolov, Dimitar B.
Fonge, Humphrey
White, Aaron P.
Foster, Leonard J.
Wang, Bingcheng
Toosi, Behzad M.
Bisson, Nicolas
Mirzabekov, Tajib A.
Vizeacoumar, Franco J.
Freywald, Andrew
A Multipronged Unbiased Strategy Guides the Development of an Anti-EGFR/EPHA2–Bispecific Antibody for Combination Cancer Therapy
title A Multipronged Unbiased Strategy Guides the Development of an Anti-EGFR/EPHA2–Bispecific Antibody for Combination Cancer Therapy
title_full A Multipronged Unbiased Strategy Guides the Development of an Anti-EGFR/EPHA2–Bispecific Antibody for Combination Cancer Therapy
title_fullStr A Multipronged Unbiased Strategy Guides the Development of an Anti-EGFR/EPHA2–Bispecific Antibody for Combination Cancer Therapy
title_full_unstemmed A Multipronged Unbiased Strategy Guides the Development of an Anti-EGFR/EPHA2–Bispecific Antibody for Combination Cancer Therapy
title_short A Multipronged Unbiased Strategy Guides the Development of an Anti-EGFR/EPHA2–Bispecific Antibody for Combination Cancer Therapy
title_sort multipronged unbiased strategy guides the development of an anti-egfr/epha2–bispecific antibody for combination cancer therapy
topic Translational Cancer Mechanisms and Therapy
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10345963/
https://www.ncbi.nlm.nih.gov/pubmed/36976175
http://dx.doi.org/10.1158/1078-0432.CCR-22-2535
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