Evaluation of a Novel Hexavalent Humanized Anti-IGF-1R Antibody and Its Bivalent Parental IgG in Diverse Cancer Cell Lines

A major mechanism of monoclonal antibodies that selectively target the insulin-like growth factor type 1 receptor (IGF-1R) to inhibit tumor growth is by downregulating the receptor, regardless whether they are capable (antagonistic) or incapable (agonistic) of blocking the binding of cognate ligands...

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Autores principales: Chang, Chien-Hsing, Wang, Yang, Trisal, Preeti, Li, Rongxiu, Rossi, Diane L., Nair, Anju, Gupta, Pankaj, Losman, Michele, Cardillo, Thomas M., Rossi, Edmund A., Goldenberg, David M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3432068/
https://www.ncbi.nlm.nih.gov/pubmed/22952934
http://dx.doi.org/10.1371/journal.pone.0044235
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author Chang, Chien-Hsing
Wang, Yang
Trisal, Preeti
Li, Rongxiu
Rossi, Diane L.
Nair, Anju
Gupta, Pankaj
Losman, Michele
Cardillo, Thomas M.
Rossi, Edmund A.
Goldenberg, David M.
author_facet Chang, Chien-Hsing
Wang, Yang
Trisal, Preeti
Li, Rongxiu
Rossi, Diane L.
Nair, Anju
Gupta, Pankaj
Losman, Michele
Cardillo, Thomas M.
Rossi, Edmund A.
Goldenberg, David M.
author_sort Chang, Chien-Hsing
collection PubMed
description A major mechanism of monoclonal antibodies that selectively target the insulin-like growth factor type 1 receptor (IGF-1R) to inhibit tumor growth is by downregulating the receptor, regardless whether they are capable (antagonistic) or incapable (agonistic) of blocking the binding of cognate ligands. We have developed and characterized a novel agonistic anti-IGF-1R humanized antibody, hR1, and used the Dock-and-Lock (DNL) method to construct Hex-hR1, the first multivalent antibody comprising 6 functional Fabs of hR1, with the aim of enhancing potency of hR1. Based on cross-blocking experiments, hR1 recognizes a region of cysteine-rich domain on the α-subunit, different from the epitopes mapped for existing anti-IGF-1R antibodies, yet hR1 is similar to other anti-IGF-1R antibodies in downregulating IGF-1R and inhibiting proliferation, colony formation, or invasion of selected cancer cell lines in vitro, as well as suppressing growth of the RH-30 rhabdomyosarcoma xenograft in nude mice when combined with the mTOR inhibitor, rapamycin. Hex-hR1 and hR1 are generally comparable in their bioactivities under the in-intro and in-vivo conditions investigated. Nevertheless, in selective experiments involving a direct comparison of potency, Hex-hR1 demonstrated a stronger effect on inhibiting cell proliferation stimulated by IGF-1 and could effectively downregulate IGF-1R at a concentration as low as 20 pM.
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spelling pubmed-34320682012-09-05 Evaluation of a Novel Hexavalent Humanized Anti-IGF-1R Antibody and Its Bivalent Parental IgG in Diverse Cancer Cell Lines Chang, Chien-Hsing Wang, Yang Trisal, Preeti Li, Rongxiu Rossi, Diane L. Nair, Anju Gupta, Pankaj Losman, Michele Cardillo, Thomas M. Rossi, Edmund A. Goldenberg, David M. PLoS One Research Article A major mechanism of monoclonal antibodies that selectively target the insulin-like growth factor type 1 receptor (IGF-1R) to inhibit tumor growth is by downregulating the receptor, regardless whether they are capable (antagonistic) or incapable (agonistic) of blocking the binding of cognate ligands. We have developed and characterized a novel agonistic anti-IGF-1R humanized antibody, hR1, and used the Dock-and-Lock (DNL) method to construct Hex-hR1, the first multivalent antibody comprising 6 functional Fabs of hR1, with the aim of enhancing potency of hR1. Based on cross-blocking experiments, hR1 recognizes a region of cysteine-rich domain on the α-subunit, different from the epitopes mapped for existing anti-IGF-1R antibodies, yet hR1 is similar to other anti-IGF-1R antibodies in downregulating IGF-1R and inhibiting proliferation, colony formation, or invasion of selected cancer cell lines in vitro, as well as suppressing growth of the RH-30 rhabdomyosarcoma xenograft in nude mice when combined with the mTOR inhibitor, rapamycin. Hex-hR1 and hR1 are generally comparable in their bioactivities under the in-intro and in-vivo conditions investigated. Nevertheless, in selective experiments involving a direct comparison of potency, Hex-hR1 demonstrated a stronger effect on inhibiting cell proliferation stimulated by IGF-1 and could effectively downregulate IGF-1R at a concentration as low as 20 pM. Public Library of Science 2012-08-31 /pmc/articles/PMC3432068/ /pubmed/22952934 http://dx.doi.org/10.1371/journal.pone.0044235 Text en © 2012 Chang et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Chang, Chien-Hsing
Wang, Yang
Trisal, Preeti
Li, Rongxiu
Rossi, Diane L.
Nair, Anju
Gupta, Pankaj
Losman, Michele
Cardillo, Thomas M.
Rossi, Edmund A.
Goldenberg, David M.
Evaluation of a Novel Hexavalent Humanized Anti-IGF-1R Antibody and Its Bivalent Parental IgG in Diverse Cancer Cell Lines
title Evaluation of a Novel Hexavalent Humanized Anti-IGF-1R Antibody and Its Bivalent Parental IgG in Diverse Cancer Cell Lines
title_full Evaluation of a Novel Hexavalent Humanized Anti-IGF-1R Antibody and Its Bivalent Parental IgG in Diverse Cancer Cell Lines
title_fullStr Evaluation of a Novel Hexavalent Humanized Anti-IGF-1R Antibody and Its Bivalent Parental IgG in Diverse Cancer Cell Lines
title_full_unstemmed Evaluation of a Novel Hexavalent Humanized Anti-IGF-1R Antibody and Its Bivalent Parental IgG in Diverse Cancer Cell Lines
title_short Evaluation of a Novel Hexavalent Humanized Anti-IGF-1R Antibody and Its Bivalent Parental IgG in Diverse Cancer Cell Lines
title_sort evaluation of a novel hexavalent humanized anti-igf-1r antibody and its bivalent parental igg in diverse cancer cell lines
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3432068/
https://www.ncbi.nlm.nih.gov/pubmed/22952934
http://dx.doi.org/10.1371/journal.pone.0044235
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