Identification of a New Epitope in uPAR as a Target for the Cancer Therapeutic Monoclonal Antibody ATN-658, a Structural Homolog of the uPAR Binding Integrin CD11b (αM)

The urokinase plasminogen activator receptor (uPAR) plays a role in tumor progression and has been proposed as a target for the treatment of cancer. We recently described the development of a novel humanized monoclonal antibody that targets uPAR and has anti-tumor activity in multiple xenograft anim...

Descripción completa

Detalles Bibliográficos
Autores principales: Xu, Xiang, Cai, Yuan, Wei, Ying, Donate, Fernando, Juarez, Jose, Parry, Graham, Chen, Liqing, Meehan, Edward J., Ahn, Richard W., Ugolkov, Andrey, Dubrovskyi, Oleksii, O'Halloran, Thomas V., Huang, Mingdong, Mazar, Andrew P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3897428/
https://www.ncbi.nlm.nih.gov/pubmed/24465541
http://dx.doi.org/10.1371/journal.pone.0085349
_version_ 1782300231691403264
author Xu, Xiang
Cai, Yuan
Wei, Ying
Donate, Fernando
Juarez, Jose
Parry, Graham
Chen, Liqing
Meehan, Edward J.
Ahn, Richard W.
Ugolkov, Andrey
Dubrovskyi, Oleksii
O'Halloran, Thomas V.
Huang, Mingdong
Mazar, Andrew P.
author_facet Xu, Xiang
Cai, Yuan
Wei, Ying
Donate, Fernando
Juarez, Jose
Parry, Graham
Chen, Liqing
Meehan, Edward J.
Ahn, Richard W.
Ugolkov, Andrey
Dubrovskyi, Oleksii
O'Halloran, Thomas V.
Huang, Mingdong
Mazar, Andrew P.
author_sort Xu, Xiang
collection PubMed
description The urokinase plasminogen activator receptor (uPAR) plays a role in tumor progression and has been proposed as a target for the treatment of cancer. We recently described the development of a novel humanized monoclonal antibody that targets uPAR and has anti-tumor activity in multiple xenograft animal tumor models. This antibody, ATN-658, does not inhibit ligand binding (i.e. uPA and vitronectin) to uPAR and its mechanism of action remains unclear. As a first step in understanding the anti-tumor activity of ATN-658, we set out to identify the epitope on uPAR to which ATN-658 binds. Guided by comparisons between primate and human uPAR, epitope mapping studies were performed using several orthogonal techniques. Systematic site directed and alanine scanning mutagenesis identified the region of aa 268–275 of uPAR as the epitope for ATN-658. No known function has previously been attributed to this epitope Structural insights into epitope recognition were obtained from structural studies of the Fab fragment of ATN-658 bound to uPAR. The structure shows that the ATN-658 binds to the DIII domain of uPAR, close to the C-terminus of the receptor, corroborating the epitope mapping results. Intriguingly, when bound to uPAR, the complementarity determining region (CDR) regions of ATN-658 closely mimic the binding regions of the integrin CD11b (αM), a previously identified uPAR ligand thought to be involved in leukocyte rolling, migration and complement fixation with no known role in tumor progression of solid tumors. These studies reveal a new functional epitope on uPAR involved in tumor progression and demonstrate a previously unrecognized strategy for the therapeutic targeting of uPAR.
format Online
Article
Text
id pubmed-3897428
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-38974282014-01-24 Identification of a New Epitope in uPAR as a Target for the Cancer Therapeutic Monoclonal Antibody ATN-658, a Structural Homolog of the uPAR Binding Integrin CD11b (αM) Xu, Xiang Cai, Yuan Wei, Ying Donate, Fernando Juarez, Jose Parry, Graham Chen, Liqing Meehan, Edward J. Ahn, Richard W. Ugolkov, Andrey Dubrovskyi, Oleksii O'Halloran, Thomas V. Huang, Mingdong Mazar, Andrew P. PLoS One Research Article The urokinase plasminogen activator receptor (uPAR) plays a role in tumor progression and has been proposed as a target for the treatment of cancer. We recently described the development of a novel humanized monoclonal antibody that targets uPAR and has anti-tumor activity in multiple xenograft animal tumor models. This antibody, ATN-658, does not inhibit ligand binding (i.e. uPA and vitronectin) to uPAR and its mechanism of action remains unclear. As a first step in understanding the anti-tumor activity of ATN-658, we set out to identify the epitope on uPAR to which ATN-658 binds. Guided by comparisons between primate and human uPAR, epitope mapping studies were performed using several orthogonal techniques. Systematic site directed and alanine scanning mutagenesis identified the region of aa 268–275 of uPAR as the epitope for ATN-658. No known function has previously been attributed to this epitope Structural insights into epitope recognition were obtained from structural studies of the Fab fragment of ATN-658 bound to uPAR. The structure shows that the ATN-658 binds to the DIII domain of uPAR, close to the C-terminus of the receptor, corroborating the epitope mapping results. Intriguingly, when bound to uPAR, the complementarity determining region (CDR) regions of ATN-658 closely mimic the binding regions of the integrin CD11b (αM), a previously identified uPAR ligand thought to be involved in leukocyte rolling, migration and complement fixation with no known role in tumor progression of solid tumors. These studies reveal a new functional epitope on uPAR involved in tumor progression and demonstrate a previously unrecognized strategy for the therapeutic targeting of uPAR. Public Library of Science 2014-01-21 /pmc/articles/PMC3897428/ /pubmed/24465541 http://dx.doi.org/10.1371/journal.pone.0085349 Text en © 2014 Xu 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
Xu, Xiang
Cai, Yuan
Wei, Ying
Donate, Fernando
Juarez, Jose
Parry, Graham
Chen, Liqing
Meehan, Edward J.
Ahn, Richard W.
Ugolkov, Andrey
Dubrovskyi, Oleksii
O'Halloran, Thomas V.
Huang, Mingdong
Mazar, Andrew P.
Identification of a New Epitope in uPAR as a Target for the Cancer Therapeutic Monoclonal Antibody ATN-658, a Structural Homolog of the uPAR Binding Integrin CD11b (αM)
title Identification of a New Epitope in uPAR as a Target for the Cancer Therapeutic Monoclonal Antibody ATN-658, a Structural Homolog of the uPAR Binding Integrin CD11b (αM)
title_full Identification of a New Epitope in uPAR as a Target for the Cancer Therapeutic Monoclonal Antibody ATN-658, a Structural Homolog of the uPAR Binding Integrin CD11b (αM)
title_fullStr Identification of a New Epitope in uPAR as a Target for the Cancer Therapeutic Monoclonal Antibody ATN-658, a Structural Homolog of the uPAR Binding Integrin CD11b (αM)
title_full_unstemmed Identification of a New Epitope in uPAR as a Target for the Cancer Therapeutic Monoclonal Antibody ATN-658, a Structural Homolog of the uPAR Binding Integrin CD11b (αM)
title_short Identification of a New Epitope in uPAR as a Target for the Cancer Therapeutic Monoclonal Antibody ATN-658, a Structural Homolog of the uPAR Binding Integrin CD11b (αM)
title_sort identification of a new epitope in upar as a target for the cancer therapeutic monoclonal antibody atn-658, a structural homolog of the upar binding integrin cd11b (αm)
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3897428/
https://www.ncbi.nlm.nih.gov/pubmed/24465541
http://dx.doi.org/10.1371/journal.pone.0085349
work_keys_str_mv AT xuxiang identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT caiyuan identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT weiying identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT donatefernando identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT juarezjose identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT parrygraham identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT chenliqing identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT meehanedwardj identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT ahnrichardw identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT ugolkovandrey identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT dubrovskyioleksii identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT ohalloranthomasv identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT huangmingdong identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam
AT mazarandrewp identificationofanewepitopeinuparasatargetforthecancertherapeuticmonoclonalantibodyatn658astructuralhomologoftheuparbindingintegrincd11bam

Ejemplares similares