Evolution of Bombesin Conjugates for Targeted PET Imaging of Tumors

Bombesin receptors are under intense investigation as molecular targets since they are overexpressed in several prevalent solid tumors. We rationally designed and synthesized a series of modified bombesin (BN) peptide analogs to study the influence of charge and spacers at the N-terminus, as well as...

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Autores principales: Zhang, Hanwen, Abiraj, Keelara, Thorek, Daniel L. J., Waser, Beatrice, Smith-Jones, Peter M., Honer, Michael, Reubi, Jean Claude, Maecke, Helmut R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3443097/
https://www.ncbi.nlm.nih.gov/pubmed/23024746
http://dx.doi.org/10.1371/journal.pone.0044046
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author Zhang, Hanwen
Abiraj, Keelara
Thorek, Daniel L. J.
Waser, Beatrice
Smith-Jones, Peter M.
Honer, Michael
Reubi, Jean Claude
Maecke, Helmut R.
author_facet Zhang, Hanwen
Abiraj, Keelara
Thorek, Daniel L. J.
Waser, Beatrice
Smith-Jones, Peter M.
Honer, Michael
Reubi, Jean Claude
Maecke, Helmut R.
author_sort Zhang, Hanwen
collection PubMed
description Bombesin receptors are under intense investigation as molecular targets since they are overexpressed in several prevalent solid tumors. We rationally designed and synthesized a series of modified bombesin (BN) peptide analogs to study the influence of charge and spacers at the N-terminus, as well as amino acid substitutions, on both receptor binding affinity and pharmacokinetics. This enabled development of a novel (64/67)Cu-labeled BN peptide for PET imaging and targeted radiotherapy of BN receptor-positive tumors. Our results show that N-terminally positively charged peptide ligands had significantly higher affinity to human gastrin releasing peptide receptor (GRPr) than negatively charged or uncharged ligands (IC(50): 3.2±0.5 vs 26.3±3.5 vs 41.5±2.5 nM). The replacement of Nle(14) by Met, and deletion of D-Tyr(6), further resulted in 8-fold higher affinity. Contrary to significant changes to human GRPr binding, modifications at the N-terminal and at the 6(th), 11(th), and 14(th) position of BN induced only slight influences on affinity to mouse GRPr. [Cu(II)]-CPTA-[βAla(11)] BN(7–14) ([Cu(II)]-BZH7) showed the highest internalization rate into PC-3 cells with relatively slow efflux because of its subnanomolar affinity to GRPr. Interestingly, [(64/67)Cu]-BZH7 also displayed similar affinities to the other 2 human BN receptor subtypes. In vivo studies showed that [(64/67)Cu]-BZH7 had a high accumulation in PC-3 xenografts and allowed for clear-cut visualization of the tumor in PET imaging. In addition, a CPTA-glycine derivative, forming a hippurane-type spacer, enhanced kidney clearance of the radiotracer. These data indicate that the species variation of BN receptor plays an important role in screening radiolabeled BN. As well, the positive charge from the metallated complex at the N-terminal significantly increases affinity to human GRPr. Application of these observations enabled the novel ligand [(64/67)Cu]-BZH7 to clearly visualize PC-3 tumors in vivo. This study provides a strong starting point for optimizing radiopeptides for targeting carcinomas that express any of the BN receptor subtypes.
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spelling pubmed-34430972012-09-28 Evolution of Bombesin Conjugates for Targeted PET Imaging of Tumors Zhang, Hanwen Abiraj, Keelara Thorek, Daniel L. J. Waser, Beatrice Smith-Jones, Peter M. Honer, Michael Reubi, Jean Claude Maecke, Helmut R. PLoS One Research Article Bombesin receptors are under intense investigation as molecular targets since they are overexpressed in several prevalent solid tumors. We rationally designed and synthesized a series of modified bombesin (BN) peptide analogs to study the influence of charge and spacers at the N-terminus, as well as amino acid substitutions, on both receptor binding affinity and pharmacokinetics. This enabled development of a novel (64/67)Cu-labeled BN peptide for PET imaging and targeted radiotherapy of BN receptor-positive tumors. Our results show that N-terminally positively charged peptide ligands had significantly higher affinity to human gastrin releasing peptide receptor (GRPr) than negatively charged or uncharged ligands (IC(50): 3.2±0.5 vs 26.3±3.5 vs 41.5±2.5 nM). The replacement of Nle(14) by Met, and deletion of D-Tyr(6), further resulted in 8-fold higher affinity. Contrary to significant changes to human GRPr binding, modifications at the N-terminal and at the 6(th), 11(th), and 14(th) position of BN induced only slight influences on affinity to mouse GRPr. [Cu(II)]-CPTA-[βAla(11)] BN(7–14) ([Cu(II)]-BZH7) showed the highest internalization rate into PC-3 cells with relatively slow efflux because of its subnanomolar affinity to GRPr. Interestingly, [(64/67)Cu]-BZH7 also displayed similar affinities to the other 2 human BN receptor subtypes. In vivo studies showed that [(64/67)Cu]-BZH7 had a high accumulation in PC-3 xenografts and allowed for clear-cut visualization of the tumor in PET imaging. In addition, a CPTA-glycine derivative, forming a hippurane-type spacer, enhanced kidney clearance of the radiotracer. These data indicate that the species variation of BN receptor plays an important role in screening radiolabeled BN. As well, the positive charge from the metallated complex at the N-terminal significantly increases affinity to human GRPr. Application of these observations enabled the novel ligand [(64/67)Cu]-BZH7 to clearly visualize PC-3 tumors in vivo. This study provides a strong starting point for optimizing radiopeptides for targeting carcinomas that express any of the BN receptor subtypes. Public Library of Science 2012-09-14 /pmc/articles/PMC3443097/ /pubmed/23024746 http://dx.doi.org/10.1371/journal.pone.0044046 Text en © 2012 Zhang 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
Zhang, Hanwen
Abiraj, Keelara
Thorek, Daniel L. J.
Waser, Beatrice
Smith-Jones, Peter M.
Honer, Michael
Reubi, Jean Claude
Maecke, Helmut R.
Evolution of Bombesin Conjugates for Targeted PET Imaging of Tumors
title Evolution of Bombesin Conjugates for Targeted PET Imaging of Tumors
title_full Evolution of Bombesin Conjugates for Targeted PET Imaging of Tumors
title_fullStr Evolution of Bombesin Conjugates for Targeted PET Imaging of Tumors
title_full_unstemmed Evolution of Bombesin Conjugates for Targeted PET Imaging of Tumors
title_short Evolution of Bombesin Conjugates for Targeted PET Imaging of Tumors
title_sort evolution of bombesin conjugates for targeted pet imaging of tumors
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3443097/
https://www.ncbi.nlm.nih.gov/pubmed/23024746
http://dx.doi.org/10.1371/journal.pone.0044046
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