Evaluation of Fluorine-18-Labeled α1(I)-N-Telopeptide Analogs as Substrate-Based Radiotracers for PET Imaging of Melanoma-Associated Lysyl Oxidase

Accumulating evidence suggests an unequivocal role of lysyl oxidases as key players of tumor progression and metastasis, which renders this enzyme family highly attractive for targeted non-invasive functional imaging of tumors. Considering their function in matrix remodeling, malignant melanoma appe...

Descripción completa

Detalles Bibliográficos
Autores principales: Kuchar, Manuela, Neuber, Christin, Belter, Birgit, Bergmann, Ralf, Lenk, Jens, Wodtke, Robert, Kniess, Torsten, Steinbach, Jörg, Pietzsch, Jens, Löser, Reik
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2018
Materias:
Chemistry
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5932954/
https://www.ncbi.nlm.nih.gov/pubmed/29755969
http://dx.doi.org/10.3389/fchem.2018.00121
_version_ 1783319908592910336
author Kuchar, Manuela
Neuber, Christin
Belter, Birgit
Bergmann, Ralf
Lenk, Jens
Wodtke, Robert
Kniess, Torsten
Steinbach, Jörg
Pietzsch, Jens
Löser, Reik
author_facet Kuchar, Manuela
Neuber, Christin
Belter, Birgit
Bergmann, Ralf
Lenk, Jens
Wodtke, Robert
Kniess, Torsten
Steinbach, Jörg
Pietzsch, Jens
Löser, Reik
author_sort Kuchar, Manuela
collection PubMed
description Accumulating evidence suggests an unequivocal role of lysyl oxidases as key players of tumor progression and metastasis, which renders this enzyme family highly attractive for targeted non-invasive functional imaging of tumors. Considering their function in matrix remodeling, malignant melanoma appears as particularly interesting neoplasia in this respect. For the development of radiotracers that enable PET imaging of the melanoma-associated lysyl oxidase activity, substrates derived from the type I collagen α1 N-telopeptide were labeled with fluorine-18 using N-succinimidyl 4-[(18)F]fluorobenzoate ([(18)F]SFB) as prosthetic reagent. With regards to potential crosslinking to tumor-associated collagen in vivo, their interaction with triple-helical type I collagen was studied by SPR. A mouse model of human melanoma was established on the basis of the A375 cell line, for which the expression of the oncologically relevant lysyl oxidase isoforms LOX and LOXL2 was demonstrated in Western blot and immunohistochemical experiments. The radiopharmacological profiles of the peptidic radiotracers were evaluated in normal rats and A375 melanoma-bearing mice by ex vivo metabolite analysis, whole-body biodistribution studies and dynamic PET imaging. Out of three (18)F-labeled telopeptide analogs, the one with the most favorable substrate properties has shown favorable tumor uptake and tumor-to-muscle ratio. Lysyl oxidase-mediated tumor uptake was proven by pharmacological inhibition using β-aminopropionitrile and by employing negative-control analogs of impeded or abolished targeting capability. The latter were obtained by substituting the lysine residue by ornithine and norleucine, respectively. Comparing the tumor uptake of the lysine-containing peptide with that of the non-functional analogs indicate the feasibility of lysyl oxidase imaging in melanoma using substrate-based radiotracers.
format Online
Article
Text
id pubmed-5932954
institution National Center for Biotechnology Information
language English
publishDate 2018
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-59329542018-05-11 Evaluation of Fluorine-18-Labeled α1(I)-N-Telopeptide Analogs as Substrate-Based Radiotracers for PET Imaging of Melanoma-Associated Lysyl Oxidase Kuchar, Manuela Neuber, Christin Belter, Birgit Bergmann, Ralf Lenk, Jens Wodtke, Robert Kniess, Torsten Steinbach, Jörg Pietzsch, Jens Löser, Reik Front Chem Chemistry Accumulating evidence suggests an unequivocal role of lysyl oxidases as key players of tumor progression and metastasis, which renders this enzyme family highly attractive for targeted non-invasive functional imaging of tumors. Considering their function in matrix remodeling, malignant melanoma appears as particularly interesting neoplasia in this respect. For the development of radiotracers that enable PET imaging of the melanoma-associated lysyl oxidase activity, substrates derived from the type I collagen α1 N-telopeptide were labeled with fluorine-18 using N-succinimidyl 4-[(18)F]fluorobenzoate ([(18)F]SFB) as prosthetic reagent. With regards to potential crosslinking to tumor-associated collagen in vivo, their interaction with triple-helical type I collagen was studied by SPR. A mouse model of human melanoma was established on the basis of the A375 cell line, for which the expression of the oncologically relevant lysyl oxidase isoforms LOX and LOXL2 was demonstrated in Western blot and immunohistochemical experiments. The radiopharmacological profiles of the peptidic radiotracers were evaluated in normal rats and A375 melanoma-bearing mice by ex vivo metabolite analysis, whole-body biodistribution studies and dynamic PET imaging. Out of three (18)F-labeled telopeptide analogs, the one with the most favorable substrate properties has shown favorable tumor uptake and tumor-to-muscle ratio. Lysyl oxidase-mediated tumor uptake was proven by pharmacological inhibition using β-aminopropionitrile and by employing negative-control analogs of impeded or abolished targeting capability. The latter were obtained by substituting the lysine residue by ornithine and norleucine, respectively. Comparing the tumor uptake of the lysine-containing peptide with that of the non-functional analogs indicate the feasibility of lysyl oxidase imaging in melanoma using substrate-based radiotracers. Frontiers Media S.A. 2018-04-26 /pmc/articles/PMC5932954/ /pubmed/29755969 http://dx.doi.org/10.3389/fchem.2018.00121 Text en Copyright © 2018 Kuchar, Neuber, Belter, Bergmann, Lenk, Wodtke, Kniess, Steinbach, Pietzsch and Löser. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Chemistry
Kuchar, Manuela
Neuber, Christin
Belter, Birgit
Bergmann, Ralf
Lenk, Jens
Wodtke, Robert
Kniess, Torsten
Steinbach, Jörg
Pietzsch, Jens
Löser, Reik
Evaluation of Fluorine-18-Labeled α1(I)-N-Telopeptide Analogs as Substrate-Based Radiotracers for PET Imaging of Melanoma-Associated Lysyl Oxidase
title Evaluation of Fluorine-18-Labeled α1(I)-N-Telopeptide Analogs as Substrate-Based Radiotracers for PET Imaging of Melanoma-Associated Lysyl Oxidase
title_full Evaluation of Fluorine-18-Labeled α1(I)-N-Telopeptide Analogs as Substrate-Based Radiotracers for PET Imaging of Melanoma-Associated Lysyl Oxidase
title_fullStr Evaluation of Fluorine-18-Labeled α1(I)-N-Telopeptide Analogs as Substrate-Based Radiotracers for PET Imaging of Melanoma-Associated Lysyl Oxidase
title_full_unstemmed Evaluation of Fluorine-18-Labeled α1(I)-N-Telopeptide Analogs as Substrate-Based Radiotracers for PET Imaging of Melanoma-Associated Lysyl Oxidase
title_short Evaluation of Fluorine-18-Labeled α1(I)-N-Telopeptide Analogs as Substrate-Based Radiotracers for PET Imaging of Melanoma-Associated Lysyl Oxidase
title_sort evaluation of fluorine-18-labeled α1(i)-n-telopeptide analogs as substrate-based radiotracers for pet imaging of melanoma-associated lysyl oxidase
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5932954/
https://www.ncbi.nlm.nih.gov/pubmed/29755969
http://dx.doi.org/10.3389/fchem.2018.00121
work_keys_str_mv AT kucharmanuela evaluationoffluorine18labeleda1intelopeptideanalogsassubstratebasedradiotracersforpetimagingofmelanomaassociatedlysyloxidase
AT neuberchristin evaluationoffluorine18labeleda1intelopeptideanalogsassubstratebasedradiotracersforpetimagingofmelanomaassociatedlysyloxidase
AT belterbirgit evaluationoffluorine18labeleda1intelopeptideanalogsassubstratebasedradiotracersforpetimagingofmelanomaassociatedlysyloxidase
AT bergmannralf evaluationoffluorine18labeleda1intelopeptideanalogsassubstratebasedradiotracersforpetimagingofmelanomaassociatedlysyloxidase
AT lenkjens evaluationoffluorine18labeleda1intelopeptideanalogsassubstratebasedradiotracersforpetimagingofmelanomaassociatedlysyloxidase
AT wodtkerobert evaluationoffluorine18labeleda1intelopeptideanalogsassubstratebasedradiotracersforpetimagingofmelanomaassociatedlysyloxidase
AT kniesstorsten evaluationoffluorine18labeleda1intelopeptideanalogsassubstratebasedradiotracersforpetimagingofmelanomaassociatedlysyloxidase
AT steinbachjorg evaluationoffluorine18labeleda1intelopeptideanalogsassubstratebasedradiotracersforpetimagingofmelanomaassociatedlysyloxidase
AT pietzschjens evaluationoffluorine18labeleda1intelopeptideanalogsassubstratebasedradiotracersforpetimagingofmelanomaassociatedlysyloxidase
AT loserreik evaluationoffluorine18labeleda1intelopeptideanalogsassubstratebasedradiotracersforpetimagingofmelanomaassociatedlysyloxidase

Ejemplares similares