Comparative Evaluation of Radiochemical and Biological Properties of (131)I- and [(99m)Tc]Tc(CO)(3)-Labeled RGD Analogues Planned to Interact with the α(v)β(3) Integrin Expressed in Glioblastoma

Radiolabeled peptides with high specificity for overexpressed receptors in tumor cells hold great promise for diagnostic and therapeutic applications. In this work, we aimed at comparing the radiolabeling efficiency and biological properties of two different RGD analogs: GRGDYV and GRGDHV, labeled w...

Descripción completa

Detalles Bibliográficos
Autores principales: Sobral, Danielle V., Fuscaldi, Leonardo L., Durante, Ana Claudia R., Mendonça, Fernanda F., de Oliveira, Larissa R., Miranda, Ana Cláudia C., Mejia, Jorge, Montor, Wagner R., de Barboza, Marycel F., Malavolta, Luciana
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8876959/
https://www.ncbi.nlm.nih.gov/pubmed/35215229
http://dx.doi.org/10.3390/ph15020116
_version_ 1784658293209169920
author Sobral, Danielle V.
Fuscaldi, Leonardo L.
Durante, Ana Claudia R.
Mendonça, Fernanda F.
de Oliveira, Larissa R.
Miranda, Ana Cláudia C.
Mejia, Jorge
Montor, Wagner R.
de Barboza, Marycel F.
Malavolta, Luciana
author_facet Sobral, Danielle V.
Fuscaldi, Leonardo L.
Durante, Ana Claudia R.
Mendonça, Fernanda F.
de Oliveira, Larissa R.
Miranda, Ana Cláudia C.
Mejia, Jorge
Montor, Wagner R.
de Barboza, Marycel F.
Malavolta, Luciana
author_sort Sobral, Danielle V.
collection PubMed
description Radiolabeled peptides with high specificity for overexpressed receptors in tumor cells hold great promise for diagnostic and therapeutic applications. In this work, we aimed at comparing the radiolabeling efficiency and biological properties of two different RGD analogs: GRGDYV and GRGDHV, labeled with iodine-131 ((131)I) and technetium-99m-tricarbonyl complex [(99m)Tc][Tc(CO)(3)](+). Additionally, we evaluated their interaction with the α(v)β(3) integrin molecule, overexpressed in a wide variety of tumors, including glioblastoma. Both peptides were chemically synthesized, purified and radiolabeled with (131)I and [(99m)Tc][Tc(CO)(3)](+) using the chloramine-T and tricarbonyl methodologies, respectively. The stability, binding to serum proteins and partition coefficient were evaluated for both radioconjugates. In addition, the binding and internalization of radiopeptides to rat C6 glioblastoma cells and rat brain homogenates from normal animals and a glioblastoma-induced model were assessed. Finally, ex vivo biodistribution studies were carried out. Radiochemical yields between 95–98% were reached for both peptides under optimized radiolabeling conditions. Both peptides were stable for up to 24 h in saline solution and in human serum. In addition, the radiopeptides have hydrophilic characteristics and a percentage of binding to serum proteins around 35% and 50% for the [(131)I]I-GRGDYV and [(99m)Tc]Tc(CO)(3)-GRGDHV fragments, respectively. Radiopeptides showed the capacity of binding and internalization both in cell culture (C6) and rat brain homogenates. Biodistribution studies corroborated the results obtained with brain homogenates and confirmed the different binding characteristics due to the exchange of radionuclides and the presence of the tricarbonyl complex. Thereby, the results showed that both radiopeptides might be considered for future clinical applications.
format Online
Article
Text
id pubmed-8876959
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-88769592022-02-26 Comparative Evaluation of Radiochemical and Biological Properties of (131)I- and [(99m)Tc]Tc(CO)(3)-Labeled RGD Analogues Planned to Interact with the α(v)β(3) Integrin Expressed in Glioblastoma Sobral, Danielle V. Fuscaldi, Leonardo L. Durante, Ana Claudia R. Mendonça, Fernanda F. de Oliveira, Larissa R. Miranda, Ana Cláudia C. Mejia, Jorge Montor, Wagner R. de Barboza, Marycel F. Malavolta, Luciana Pharmaceuticals (Basel) Article Radiolabeled peptides with high specificity for overexpressed receptors in tumor cells hold great promise for diagnostic and therapeutic applications. In this work, we aimed at comparing the radiolabeling efficiency and biological properties of two different RGD analogs: GRGDYV and GRGDHV, labeled with iodine-131 ((131)I) and technetium-99m-tricarbonyl complex [(99m)Tc][Tc(CO)(3)](+). Additionally, we evaluated their interaction with the α(v)β(3) integrin molecule, overexpressed in a wide variety of tumors, including glioblastoma. Both peptides were chemically synthesized, purified and radiolabeled with (131)I and [(99m)Tc][Tc(CO)(3)](+) using the chloramine-T and tricarbonyl methodologies, respectively. The stability, binding to serum proteins and partition coefficient were evaluated for both radioconjugates. In addition, the binding and internalization of radiopeptides to rat C6 glioblastoma cells and rat brain homogenates from normal animals and a glioblastoma-induced model were assessed. Finally, ex vivo biodistribution studies were carried out. Radiochemical yields between 95–98% were reached for both peptides under optimized radiolabeling conditions. Both peptides were stable for up to 24 h in saline solution and in human serum. In addition, the radiopeptides have hydrophilic characteristics and a percentage of binding to serum proteins around 35% and 50% for the [(131)I]I-GRGDYV and [(99m)Tc]Tc(CO)(3)-GRGDHV fragments, respectively. Radiopeptides showed the capacity of binding and internalization both in cell culture (C6) and rat brain homogenates. Biodistribution studies corroborated the results obtained with brain homogenates and confirmed the different binding characteristics due to the exchange of radionuclides and the presence of the tricarbonyl complex. Thereby, the results showed that both radiopeptides might be considered for future clinical applications. MDPI 2022-01-18 /pmc/articles/PMC8876959/ /pubmed/35215229 http://dx.doi.org/10.3390/ph15020116 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Sobral, Danielle V.
Fuscaldi, Leonardo L.
Durante, Ana Claudia R.
Mendonça, Fernanda F.
de Oliveira, Larissa R.
Miranda, Ana Cláudia C.
Mejia, Jorge
Montor, Wagner R.
de Barboza, Marycel F.
Malavolta, Luciana
Comparative Evaluation of Radiochemical and Biological Properties of (131)I- and [(99m)Tc]Tc(CO)(3)-Labeled RGD Analogues Planned to Interact with the α(v)β(3) Integrin Expressed in Glioblastoma
title Comparative Evaluation of Radiochemical and Biological Properties of (131)I- and [(99m)Tc]Tc(CO)(3)-Labeled RGD Analogues Planned to Interact with the α(v)β(3) Integrin Expressed in Glioblastoma
title_full Comparative Evaluation of Radiochemical and Biological Properties of (131)I- and [(99m)Tc]Tc(CO)(3)-Labeled RGD Analogues Planned to Interact with the α(v)β(3) Integrin Expressed in Glioblastoma
title_fullStr Comparative Evaluation of Radiochemical and Biological Properties of (131)I- and [(99m)Tc]Tc(CO)(3)-Labeled RGD Analogues Planned to Interact with the α(v)β(3) Integrin Expressed in Glioblastoma
title_full_unstemmed Comparative Evaluation of Radiochemical and Biological Properties of (131)I- and [(99m)Tc]Tc(CO)(3)-Labeled RGD Analogues Planned to Interact with the α(v)β(3) Integrin Expressed in Glioblastoma
title_short Comparative Evaluation of Radiochemical and Biological Properties of (131)I- and [(99m)Tc]Tc(CO)(3)-Labeled RGD Analogues Planned to Interact with the α(v)β(3) Integrin Expressed in Glioblastoma
title_sort comparative evaluation of radiochemical and biological properties of (131)i- and [(99m)tc]tc(co)(3)-labeled rgd analogues planned to interact with the α(v)β(3) integrin expressed in glioblastoma
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8876959/
https://www.ncbi.nlm.nih.gov/pubmed/35215229
http://dx.doi.org/10.3390/ph15020116
work_keys_str_mv AT sobraldaniellev comparativeevaluationofradiochemicalandbiologicalpropertiesof131iand99mtctcco3labeledrgdanaloguesplannedtointeractwiththeavb3integrinexpressedinglioblastoma
AT fuscaldileonardol comparativeevaluationofradiochemicalandbiologicalpropertiesof131iand99mtctcco3labeledrgdanaloguesplannedtointeractwiththeavb3integrinexpressedinglioblastoma
AT duranteanaclaudiar comparativeevaluationofradiochemicalandbiologicalpropertiesof131iand99mtctcco3labeledrgdanaloguesplannedtointeractwiththeavb3integrinexpressedinglioblastoma
AT mendoncafernandaf comparativeevaluationofradiochemicalandbiologicalpropertiesof131iand99mtctcco3labeledrgdanaloguesplannedtointeractwiththeavb3integrinexpressedinglioblastoma
AT deoliveiralarissar comparativeevaluationofradiochemicalandbiologicalpropertiesof131iand99mtctcco3labeledrgdanaloguesplannedtointeractwiththeavb3integrinexpressedinglioblastoma
AT mirandaanaclaudiac comparativeevaluationofradiochemicalandbiologicalpropertiesof131iand99mtctcco3labeledrgdanaloguesplannedtointeractwiththeavb3integrinexpressedinglioblastoma
AT mejiajorge comparativeevaluationofradiochemicalandbiologicalpropertiesof131iand99mtctcco3labeledrgdanaloguesplannedtointeractwiththeavb3integrinexpressedinglioblastoma
AT montorwagnerr comparativeevaluationofradiochemicalandbiologicalpropertiesof131iand99mtctcco3labeledrgdanaloguesplannedtointeractwiththeavb3integrinexpressedinglioblastoma
AT debarbozamarycelf comparativeevaluationofradiochemicalandbiologicalpropertiesof131iand99mtctcco3labeledrgdanaloguesplannedtointeractwiththeavb3integrinexpressedinglioblastoma
AT malavoltaluciana comparativeevaluationofradiochemicalandbiologicalpropertiesof131iand99mtctcco3labeledrgdanaloguesplannedtointeractwiththeavb3integrinexpressedinglioblastoma

Ejemplares similares