Radiolabeled nano-peptides show specificity for an animal model of human PC3 prostate cancer cells

Detalhes bibliográficos
Autor(a) principal: Faintuch, Bluma Linkowski
Data de Publicação: 2011
Outros Autores: Núñez, Gustavo Eutimio Fernandez, Teodoro, Rodrigo, Moro, Ana M., Mengatti, Jair
Tipo de documento: Artigo
Idioma: eng
Título da fonte: Clinics
Texto Completo: https://www.revistas.usp.br/clinics/article/view/19311
Resumo: OBJECTIVES: Cancer has been investigated using various pre-targeting techniques or models focusing on radiobombesin analogues; however, both are not offered together. In this study, nano-bombesin labeling by a pre-targeting system was undertaken to develop an alternative approach for prostate tumor treatment. METHODS: A two-step pre-targeting system utilizing a combination of streptavidin (SA), biotinylated morpholino (B-MORF), biotinylated BBN (B-BBN) with two different spacers (b-Ala and PEG), and a radiolabeled cMORF was evaluated in vitro and in vivo. RESULTS: Final conjugation conditions consisted of a 1:1:2 ratio of SA:B-MORF:B-BBN, followed by addition of 99mTc-cMORF to compensate for free MORF. In vitro binding experiments with prostate cancer cells (PC-3) revealed that total binding was time-dependent for the Ala spacer but not for the PEG spacer. The highest accumulation (5.06 ± 1.98 %) was achieved with 1 hour of incubation, decreasing as time progressed. Specific binding fell to 1.05 ± 0.35 %. The pre-targeting biodistribution in healthy Swiss mice was measured at different time points, with the best responses observed for 7-h and 15-h incubations. The effector, 99mTc-MAG3-cMORF, was administered 2 h later. Strong kidney excretion was always documented. The greatest tumor uptake was 2.58 ± 0.59 %ID/g at 7 h for B-bAla-BBN, with a region of interest (ROI) value of 3.9 % during imaging. The tumor/blood ratio was low due to the slow blood clearance; however, the tumor/muscle ratio was 5.95. CONCLUSIONS: The pre-targeting approach with a peptide was a viable concept. Further evaluation with modified sequences of MORF, including less cytosine, and additional test intervals could be worthwhile.
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spelling Radiolabeled nano-peptides show specificity for an animal model of human PC3 prostate cancer cells RadiolabelingTechnetium-99mHuman tumor PC-3 cellsPeptideTumor uptake OBJECTIVES: Cancer has been investigated using various pre-targeting techniques or models focusing on radiobombesin analogues; however, both are not offered together. In this study, nano-bombesin labeling by a pre-targeting system was undertaken to develop an alternative approach for prostate tumor treatment. METHODS: A two-step pre-targeting system utilizing a combination of streptavidin (SA), biotinylated morpholino (B-MORF), biotinylated BBN (B-BBN) with two different spacers (b-Ala and PEG), and a radiolabeled cMORF was evaluated in vitro and in vivo. RESULTS: Final conjugation conditions consisted of a 1:1:2 ratio of SA:B-MORF:B-BBN, followed by addition of 99mTc-cMORF to compensate for free MORF. In vitro binding experiments with prostate cancer cells (PC-3) revealed that total binding was time-dependent for the Ala spacer but not for the PEG spacer. The highest accumulation (5.06 ± 1.98 %) was achieved with 1 hour of incubation, decreasing as time progressed. Specific binding fell to 1.05 ± 0.35 %. The pre-targeting biodistribution in healthy Swiss mice was measured at different time points, with the best responses observed for 7-h and 15-h incubations. The effector, 99mTc-MAG3-cMORF, was administered 2 h later. Strong kidney excretion was always documented. The greatest tumor uptake was 2.58 ± 0.59 %ID/g at 7 h for B-bAla-BBN, with a region of interest (ROI) value of 3.9 % during imaging. The tumor/blood ratio was low due to the slow blood clearance; however, the tumor/muscle ratio was 5.95. CONCLUSIONS: The pre-targeting approach with a peptide was a viable concept. Further evaluation with modified sequences of MORF, including less cytosine, and additional test intervals could be worthwhile. Hospital das Clínicas, Faculdade de Medicina, Universidade de São Paulo2011-01-01info:eu-repo/semantics/articleinfo:eu-repo/semantics/publishedVersionapplication/pdfhttps://www.revistas.usp.br/clinics/article/view/1931110.1590/S1807-59322011000200024Clinics; Vol. 66 No. 2 (2011); 327-336 Clinics; v. 66 n. 2 (2011); 327-336 Clinics; Vol. 66 Núm. 2 (2011); 327-336 1980-53221807-5932reponame:Clinicsinstname:Universidade de São Paulo (USP)instacron:USPenghttps://www.revistas.usp.br/clinics/article/view/19311/21374Faintuch, Bluma LinkowskiNúñez, Gustavo Eutimio FernandezTeodoro, RodrigoMoro, Ana M.Mengatti, Jairinfo:eu-repo/semantics/openAccess2012-05-23T16:33:31Zoai:revistas.usp.br:article/19311Revistahttps://www.revistas.usp.br/clinicsPUBhttps://www.revistas.usp.br/clinics/oai||clinics@hc.fm.usp.br1980-53221807-5932opendoar:2012-05-23T16:33:31Clinics - Universidade de São Paulo (USP)false
dc.title.none.fl_str_mv Radiolabeled nano-peptides show specificity for an animal model of human PC3 prostate cancer cells
title Radiolabeled nano-peptides show specificity for an animal model of human PC3 prostate cancer cells
spellingShingle Radiolabeled nano-peptides show specificity for an animal model of human PC3 prostate cancer cells
Faintuch, Bluma Linkowski
Radiolabeling
Technetium-99m
Human tumor PC-3 cells
Peptide
Tumor uptake
title_short Radiolabeled nano-peptides show specificity for an animal model of human PC3 prostate cancer cells
title_full Radiolabeled nano-peptides show specificity for an animal model of human PC3 prostate cancer cells
title_fullStr Radiolabeled nano-peptides show specificity for an animal model of human PC3 prostate cancer cells
title_full_unstemmed Radiolabeled nano-peptides show specificity for an animal model of human PC3 prostate cancer cells
title_sort Radiolabeled nano-peptides show specificity for an animal model of human PC3 prostate cancer cells
author Faintuch, Bluma Linkowski
author_facet Faintuch, Bluma Linkowski
Núñez, Gustavo Eutimio Fernandez
Teodoro, Rodrigo
Moro, Ana M.
Mengatti, Jair
author_role author
author2 Núñez, Gustavo Eutimio Fernandez
Teodoro, Rodrigo
Moro, Ana M.
Mengatti, Jair
author2_role author
author
author
author
dc.contributor.author.fl_str_mv Faintuch, Bluma Linkowski
Núñez, Gustavo Eutimio Fernandez
Teodoro, Rodrigo
Moro, Ana M.
Mengatti, Jair
dc.subject.por.fl_str_mv Radiolabeling
Technetium-99m
Human tumor PC-3 cells
Peptide
Tumor uptake
topic Radiolabeling
Technetium-99m
Human tumor PC-3 cells
Peptide
Tumor uptake
description OBJECTIVES: Cancer has been investigated using various pre-targeting techniques or models focusing on radiobombesin analogues; however, both are not offered together. In this study, nano-bombesin labeling by a pre-targeting system was undertaken to develop an alternative approach for prostate tumor treatment. METHODS: A two-step pre-targeting system utilizing a combination of streptavidin (SA), biotinylated morpholino (B-MORF), biotinylated BBN (B-BBN) with two different spacers (b-Ala and PEG), and a radiolabeled cMORF was evaluated in vitro and in vivo. RESULTS: Final conjugation conditions consisted of a 1:1:2 ratio of SA:B-MORF:B-BBN, followed by addition of 99mTc-cMORF to compensate for free MORF. In vitro binding experiments with prostate cancer cells (PC-3) revealed that total binding was time-dependent for the Ala spacer but not for the PEG spacer. The highest accumulation (5.06 ± 1.98 %) was achieved with 1 hour of incubation, decreasing as time progressed. Specific binding fell to 1.05 ± 0.35 %. The pre-targeting biodistribution in healthy Swiss mice was measured at different time points, with the best responses observed for 7-h and 15-h incubations. The effector, 99mTc-MAG3-cMORF, was administered 2 h later. Strong kidney excretion was always documented. The greatest tumor uptake was 2.58 ± 0.59 %ID/g at 7 h for B-bAla-BBN, with a region of interest (ROI) value of 3.9 % during imaging. The tumor/blood ratio was low due to the slow blood clearance; however, the tumor/muscle ratio was 5.95. CONCLUSIONS: The pre-targeting approach with a peptide was a viable concept. Further evaluation with modified sequences of MORF, including less cytosine, and additional test intervals could be worthwhile.
publishDate 2011
dc.date.none.fl_str_mv 2011-01-01
dc.type.driver.fl_str_mv info:eu-repo/semantics/article
info:eu-repo/semantics/publishedVersion
format article
status_str publishedVersion
dc.identifier.uri.fl_str_mv https://www.revistas.usp.br/clinics/article/view/19311
10.1590/S1807-59322011000200024
url https://www.revistas.usp.br/clinics/article/view/19311
identifier_str_mv 10.1590/S1807-59322011000200024
dc.language.iso.fl_str_mv eng
language eng
dc.relation.none.fl_str_mv https://www.revistas.usp.br/clinics/article/view/19311/21374
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
dc.publisher.none.fl_str_mv Hospital das Clínicas, Faculdade de Medicina, Universidade de São Paulo
publisher.none.fl_str_mv Hospital das Clínicas, Faculdade de Medicina, Universidade de São Paulo
dc.source.none.fl_str_mv Clinics; Vol. 66 No. 2 (2011); 327-336
Clinics; v. 66 n. 2 (2011); 327-336
Clinics; Vol. 66 Núm. 2 (2011); 327-336
1980-5322
1807-5932
reponame:Clinics
instname:Universidade de São Paulo (USP)
instacron:USP
instname_str Universidade de São Paulo (USP)
instacron_str USP
institution USP
reponame_str Clinics
collection Clinics
repository.name.fl_str_mv Clinics - Universidade de São Paulo (USP)
repository.mail.fl_str_mv ||clinics@hc.fm.usp.br
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