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Optimizing CIGB-300 intralesional delivery in locally advanced cervical cancer

BACKGROUND: We conducted a phase 1 trial in patients with locally advanced cervical cancer by injecting 0.5 ml of the CK2-antagonist CIGB-300 in two different sites on tumours to assess tumour uptake, safety, pharmacodynamic activity and identify the recommended dose. METHODS: Fourteen patients were...

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Autores principales: Sarduy, M R, García, I, Coca, M A, Perera, A, Torres, L A, Valenzuela, C M, Baladrón, I, Solares, M, Reyes, V, Hernández, I, Perera, Y, Martínez, Y M, Molina, L, González, Y M, Ancízar, J A, Prats, A, González, L, Casacó, C A, Acevedo, B E, López-Saura, P A, Alonso, D F, Gómez, R, Perea-Rodríguez, S E
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4430720/
https://www.ncbi.nlm.nih.gov/pubmed/25880012
http://dx.doi.org/10.1038/bjc.2015.137
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author Sarduy, M R
García, I
Coca, M A
Perera, A
Torres, L A
Valenzuela, C M
Baladrón, I
Solares, M
Reyes, V
Hernández, I
Perera, Y
Martínez, Y M
Molina, L
González, Y M
Ancízar, J A
Prats, A
González, L
Casacó, C A
Acevedo, B E
López-Saura, P A
Alonso, D F
Gómez, R
Perea-Rodríguez, S E
author_facet Sarduy, M R
García, I
Coca, M A
Perera, A
Torres, L A
Valenzuela, C M
Baladrón, I
Solares, M
Reyes, V
Hernández, I
Perera, Y
Martínez, Y M
Molina, L
González, Y M
Ancízar, J A
Prats, A
González, L
Casacó, C A
Acevedo, B E
López-Saura, P A
Alonso, D F
Gómez, R
Perea-Rodríguez, S E
author_sort Sarduy, M R
collection PubMed
description BACKGROUND: We conducted a phase 1 trial in patients with locally advanced cervical cancer by injecting 0.5 ml of the CK2-antagonist CIGB-300 in two different sites on tumours to assess tumour uptake, safety, pharmacodynamic activity and identify the recommended dose. METHODS: Fourteen patients were treated with intralesional injections containing 35 or 70 mg of CIGB-300 in three alternate cycles of three consecutive days each before standard chemoradiotherapy. Tumour uptake was determined using (99)Tc-radiolabelled peptide. In situ B23/nucleophosmin was determined by immunohistochemistry. RESULTS: Maximum tumour uptake for CIGB-300 70-mg dose was significantly higher than the one observed for 35 mg: 16.1±8.9 vs 31.3±12.9 mg (P=0.01). Both, AUC(24h) and biological half-life were also significantly higher using 70 mg of CIGB-300 (P<0.001). Unincorporated CIGB-300 diffused rapidly to blood and was mainly distributed towards kidneys, and marginally in liver, lungs, heart and spleen. There was no DLT and moderate allergic-like reactions were the most common systemic side effect with strong correlation between unincorporated CIGB-300 and histamine levels in blood. CIGB-300, 70 mg, downregulated B23/nucleophosmin (P=0.03) in tumour specimens. CONCLUSION: Intralesional injections of 70 mg CIGB-300 in two sites (0.5 ml per injection) and this treatment plan are recommended to be evaluated in phase 2 studies.
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spelling pubmed-44307202016-05-12 Optimizing CIGB-300 intralesional delivery in locally advanced cervical cancer Sarduy, M R García, I Coca, M A Perera, A Torres, L A Valenzuela, C M Baladrón, I Solares, M Reyes, V Hernández, I Perera, Y Martínez, Y M Molina, L González, Y M Ancízar, J A Prats, A González, L Casacó, C A Acevedo, B E López-Saura, P A Alonso, D F Gómez, R Perea-Rodríguez, S E Br J Cancer Clinical Study BACKGROUND: We conducted a phase 1 trial in patients with locally advanced cervical cancer by injecting 0.5 ml of the CK2-antagonist CIGB-300 in two different sites on tumours to assess tumour uptake, safety, pharmacodynamic activity and identify the recommended dose. METHODS: Fourteen patients were treated with intralesional injections containing 35 or 70 mg of CIGB-300 in three alternate cycles of three consecutive days each before standard chemoradiotherapy. Tumour uptake was determined using (99)Tc-radiolabelled peptide. In situ B23/nucleophosmin was determined by immunohistochemistry. RESULTS: Maximum tumour uptake for CIGB-300 70-mg dose was significantly higher than the one observed for 35 mg: 16.1±8.9 vs 31.3±12.9 mg (P=0.01). Both, AUC(24h) and biological half-life were also significantly higher using 70 mg of CIGB-300 (P<0.001). Unincorporated CIGB-300 diffused rapidly to blood and was mainly distributed towards kidneys, and marginally in liver, lungs, heart and spleen. There was no DLT and moderate allergic-like reactions were the most common systemic side effect with strong correlation between unincorporated CIGB-300 and histamine levels in blood. CIGB-300, 70 mg, downregulated B23/nucleophosmin (P=0.03) in tumour specimens. CONCLUSION: Intralesional injections of 70 mg CIGB-300 in two sites (0.5 ml per injection) and this treatment plan are recommended to be evaluated in phase 2 studies. Nature Publishing Group 2015-05-12 2015-04-16 /pmc/articles/PMC4430720/ /pubmed/25880012 http://dx.doi.org/10.1038/bjc.2015.137 Text en Copyright © 2015 Cancer Research UK http://creativecommons.org/licenses/by-nc-sa/4.0/ From twelve months after its original publication, this work is licensed under the Creative Commons Attribution-NonCommercial-Share Alike 4.0 Unported License. To view a copy of this license, visit http://creativecommons.org/licenses/by-nc-sa/4.0/
spellingShingle Clinical Study
Sarduy, M R
García, I
Coca, M A
Perera, A
Torres, L A
Valenzuela, C M
Baladrón, I
Solares, M
Reyes, V
Hernández, I
Perera, Y
Martínez, Y M
Molina, L
González, Y M
Ancízar, J A
Prats, A
González, L
Casacó, C A
Acevedo, B E
López-Saura, P A
Alonso, D F
Gómez, R
Perea-Rodríguez, S E
Optimizing CIGB-300 intralesional delivery in locally advanced cervical cancer
title Optimizing CIGB-300 intralesional delivery in locally advanced cervical cancer
title_full Optimizing CIGB-300 intralesional delivery in locally advanced cervical cancer
title_fullStr Optimizing CIGB-300 intralesional delivery in locally advanced cervical cancer
title_full_unstemmed Optimizing CIGB-300 intralesional delivery in locally advanced cervical cancer
title_short Optimizing CIGB-300 intralesional delivery in locally advanced cervical cancer
title_sort optimizing cigb-300 intralesional delivery in locally advanced cervical cancer
topic Clinical Study
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4430720/
https://www.ncbi.nlm.nih.gov/pubmed/25880012
http://dx.doi.org/10.1038/bjc.2015.137
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