The oncogenic role of the In1-ghrelin splicing variant in prostate cancer aggressiveness

BACKGROUND: The Ghrelin-system is a complex, pleiotropic family composed of several peptides, including native-ghrelin and its In1-ghrelin splicing variant, and receptors (GHSR 1a/b), which are dysregulated in various endocrine-related tumors, where they associate to pathophysiological features, but...

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Autores principales: Hormaechea-Agulla, Daniel, Gahete, Manuel D., Jiménez-Vacas, Juan M., Gómez-Gómez, Enrique, Ibáñez-Costa, Alejandro, L-López, Fernando, Rivero-Cortés, Esther, Sarmento-Cabral, André, Valero-Rosa, José, Carrasco-Valiente, Julia, Sánchez-Sánchez, Rafael, Ortega-Salas, Rosa, Moreno, María M., Tsomaia, Natia, Swanson, Steve M., Culler, Michael D., Requena, María J., Castaño, Justo P., Luque, Raúl M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2017
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5576296/
https://www.ncbi.nlm.nih.gov/pubmed/28851363
http://dx.doi.org/10.1186/s12943-017-0713-9
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author Hormaechea-Agulla, Daniel
Gahete, Manuel D.
Jiménez-Vacas, Juan M.
Gómez-Gómez, Enrique
Ibáñez-Costa, Alejandro
L-López, Fernando
Rivero-Cortés, Esther
Sarmento-Cabral, André
Valero-Rosa, José
Carrasco-Valiente, Julia
Sánchez-Sánchez, Rafael
Ortega-Salas, Rosa
Moreno, María M.
Tsomaia, Natia
Swanson, Steve M.
Culler, Michael D.
Requena, María J.
Castaño, Justo P.
Luque, Raúl M.
author_facet Hormaechea-Agulla, Daniel
Gahete, Manuel D.
Jiménez-Vacas, Juan M.
Gómez-Gómez, Enrique
Ibáñez-Costa, Alejandro
L-López, Fernando
Rivero-Cortés, Esther
Sarmento-Cabral, André
Valero-Rosa, José
Carrasco-Valiente, Julia
Sánchez-Sánchez, Rafael
Ortega-Salas, Rosa
Moreno, María M.
Tsomaia, Natia
Swanson, Steve M.
Culler, Michael D.
Requena, María J.
Castaño, Justo P.
Luque, Raúl M.
author_sort Hormaechea-Agulla, Daniel
collection PubMed
description BACKGROUND: The Ghrelin-system is a complex, pleiotropic family composed of several peptides, including native-ghrelin and its In1-ghrelin splicing variant, and receptors (GHSR 1a/b), which are dysregulated in various endocrine-related tumors, where they associate to pathophysiological features, but the presence, functional role, and mechanisms of actions of In1-ghrelin splicing variant in prostate-cancer (PCa), is completely unexplored. Herein, we aimed to determine the presence of key ghrelin-system components (native-ghrelin, In1-ghrelin, GHSR1a/1b) and their potential pathophysiological role in prostate cancer (PCa). METHODS: In1-ghrelin and native-ghrelin expression was evaluated by qPCR in prostate tissues from patients with high PCa-risk (n = 52; fresh-tumoral biopsies), and healthy-prostates (n = 12; from cystoprostatectomies) and correlated with clinical parameters using Spearman-test. In addition, In1-ghrelin and native-ghrelin was measured in plasma from an additional cohort of PCa-patients with different risk levels (n = 30) and control-healthy patients (n = 20). In vivo functional (proliferation/migration) and mechanistic (gene expression/signaling-pathways) assays were performed in PCa-cell lines in response to In1-ghrelin and native-ghrelin treatment, overexpression and/or silencing. Finally, tumor progression was monitored in nude-mice injected with PCa-cells overexpressing In1-ghrelin, native-ghrelin and empty vector (control). RESULTS: In1-ghrelin, but not native-ghrelin, was overexpressed in high-risk PCa-samples compared to normal-prostate (NP), and this expression correlated with that of PSA. Conversely, GHSR1a/1b expression was virtually absent. Remarkably, plasmatic In1-ghrelin, but not native-ghrelin, levels were also higher in PCa-patients compared to healthy-controls. Furthermore, In1-ghrelin treatment/overexpression, and to a much lesser extent native-ghrelin, increased aggressiveness features (cell-proliferation, migration and PSA secretion) of NP and PCa cells. Consistently, nude-mice injected with PC-3-cells stably-transfected with In1-ghrelin, but not native-ghrelin, presented larger tumors. These effects were likely mediated by ERK1/2-signaling activation and involved altered expression of key oncogenes/tumor suppressor genes. Finally, In1-ghrelin silencing reduced cell-proliferation and PSA secretion from PCa cells. CONCLUSIONS: Altogether, our results indicate that In1-ghrelin levels (in tissue) and circulating levels (in plasma) are increased in PCa where it can regulate key pathophysiological processes, thus suggesting that In1-ghrelin may represent a novel biomarker and a new therapeutic target in PCa. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s12943-017-0713-9) contains supplementary material, which is available to authorized users.
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spelling pubmed-55762962017-08-30 The oncogenic role of the In1-ghrelin splicing variant in prostate cancer aggressiveness Hormaechea-Agulla, Daniel Gahete, Manuel D. Jiménez-Vacas, Juan M. Gómez-Gómez, Enrique Ibáñez-Costa, Alejandro L-López, Fernando Rivero-Cortés, Esther Sarmento-Cabral, André Valero-Rosa, José Carrasco-Valiente, Julia Sánchez-Sánchez, Rafael Ortega-Salas, Rosa Moreno, María M. Tsomaia, Natia Swanson, Steve M. Culler, Michael D. Requena, María J. Castaño, Justo P. Luque, Raúl M. Mol Cancer Research BACKGROUND: The Ghrelin-system is a complex, pleiotropic family composed of several peptides, including native-ghrelin and its In1-ghrelin splicing variant, and receptors (GHSR 1a/b), which are dysregulated in various endocrine-related tumors, where they associate to pathophysiological features, but the presence, functional role, and mechanisms of actions of In1-ghrelin splicing variant in prostate-cancer (PCa), is completely unexplored. Herein, we aimed to determine the presence of key ghrelin-system components (native-ghrelin, In1-ghrelin, GHSR1a/1b) and their potential pathophysiological role in prostate cancer (PCa). METHODS: In1-ghrelin and native-ghrelin expression was evaluated by qPCR in prostate tissues from patients with high PCa-risk (n = 52; fresh-tumoral biopsies), and healthy-prostates (n = 12; from cystoprostatectomies) and correlated with clinical parameters using Spearman-test. In addition, In1-ghrelin and native-ghrelin was measured in plasma from an additional cohort of PCa-patients with different risk levels (n = 30) and control-healthy patients (n = 20). In vivo functional (proliferation/migration) and mechanistic (gene expression/signaling-pathways) assays were performed in PCa-cell lines in response to In1-ghrelin and native-ghrelin treatment, overexpression and/or silencing. Finally, tumor progression was monitored in nude-mice injected with PCa-cells overexpressing In1-ghrelin, native-ghrelin and empty vector (control). RESULTS: In1-ghrelin, but not native-ghrelin, was overexpressed in high-risk PCa-samples compared to normal-prostate (NP), and this expression correlated with that of PSA. Conversely, GHSR1a/1b expression was virtually absent. Remarkably, plasmatic In1-ghrelin, but not native-ghrelin, levels were also higher in PCa-patients compared to healthy-controls. Furthermore, In1-ghrelin treatment/overexpression, and to a much lesser extent native-ghrelin, increased aggressiveness features (cell-proliferation, migration and PSA secretion) of NP and PCa cells. Consistently, nude-mice injected with PC-3-cells stably-transfected with In1-ghrelin, but not native-ghrelin, presented larger tumors. These effects were likely mediated by ERK1/2-signaling activation and involved altered expression of key oncogenes/tumor suppressor genes. Finally, In1-ghrelin silencing reduced cell-proliferation and PSA secretion from PCa cells. CONCLUSIONS: Altogether, our results indicate that In1-ghrelin levels (in tissue) and circulating levels (in plasma) are increased in PCa where it can regulate key pathophysiological processes, thus suggesting that In1-ghrelin may represent a novel biomarker and a new therapeutic target in PCa. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s12943-017-0713-9) contains supplementary material, which is available to authorized users. BioMed Central 2017-08-29 /pmc/articles/PMC5576296/ /pubmed/28851363 http://dx.doi.org/10.1186/s12943-017-0713-9 Text en © The Author(s). 2017 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Hormaechea-Agulla, Daniel
Gahete, Manuel D.
Jiménez-Vacas, Juan M.
Gómez-Gómez, Enrique
Ibáñez-Costa, Alejandro
L-López, Fernando
Rivero-Cortés, Esther
Sarmento-Cabral, André
Valero-Rosa, José
Carrasco-Valiente, Julia
Sánchez-Sánchez, Rafael
Ortega-Salas, Rosa
Moreno, María M.
Tsomaia, Natia
Swanson, Steve M.
Culler, Michael D.
Requena, María J.
Castaño, Justo P.
Luque, Raúl M.
The oncogenic role of the In1-ghrelin splicing variant in prostate cancer aggressiveness
title The oncogenic role of the In1-ghrelin splicing variant in prostate cancer aggressiveness
title_full The oncogenic role of the In1-ghrelin splicing variant in prostate cancer aggressiveness
title_fullStr The oncogenic role of the In1-ghrelin splicing variant in prostate cancer aggressiveness
title_full_unstemmed The oncogenic role of the In1-ghrelin splicing variant in prostate cancer aggressiveness
title_short The oncogenic role of the In1-ghrelin splicing variant in prostate cancer aggressiveness
title_sort oncogenic role of the in1-ghrelin splicing variant in prostate cancer aggressiveness
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5576296/
https://www.ncbi.nlm.nih.gov/pubmed/28851363
http://dx.doi.org/10.1186/s12943-017-0713-9
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