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BIM-23A760 influences key functional endpoints in pituitary adenomas and normal pituitaries: molecular mechanisms underlying the differential response in adenomas

Chimeric somatostatin/dopamine compounds such as BIM-23A760, an sst2/sst5/D(2) receptors-agonist, have emerged as promising new approaches to treat pituitary adenomas. However, information on direct in vitro effects of BIM-23A760 in normal and tumoral pituitaries remains incomplete. The objective of...

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Autores principales: Ibáñez-Costa, Alejandro, López-Sánchez, Laura M., Gahete, Manuel D., Rivero-Cortés, Esther, Vázquez-Borrego, Mari C., Gálvez, María A., de la Riva, Andrés, Venegas-Moreno, Eva, Jiménez-Reina, Luis, Moreno-Carazo, Alberto, Tinahones, Francisco J., Maraver-Selfa, Silvia, Japón, Miguel A., García-Arnés, Juan A., Soto-Moreno, Alfonso, Webb, Susan M., Kineman, Rhonda D., Culler, Michael D., Castaño, Justo P., Luque, Raúl M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5299479/
https://www.ncbi.nlm.nih.gov/pubmed/28181484
http://dx.doi.org/10.1038/srep42002
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author Ibáñez-Costa, Alejandro
López-Sánchez, Laura M.
Gahete, Manuel D.
Rivero-Cortés, Esther
Vázquez-Borrego, Mari C.
Gálvez, María A.
de la Riva, Andrés
Venegas-Moreno, Eva
Jiménez-Reina, Luis
Moreno-Carazo, Alberto
Tinahones, Francisco J.
Maraver-Selfa, Silvia
Japón, Miguel A.
García-Arnés, Juan A.
Soto-Moreno, Alfonso
Webb, Susan M.
Kineman, Rhonda D.
Culler, Michael D.
Castaño, Justo P.
Luque, Raúl M.
author_facet Ibáñez-Costa, Alejandro
López-Sánchez, Laura M.
Gahete, Manuel D.
Rivero-Cortés, Esther
Vázquez-Borrego, Mari C.
Gálvez, María A.
de la Riva, Andrés
Venegas-Moreno, Eva
Jiménez-Reina, Luis
Moreno-Carazo, Alberto
Tinahones, Francisco J.
Maraver-Selfa, Silvia
Japón, Miguel A.
García-Arnés, Juan A.
Soto-Moreno, Alfonso
Webb, Susan M.
Kineman, Rhonda D.
Culler, Michael D.
Castaño, Justo P.
Luque, Raúl M.
author_sort Ibáñez-Costa, Alejandro
collection PubMed
description Chimeric somatostatin/dopamine compounds such as BIM-23A760, an sst2/sst5/D(2) receptors-agonist, have emerged as promising new approaches to treat pituitary adenomas. However, information on direct in vitro effects of BIM-23A760 in normal and tumoral pituitaries remains incomplete. The objective of this study was to analyze BIM-23A760 effects on functional parameters (Ca(2+) signaling, hormone expression/secretion, cell viability and apoptosis) in pituitary adenomas (n = 74), and to compare with the responses of normal primate and human pituitaries (n = 3–5). Primate and human normal pituitaries exhibited similar sst2/sst5/D2 expression patterns, wherein BIM-23A760 inhibited the expression/secretion of several pituitary hormones (specially GH/PRL), which was accompanied by increased sst2/sst5/D2 expression in primates and decreased Ca(2+) concentration in human cells. In tumoral pituitaries, BIM-23A760 also inhibited Ca(2+) concentration, hormone secretion/expression and proliferation. However, BIM-23A760 elicited stimulatory effects in a subset of GHomas, ACTHomas and NFPAs in terms of Ca(2+) signaling and/or hormone secretion, which was associated with the relative somatostatin/dopamine-receptors levels, especially sst5 and sst5TMD4. The chimeric sst2/sst5/D(2) compound BIM-23A760 affects multiple, clinically relevant parameters on pituitary adenomas and may represent a valuable therapeutic tool. The relative ssts/D(2) expression profile, particularly sst5 and/or sst5TMD4 levels, might represent useful molecular markers to predict the ultimate response of pituitary adenomas to BIM-23A760.
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spelling pubmed-52994792017-02-13 BIM-23A760 influences key functional endpoints in pituitary adenomas and normal pituitaries: molecular mechanisms underlying the differential response in adenomas Ibáñez-Costa, Alejandro López-Sánchez, Laura M. Gahete, Manuel D. Rivero-Cortés, Esther Vázquez-Borrego, Mari C. Gálvez, María A. de la Riva, Andrés Venegas-Moreno, Eva Jiménez-Reina, Luis Moreno-Carazo, Alberto Tinahones, Francisco J. Maraver-Selfa, Silvia Japón, Miguel A. García-Arnés, Juan A. Soto-Moreno, Alfonso Webb, Susan M. Kineman, Rhonda D. Culler, Michael D. Castaño, Justo P. Luque, Raúl M. Sci Rep Article Chimeric somatostatin/dopamine compounds such as BIM-23A760, an sst2/sst5/D(2) receptors-agonist, have emerged as promising new approaches to treat pituitary adenomas. However, information on direct in vitro effects of BIM-23A760 in normal and tumoral pituitaries remains incomplete. The objective of this study was to analyze BIM-23A760 effects on functional parameters (Ca(2+) signaling, hormone expression/secretion, cell viability and apoptosis) in pituitary adenomas (n = 74), and to compare with the responses of normal primate and human pituitaries (n = 3–5). Primate and human normal pituitaries exhibited similar sst2/sst5/D2 expression patterns, wherein BIM-23A760 inhibited the expression/secretion of several pituitary hormones (specially GH/PRL), which was accompanied by increased sst2/sst5/D2 expression in primates and decreased Ca(2+) concentration in human cells. In tumoral pituitaries, BIM-23A760 also inhibited Ca(2+) concentration, hormone secretion/expression and proliferation. However, BIM-23A760 elicited stimulatory effects in a subset of GHomas, ACTHomas and NFPAs in terms of Ca(2+) signaling and/or hormone secretion, which was associated with the relative somatostatin/dopamine-receptors levels, especially sst5 and sst5TMD4. The chimeric sst2/sst5/D(2) compound BIM-23A760 affects multiple, clinically relevant parameters on pituitary adenomas and may represent a valuable therapeutic tool. The relative ssts/D(2) expression profile, particularly sst5 and/or sst5TMD4 levels, might represent useful molecular markers to predict the ultimate response of pituitary adenomas to BIM-23A760. Nature Publishing Group 2017-02-09 /pmc/articles/PMC5299479/ /pubmed/28181484 http://dx.doi.org/10.1038/srep42002 Text en Copyright © 2017, The Author(s) http://creativecommons.org/licenses/by/4.0/ This work is licensed under a Creative Commons Attribution 4.0 International License. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in the credit line; if the material is not included under the Creative Commons license, users will need to obtain permission from the license holder to reproduce the material. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/
spellingShingle Article
Ibáñez-Costa, Alejandro
López-Sánchez, Laura M.
Gahete, Manuel D.
Rivero-Cortés, Esther
Vázquez-Borrego, Mari C.
Gálvez, María A.
de la Riva, Andrés
Venegas-Moreno, Eva
Jiménez-Reina, Luis
Moreno-Carazo, Alberto
Tinahones, Francisco J.
Maraver-Selfa, Silvia
Japón, Miguel A.
García-Arnés, Juan A.
Soto-Moreno, Alfonso
Webb, Susan M.
Kineman, Rhonda D.
Culler, Michael D.
Castaño, Justo P.
Luque, Raúl M.
BIM-23A760 influences key functional endpoints in pituitary adenomas and normal pituitaries: molecular mechanisms underlying the differential response in adenomas
title BIM-23A760 influences key functional endpoints in pituitary adenomas and normal pituitaries: molecular mechanisms underlying the differential response in adenomas
title_full BIM-23A760 influences key functional endpoints in pituitary adenomas and normal pituitaries: molecular mechanisms underlying the differential response in adenomas
title_fullStr BIM-23A760 influences key functional endpoints in pituitary adenomas and normal pituitaries: molecular mechanisms underlying the differential response in adenomas
title_full_unstemmed BIM-23A760 influences key functional endpoints in pituitary adenomas and normal pituitaries: molecular mechanisms underlying the differential response in adenomas
title_short BIM-23A760 influences key functional endpoints in pituitary adenomas and normal pituitaries: molecular mechanisms underlying the differential response in adenomas
title_sort bim-23a760 influences key functional endpoints in pituitary adenomas and normal pituitaries: molecular mechanisms underlying the differential response in adenomas
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5299479/
https://www.ncbi.nlm.nih.gov/pubmed/28181484
http://dx.doi.org/10.1038/srep42002
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