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Pegvisomant in acromegaly: a multicenter real-life study in Argentina

OBJECTIVE: To describe the long term safety and efficacy of pegvisomant (PEGV), and the predictors of treatment response in patients with acromegaly in the real life setting. SUBJECTS AND METHODS: We retrospectively reviewed the clinical, hormonal and radiological data of acromegalic patients treate...

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Autores principales: Basavilbaso, Natalia Ximena Garcia, Ballarino, Maria Carolina, Bruera, Darío, Bruno, Oscar D., Chervin, Alberto B., Danilowicz, Karina, Fainstein-Day, Patricia, Fidalgo, Silvina Gabriela, Frigeri, Adriana, Glerean, Mariela, Guelman, Rodolfo, Isaac, Gabriel, Katz, Debora Adela, Knoblovits, Pablo, Librandi, Fabiana, Montes, Monica López, Mallea-Gil, Maria Susana, Manavela, Marcos, Mereshian, Paula, Moncet, Daniel, Pignatta, Analia, Rogozinsky, Amelia, Sago, Laura R., Servidio, Marisa, Spezzi, Monica, Stalldecker, Graciela, Tkatch, Julieta, Vitale, Nicolas Marcelo, Guitelman, Mirtha
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Sociedade Brasileira de Endocrinologia e Metabologia 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10528651/
https://www.ncbi.nlm.nih.gov/pubmed/31460622
http://dx.doi.org/10.20945/2359-3997000000160
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author Basavilbaso, Natalia Ximena Garcia
Ballarino, Maria Carolina
Bruera, Darío
Bruno, Oscar D.
Chervin, Alberto B.
Danilowicz, Karina
Fainstein-Day, Patricia
Fidalgo, Silvina Gabriela
Frigeri, Adriana
Glerean, Mariela
Guelman, Rodolfo
Isaac, Gabriel
Katz, Debora Adela
Knoblovits, Pablo
Librandi, Fabiana
Montes, Monica López
Mallea-Gil, Maria Susana
Manavela, Marcos
Mereshian, Paula
Moncet, Daniel
Pignatta, Analia
Rogozinsky, Amelia
Sago, Laura R.
Servidio, Marisa
Spezzi, Monica
Stalldecker, Graciela
Tkatch, Julieta
Vitale, Nicolas Marcelo
Guitelman, Mirtha
author_facet Basavilbaso, Natalia Ximena Garcia
Ballarino, Maria Carolina
Bruera, Darío
Bruno, Oscar D.
Chervin, Alberto B.
Danilowicz, Karina
Fainstein-Day, Patricia
Fidalgo, Silvina Gabriela
Frigeri, Adriana
Glerean, Mariela
Guelman, Rodolfo
Isaac, Gabriel
Katz, Debora Adela
Knoblovits, Pablo
Librandi, Fabiana
Montes, Monica López
Mallea-Gil, Maria Susana
Manavela, Marcos
Mereshian, Paula
Moncet, Daniel
Pignatta, Analia
Rogozinsky, Amelia
Sago, Laura R.
Servidio, Marisa
Spezzi, Monica
Stalldecker, Graciela
Tkatch, Julieta
Vitale, Nicolas Marcelo
Guitelman, Mirtha
author_sort Basavilbaso, Natalia Ximena Garcia
collection PubMed
description OBJECTIVE: To describe the long term safety and efficacy of pegvisomant (PEGV), and the predictors of treatment response in patients with acromegaly in the real life setting. SUBJECTS AND METHODS: We retrospectively reviewed the clinical, hormonal and radiological data of acromegalic patients treated with PEGV in 17 Argentine centers. RESULTS: Seventy-five patients (age range 22-77, 51 females) with acromegaly have been treated with PEGV for up to 118 months (median 27 months). Before PEGV, 97.3% of patients had been treated with medical therapy, surgery and/or radiotherapy, two patients had no previous treatment. At that time, all patients had an IGF-1 above the upper normal limit (ULN) (mean 2.4 x ULN ± 0.98, range 1.25-7). At diagnosis of acromegaly 84% presented macroadenomas, prior to PEGV only 23,5% of patients remained with tumor remnant > 1 cm, the remaining showed normal or less than 1 cm images. Disease control (IGF-1 ≤ 1.2 x ULN) was achieved in 62.9% of patients with a mean dose of 11.8 mg/day. Thirty-four patients (45%) received PEGV monotherapy, while 41 (55%) received combined therapy with either somatostatin analogues and/or cabergoline. Adverse events related to PEGV were: local injection site reaction in 5.3%, elevated liver enzymes in 9.3%, and tumor size growth in 9.8%. Pre-PEGV IGF-I level was the only predictor of treatment response: 2.1 x ULN vs 2.8 x ULN in controlled and uncontrolled patients respectively (p < 0.001). CONCLUSION: this long term experience indicates PEGV treatment was highly effective and safe in our series of Argentine patients with acromegaly refractory to standard therapies. Arch Endocrinol Metab. 2019;63(4):320-7
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spelling pubmed-105286512023-09-28 Pegvisomant in acromegaly: a multicenter real-life study in Argentina Basavilbaso, Natalia Ximena Garcia Ballarino, Maria Carolina Bruera, Darío Bruno, Oscar D. Chervin, Alberto B. Danilowicz, Karina Fainstein-Day, Patricia Fidalgo, Silvina Gabriela Frigeri, Adriana Glerean, Mariela Guelman, Rodolfo Isaac, Gabriel Katz, Debora Adela Knoblovits, Pablo Librandi, Fabiana Montes, Monica López Mallea-Gil, Maria Susana Manavela, Marcos Mereshian, Paula Moncet, Daniel Pignatta, Analia Rogozinsky, Amelia Sago, Laura R. Servidio, Marisa Spezzi, Monica Stalldecker, Graciela Tkatch, Julieta Vitale, Nicolas Marcelo Guitelman, Mirtha Arch Endocrinol Metab Original Articles OBJECTIVE: To describe the long term safety and efficacy of pegvisomant (PEGV), and the predictors of treatment response in patients with acromegaly in the real life setting. SUBJECTS AND METHODS: We retrospectively reviewed the clinical, hormonal and radiological data of acromegalic patients treated with PEGV in 17 Argentine centers. RESULTS: Seventy-five patients (age range 22-77, 51 females) with acromegaly have been treated with PEGV for up to 118 months (median 27 months). Before PEGV, 97.3% of patients had been treated with medical therapy, surgery and/or radiotherapy, two patients had no previous treatment. At that time, all patients had an IGF-1 above the upper normal limit (ULN) (mean 2.4 x ULN ± 0.98, range 1.25-7). At diagnosis of acromegaly 84% presented macroadenomas, prior to PEGV only 23,5% of patients remained with tumor remnant > 1 cm, the remaining showed normal or less than 1 cm images. Disease control (IGF-1 ≤ 1.2 x ULN) was achieved in 62.9% of patients with a mean dose of 11.8 mg/day. Thirty-four patients (45%) received PEGV monotherapy, while 41 (55%) received combined therapy with either somatostatin analogues and/or cabergoline. Adverse events related to PEGV were: local injection site reaction in 5.3%, elevated liver enzymes in 9.3%, and tumor size growth in 9.8%. Pre-PEGV IGF-I level was the only predictor of treatment response: 2.1 x ULN vs 2.8 x ULN in controlled and uncontrolled patients respectively (p < 0.001). CONCLUSION: this long term experience indicates PEGV treatment was highly effective and safe in our series of Argentine patients with acromegaly refractory to standard therapies. Arch Endocrinol Metab. 2019;63(4):320-7 Sociedade Brasileira de Endocrinologia e Metabologia 2019-08-14 /pmc/articles/PMC10528651/ /pubmed/31460622 http://dx.doi.org/10.20945/2359-3997000000160 Text en https://creativecommons.org/licenses/by/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Basavilbaso, Natalia Ximena Garcia
Ballarino, Maria Carolina
Bruera, Darío
Bruno, Oscar D.
Chervin, Alberto B.
Danilowicz, Karina
Fainstein-Day, Patricia
Fidalgo, Silvina Gabriela
Frigeri, Adriana
Glerean, Mariela
Guelman, Rodolfo
Isaac, Gabriel
Katz, Debora Adela
Knoblovits, Pablo
Librandi, Fabiana
Montes, Monica López
Mallea-Gil, Maria Susana
Manavela, Marcos
Mereshian, Paula
Moncet, Daniel
Pignatta, Analia
Rogozinsky, Amelia
Sago, Laura R.
Servidio, Marisa
Spezzi, Monica
Stalldecker, Graciela
Tkatch, Julieta
Vitale, Nicolas Marcelo
Guitelman, Mirtha
Pegvisomant in acromegaly: a multicenter real-life study in Argentina
title Pegvisomant in acromegaly: a multicenter real-life study in Argentina
title_full Pegvisomant in acromegaly: a multicenter real-life study in Argentina
title_fullStr Pegvisomant in acromegaly: a multicenter real-life study in Argentina
title_full_unstemmed Pegvisomant in acromegaly: a multicenter real-life study in Argentina
title_short Pegvisomant in acromegaly: a multicenter real-life study in Argentina
title_sort pegvisomant in acromegaly: a multicenter real-life study in argentina
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10528651/
https://www.ncbi.nlm.nih.gov/pubmed/31460622
http://dx.doi.org/10.20945/2359-3997000000160
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