Cellular and Molecular Mechanisms of MEK1 Inhibitor–Induced Cardiotoxicity

BACKGROUND: Trametinib is a MEK1 (mitogen-activated extracellular signal-related kinase kinase 1) inhibitor used in the treatment of BRAF (rapid accelerated fibrosarcoma B-type)–mutated metastatic melanoma. Roughly 11% of patients develop cardiomyopathy following long-term trametinib exposure. Altho...

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Autores principales: Beck, Tyler C., Arhontoulis, Dimitrios C., Morningstar, Jordan E., Hyams, Nathaniel, Stoddard, Andrew, Springs, Kendra, Mukherjee, Rupak, Helke, Kris, Guo, Lilong, Moore, Kelsey, Gensemer, Cortney, Biggs, Rachel, Petrucci, Taylor, Kwon, Jennie, Stayer, Kristina, Koren, Natalie, Harvey, Andrew, Holman, Heather, Dunne, Jaclyn, Fulmer, Diana, Vohra, Ayesha, Mai, Le, Dooley, Sarah, Weninger, Julianna, Vaena, Silvia, Romeo, Martin, Muise-Helmericks, Robin C., Mei, Ying, Norris, Russell A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9700254/
https://www.ncbi.nlm.nih.gov/pubmed/36444237
http://dx.doi.org/10.1016/j.jaccao.2022.07.009
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author Beck, Tyler C.
Arhontoulis, Dimitrios C.
Morningstar, Jordan E.
Hyams, Nathaniel
Stoddard, Andrew
Springs, Kendra
Mukherjee, Rupak
Helke, Kris
Guo, Lilong
Moore, Kelsey
Gensemer, Cortney
Biggs, Rachel
Petrucci, Taylor
Kwon, Jennie
Stayer, Kristina
Koren, Natalie
Harvey, Andrew
Holman, Heather
Dunne, Jaclyn
Fulmer, Diana
Vohra, Ayesha
Mai, Le
Dooley, Sarah
Weninger, Julianna
Vaena, Silvia
Romeo, Martin
Muise-Helmericks, Robin C.
Mei, Ying
Norris, Russell A.
author_facet Beck, Tyler C.
Arhontoulis, Dimitrios C.
Morningstar, Jordan E.
Hyams, Nathaniel
Stoddard, Andrew
Springs, Kendra
Mukherjee, Rupak
Helke, Kris
Guo, Lilong
Moore, Kelsey
Gensemer, Cortney
Biggs, Rachel
Petrucci, Taylor
Kwon, Jennie
Stayer, Kristina
Koren, Natalie
Harvey, Andrew
Holman, Heather
Dunne, Jaclyn
Fulmer, Diana
Vohra, Ayesha
Mai, Le
Dooley, Sarah
Weninger, Julianna
Vaena, Silvia
Romeo, Martin
Muise-Helmericks, Robin C.
Mei, Ying
Norris, Russell A.
author_sort Beck, Tyler C.
collection PubMed
description BACKGROUND: Trametinib is a MEK1 (mitogen-activated extracellular signal-related kinase kinase 1) inhibitor used in the treatment of BRAF (rapid accelerated fibrosarcoma B-type)–mutated metastatic melanoma. Roughly 11% of patients develop cardiomyopathy following long-term trametinib exposure. Although described clinically, the molecular landscape of trametinib cardiotoxicity has not been characterized. OBJECTIVES: The aim of this study was to test the hypothesis that trametinib promotes widespread transcriptomic and cellular changes consistent with oxidative stress and impairs cardiac function. METHODS: Mice were treated with trametinib (1 mg/kg/d). Echocardiography was performed pre- and post-treatment. Gross, histopathologic, and biochemical assessments were performed to probe for molecular and cellular changes. Human cardiac organoids were used as an in vitro measurement of cardiotoxicity and recovery. RESULTS: Long-term administration of trametinib was associated with significant reductions in survival and left ventricular ejection fraction. Histologic analyses of the heart revealed myocardial vacuolization and calcification in 28% of animals. Bulk RNA sequencing identified 435 differentially expressed genes and 116 differential signaling pathways following trametinib treatment. Upstream gene analysis predicted interleukin-6 as a regulator of 17 relevant differentially expressed genes, suggestive of PI3K/AKT and JAK/STAT activation, which was subsequently validated. Trametinib hearts displayed elevated markers of oxidative stress, myofibrillar degeneration, an 11-fold down-regulation of the apelin receptor, and connexin-43 mislocalization. To confirm the direct cardiotoxic effects of trametinib, human cardiac organoids were treated for 6 days, followed by a 6-day media-only recovery. Trametinib-treated organoids exhibited reductions in diameter and contractility, followed by partial recovery with removal of treatment. CONCLUSIONS: These data describe pathologic changes observed in trametinib cardiotoxicity, supporting the exploration of drug holidays and alternative pharmacologic strategies for disease prevention.
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spelling pubmed-97002542022-11-27 Cellular and Molecular Mechanisms of MEK1 Inhibitor–Induced Cardiotoxicity Beck, Tyler C. Arhontoulis, Dimitrios C. Morningstar, Jordan E. Hyams, Nathaniel Stoddard, Andrew Springs, Kendra Mukherjee, Rupak Helke, Kris Guo, Lilong Moore, Kelsey Gensemer, Cortney Biggs, Rachel Petrucci, Taylor Kwon, Jennie Stayer, Kristina Koren, Natalie Harvey, Andrew Holman, Heather Dunne, Jaclyn Fulmer, Diana Vohra, Ayesha Mai, Le Dooley, Sarah Weninger, Julianna Vaena, Silvia Romeo, Martin Muise-Helmericks, Robin C. Mei, Ying Norris, Russell A. JACC CardioOncol Original Research BACKGROUND: Trametinib is a MEK1 (mitogen-activated extracellular signal-related kinase kinase 1) inhibitor used in the treatment of BRAF (rapid accelerated fibrosarcoma B-type)–mutated metastatic melanoma. Roughly 11% of patients develop cardiomyopathy following long-term trametinib exposure. Although described clinically, the molecular landscape of trametinib cardiotoxicity has not been characterized. OBJECTIVES: The aim of this study was to test the hypothesis that trametinib promotes widespread transcriptomic and cellular changes consistent with oxidative stress and impairs cardiac function. METHODS: Mice were treated with trametinib (1 mg/kg/d). Echocardiography was performed pre- and post-treatment. Gross, histopathologic, and biochemical assessments were performed to probe for molecular and cellular changes. Human cardiac organoids were used as an in vitro measurement of cardiotoxicity and recovery. RESULTS: Long-term administration of trametinib was associated with significant reductions in survival and left ventricular ejection fraction. Histologic analyses of the heart revealed myocardial vacuolization and calcification in 28% of animals. Bulk RNA sequencing identified 435 differentially expressed genes and 116 differential signaling pathways following trametinib treatment. Upstream gene analysis predicted interleukin-6 as a regulator of 17 relevant differentially expressed genes, suggestive of PI3K/AKT and JAK/STAT activation, which was subsequently validated. Trametinib hearts displayed elevated markers of oxidative stress, myofibrillar degeneration, an 11-fold down-regulation of the apelin receptor, and connexin-43 mislocalization. To confirm the direct cardiotoxic effects of trametinib, human cardiac organoids were treated for 6 days, followed by a 6-day media-only recovery. Trametinib-treated organoids exhibited reductions in diameter and contractility, followed by partial recovery with removal of treatment. CONCLUSIONS: These data describe pathologic changes observed in trametinib cardiotoxicity, supporting the exploration of drug holidays and alternative pharmacologic strategies for disease prevention. Elsevier 2022-11-15 /pmc/articles/PMC9700254/ /pubmed/36444237 http://dx.doi.org/10.1016/j.jaccao.2022.07.009 Text en © 2022 Published by Elsevier on behalf of the American College of Cardiology Foundation. https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Original Research
Beck, Tyler C.
Arhontoulis, Dimitrios C.
Morningstar, Jordan E.
Hyams, Nathaniel
Stoddard, Andrew
Springs, Kendra
Mukherjee, Rupak
Helke, Kris
Guo, Lilong
Moore, Kelsey
Gensemer, Cortney
Biggs, Rachel
Petrucci, Taylor
Kwon, Jennie
Stayer, Kristina
Koren, Natalie
Harvey, Andrew
Holman, Heather
Dunne, Jaclyn
Fulmer, Diana
Vohra, Ayesha
Mai, Le
Dooley, Sarah
Weninger, Julianna
Vaena, Silvia
Romeo, Martin
Muise-Helmericks, Robin C.
Mei, Ying
Norris, Russell A.
Cellular and Molecular Mechanisms of MEK1 Inhibitor–Induced Cardiotoxicity
title Cellular and Molecular Mechanisms of MEK1 Inhibitor–Induced Cardiotoxicity
title_full Cellular and Molecular Mechanisms of MEK1 Inhibitor–Induced Cardiotoxicity
title_fullStr Cellular and Molecular Mechanisms of MEK1 Inhibitor–Induced Cardiotoxicity
title_full_unstemmed Cellular and Molecular Mechanisms of MEK1 Inhibitor–Induced Cardiotoxicity
title_short Cellular and Molecular Mechanisms of MEK1 Inhibitor–Induced Cardiotoxicity
title_sort cellular and molecular mechanisms of mek1 inhibitor–induced cardiotoxicity
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9700254/
https://www.ncbi.nlm.nih.gov/pubmed/36444237
http://dx.doi.org/10.1016/j.jaccao.2022.07.009
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