Silencing of CCR4-NOT complex subunits affects heart structure and function

The identification of genetic variants that predispose individuals to cardiovascular disease and a better understanding of their targets would be highly advantageous. Genome-wide association studies have identified variants that associate with QT-interval length (a measure of myocardial repolarizati...

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Autores principales: Elmén, Lisa, Volpato, Claudia B., Kervadec, Anaïs, Pineda, Santiago, Kalvakuri, Sreehari, Alayari, Nakissa N., Foco, Luisa, Pramstaller, Peter P., Ocorr, Karen, Rossini, Alessandra, Cammarato, Anthony, Colas, Alexandre R., Hicks, Andrew A., Bodmer, Rolf
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Company of Biologists Ltd 2020
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7390626/
https://www.ncbi.nlm.nih.gov/pubmed/32471864
http://dx.doi.org/10.1242/dmm.044727
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author Elmén, Lisa
Volpato, Claudia B.
Kervadec, Anaïs
Pineda, Santiago
Kalvakuri, Sreehari
Alayari, Nakissa N.
Foco, Luisa
Pramstaller, Peter P.
Ocorr, Karen
Rossini, Alessandra
Cammarato, Anthony
Colas, Alexandre R.
Hicks, Andrew A.
Bodmer, Rolf
author_facet Elmén, Lisa
Volpato, Claudia B.
Kervadec, Anaïs
Pineda, Santiago
Kalvakuri, Sreehari
Alayari, Nakissa N.
Foco, Luisa
Pramstaller, Peter P.
Ocorr, Karen
Rossini, Alessandra
Cammarato, Anthony
Colas, Alexandre R.
Hicks, Andrew A.
Bodmer, Rolf
author_sort Elmén, Lisa
collection PubMed
description The identification of genetic variants that predispose individuals to cardiovascular disease and a better understanding of their targets would be highly advantageous. Genome-wide association studies have identified variants that associate with QT-interval length (a measure of myocardial repolarization). Three of the strongest associating variants (single-nucleotide polymorphisms) are located in the putative promotor region of CNOT1, a gene encoding the central CNOT1 subunit of CCR4-NOT: a multifunctional, conserved complex regulating gene expression and mRNA stability and turnover. We isolated the minimum fragment of the CNOT1 promoter containing all three variants from individuals homozygous for the QT risk alleles and demonstrated that the haplotype associating with longer QT interval caused reduced reporter expression in a cardiac cell line, suggesting that reduced CNOT1 expression might contribute to abnormal QT intervals. Systematic siRNA-mediated knockdown of CCR4-NOT components in human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) revealed that silencing CNOT1 and other CCR4-NOT genes reduced their proliferative capacity. Silencing CNOT7 also shortened action potential duration. Furthermore, the cardiac-specific knockdown of Drosophila orthologs of CCR4-NOT genes in vivo (CNOT1/Not1 and CNOT7/8/Pop2) was either lethal or resulted in dilated cardiomyopathy, reduced contractility or a propensity for arrhythmia. Silencing CNOT2/Not2, CNOT4/Not4 and CNOT6/6L/twin also affected cardiac chamber size and contractility. Developmental studies suggested that CNOT1/Not1 and CNOT7/8/Pop2 are required during cardiac remodeling from larval to adult stages. To summarize, we have demonstrated how disease-associated genes identified by GWAS can be investigated by combining human cardiomyocyte cell-based and whole-organism in vivo heart models. Our results also suggest a potential link of CNOT1 and CNOT7/8 to QT alterations and further establish a crucial role of the CCR4-NOT complex in heart development and function. This article has an associated First Person interview with the first author of the paper.
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spelling pubmed-73906262020-07-30 Silencing of CCR4-NOT complex subunits affects heart structure and function Elmén, Lisa Volpato, Claudia B. Kervadec, Anaïs Pineda, Santiago Kalvakuri, Sreehari Alayari, Nakissa N. Foco, Luisa Pramstaller, Peter P. Ocorr, Karen Rossini, Alessandra Cammarato, Anthony Colas, Alexandre R. Hicks, Andrew A. Bodmer, Rolf Dis Model Mech Research Article The identification of genetic variants that predispose individuals to cardiovascular disease and a better understanding of their targets would be highly advantageous. Genome-wide association studies have identified variants that associate with QT-interval length (a measure of myocardial repolarization). Three of the strongest associating variants (single-nucleotide polymorphisms) are located in the putative promotor region of CNOT1, a gene encoding the central CNOT1 subunit of CCR4-NOT: a multifunctional, conserved complex regulating gene expression and mRNA stability and turnover. We isolated the minimum fragment of the CNOT1 promoter containing all three variants from individuals homozygous for the QT risk alleles and demonstrated that the haplotype associating with longer QT interval caused reduced reporter expression in a cardiac cell line, suggesting that reduced CNOT1 expression might contribute to abnormal QT intervals. Systematic siRNA-mediated knockdown of CCR4-NOT components in human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) revealed that silencing CNOT1 and other CCR4-NOT genes reduced their proliferative capacity. Silencing CNOT7 also shortened action potential duration. Furthermore, the cardiac-specific knockdown of Drosophila orthologs of CCR4-NOT genes in vivo (CNOT1/Not1 and CNOT7/8/Pop2) was either lethal or resulted in dilated cardiomyopathy, reduced contractility or a propensity for arrhythmia. Silencing CNOT2/Not2, CNOT4/Not4 and CNOT6/6L/twin also affected cardiac chamber size and contractility. Developmental studies suggested that CNOT1/Not1 and CNOT7/8/Pop2 are required during cardiac remodeling from larval to adult stages. To summarize, we have demonstrated how disease-associated genes identified by GWAS can be investigated by combining human cardiomyocyte cell-based and whole-organism in vivo heart models. Our results also suggest a potential link of CNOT1 and CNOT7/8 to QT alterations and further establish a crucial role of the CCR4-NOT complex in heart development and function. This article has an associated First Person interview with the first author of the paper. The Company of Biologists Ltd 2020-07-20 /pmc/articles/PMC7390626/ /pubmed/32471864 http://dx.doi.org/10.1242/dmm.044727 Text en © 2020. Published by The Company of Biologists Ltd http://creativecommons.org/licenses/by/4.0This is an Open Access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0), which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.
spellingShingle Research Article
Elmén, Lisa
Volpato, Claudia B.
Kervadec, Anaïs
Pineda, Santiago
Kalvakuri, Sreehari
Alayari, Nakissa N.
Foco, Luisa
Pramstaller, Peter P.
Ocorr, Karen
Rossini, Alessandra
Cammarato, Anthony
Colas, Alexandre R.
Hicks, Andrew A.
Bodmer, Rolf
Silencing of CCR4-NOT complex subunits affects heart structure and function
title Silencing of CCR4-NOT complex subunits affects heart structure and function
title_full Silencing of CCR4-NOT complex subunits affects heart structure and function
title_fullStr Silencing of CCR4-NOT complex subunits affects heart structure and function
title_full_unstemmed Silencing of CCR4-NOT complex subunits affects heart structure and function
title_short Silencing of CCR4-NOT complex subunits affects heart structure and function
title_sort silencing of ccr4-not complex subunits affects heart structure and function
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7390626/
https://www.ncbi.nlm.nih.gov/pubmed/32471864
http://dx.doi.org/10.1242/dmm.044727
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