MYC disrupts transcriptional and metabolic circadian oscillations in cancer and promotes enhanced biosynthesis

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The molecular circadian clock, which controls rhythmic 24-hour oscillation of genes, proteins, and metabolites in healthy tissues, is disrupted across many human cancers. Deregulated expression of the MYC oncoprotein has been shown to alter expression of molecular clock genes, leading to a disruptio...

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Autores principales: Cazarin, Juliana, DeRollo, Rachel E., Ahmad Shahidan, Siti Noor Ain Binti, Burchett, Jamison B., Mwangi, Daniel, Krishnaiah, Saikumari, Hsieh, Annie L., Walton, Zandra E., Brooks, Rebekah, Mello, Stephano S., Weljie, Aalim M., Dang, Chi V., Altman, Brian J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9881876/
https://www.ncbi.nlm.nih.gov/pubmed/36711638
http://dx.doi.org/10.1101/2023.01.03.522637
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author Cazarin, Juliana
DeRollo, Rachel E.
Ahmad Shahidan, Siti Noor Ain Binti
Burchett, Jamison B.
Mwangi, Daniel
Krishnaiah, Saikumari
Hsieh, Annie L.
Walton, Zandra E.
Brooks, Rebekah
Mello, Stephano S.
Weljie, Aalim M.
Dang, Chi V.
Altman, Brian J.
author_facet Cazarin, Juliana
DeRollo, Rachel E.
Ahmad Shahidan, Siti Noor Ain Binti
Burchett, Jamison B.
Mwangi, Daniel
Krishnaiah, Saikumari
Hsieh, Annie L.
Walton, Zandra E.
Brooks, Rebekah
Mello, Stephano S.
Weljie, Aalim M.
Dang, Chi V.
Altman, Brian J.
author_sort Cazarin, Juliana
collection PubMed
description The molecular circadian clock, which controls rhythmic 24-hour oscillation of genes, proteins, and metabolites in healthy tissues, is disrupted across many human cancers. Deregulated expression of the MYC oncoprotein has been shown to alter expression of molecular clock genes, leading to a disruption of molecular clock oscillation across cancer types. It remains unclear what benefit cancer cells gain from suppressing clock oscillation, and how this loss of molecular clock oscillation impacts global gene expression and metabolism in cancer. We hypothesized that MYC or its paralog N-MYC (collectively termed MYC herein) suppress oscillation of gene expression and metabolism to upregulate pathways involved in biosynthesis in a static, non-oscillatory fashion. To test this, cells from distinct cancer types with inducible MYC were examined, using time-series RNA-sequencing and metabolomics, to determine the extent to which MYC activation disrupts global oscillation of genes, gene expression pathways, and metabolites. We focused our analyses on genes, pathways, and metabolites that changed in common across multiple cancer cell line models. We report here that MYC disrupted over 85% of oscillating genes, while instead promoting enhanced ribosomal and mitochondrial biogenesis and suppressed cell attachment pathways. Notably, when MYC is activated, biosynthetic programs that were formerly circadian flipped to being upregulated in an oscillation-free manner. Further, activation of MYC ablates the oscillation of nutrient transporter proteins while greatly upregulating transporter expression, cell surface localization, and intracellular amino acid pools. Finally, we report that MYC disrupts metabolite oscillations and the temporal segregation of amino acid metabolism from nucleotide metabolism. Our results demonstrate that MYC disruption of the molecular circadian clock releases metabolic and biosynthetic processes from circadian control, which may provide a distinct advantage to cancer cells.
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spelling pubmed-98818762023-01-28 MYC disrupts transcriptional and metabolic circadian oscillations in cancer and promotes enhanced biosynthesis Cazarin, Juliana DeRollo, Rachel E. Ahmad Shahidan, Siti Noor Ain Binti Burchett, Jamison B. Mwangi, Daniel Krishnaiah, Saikumari Hsieh, Annie L. Walton, Zandra E. Brooks, Rebekah Mello, Stephano S. Weljie, Aalim M. Dang, Chi V. Altman, Brian J. bioRxiv Article The molecular circadian clock, which controls rhythmic 24-hour oscillation of genes, proteins, and metabolites in healthy tissues, is disrupted across many human cancers. Deregulated expression of the MYC oncoprotein has been shown to alter expression of molecular clock genes, leading to a disruption of molecular clock oscillation across cancer types. It remains unclear what benefit cancer cells gain from suppressing clock oscillation, and how this loss of molecular clock oscillation impacts global gene expression and metabolism in cancer. We hypothesized that MYC or its paralog N-MYC (collectively termed MYC herein) suppress oscillation of gene expression and metabolism to upregulate pathways involved in biosynthesis in a static, non-oscillatory fashion. To test this, cells from distinct cancer types with inducible MYC were examined, using time-series RNA-sequencing and metabolomics, to determine the extent to which MYC activation disrupts global oscillation of genes, gene expression pathways, and metabolites. We focused our analyses on genes, pathways, and metabolites that changed in common across multiple cancer cell line models. We report here that MYC disrupted over 85% of oscillating genes, while instead promoting enhanced ribosomal and mitochondrial biogenesis and suppressed cell attachment pathways. Notably, when MYC is activated, biosynthetic programs that were formerly circadian flipped to being upregulated in an oscillation-free manner. Further, activation of MYC ablates the oscillation of nutrient transporter proteins while greatly upregulating transporter expression, cell surface localization, and intracellular amino acid pools. Finally, we report that MYC disrupts metabolite oscillations and the temporal segregation of amino acid metabolism from nucleotide metabolism. Our results demonstrate that MYC disruption of the molecular circadian clock releases metabolic and biosynthetic processes from circadian control, which may provide a distinct advantage to cancer cells. Cold Spring Harbor Laboratory 2023-08-08 /pmc/articles/PMC9881876/ /pubmed/36711638 http://dx.doi.org/10.1101/2023.01.03.522637 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Article
Cazarin, Juliana
DeRollo, Rachel E.
Ahmad Shahidan, Siti Noor Ain Binti
Burchett, Jamison B.
Mwangi, Daniel
Krishnaiah, Saikumari
Hsieh, Annie L.
Walton, Zandra E.
Brooks, Rebekah
Mello, Stephano S.
Weljie, Aalim M.
Dang, Chi V.
Altman, Brian J.
MYC disrupts transcriptional and metabolic circadian oscillations in cancer and promotes enhanced biosynthesis
title MYC disrupts transcriptional and metabolic circadian oscillations in cancer and promotes enhanced biosynthesis
title_full MYC disrupts transcriptional and metabolic circadian oscillations in cancer and promotes enhanced biosynthesis
title_fullStr MYC disrupts transcriptional and metabolic circadian oscillations in cancer and promotes enhanced biosynthesis
title_full_unstemmed MYC disrupts transcriptional and metabolic circadian oscillations in cancer and promotes enhanced biosynthesis
title_short MYC disrupts transcriptional and metabolic circadian oscillations in cancer and promotes enhanced biosynthesis
title_sort myc disrupts transcriptional and metabolic circadian oscillations in cancer and promotes enhanced biosynthesis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9881876/
https://www.ncbi.nlm.nih.gov/pubmed/36711638
http://dx.doi.org/10.1101/2023.01.03.522637
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