Mitochondrial DNA Affects the Expression of Nuclear Genes Involved in Immune and Stress Responses in a Breast Cancer Model

Tumor cells without mitochondrial (mt) DNA (ρ(0) cells) are auxotrophic for uridine, and their growth is supported by pyruvate. While ATP synthesis in ρ(0) cells relies on glycolysis, they fail to form tumors unless they acquire mitochondria from stromal cells. Mitochondrial acquisition restores res...

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Autores principales: Grasso, Carole, Eccles, David A., Boukalova, Stepana, Fabre, Marie-Sophie, Dawson, Rebecca H., Neuzil, Jiri, Herst, Patries M., Berridge, Michael V.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2020
Materias:
Physiology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7732479/
https://www.ncbi.nlm.nih.gov/pubmed/33329014
http://dx.doi.org/10.3389/fphys.2020.543962
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author Grasso, Carole
Eccles, David A.
Boukalova, Stepana
Fabre, Marie-Sophie
Dawson, Rebecca H.
Neuzil, Jiri
Herst, Patries M.
Berridge, Michael V.
author_facet Grasso, Carole
Eccles, David A.
Boukalova, Stepana
Fabre, Marie-Sophie
Dawson, Rebecca H.
Neuzil, Jiri
Herst, Patries M.
Berridge, Michael V.
author_sort Grasso, Carole
collection PubMed
description Tumor cells without mitochondrial (mt) DNA (ρ(0) cells) are auxotrophic for uridine, and their growth is supported by pyruvate. While ATP synthesis in ρ(0) cells relies on glycolysis, they fail to form tumors unless they acquire mitochondria from stromal cells. Mitochondrial acquisition restores respiration that is essential for de novo pyrimidine biosynthesis and for mitochondrial ATP production. The physiological processes that underpin intercellular mitochondrial transfer to tumor cells lacking mtDNA and the metabolic remodeling and restored tumorigenic properties of cells that acquire mitochondria are not well understood. Here, we investigated the changes in mitochondrial and nuclear gene expression that accompany mtDNA deletion and acquisition in metastatic murine 4T1 breast cancer cells. Loss of mitochondrial gene expression in 4T1ρ(0) cells was restored in cells recovered from subcutaneous tumors that grew from 4T1ρ(0) cells following acquisition of mtDNA from host cells. In contrast, the expression of most nuclear genes that encode respiratory complex subunits and mitochondrial ribosomal subunits was not greatly affected by loss of mtDNA, indicating ineffective mitochondria-to-nucleus communication systems for these nuclear genes. Further, analysis of nuclear genes whose expression was compromised in 4T1ρ(0) cells showed that immune- and stress-related genes were the most highly differentially expressed, representing over 70% of those with greater than 16-fold higher expression in 4T1 compared with 4T1ρ(0) cells. The monocyte recruiting chemokine, Ccl2, and Psmb8, a subunit of the immunoproteasome that generates MHCI-binding peptides, were the most highly differentially expressed. Early monocyte/macrophage recruitment into the tumor mass was compromised in 4T1ρ(0) cells but recovered before mtDNA could be detected. Taken together, our results show that mitochondrial acquisition by tumor cells without mtDNA results in bioenergetic remodeling and re-expression of genes involved in immune function and stress adaptation.
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spelling pubmed-77324792020-12-15 Mitochondrial DNA Affects the Expression of Nuclear Genes Involved in Immune and Stress Responses in a Breast Cancer Model Grasso, Carole Eccles, David A. Boukalova, Stepana Fabre, Marie-Sophie Dawson, Rebecca H. Neuzil, Jiri Herst, Patries M. Berridge, Michael V. Front Physiol Physiology Tumor cells without mitochondrial (mt) DNA (ρ(0) cells) are auxotrophic for uridine, and their growth is supported by pyruvate. While ATP synthesis in ρ(0) cells relies on glycolysis, they fail to form tumors unless they acquire mitochondria from stromal cells. Mitochondrial acquisition restores respiration that is essential for de novo pyrimidine biosynthesis and for mitochondrial ATP production. The physiological processes that underpin intercellular mitochondrial transfer to tumor cells lacking mtDNA and the metabolic remodeling and restored tumorigenic properties of cells that acquire mitochondria are not well understood. Here, we investigated the changes in mitochondrial and nuclear gene expression that accompany mtDNA deletion and acquisition in metastatic murine 4T1 breast cancer cells. Loss of mitochondrial gene expression in 4T1ρ(0) cells was restored in cells recovered from subcutaneous tumors that grew from 4T1ρ(0) cells following acquisition of mtDNA from host cells. In contrast, the expression of most nuclear genes that encode respiratory complex subunits and mitochondrial ribosomal subunits was not greatly affected by loss of mtDNA, indicating ineffective mitochondria-to-nucleus communication systems for these nuclear genes. Further, analysis of nuclear genes whose expression was compromised in 4T1ρ(0) cells showed that immune- and stress-related genes were the most highly differentially expressed, representing over 70% of those with greater than 16-fold higher expression in 4T1 compared with 4T1ρ(0) cells. The monocyte recruiting chemokine, Ccl2, and Psmb8, a subunit of the immunoproteasome that generates MHCI-binding peptides, were the most highly differentially expressed. Early monocyte/macrophage recruitment into the tumor mass was compromised in 4T1ρ(0) cells but recovered before mtDNA could be detected. Taken together, our results show that mitochondrial acquisition by tumor cells without mtDNA results in bioenergetic remodeling and re-expression of genes involved in immune function and stress adaptation. Frontiers Media S.A. 2020-11-24 /pmc/articles/PMC7732479/ /pubmed/33329014 http://dx.doi.org/10.3389/fphys.2020.543962 Text en Copyright © 2020 Grasso, Eccles, Boukalova, Fabre, Dawson, Neuzil, Herst and Berridge. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Physiology
Grasso, Carole
Eccles, David A.
Boukalova, Stepana
Fabre, Marie-Sophie
Dawson, Rebecca H.
Neuzil, Jiri
Herst, Patries M.
Berridge, Michael V.
Mitochondrial DNA Affects the Expression of Nuclear Genes Involved in Immune and Stress Responses in a Breast Cancer Model
title Mitochondrial DNA Affects the Expression of Nuclear Genes Involved in Immune and Stress Responses in a Breast Cancer Model
title_full Mitochondrial DNA Affects the Expression of Nuclear Genes Involved in Immune and Stress Responses in a Breast Cancer Model
title_fullStr Mitochondrial DNA Affects the Expression of Nuclear Genes Involved in Immune and Stress Responses in a Breast Cancer Model
title_full_unstemmed Mitochondrial DNA Affects the Expression of Nuclear Genes Involved in Immune and Stress Responses in a Breast Cancer Model
title_short Mitochondrial DNA Affects the Expression of Nuclear Genes Involved in Immune and Stress Responses in a Breast Cancer Model
title_sort mitochondrial dna affects the expression of nuclear genes involved in immune and stress responses in a breast cancer model
topic Physiology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7732479/
https://www.ncbi.nlm.nih.gov/pubmed/33329014
http://dx.doi.org/10.3389/fphys.2020.543962
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