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Mitochondrial Respiration in Human Colorectal and Breast Cancer Clinical Material Is Regulated Differently

We conducted quantitative cellular respiration analysis on samples taken from human breast cancer (HBC) and human colorectal cancer (HCC) patients. Respiratory capacity is not lost as a result of tumor formation and even though, functionally, complex I in HCC was found to be suppressed, it was not e...

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Autores principales: Koit, Andre, Shevchuk, Igor, Ounpuu, Lyudmila, Klepinin, Aleksandr, Chekulayev, Vladimir, Timohhina, Natalja, Tepp, Kersti, Puurand, Marju, Truu, Laura, Heck, Karoliina, Valvere, Vahur, Guzun, Rita, Kaambre, Tuuli
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5525093/
https://www.ncbi.nlm.nih.gov/pubmed/28781720
http://dx.doi.org/10.1155/2017/1372640
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author Koit, Andre
Shevchuk, Igor
Ounpuu, Lyudmila
Klepinin, Aleksandr
Chekulayev, Vladimir
Timohhina, Natalja
Tepp, Kersti
Puurand, Marju
Truu, Laura
Heck, Karoliina
Valvere, Vahur
Guzun, Rita
Kaambre, Tuuli
author_facet Koit, Andre
Shevchuk, Igor
Ounpuu, Lyudmila
Klepinin, Aleksandr
Chekulayev, Vladimir
Timohhina, Natalja
Tepp, Kersti
Puurand, Marju
Truu, Laura
Heck, Karoliina
Valvere, Vahur
Guzun, Rita
Kaambre, Tuuli
author_sort Koit, Andre
collection PubMed
description We conducted quantitative cellular respiration analysis on samples taken from human breast cancer (HBC) and human colorectal cancer (HCC) patients. Respiratory capacity is not lost as a result of tumor formation and even though, functionally, complex I in HCC was found to be suppressed, it was not evident on the protein level. Additionally, metabolic control analysis was used to quantify the role of components of mitochondrial interactosome. The main rate-controlling steps in HBC are complex IV and adenine nucleotide transporter, but in HCC, complexes I and III. Our kinetic measurements confirmed previous studies that respiratory chain complexes I and III in HBC and HCC can be assembled into supercomplexes with a possible partial addition from the complex IV pool. Therefore, the kinetic method can be a useful addition in studying supercomplexes in cell lines or human samples. In addition, when results from culture cells were compared to those from clinical samples, clear differences were present, but we also detected two different types of mitochondria within clinical HBC samples, possibly linked to two-compartment metabolism. Taken together, our data show that mitochondrial respiration and regulation of mitochondrial membrane permeability have substantial differences between these two cancer types when compared to each other to their adjacent healthy tissue or to respective cell cultures.
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spelling pubmed-55250932017-08-06 Mitochondrial Respiration in Human Colorectal and Breast Cancer Clinical Material Is Regulated Differently Koit, Andre Shevchuk, Igor Ounpuu, Lyudmila Klepinin, Aleksandr Chekulayev, Vladimir Timohhina, Natalja Tepp, Kersti Puurand, Marju Truu, Laura Heck, Karoliina Valvere, Vahur Guzun, Rita Kaambre, Tuuli Oxid Med Cell Longev Research Article We conducted quantitative cellular respiration analysis on samples taken from human breast cancer (HBC) and human colorectal cancer (HCC) patients. Respiratory capacity is not lost as a result of tumor formation and even though, functionally, complex I in HCC was found to be suppressed, it was not evident on the protein level. Additionally, metabolic control analysis was used to quantify the role of components of mitochondrial interactosome. The main rate-controlling steps in HBC are complex IV and adenine nucleotide transporter, but in HCC, complexes I and III. Our kinetic measurements confirmed previous studies that respiratory chain complexes I and III in HBC and HCC can be assembled into supercomplexes with a possible partial addition from the complex IV pool. Therefore, the kinetic method can be a useful addition in studying supercomplexes in cell lines or human samples. In addition, when results from culture cells were compared to those from clinical samples, clear differences were present, but we also detected two different types of mitochondria within clinical HBC samples, possibly linked to two-compartment metabolism. Taken together, our data show that mitochondrial respiration and regulation of mitochondrial membrane permeability have substantial differences between these two cancer types when compared to each other to their adjacent healthy tissue or to respective cell cultures. Hindawi 2017 2017-07-11 /pmc/articles/PMC5525093/ /pubmed/28781720 http://dx.doi.org/10.1155/2017/1372640 Text en Copyright © 2017 Andre Koit et al. http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Koit, Andre
Shevchuk, Igor
Ounpuu, Lyudmila
Klepinin, Aleksandr
Chekulayev, Vladimir
Timohhina, Natalja
Tepp, Kersti
Puurand, Marju
Truu, Laura
Heck, Karoliina
Valvere, Vahur
Guzun, Rita
Kaambre, Tuuli
Mitochondrial Respiration in Human Colorectal and Breast Cancer Clinical Material Is Regulated Differently
title Mitochondrial Respiration in Human Colorectal and Breast Cancer Clinical Material Is Regulated Differently
title_full Mitochondrial Respiration in Human Colorectal and Breast Cancer Clinical Material Is Regulated Differently
title_fullStr Mitochondrial Respiration in Human Colorectal and Breast Cancer Clinical Material Is Regulated Differently
title_full_unstemmed Mitochondrial Respiration in Human Colorectal and Breast Cancer Clinical Material Is Regulated Differently
title_short Mitochondrial Respiration in Human Colorectal and Breast Cancer Clinical Material Is Regulated Differently
title_sort mitochondrial respiration in human colorectal and breast cancer clinical material is regulated differently
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5525093/
https://www.ncbi.nlm.nih.gov/pubmed/28781720
http://dx.doi.org/10.1155/2017/1372640
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