Effect of TP53 deficiency and KRAS signaling on the bioenergetics of colon cancer cells in response to different substrates: A single cell study

Metabolic reprogramming is a hallmark of cancer. Somatic mutations in genes involved in oncogenic signaling pathways, including KRAS and TP53, rewire the metabolic machinery in cancer cells. We here set out to determine, at the single cell level, metabolic signatures in human colon cancer cells engi...

Descripción completa

Detalles Bibliográficos
Autores principales: Kealey, James, Düssmann, Heiko, Llorente-Folch, Irene, Niewidok, Natalia, Salvucci, Manuela, Prehn, Jochen H. M., D’Orsi, Beatrice
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Cell and Developmental Biology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9550869/
https://www.ncbi.nlm.nih.gov/pubmed/36238683
http://dx.doi.org/10.3389/fcell.2022.893677
_version_ 1784805979241578496
author Kealey, James
Düssmann, Heiko
Llorente-Folch, Irene
Niewidok, Natalia
Salvucci, Manuela
Prehn, Jochen H. M.
D’Orsi, Beatrice
author_facet Kealey, James
Düssmann, Heiko
Llorente-Folch, Irene
Niewidok, Natalia
Salvucci, Manuela
Prehn, Jochen H. M.
D’Orsi, Beatrice
author_sort Kealey, James
collection PubMed
description Metabolic reprogramming is a hallmark of cancer. Somatic mutations in genes involved in oncogenic signaling pathways, including KRAS and TP53, rewire the metabolic machinery in cancer cells. We here set out to determine, at the single cell level, metabolic signatures in human colon cancer cells engineered to express combinations of activating KRAS gene mutations and TP53 gene deletions. Specifically, we explored how somatic mutations in these genes and substrate availability (lactate, glucose, substrate deprivation) from the extracellular microenvironment affect bioenergetic parameters, including cellular ATP, NADH and mitochondrial membrane potential dynamics. Employing cytosolic and mitochondrial FRET-based ATP probes, fluorescent NADH sensors, and the membrane-permeant cationic fluorescent probe TMRM in HCT-116 cells as a model system, we observed that TP53 deletion and KRAS mutations drive a shift in metabolic signatures enabling lactate to become an efficient metabolite to replenish both ATP and NADH following nutrient deprivation. Intriguingly, cytosolic, mitochondrial and overall cellular ATP measurements revealed that, in WT KRAS cells, TP53 deficiency leads to an enhanced ATP production in the presence of extracellular lactate and glucose, and to the greatest increase in ATP following a starvation period. On the other hand, oncogenic KRAS in TP53-deficient cells reversed the alterations in cellular ATP levels. Moreover, cell population measurements of mitochondrial and glycolytic metabolism using a Seahorse analyzer demonstrated that WT KRAS TP53-silenced cells display an increase of the basal respiration and tightly-coupled mitochondria, in the presence of glucose as substrate, compared to TP53 competent cells. Furthermore, cells possessing oncogenic KRAS, independently of TP53 status, showed less pronounced mitochondrial membrane potential changes in response to metabolic nutrients. Furthermore, analysis of cytosolic and mitochondrial NADH levels revealed that the simultaneous presence of TP53 deletion and oncogenic KRAS showed the most pronounced alteration in cytosolic and mitochondrial NADH during metabolic stress. In conclusion, our findings demonstrate how activating KRAS mutation and loss of TP53 remodel cancer metabolism and lead to alterations in bioenergetics under metabolic stress conditions by modulating cellular ATP production, NADH oxidation, mitochondrial respiration and function.
format Online
Article
Text
id pubmed-9550869
institution National Center for Biotechnology Information
language English
publishDate 2022
publisher Frontiers Media S.A.
record_format MEDLINE/PubMed
spelling pubmed-95508692022-10-12 Effect of TP53 deficiency and KRAS signaling on the bioenergetics of colon cancer cells in response to different substrates: A single cell study Kealey, James Düssmann, Heiko Llorente-Folch, Irene Niewidok, Natalia Salvucci, Manuela Prehn, Jochen H. M. D’Orsi, Beatrice Front Cell Dev Biol Cell and Developmental Biology Metabolic reprogramming is a hallmark of cancer. Somatic mutations in genes involved in oncogenic signaling pathways, including KRAS and TP53, rewire the metabolic machinery in cancer cells. We here set out to determine, at the single cell level, metabolic signatures in human colon cancer cells engineered to express combinations of activating KRAS gene mutations and TP53 gene deletions. Specifically, we explored how somatic mutations in these genes and substrate availability (lactate, glucose, substrate deprivation) from the extracellular microenvironment affect bioenergetic parameters, including cellular ATP, NADH and mitochondrial membrane potential dynamics. Employing cytosolic and mitochondrial FRET-based ATP probes, fluorescent NADH sensors, and the membrane-permeant cationic fluorescent probe TMRM in HCT-116 cells as a model system, we observed that TP53 deletion and KRAS mutations drive a shift in metabolic signatures enabling lactate to become an efficient metabolite to replenish both ATP and NADH following nutrient deprivation. Intriguingly, cytosolic, mitochondrial and overall cellular ATP measurements revealed that, in WT KRAS cells, TP53 deficiency leads to an enhanced ATP production in the presence of extracellular lactate and glucose, and to the greatest increase in ATP following a starvation period. On the other hand, oncogenic KRAS in TP53-deficient cells reversed the alterations in cellular ATP levels. Moreover, cell population measurements of mitochondrial and glycolytic metabolism using a Seahorse analyzer demonstrated that WT KRAS TP53-silenced cells display an increase of the basal respiration and tightly-coupled mitochondria, in the presence of glucose as substrate, compared to TP53 competent cells. Furthermore, cells possessing oncogenic KRAS, independently of TP53 status, showed less pronounced mitochondrial membrane potential changes in response to metabolic nutrients. Furthermore, analysis of cytosolic and mitochondrial NADH levels revealed that the simultaneous presence of TP53 deletion and oncogenic KRAS showed the most pronounced alteration in cytosolic and mitochondrial NADH during metabolic stress. In conclusion, our findings demonstrate how activating KRAS mutation and loss of TP53 remodel cancer metabolism and lead to alterations in bioenergetics under metabolic stress conditions by modulating cellular ATP production, NADH oxidation, mitochondrial respiration and function. Frontiers Media S.A. 2022-09-27 /pmc/articles/PMC9550869/ /pubmed/36238683 http://dx.doi.org/10.3389/fcell.2022.893677 Text en Copyright © 2022 Kealey, Düssmann, Llorente-Folch, Niewidok, Salvucci, Prehn and D’Orsi. https://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 Cell and Developmental Biology
Kealey, James
Düssmann, Heiko
Llorente-Folch, Irene
Niewidok, Natalia
Salvucci, Manuela
Prehn, Jochen H. M.
D’Orsi, Beatrice
Effect of TP53 deficiency and KRAS signaling on the bioenergetics of colon cancer cells in response to different substrates: A single cell study
title Effect of TP53 deficiency and KRAS signaling on the bioenergetics of colon cancer cells in response to different substrates: A single cell study
title_full Effect of TP53 deficiency and KRAS signaling on the bioenergetics of colon cancer cells in response to different substrates: A single cell study
title_fullStr Effect of TP53 deficiency and KRAS signaling on the bioenergetics of colon cancer cells in response to different substrates: A single cell study
title_full_unstemmed Effect of TP53 deficiency and KRAS signaling on the bioenergetics of colon cancer cells in response to different substrates: A single cell study
title_short Effect of TP53 deficiency and KRAS signaling on the bioenergetics of colon cancer cells in response to different substrates: A single cell study
title_sort effect of tp53 deficiency and kras signaling on the bioenergetics of colon cancer cells in response to different substrates: a single cell study
topic Cell and Developmental Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9550869/
https://www.ncbi.nlm.nih.gov/pubmed/36238683
http://dx.doi.org/10.3389/fcell.2022.893677
work_keys_str_mv AT kealeyjames effectoftp53deficiencyandkrassignalingonthebioenergeticsofcoloncancercellsinresponsetodifferentsubstratesasinglecellstudy
AT dussmannheiko effectoftp53deficiencyandkrassignalingonthebioenergeticsofcoloncancercellsinresponsetodifferentsubstratesasinglecellstudy
AT llorentefolchirene effectoftp53deficiencyandkrassignalingonthebioenergeticsofcoloncancercellsinresponsetodifferentsubstratesasinglecellstudy
AT niewidoknatalia effectoftp53deficiencyandkrassignalingonthebioenergeticsofcoloncancercellsinresponsetodifferentsubstratesasinglecellstudy
AT salvuccimanuela effectoftp53deficiencyandkrassignalingonthebioenergeticsofcoloncancercellsinresponsetodifferentsubstratesasinglecellstudy
AT prehnjochenhm effectoftp53deficiencyandkrassignalingonthebioenergeticsofcoloncancercellsinresponsetodifferentsubstratesasinglecellstudy
AT dorsibeatrice effectoftp53deficiencyandkrassignalingonthebioenergeticsofcoloncancercellsinresponsetodifferentsubstratesasinglecellstudy

Ejemplares similares