Reductive carboxylation supports redox homeostasis during anchorage-independent growth

Epithelial cells receive growth and survival stimuli through their attachment to an extracellular matrix (ECM)(1). Overcoming the addiction to ECM-induced signals is required for anchorage-independent growth, a property of most malignant cells(2). Detachment from ECM is associated with enhanced reac...

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Autores principales: Jiang, Lei, Shestov, Alexander A., Swain, Pamela, Yang, Chendong, Parker, Seth J., Wang, Qiong A., Terada, Lance S., Adams, Nicholas D., McCabe, Michael T., Pietrak, Beth, Schmidt, Stan, Metallo, Christian M., Dranka, Brian P., Schwartz, Benjamin, DeBerardinis, Ralph J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2016
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4860952/
https://www.ncbi.nlm.nih.gov/pubmed/27049945
http://dx.doi.org/10.1038/nature17393
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author Jiang, Lei
Shestov, Alexander A.
Swain, Pamela
Yang, Chendong
Parker, Seth J.
Wang, Qiong A.
Terada, Lance S.
Adams, Nicholas D.
McCabe, Michael T.
Pietrak, Beth
Schmidt, Stan
Metallo, Christian M.
Dranka, Brian P.
Schwartz, Benjamin
DeBerardinis, Ralph J.
author_facet Jiang, Lei
Shestov, Alexander A.
Swain, Pamela
Yang, Chendong
Parker, Seth J.
Wang, Qiong A.
Terada, Lance S.
Adams, Nicholas D.
McCabe, Michael T.
Pietrak, Beth
Schmidt, Stan
Metallo, Christian M.
Dranka, Brian P.
Schwartz, Benjamin
DeBerardinis, Ralph J.
author_sort Jiang, Lei
collection PubMed
description Epithelial cells receive growth and survival stimuli through their attachment to an extracellular matrix (ECM)(1). Overcoming the addiction to ECM-induced signals is required for anchorage-independent growth, a property of most malignant cells(2). Detachment from ECM is associated with enhanced reactive oxygen species (ROS) due to altered glucose metabolism(2). Here we identify an unconventional pathway that supports redox homeostasis and growth during adaptation to anchorage independence. We observed that detachment from monolayer culture and growth as anchorage-independent tumor spheroids was accompanied by changes in both glucose and glutamine metabolism. Specifically, oxidation of both nutrients was suppressed in spheroids, whereas reductive formation of citrate from glutamine was enhanced. Reductive glutamine metabolism was highly dependent on cytosolic isocitrate dehydrogenase-1 (IDH1), because the activity was suppressed in cells homozygous null for IDH1 or treated with an IDH1 inhibitor. This activity occurred in absence of hypoxia, a well-known inducer of reductive metabolism. Rather, IDH1 mitigated mitochondrial ROS in spheroids, and suppressing IDH1 reduced spheroid growth through a mechanism requiring mitochondrial ROS. Isotope tracing revealed that in spheroids, isocitrate/citrate produced reductively in the cytosol could enter the mitochondria and participate in oxidative metabolism, including oxidation by IDH2. This generates NADPH in the mitochondria, enabling cells to mitigate mitochondrial ROS and maximize growth. Neither IDH1 nor IDH2 was necessary for monolayer growth, but deleting either one enhanced mitochondrial ROS and reduced spheroid size, as did deletion of the mitochondrial citrate transporter protein. Together, the data indicate that adaptation to anchorage independence requires a fundamental change in citrate metabolism, initiated by IDH1-dependent reductive carboxylation and culminating in suppression of mitochondrial ROS.
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spelling pubmed-48609522016-05-09 Reductive carboxylation supports redox homeostasis during anchorage-independent growth Jiang, Lei Shestov, Alexander A. Swain, Pamela Yang, Chendong Parker, Seth J. Wang, Qiong A. Terada, Lance S. Adams, Nicholas D. McCabe, Michael T. Pietrak, Beth Schmidt, Stan Metallo, Christian M. Dranka, Brian P. Schwartz, Benjamin DeBerardinis, Ralph J. Nature Article Epithelial cells receive growth and survival stimuli through their attachment to an extracellular matrix (ECM)(1). Overcoming the addiction to ECM-induced signals is required for anchorage-independent growth, a property of most malignant cells(2). Detachment from ECM is associated with enhanced reactive oxygen species (ROS) due to altered glucose metabolism(2). Here we identify an unconventional pathway that supports redox homeostasis and growth during adaptation to anchorage independence. We observed that detachment from monolayer culture and growth as anchorage-independent tumor spheroids was accompanied by changes in both glucose and glutamine metabolism. Specifically, oxidation of both nutrients was suppressed in spheroids, whereas reductive formation of citrate from glutamine was enhanced. Reductive glutamine metabolism was highly dependent on cytosolic isocitrate dehydrogenase-1 (IDH1), because the activity was suppressed in cells homozygous null for IDH1 or treated with an IDH1 inhibitor. This activity occurred in absence of hypoxia, a well-known inducer of reductive metabolism. Rather, IDH1 mitigated mitochondrial ROS in spheroids, and suppressing IDH1 reduced spheroid growth through a mechanism requiring mitochondrial ROS. Isotope tracing revealed that in spheroids, isocitrate/citrate produced reductively in the cytosol could enter the mitochondria and participate in oxidative metabolism, including oxidation by IDH2. This generates NADPH in the mitochondria, enabling cells to mitigate mitochondrial ROS and maximize growth. Neither IDH1 nor IDH2 was necessary for monolayer growth, but deleting either one enhanced mitochondrial ROS and reduced spheroid size, as did deletion of the mitochondrial citrate transporter protein. Together, the data indicate that adaptation to anchorage independence requires a fundamental change in citrate metabolism, initiated by IDH1-dependent reductive carboxylation and culminating in suppression of mitochondrial ROS. 2016-04-06 2016-04-14 /pmc/articles/PMC4860952/ /pubmed/27049945 http://dx.doi.org/10.1038/nature17393 Text en Reprints and permissions information is available at www.nature.com/reprints (http://www.nature.com/reprints) .
spellingShingle Article
Jiang, Lei
Shestov, Alexander A.
Swain, Pamela
Yang, Chendong
Parker, Seth J.
Wang, Qiong A.
Terada, Lance S.
Adams, Nicholas D.
McCabe, Michael T.
Pietrak, Beth
Schmidt, Stan
Metallo, Christian M.
Dranka, Brian P.
Schwartz, Benjamin
DeBerardinis, Ralph J.
Reductive carboxylation supports redox homeostasis during anchorage-independent growth
title Reductive carboxylation supports redox homeostasis during anchorage-independent growth
title_full Reductive carboxylation supports redox homeostasis during anchorage-independent growth
title_fullStr Reductive carboxylation supports redox homeostasis during anchorage-independent growth
title_full_unstemmed Reductive carboxylation supports redox homeostasis during anchorage-independent growth
title_short Reductive carboxylation supports redox homeostasis during anchorage-independent growth
title_sort reductive carboxylation supports redox homeostasis during anchorage-independent growth
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4860952/
https://www.ncbi.nlm.nih.gov/pubmed/27049945
http://dx.doi.org/10.1038/nature17393
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