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The Sedoheptulose Kinase CARKL Directs Macrophage Polarization through Control of Glucose Metabolism

Immune cells are somewhat unique in that activation responses can alter quantitative phenotypes upwards of 100,000-fold. To date little is known about the metabolic adaptations necessary to mount such dramatic phenotypic shifts. Screening for novel regulators of macrophage activation, we found nonpr...

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Autores principales: Haschemi, Arvand, Kosma, Paul, Gille, Lars, Evans, Charles R., Burant, Charles F., Starkl, Philipp, Knapp, Bernhard, Haas, Robert, Schmid, Johannes A., Jandl, Christoph, Amir, Shahzada, Lubec, Gert, Park, Jaehong, Esterbauer, Harald, Bilban, Martin, Brizuela, Leonardo, Pospisilik, J. Andrew, Otterbein, Leo E., Wagner, Oswald
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3370649/
https://www.ncbi.nlm.nih.gov/pubmed/22682222
http://dx.doi.org/10.1016/j.cmet.2012.04.023
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author Haschemi, Arvand
Kosma, Paul
Gille, Lars
Evans, Charles R.
Burant, Charles F.
Starkl, Philipp
Knapp, Bernhard
Haas, Robert
Schmid, Johannes A.
Jandl, Christoph
Amir, Shahzada
Lubec, Gert
Park, Jaehong
Esterbauer, Harald
Bilban, Martin
Brizuela, Leonardo
Pospisilik, J. Andrew
Otterbein, Leo E.
Wagner, Oswald
author_facet Haschemi, Arvand
Kosma, Paul
Gille, Lars
Evans, Charles R.
Burant, Charles F.
Starkl, Philipp
Knapp, Bernhard
Haas, Robert
Schmid, Johannes A.
Jandl, Christoph
Amir, Shahzada
Lubec, Gert
Park, Jaehong
Esterbauer, Harald
Bilban, Martin
Brizuela, Leonardo
Pospisilik, J. Andrew
Otterbein, Leo E.
Wagner, Oswald
author_sort Haschemi, Arvand
collection PubMed
description Immune cells are somewhat unique in that activation responses can alter quantitative phenotypes upwards of 100,000-fold. To date little is known about the metabolic adaptations necessary to mount such dramatic phenotypic shifts. Screening for novel regulators of macrophage activation, we found nonprotein kinases of glucose metabolism among the most enriched classes of candidate immune modulators. We find that one of these, the carbohydrate kinase-like protein CARKL, is rapidly downregulated in vitro and in vivo upon LPS stimulation in both mice and humans. Interestingly, CARKL catalyzes an orphan reaction in the pentose phosphate pathway, refocusing cellular metabolism to a high-redox state upon physiological or artificial downregulation. We find that CARKL-dependent metabolic reprogramming is required for proper M1- and M2-like macrophage polarization and uncover a rate-limiting requirement for appropriate glucose flux in macrophage polarization.
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spelling pubmed-33706492012-06-18 The Sedoheptulose Kinase CARKL Directs Macrophage Polarization through Control of Glucose Metabolism Haschemi, Arvand Kosma, Paul Gille, Lars Evans, Charles R. Burant, Charles F. Starkl, Philipp Knapp, Bernhard Haas, Robert Schmid, Johannes A. Jandl, Christoph Amir, Shahzada Lubec, Gert Park, Jaehong Esterbauer, Harald Bilban, Martin Brizuela, Leonardo Pospisilik, J. Andrew Otterbein, Leo E. Wagner, Oswald Cell Metab Article Immune cells are somewhat unique in that activation responses can alter quantitative phenotypes upwards of 100,000-fold. To date little is known about the metabolic adaptations necessary to mount such dramatic phenotypic shifts. Screening for novel regulators of macrophage activation, we found nonprotein kinases of glucose metabolism among the most enriched classes of candidate immune modulators. We find that one of these, the carbohydrate kinase-like protein CARKL, is rapidly downregulated in vitro and in vivo upon LPS stimulation in both mice and humans. Interestingly, CARKL catalyzes an orphan reaction in the pentose phosphate pathway, refocusing cellular metabolism to a high-redox state upon physiological or artificial downregulation. We find that CARKL-dependent metabolic reprogramming is required for proper M1- and M2-like macrophage polarization and uncover a rate-limiting requirement for appropriate glucose flux in macrophage polarization. Cell Press 2012-06-06 /pmc/articles/PMC3370649/ /pubmed/22682222 http://dx.doi.org/10.1016/j.cmet.2012.04.023 Text en © 2012 ELL & Excerpta Medica. https://creativecommons.org/licenses/by-nc-nd/3.0/ Open Access under CC BY-NC-ND 3.0 (https://creativecommons.org/licenses/by-nc-nd/3.0/) license
spellingShingle Article
Haschemi, Arvand
Kosma, Paul
Gille, Lars
Evans, Charles R.
Burant, Charles F.
Starkl, Philipp
Knapp, Bernhard
Haas, Robert
Schmid, Johannes A.
Jandl, Christoph
Amir, Shahzada
Lubec, Gert
Park, Jaehong
Esterbauer, Harald
Bilban, Martin
Brizuela, Leonardo
Pospisilik, J. Andrew
Otterbein, Leo E.
Wagner, Oswald
The Sedoheptulose Kinase CARKL Directs Macrophage Polarization through Control of Glucose Metabolism
title The Sedoheptulose Kinase CARKL Directs Macrophage Polarization through Control of Glucose Metabolism
title_full The Sedoheptulose Kinase CARKL Directs Macrophage Polarization through Control of Glucose Metabolism
title_fullStr The Sedoheptulose Kinase CARKL Directs Macrophage Polarization through Control of Glucose Metabolism
title_full_unstemmed The Sedoheptulose Kinase CARKL Directs Macrophage Polarization through Control of Glucose Metabolism
title_short The Sedoheptulose Kinase CARKL Directs Macrophage Polarization through Control of Glucose Metabolism
title_sort sedoheptulose kinase carkl directs macrophage polarization through control of glucose metabolism
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3370649/
https://www.ncbi.nlm.nih.gov/pubmed/22682222
http://dx.doi.org/10.1016/j.cmet.2012.04.023
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