Acly Deficiency Enhances Myelopoiesis through Acetyl Coenzyme A and Metabolic–Epigenetic Cross-Talk

Hematopoiesis integrates cytokine signaling, metabolism, and epigenetic modifications to regulate blood cell generation. These processes are linked, as metabolites provide essential substrates for epigenetic marks. In this study, we demonstrate that ATP citrate lyase (Acly), which metabolizes citrat...

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Autores principales: Greenwood, Dalton L., Ramsey, Haley E., Nguyen, Phuong T. T., Patterson, Andrew R., Voss, Kelsey, Bader, Jackie E., Sugiura, Ayaka, Bacigalupa, Zachary A., Schaefer, Samuel, Ye, Xiang, Dahunsi, Debolanle O., Madden, Matthew Z., Wellen, Kathryn E., Savona, Michael R., Ferrell, P. Brent, Rathmell, Jeffrey C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2022
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9935084/
https://www.ncbi.nlm.nih.gov/pubmed/36547387
http://dx.doi.org/10.4049/immunohorizons.2200086
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author Greenwood, Dalton L.
Ramsey, Haley E.
Nguyen, Phuong T. T.
Patterson, Andrew R.
Voss, Kelsey
Bader, Jackie E.
Sugiura, Ayaka
Bacigalupa, Zachary A.
Schaefer, Samuel
Ye, Xiang
Dahunsi, Debolanle O.
Madden, Matthew Z.
Wellen, Kathryn E.
Savona, Michael R.
Ferrell, P. Brent
Rathmell, Jeffrey C.
author_facet Greenwood, Dalton L.
Ramsey, Haley E.
Nguyen, Phuong T. T.
Patterson, Andrew R.
Voss, Kelsey
Bader, Jackie E.
Sugiura, Ayaka
Bacigalupa, Zachary A.
Schaefer, Samuel
Ye, Xiang
Dahunsi, Debolanle O.
Madden, Matthew Z.
Wellen, Kathryn E.
Savona, Michael R.
Ferrell, P. Brent
Rathmell, Jeffrey C.
author_sort Greenwood, Dalton L.
collection PubMed
description Hematopoiesis integrates cytokine signaling, metabolism, and epigenetic modifications to regulate blood cell generation. These processes are linked, as metabolites provide essential substrates for epigenetic marks. In this study, we demonstrate that ATP citrate lyase (Acly), which metabolizes citrate to generate cytosolic acetyl-CoA and is of clinical interest, can regulate chromatin accessibility to limit myeloid differentiation. Acly was tested for a role in murine hematopoiesis by small-molecule inhibition or genetic deletion in lineage-depleted, c-Kit–enriched hematopoietic stem and progenitor cells from Mus musculus. Treatments increased the abundance of cell populations that expressed the myeloid integrin CD11b and other markers of myeloid differentiation. When single-cell RNA sequencing was performed, we found that Acly inhibitor–treated hematopoietic stem and progenitor cells exhibited greater gene expression signatures for macrophages and enrichment of these populations. Similarly, the single-cell assay for transposase-accessible chromatin sequencing showed increased chromatin accessibility at genes associated with myeloid differentiation, including CD11b, CD11c, and IRF8. Mechanistically, Acly deficiency altered chromatin accessibility and expression of multiple C/EBP family transcription factors known to regulate myeloid differentiation and cell metabolism, with increased Cebpe and decreased Cebpa and Cebpb. This effect of Acly deficiency was accompanied by altered mitochondrial metabolism with decreased mitochondrial polarization but increased mitochondrial content and production of reactive oxygen species. The bias to myeloid differentiation appeared due to insufficient generation of acetyl-CoA, as exogenous acetate to support alternate compensatory pathways to produce acetyl-CoA reversed this phenotype. Acly inhibition thus can promote myelopoiesis through deprivation of acetyl-CoA and altered histone acetylome to regulate C/EBP transcription factor family activity for myeloid differentiation.
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spelling pubmed-99350842023-12-01 Acly Deficiency Enhances Myelopoiesis through Acetyl Coenzyme A and Metabolic–Epigenetic Cross-Talk Greenwood, Dalton L. Ramsey, Haley E. Nguyen, Phuong T. T. Patterson, Andrew R. Voss, Kelsey Bader, Jackie E. Sugiura, Ayaka Bacigalupa, Zachary A. Schaefer, Samuel Ye, Xiang Dahunsi, Debolanle O. Madden, Matthew Z. Wellen, Kathryn E. Savona, Michael R. Ferrell, P. Brent Rathmell, Jeffrey C. Immunohorizons Article Hematopoiesis integrates cytokine signaling, metabolism, and epigenetic modifications to regulate blood cell generation. These processes are linked, as metabolites provide essential substrates for epigenetic marks. In this study, we demonstrate that ATP citrate lyase (Acly), which metabolizes citrate to generate cytosolic acetyl-CoA and is of clinical interest, can regulate chromatin accessibility to limit myeloid differentiation. Acly was tested for a role in murine hematopoiesis by small-molecule inhibition or genetic deletion in lineage-depleted, c-Kit–enriched hematopoietic stem and progenitor cells from Mus musculus. Treatments increased the abundance of cell populations that expressed the myeloid integrin CD11b and other markers of myeloid differentiation. When single-cell RNA sequencing was performed, we found that Acly inhibitor–treated hematopoietic stem and progenitor cells exhibited greater gene expression signatures for macrophages and enrichment of these populations. Similarly, the single-cell assay for transposase-accessible chromatin sequencing showed increased chromatin accessibility at genes associated with myeloid differentiation, including CD11b, CD11c, and IRF8. Mechanistically, Acly deficiency altered chromatin accessibility and expression of multiple C/EBP family transcription factors known to regulate myeloid differentiation and cell metabolism, with increased Cebpe and decreased Cebpa and Cebpb. This effect of Acly deficiency was accompanied by altered mitochondrial metabolism with decreased mitochondrial polarization but increased mitochondrial content and production of reactive oxygen species. The bias to myeloid differentiation appeared due to insufficient generation of acetyl-CoA, as exogenous acetate to support alternate compensatory pathways to produce acetyl-CoA reversed this phenotype. Acly inhibition thus can promote myelopoiesis through deprivation of acetyl-CoA and altered histone acetylome to regulate C/EBP transcription factor family activity for myeloid differentiation. 2022-12-01 /pmc/articles/PMC9935084/ /pubmed/36547387 http://dx.doi.org/10.4049/immunohorizons.2200086 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This article is distributed under the terms of the CC BY-NC-ND 4.0 Unported license (https://creativecommons.org/licenses/by-nc-nd/4.0/) .
spellingShingle Article
Greenwood, Dalton L.
Ramsey, Haley E.
Nguyen, Phuong T. T.
Patterson, Andrew R.
Voss, Kelsey
Bader, Jackie E.
Sugiura, Ayaka
Bacigalupa, Zachary A.
Schaefer, Samuel
Ye, Xiang
Dahunsi, Debolanle O.
Madden, Matthew Z.
Wellen, Kathryn E.
Savona, Michael R.
Ferrell, P. Brent
Rathmell, Jeffrey C.
Acly Deficiency Enhances Myelopoiesis through Acetyl Coenzyme A and Metabolic–Epigenetic Cross-Talk
title Acly Deficiency Enhances Myelopoiesis through Acetyl Coenzyme A and Metabolic–Epigenetic Cross-Talk
title_full Acly Deficiency Enhances Myelopoiesis through Acetyl Coenzyme A and Metabolic–Epigenetic Cross-Talk
title_fullStr Acly Deficiency Enhances Myelopoiesis through Acetyl Coenzyme A and Metabolic–Epigenetic Cross-Talk
title_full_unstemmed Acly Deficiency Enhances Myelopoiesis through Acetyl Coenzyme A and Metabolic–Epigenetic Cross-Talk
title_short Acly Deficiency Enhances Myelopoiesis through Acetyl Coenzyme A and Metabolic–Epigenetic Cross-Talk
title_sort acly deficiency enhances myelopoiesis through acetyl coenzyme a and metabolic–epigenetic cross-talk
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9935084/
https://www.ncbi.nlm.nih.gov/pubmed/36547387
http://dx.doi.org/10.4049/immunohorizons.2200086
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