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After myocardial infarction (MI), emergency hematopoiesis produces inflammatory myeloid cells that accelerate atherosclerosis and promote heart failure. Because the balance between glycolysis and mitochondrial metabolism regulates hematopoietic stem cell homeostasis, metabolic cues may influence emergency myelopoiesis. Here we show, in humans and female mice, that hematopoietic progenitor cells increase fatty acid metabolism after MI. Blockade of fatty acid oxidation by deleting carnitine palmitoyltransferase (Cpt1a) in hematopoietic cells of Vav1Cre/+Cpt1afl/fl mice limited hematopoietic progenitor proliferation and myeloid cell expansion after MI. We also observed reduced bone marrow adiposity in humans, pigs and mice after MI. Inhibiting lipolysis in adipocytes using AdipoqCreERT2Atglfl/fl mice or local depletion of bone marrow adipocytes in AdipoqCreERT2iDTR mice also curbed emergency hematopoiesis. Furthermore, systemic and regional sympathectomy prevented bone marrow adipocyte shrinkage after MI. These data establish a critical role for fatty acid metabolism in post-MI emergency hematopoiesis.Zhang et al. show that bone marrow fatty acid metabolism fuels expanded leukocyte production after myocardial infarction and, based on mouse, pig and human data, suggest that lipolysis in marrow adipocytes provides fatty acids to hematopoietic stem cells.

Bone marrow adipocytes fuel emergency hematopoiesis after myocardial infarction / Zhang, Shuang; Paccalet, Alexandre; Rohde, David; Cremer, Sebastian; Hulsmans, Maarten; Lee, I-Hsiu; Mentkowski, Kyle; Grune, Jana; Schloss, Maximilian J.; Honold, Lisa; Iwamoto, Yoshiko; Zheng, Yi; Bredella, Miriam A.; Buckless, Colleen; Ghoshhajra, Brian; Thondapu, Vikas; van der Laan, Anja M.; Piek, Jan J.; Niessen, Hans W. M.; Pallante, Fabio; Carnevale, Raimondo; Perrotta, Sara; Carnevale, Daniela; Iborra-Egea, Oriol; Muñoz-Guijosa, Christian; Galvez-Monton, Carolina; Bayes-Genis, Antoni; Vidoudez, Charles; Trauger, Sunia A.; Scadden, David T.; Swirski, Filip K.; Moskowitz, Michael A.; Naxerova, Kamila; Nahrendorf, Matthias. - In: NATURE CARDIOVASCULAR RESEARCH. - ISSN 2731-0590. - 2:12(2023), pp. 1277-1290. [10.1038/s44161-023-00388-7]

Bone marrow adipocytes fuel emergency hematopoiesis after myocardial infarction

Perrotta, Sara;Carnevale, Daniela
Investigation
;
2023

Abstract

After myocardial infarction (MI), emergency hematopoiesis produces inflammatory myeloid cells that accelerate atherosclerosis and promote heart failure. Because the balance between glycolysis and mitochondrial metabolism regulates hematopoietic stem cell homeostasis, metabolic cues may influence emergency myelopoiesis. Here we show, in humans and female mice, that hematopoietic progenitor cells increase fatty acid metabolism after MI. Blockade of fatty acid oxidation by deleting carnitine palmitoyltransferase (Cpt1a) in hematopoietic cells of Vav1Cre/+Cpt1afl/fl mice limited hematopoietic progenitor proliferation and myeloid cell expansion after MI. We also observed reduced bone marrow adiposity in humans, pigs and mice after MI. Inhibiting lipolysis in adipocytes using AdipoqCreERT2Atglfl/fl mice or local depletion of bone marrow adipocytes in AdipoqCreERT2iDTR mice also curbed emergency hematopoiesis. Furthermore, systemic and regional sympathectomy prevented bone marrow adipocyte shrinkage after MI. These data establish a critical role for fatty acid metabolism in post-MI emergency hematopoiesis.Zhang et al. show that bone marrow fatty acid metabolism fuels expanded leukocyte production after myocardial infarction and, based on mouse, pig and human data, suggest that lipolysis in marrow adipocytes provides fatty acids to hematopoietic stem cells.
2023
myocardial infarction; adipocytes; bone marrow; emergency hematopoiesis; fatty acid oxidation; lipolysis
01 Pubblicazione su rivista::01a Articolo in rivista
Bone marrow adipocytes fuel emergency hematopoiesis after myocardial infarction / Zhang, Shuang; Paccalet, Alexandre; Rohde, David; Cremer, Sebastian; Hulsmans, Maarten; Lee, I-Hsiu; Mentkowski, Kyle; Grune, Jana; Schloss, Maximilian J.; Honold, Lisa; Iwamoto, Yoshiko; Zheng, Yi; Bredella, Miriam A.; Buckless, Colleen; Ghoshhajra, Brian; Thondapu, Vikas; van der Laan, Anja M.; Piek, Jan J.; Niessen, Hans W. M.; Pallante, Fabio; Carnevale, Raimondo; Perrotta, Sara; Carnevale, Daniela; Iborra-Egea, Oriol; Muñoz-Guijosa, Christian; Galvez-Monton, Carolina; Bayes-Genis, Antoni; Vidoudez, Charles; Trauger, Sunia A.; Scadden, David T.; Swirski, Filip K.; Moskowitz, Michael A.; Naxerova, Kamila; Nahrendorf, Matthias. - In: NATURE CARDIOVASCULAR RESEARCH. - ISSN 2731-0590. - 2:12(2023), pp. 1277-1290. [10.1038/s44161-023-00388-7]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1702075
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