Adiponectin receptors sustain haematopoietic stem cells throughout adulthood by protecting them from inflammation

Corbin E. Meacham; Elise C. Jeffery; Rebecca J. Burgess; Charukesi D. Sivakumar; Madison A. Arora; Anne Marie Stanley; Emily M. Colby; Genevieve M. Crane; Zhiyu Zhao; Sean J. Morrison

doi:10.1038/s41556-022-00909-9

Adiponectin receptors sustain haematopoietic stem cells throughout adulthood by protecting them from inflammation

Corbin E. Meacham, Elise C. Jeffery, Rebecca J. Burgess, Charukesi D. Sivakumar, Madison A. Arora, Anne Marie Stanley, Emily M. Colby, Genevieve M. Crane, Zhiyu Zhao, Sean J. Morrison

Research output: Contribution to journal › Article › peer-review

1 Scopus citations

Abstract

How are haematopoietic stem cells (HSCs) protected from inflammation, which increases with age and can deplete HSCs? Adiponectin, an anti-inflammatory factor that is not required for HSC function or haematopoiesis, promotes stem/progenitor cell proliferation after bacterial infection and myeloablation. Adiponectin binds two receptors, AdipoR1 and AdipoR2, which have ceramidase activity that increases upon adiponectin binding. Here we found that adiponectin receptors are non-cell-autonomously required in haematopoietic cells to promote HSC quiescence and self-renewal. Adiponectin receptor signalling suppresses inflammatory cytokine expression by myeloid cells and T cells, including interferon-γ and tumour necrosis factor. Without adiponectin receptors, the levels of these factors increase, chronically activating HSCs, reducing their self-renewal potential and depleting them during ageing. Pathogen infection accelerates this loss of HSC self-renewal potential. Blocking interferon-γ or tumour necrosis factor signalling partially rescues these effects. Adiponectin receptors are thus required in immune cells to sustain HSC quiescence and to prevent premature HSC depletion by reducing inflammation.

Original language	English (US)
Pages (from-to)	697-707
Number of pages	11
Journal	Nature cell biology
Volume	24
Issue number	5
DOIs	https://doi.org/10.1038/s41556-022-00909-9
State	Published - May 2022

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Cell Biology

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10.1038/s41556-022-00909-9

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@article{7da87cba2139428999c85e3f1dcc077f,

title = "Adiponectin receptors sustain haematopoietic stem cells throughout adulthood by protecting them from inflammation",

abstract = "How are haematopoietic stem cells (HSCs) protected from inflammation, which increases with age and can deplete HSCs? Adiponectin, an anti-inflammatory factor that is not required for HSC function or haematopoiesis, promotes stem/progenitor cell proliferation after bacterial infection and myeloablation. Adiponectin binds two receptors, AdipoR1 and AdipoR2, which have ceramidase activity that increases upon adiponectin binding. Here we found that adiponectin receptors are non-cell-autonomously required in haematopoietic cells to promote HSC quiescence and self-renewal. Adiponectin receptor signalling suppresses inflammatory cytokine expression by myeloid cells and T cells, including interferon-γ and tumour necrosis factor. Without adiponectin receptors, the levels of these factors increase, chronically activating HSCs, reducing their self-renewal potential and depleting them during ageing. Pathogen infection accelerates this loss of HSC self-renewal potential. Blocking interferon-γ or tumour necrosis factor signalling partially rescues these effects. Adiponectin receptors are thus required in immune cells to sustain HSC quiescence and to prevent premature HSC depletion by reducing inflammation.",

author = "Meacham, {Corbin E.} and Jeffery, {Elise C.} and Burgess, {Rebecca J.} and Sivakumar, {Charukesi D.} and Arora, {Madison A.} and Stanley, {Anne Marie} and Colby, {Emily M.} and Crane, {Genevieve M.} and Zhiyu Zhao and Morrison, {Sean J.}",

note = "Funding Information: S.J.M. is a Howard Hughes Medical Institute (HHMI) Investigator, the Mary McDermott Cook Chair in Pediatric Genetics, the Kathryn and Gene Bishop Distinguished Chair in Pediatric Research, the director of the Hamon Laboratory for Stem Cells and Cancer and a Cancer Prevention and Research Institute of Texas Scholar. This work was supported by the National Institutes of Health (DK118745), the Moody Medical Research Institute, the Josephine Hughes Sterling Foundation and the Robert J. Kleberg, Jr. and Helen C. Kleberg Foundation (all to S.J.M.). C.E.M. was supported by a Postdoctoral Fellowship from the American Cancer Society (PF-13-245-01-LIB). E.C.J. was supported by a Postdoctoral Fellowship from the Damon Runyon Cancer Research Foundation (2278-16). R.J.B. was supported by Ruth L. Kirschstein National Research Service Award Postdoctoral Fellowship from the National Heart, Lung, and Blood Institute (F32HL122095-01). Funding for the UT Dallas/UT Southwestern Green Fellows Program (C.D.S.) was supported, in part, by the Cecil and Ida Green Foundation. We thank G. Karsenty for providing the Adipor1fl/fland Adipor2fl/flmice, N. Loof, C. Cantu, T. Shih, G. Wilson and the Moody Foundation Flow Cytometry Facility, M. Mulkey for mouse colony management, and the BioHPC high-performance computing cloud at the University of Texas Southwestern Medical Center for providing computational resources. Funding Information: S.J.M. is a Howard Hughes Medical Institute (HHMI) Investigator, the Mary McDermott Cook Chair in Pediatric Genetics, the Kathryn and Gene Bishop Distinguished Chair in Pediatric Research, the director of the Hamon Laboratory for Stem Cells and Cancer and a Cancer Prevention and Research Institute of Texas Scholar. This work was supported by the National Institutes of Health (DK118745), the Moody Medical Research Institute, the Josephine Hughes Sterling Foundation and the Robert J. Kleberg, Jr. and Helen C. Kleberg Foundation (all to S.J.M.). C.E.M. was supported by a Postdoctoral Fellowship from the American Cancer Society (PF-13-245-01-LIB). E.C.J. was supported by a Postdoctoral Fellowship from the Damon Runyon Cancer Research Foundation (2278-16). R.J.B. was supported by Ruth L. Kirschstein National Research Service Award Postdoctoral Fellowship from the National Heart, Lung, and Blood Institute (F32HL122095-01). Funding for the UT Dallas/UT Southwestern Green Fellows Program (C.D.S.) was supported, in part, by the Cecil and Ida Green Foundation. We thank G. Karsenty for providing the Adipor1and Adipor2 mice, N. Loof, C. Cantu, T. Shih, G. Wilson and the Moody Foundation Flow Cytometry Facility, M. Mulkey for mouse colony management, and the BioHPC high-performance computing cloud at the University of Texas Southwestern Medical Center for providing computational resources. fl/fl fl/fl Publisher Copyright: {\textcopyright} 2022, The Author(s), under exclusive licence to Springer Nature Limited.",

year = "2022",

month = may,

doi = "10.1038/s41556-022-00909-9",

language = "English (US)",

volume = "24",

pages = "697--707",

journal = "Nature Cell Biology",

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T1 - Adiponectin receptors sustain haematopoietic stem cells throughout adulthood by protecting them from inflammation

AU - Meacham, Corbin E.

AU - Jeffery, Elise C.

AU - Burgess, Rebecca J.

AU - Sivakumar, Charukesi D.

AU - Arora, Madison A.

AU - Stanley, Anne Marie

AU - Colby, Emily M.

AU - Crane, Genevieve M.

AU - Zhao, Zhiyu

AU - Morrison, Sean J.

N1 - Funding Information: S.J.M. is a Howard Hughes Medical Institute (HHMI) Investigator, the Mary McDermott Cook Chair in Pediatric Genetics, the Kathryn and Gene Bishop Distinguished Chair in Pediatric Research, the director of the Hamon Laboratory for Stem Cells and Cancer and a Cancer Prevention and Research Institute of Texas Scholar. This work was supported by the National Institutes of Health (DK118745), the Moody Medical Research Institute, the Josephine Hughes Sterling Foundation and the Robert J. Kleberg, Jr. and Helen C. Kleberg Foundation (all to S.J.M.). C.E.M. was supported by a Postdoctoral Fellowship from the American Cancer Society (PF-13-245-01-LIB). E.C.J. was supported by a Postdoctoral Fellowship from the Damon Runyon Cancer Research Foundation (2278-16). R.J.B. was supported by Ruth L. Kirschstein National Research Service Award Postdoctoral Fellowship from the National Heart, Lung, and Blood Institute (F32HL122095-01). Funding for the UT Dallas/UT Southwestern Green Fellows Program (C.D.S.) was supported, in part, by the Cecil and Ida Green Foundation. We thank G. Karsenty for providing the Adipor1fl/fland Adipor2fl/flmice, N. Loof, C. Cantu, T. Shih, G. Wilson and the Moody Foundation Flow Cytometry Facility, M. Mulkey for mouse colony management, and the BioHPC high-performance computing cloud at the University of Texas Southwestern Medical Center for providing computational resources. Funding Information: S.J.M. is a Howard Hughes Medical Institute (HHMI) Investigator, the Mary McDermott Cook Chair in Pediatric Genetics, the Kathryn and Gene Bishop Distinguished Chair in Pediatric Research, the director of the Hamon Laboratory for Stem Cells and Cancer and a Cancer Prevention and Research Institute of Texas Scholar. This work was supported by the National Institutes of Health (DK118745), the Moody Medical Research Institute, the Josephine Hughes Sterling Foundation and the Robert J. Kleberg, Jr. and Helen C. Kleberg Foundation (all to S.J.M.). C.E.M. was supported by a Postdoctoral Fellowship from the American Cancer Society (PF-13-245-01-LIB). E.C.J. was supported by a Postdoctoral Fellowship from the Damon Runyon Cancer Research Foundation (2278-16). R.J.B. was supported by Ruth L. Kirschstein National Research Service Award Postdoctoral Fellowship from the National Heart, Lung, and Blood Institute (F32HL122095-01). Funding for the UT Dallas/UT Southwestern Green Fellows Program (C.D.S.) was supported, in part, by the Cecil and Ida Green Foundation. We thank G. Karsenty for providing the Adipor1and Adipor2 mice, N. Loof, C. Cantu, T. Shih, G. Wilson and the Moody Foundation Flow Cytometry Facility, M. Mulkey for mouse colony management, and the BioHPC high-performance computing cloud at the University of Texas Southwestern Medical Center for providing computational resources. fl/fl fl/fl Publisher Copyright: © 2022, The Author(s), under exclusive licence to Springer Nature Limited.

PY - 2022/5

Y1 - 2022/5

N2 - How are haematopoietic stem cells (HSCs) protected from inflammation, which increases with age and can deplete HSCs? Adiponectin, an anti-inflammatory factor that is not required for HSC function or haematopoiesis, promotes stem/progenitor cell proliferation after bacterial infection and myeloablation. Adiponectin binds two receptors, AdipoR1 and AdipoR2, which have ceramidase activity that increases upon adiponectin binding. Here we found that adiponectin receptors are non-cell-autonomously required in haematopoietic cells to promote HSC quiescence and self-renewal. Adiponectin receptor signalling suppresses inflammatory cytokine expression by myeloid cells and T cells, including interferon-γ and tumour necrosis factor. Without adiponectin receptors, the levels of these factors increase, chronically activating HSCs, reducing their self-renewal potential and depleting them during ageing. Pathogen infection accelerates this loss of HSC self-renewal potential. Blocking interferon-γ or tumour necrosis factor signalling partially rescues these effects. Adiponectin receptors are thus required in immune cells to sustain HSC quiescence and to prevent premature HSC depletion by reducing inflammation.

AB - How are haematopoietic stem cells (HSCs) protected from inflammation, which increases with age and can deplete HSCs? Adiponectin, an anti-inflammatory factor that is not required for HSC function or haematopoiesis, promotes stem/progenitor cell proliferation after bacterial infection and myeloablation. Adiponectin binds two receptors, AdipoR1 and AdipoR2, which have ceramidase activity that increases upon adiponectin binding. Here we found that adiponectin receptors are non-cell-autonomously required in haematopoietic cells to promote HSC quiescence and self-renewal. Adiponectin receptor signalling suppresses inflammatory cytokine expression by myeloid cells and T cells, including interferon-γ and tumour necrosis factor. Without adiponectin receptors, the levels of these factors increase, chronically activating HSCs, reducing their self-renewal potential and depleting them during ageing. Pathogen infection accelerates this loss of HSC self-renewal potential. Blocking interferon-γ or tumour necrosis factor signalling partially rescues these effects. Adiponectin receptors are thus required in immune cells to sustain HSC quiescence and to prevent premature HSC depletion by reducing inflammation.

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Adiponectin receptors sustain haematopoietic stem cells throughout adulthood by protecting them from inflammation

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