The glial cell response is an essential component of hypoxia-induced erythropoiesis in mice

Alexander Weidemann; Yann M. Kerdiles; Karl X. Knaup; Christopher A. Rafie; Adam T. Boutin; Christian Stockmann; Norihiko Takeda; Miriam Scadeng; Andy Y. Shih; Volker H. Haase; M. Celeste Simon; David Kleinfeld; Randall S. Johnson

doi:10.1172/JCI39378

The glial cell response is an essential component of hypoxia-induced erythropoiesis in mice

Alexander Weidemann, Yann M. Kerdiles, Karl X. Knaup, Christopher A. Rafie, Adam T. Boutin, Christian Stockmann, Norihiko Takeda, Miriam Scadeng, Andy Y. Shih, Volker H. Haase, M. Celeste Simon, David Kleinfeld, Randall S. Johnson

Genomic Medicine

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83 Scopus citations

Abstract

A key adaptation to environmental hypoxia is an increase in erythropoiesis, driven by the hormone erythropoietin (EPO) through what is traditionally thought to be primarily a renal response. However, both neurons and astrocytes (the largest subpopulation of glial cells in the CNS) also express EPO following ischemic injury, and this response is known to ameliorate damage to the brain. To investigate the role of glial cells as a component of the systemic response to hypoxia, we created astrocyte-specific deletions of the murine genes encoding the hypoxia-inducible transcription factors HIF-1α and HIF-2α and their negative regulator von Hippel-Lindau (VHL) as well as astrocyte-specific deletion of the HIF target gene Vegf. We found that loss of the hypoxic response in astrocytes does not cause anemia in mice but is necessary for approximately 50% of the acute erythropoietic response to hypoxic stress. In accord with this, erythroid progenitor cells and reticulocytes were substantially reduced in number in mice lacking HIF function in astrocytes following hypoxic stress. Thus, we have demonstrated that the glial component of the CNS is an essential component of hypoxia-induced erythropoiesis.

Original language	English (US)
Pages (from-to)	3373-3383
Number of pages	11
Journal	Journal of Clinical Investigation
Volume	119
Issue number	11
DOIs	https://doi.org/10.1172/JCI39378
State	Published - Nov 2 2009

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General Medicine

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Weidemann, A., Kerdiles, Y. M., Knaup, K. X., Rafie, C. A., Boutin, A. T., Stockmann, C., Takeda, N., Scadeng, M., Shih, A. Y., Haase, V. H., Simon, M. C., Kleinfeld, D., & Johnson, R. S. (2009). The glial cell response is an essential component of hypoxia-induced erythropoiesis in mice. Journal of Clinical Investigation, 119(11), 3373-3383. https://doi.org/10.1172/JCI39378

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abstract = "A key adaptation to environmental hypoxia is an increase in erythropoiesis, driven by the hormone erythropoietin (EPO) through what is traditionally thought to be primarily a renal response. However, both neurons and astrocytes (the largest subpopulation of glial cells in the CNS) also express EPO following ischemic injury, and this response is known to ameliorate damage to the brain. To investigate the role of glial cells as a component of the systemic response to hypoxia, we created astrocyte-specific deletions of the murine genes encoding the hypoxia-inducible transcription factors HIF-1α and HIF-2α and their negative regulator von Hippel-Lindau (VHL) as well as astrocyte-specific deletion of the HIF target gene Vegf. We found that loss of the hypoxic response in astrocytes does not cause anemia in mice but is necessary for approximately 50% of the acute erythropoietic response to hypoxic stress. In accord with this, erythroid progenitor cells and reticulocytes were substantially reduced in number in mice lacking HIF function in astrocytes following hypoxic stress. Thus, we have demonstrated that the glial component of the CNS is an essential component of hypoxia-induced erythropoiesis.",

author = "Alexander Weidemann and Kerdiles, {Yann M.} and Knaup, {Karl X.} and Rafie, {Christopher A.} and Boutin, {Adam T.} and Christian Stockmann and Norihiko Takeda and Miriam Scadeng and Shih, {Andy Y.} and Haase, {Volker H.} and Simon, {M. Celeste} and David Kleinfeld and Johnson, {Randall S.}",

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AU - Boutin, Adam T.

AU - Stockmann, Christian

AU - Takeda, Norihiko

AU - Scadeng, Miriam

AU - Shih, Andy Y.

AU - Haase, Volker H.

AU - Simon, M. Celeste

AU - Kleinfeld, David

AU - Johnson, Randall S.

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N2 - A key adaptation to environmental hypoxia is an increase in erythropoiesis, driven by the hormone erythropoietin (EPO) through what is traditionally thought to be primarily a renal response. However, both neurons and astrocytes (the largest subpopulation of glial cells in the CNS) also express EPO following ischemic injury, and this response is known to ameliorate damage to the brain. To investigate the role of glial cells as a component of the systemic response to hypoxia, we created astrocyte-specific deletions of the murine genes encoding the hypoxia-inducible transcription factors HIF-1α and HIF-2α and their negative regulator von Hippel-Lindau (VHL) as well as astrocyte-specific deletion of the HIF target gene Vegf. We found that loss of the hypoxic response in astrocytes does not cause anemia in mice but is necessary for approximately 50% of the acute erythropoietic response to hypoxic stress. In accord with this, erythroid progenitor cells and reticulocytes were substantially reduced in number in mice lacking HIF function in astrocytes following hypoxic stress. Thus, we have demonstrated that the glial component of the CNS is an essential component of hypoxia-induced erythropoiesis.

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The glial cell response is an essential component of hypoxia-induced erythropoiesis in mice

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