Functional conservation of erythropoietin signaling in zebrafish

Paffett-Lugassy, Noëlle; Hsia, Nelson; Fraenkel, Paula G.; Paw, Barry H.; Leshinsky, Irene; Barut, Bruce A.; Bahary, Nathan; Caro, Jaime; Handin, Robert I.; Zon, Leonard I.

doi:10.1182/blood-2006-04-016535

Cited by 125 publications

(118 citation statements)

References 64 publications

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“…We further have discovered that a major source of Epo for primitive erythropoiesis might be a subpopulation of neural and neural crest cells, which we refer to as NEP cells. Consistent with our observation, the principal Epo-producing tissue in zebrafish larvae is neural tissue, and Epo production moves to the heart and liver during adulthood 40,41 . We also observed that a subpopulation of NEP cells migrate along the blood vessels in the intersomitic space.…”

Section: Discussionsupporting

confidence: 77%

“…We have also observed that Epo-KO embryos exhibit no apparent abnormality until E11.5 in non-haematopoietic organs. In zebrafish, the overexpression and knockdown of Epo dramatically alter erythropoiesis in the embryonic intermediate cell mass and the adult kidney, but these alterations in Epo levels do not affect the development of non-haematopoietic systems 41 . Moreover, NEP cells express low EpoR mRNA levels compared with haematopoietic cells.…”

Section: Discussionmentioning

confidence: 99%

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Erythropoietin production in neuroepithelial and neural crest cells during primitive erythropoiesis

et al. 2013

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Erythropoietin (Epo) supports both primitive erythropoiesis in the yolk sac and definitive erythropoiesis in the fetal liver and bone marrow. Although definitive erythropoiesis requires kidney-and liver-secreted Epo, it is unclear which cells produce Epo for primitive erythropoiesis. Here we find neural Epo-producing (NEP) cells in mid-gestational stage embryos using mouse lines that express green fluorescent protein (GFP) under the Epo gene regulation. In these mice, GFP is expressed exclusively in a subpopulation of neural and neural crest cells at embryonic day 9.0 when Epo-deficient embryos exhibit abnormalities in primitive erythropoiesis. The GFP-positive NEP cells express Epo mRNA and the ex vivo culture of embryonic day 8.5 neural tubes results in the secretion of Epo, which is able to induce the proliferation and differentiation of yolk sac-derived erythroid cells. These results thus suggest that NEP cells secrete Epo and might support the development of primitive erythropoiesis.

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Section: Discussionsupporting

confidence: 77%

Section: Discussionmentioning

confidence: 99%

Erythropoietin production in neuroepithelial and neural crest cells during primitive erythropoiesis

et al. 2013

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“…This evidence suggests that NEP-derived cells in organs other than the kidney and liver may retain their ability to produce Epo under pathological conditions. Interestingly, in Zebrafish, one of the major Epo-producing sites is the brain (Paffett-Lugassy et al 2007). Therefore, transient Epo production by NEP cells in mouse embryos may support the so-called "recapitulation theory", which argues that ontogeny recapitulates phylogeny (Sander 2002).…”

Section: Neural Epo-producing (Nep) Cellsmentioning

confidence: 99%

“…At the transcriptional level, Epo gene expression is tightly regulated by hypoxia-inducible factors (HIFs), which are the master transcription factors for oxygen-dependent gene regulation (Suzuki et al 2007;Miyata et al 2013;Franke et al 2013). Because non-mammalian Epo genes also respond to hypoxic stimuli (Paffett-Lugassy et al 2007), Epo is considered to be evolutionarily indispensable for maintaining oxygen homeostasis in animals with hemoglobins encapsulated by erythrocytes.…”

Section: Introductionmentioning

confidence: 99%

“…Epo binding to the receptors causes conformation changes in the intracellular domains of an EpoR homodimer, bringing it into close proximity to initiate Epo-EpoR signal transduction (Suzuki et al 2015). Because EpoR is highly expressed only in committed erythroid progenitors and erythroblastic cells, the principal function of Epo is fundamentally restricted to erythropoiesis; it is not involved in the growth of other cell lineages (Suzuki et al 2002;Paffett-Lugassy et al 2007). Additionally, Epo signaling is important for the growth and terminal maturation of erythroid cells and not for the commitment of hematopoietic stem cells to the erythroid lineage (Wu et al 1995).…”

Section: Introductionmentioning

confidence: 99%

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Erythropoietin Gene Expression: Developmental-Stage Specificity, Cell-Type Specificity, and Hypoxia Inducibility

Suzuki

2015

Tohoku J. Exp. Med.

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Erythrocytes play an essential role in the delivery of oxygen from the lung to every organ; a decrease in erythrocytes (anemia) causes hypoxic stress and tissue damage. To maintain oxygen homeostasis in adult mammals, when the kidney senses hypoxia, it secretes an erythroid growth factor, erythropoietin (Epo), which stimulates erythropoiesis in the bone marrow. Recently, studies using genetically modified mice have shown that the in vivo expression profile of the Epo gene changes dramatically during development. The first Epo-producing cells emerge in the neural crest and neuroepithelium of mid-stage embryos and support primitive erythropoiesis in the yolk sac. Subsequently, Epo from the hepatocytes stimulates erythropoiesis in the fetal liver of later stage embryos in a paracrine manner. In fact, erythroid lineage cells comprise the largest cell population in the fetal liver, and hepatocytes are distributed among the erythroid cell clusters. Adult erythropoiesis in the bone marrow requires Epo that is secreted by renal Epo-producing cells (REP cells). REP cells are widely distributed in the renal cortex and outer medulla. Hypoxia-inducible Epo production both in hepatocytes and REP cells is controlled at the gene transcription level that is mainly mediated by the hypoxia-inducible transcription factor (HIF) pathway. These mouse studies further provide insights into the molecular mechanisms of the cell-type specific, hypoxia-inducible expression of the Epo gene, which involves multiple sets of cis-and trans-regulatory elements.

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Zebrafish blood stem cells

Chen

Zon

2009

J of Cellular Biochemistry

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141

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Within the past two decades, the zebrafish (Danio rerio) has become an excellent model to study the development of hematopoietic stem cells (HSCs). All vertebrates including zebrafish have primitive and definitive waves of hematopoiesis, but self-renewing pluripotent HSCs are only produced by the definitive wave. The primitive wave occurs in two intraembryonic locations called the intermediate cell mass (ICM) and the anterior lateral mesoderm (ALM). Primitive erythropoiesis is in the ICM, whereas myelopoiesis initiates in the ALM. After circulation starts at 24 h post-fertilization, hematopoiesis shifts to the posterior blood island (PBI) for a brief period. The definitive wave starts in the aorta-gonad-mesonephros (AGM). There are three different HSC migration and colonization events that begin 2 days post-fertilization: AGM progenitor cells migrate to (1) the caudal hematopoietic tissue (CHT), which is an intermediate site of blood development; (2) the thymus, which is a site of lymphocyte maturation; and (3) the developing kidney marrow, which is the larval and adult location for production of all hematopoietic cell types, and is comparable to the bone marrow of mammals. Many of the transcription factors and signaling pathways that regulate the formation of HSCs in a zebrafish are conserved with mammals. Large-scale forward and reverse genetic screens have identified zebrafish blood and HSC mutants that represent models for known human diseases. Along with the technological advancements in the field of zebrafish research, future HSC studies in zebrafish will help us illuminate the genetic network controlling the development and function of stem cells in all vertebrates.

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Functional conservation of erythropoietin signaling in zebrafish

Cited by 125 publications

References 64 publications

Erythropoietin production in neuroepithelial and neural crest cells during primitive erythropoiesis

Erythropoietin production in neuroepithelial and neural crest cells during primitive erythropoiesis

Erythropoietin Gene Expression: Developmental-Stage Specificity, Cell-Type Specificity, and Hypoxia Inducibility

Zebrafish blood stem cells

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