Literature DB >> 27920250

Renal Anemia Model Mouse Established by Transgenic Rescue with an Erythropoietin Gene Lacking Kidney-Specific Regulatory Elements.

Ikuo Hirano1, Norio Suzuki2, Shun Yamazaki3, Hiroki Sekine4, Naoko Minegishi5, Ritsuko Shimizu6,5, Masayuki Yamamoto7,5.   

Abstract

The erythropoietin (Epo) gene is under tissue-specific inducible regulation. Because the kidney is the primary EPO-producing tissue in adults, impaired EPO production in chronic kidney disorders results in serious renal anemia. The Epo gene contains a liver-specific enhancer in the 3' region, but the kidney-specific enhancer for gene expression in renal EPO-producing (REP) cells remains elusive. Here, we examined a conserved upstream element for renal Epo regulation (CURE) region that spans 17.4 kb to 3.6 kb upstream of the Epo gene and harbors several phylogenetically conserved elements. We prepared various Epo gene-reporter constructs utilizing a bacterial artificial chromosome and generated a number of transgenic-mouse lines. We observed that deletion of the CURE region (δCURE) abrogated Epo gene expression in REP cells. Although transgenic expression of the δCURE construct rescued Epo-deficient mice from embryonic lethality, the rescued mice had severe EPO-dependent anemia. These mouse lines serve as an elaborate model for the search for erythroid stimulatory activity and are referred to as AnRED (anemic model with renal EPO deficiency) mice. We also dissected the CURE region by exploiting a minigene harboring four phylogenetically conserved elements in reporter transgenic-mouse analyses. Our analyses revealed that Epo gene regulation in REP cells is a complex process that utilizes multiple regulatory influences.
Copyright © 2017 American Society for Microbiology.

Entities:  

Keywords:  HIF; HRE; erythropoietin; hypoxia; kidney; renal anemia

Mesh:

Substances:

Year:  2017        PMID: 27920250      PMCID: PMC5288576          DOI: 10.1128/MCB.00451-16

Source DB:  PubMed          Journal:  Mol Cell Biol        ISSN: 0270-7306            Impact factor:   4.272


  44 in total

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Journal:  Haematologica       Date:  2014-02-07       Impact factor: 9.941

3.  Plasticity of renal erythropoietin-producing cells governs fibrosis.

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Journal:  J Am Soc Nephrol       Date:  2013-07-05       Impact factor: 10.121

4.  Purification of human erythropoietin.

Authors:  T Miyake; C K Kung; E Goldwasser
Journal:  J Biol Chem       Date:  1977-08-10       Impact factor: 5.157

5.  Repression via the GATA box is essential for tissue-specific erythropoietin gene expression.

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6.  Erythropoietin mRNA expression in human fetal and neonatal tissue.

Authors:  C Dame; H Fahnenstich; P Freitag; D Hofmann; T Abdul-Nour; P Bartmann; J Fandrey
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Review 8.  Nonrenal regulation of EPO synthesis.

Authors:  Alexander Weidemann; Randall S Johnson
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9.  Regulated basal, inducible, and tissue-specific human erythropoietin gene expression in transgenic mice requires multiple cis DNA sequences.

Authors:  A Madan; C Lin; S L Hatch; P T Curtin
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10.  Isolation and characterization of renal erythropoietin-producing cells from genetically produced anemia mice.

Authors:  Xiaoqing Pan; Norio Suzuki; Ikuo Hirano; Shun Yamazaki; Naoko Minegishi; Masayuki Yamamoto
Journal:  PLoS One       Date:  2011-10-11       Impact factor: 3.240

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2.  Retinoic acid regulates erythropoietin production cooperatively with hypoxia-inducible factors in human iPSC-derived erythropoietin-producing cells.

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3.  Fate-mapping of erythropoietin-producing cells in mouse models of hypoxaemia and renal tissue remodelling reveals repeated recruitment and persistent functionality.

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5.  Erythropoietin in bone homeostasis-Implications for efficacious anemia therapy.

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6.  Blockade of the interaction between BMP9 and endoglin on erythroid progenitors promotes erythropoiesis in mice.

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Journal:  Genes Cells       Date:  2021-08-12       Impact factor: 2.300

7.  An immortalized cell line derived from renal erythropoietin-producing (REP) cells demonstrates their potential to transform into myofibroblasts.

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Review 8.  Alteration of the DNA Methylation Signature of Renal Erythropoietin-Producing Cells Governs the Sensitivity to Drugs Targeting the Hypoxia-Response Pathway in Kidney Disease Progression.

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Review 9.  Hypoxia Pathway Proteins are Master Regulators of Erythropoiesis.

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10.  Efficient isolation of interstitial fibroblasts directly from mouse kidneys or indirectly after ex vivo expansion.

Authors:  Taku Nakai; Yuma Iwamura; Norio Suzuki
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