Literature DB >> 23602701

Signaling pathways of cell proliferation are involved in the differential effect of erythropoietin and its carbamylated derivative.

María Eugenia Chamorro1, Shirley Denise Wenker, Daiana Marina Vota, Daniela Cecilia Vittori, Alcira Beatriz Nesse.   

Abstract

It is now recognized that in addition to its activity upon erythroid progenitor cells, erythropoietin (Epo) is capable of stimulating survival of different non-erythroid cells. Since stimulation of erythropoiesis is unwanted for neuroprotection, Epo-like compounds with a more selective action are under investigation. Although the carbamylated derivative of erythropoietin (cEpo) has demonstrated non-hematopoietic tissue protection without erythropoietic effect, little is known about differential mechanisms between Epo and cEpo. Therefore, we investigated signaling pathways which play a key role in Epo-induced proliferation. Here we show that cEpo blocked FOXO3a phosphorylation, allowing expression of downstream target p27(kip1) in UT-7 and TF-1 cells capable of erythroid differentiation. This is consistent with the involvement of cEpo in slowing down G1-to-S-phase progression compared with the effect of Epo upon cell cycle. In contrast, similar antiapoptotic actions of cEpo and Epo were observed in neuronal SH-SY5Y cells. Inhibition and competition assays suggest that Epo may act through both, the homodimeric (EpoR/EpoR) and the heterodimeric (EpoR/βcR) receptors in neuronal SH-SY5Y cells and probably in the TF-1 cell type as well. Results also indicate that cEpo needs both the EpoR and βcR subunits to prevent apoptosis of neuronal cells. Based on evidence suggesting that cell proliferation pathways were involved in the differential effect of Epo and cEpo, we went forward to studying downstream signals. Here we provide the first evidence that unlike Epo, cEpo failed to induce FOXO3a inactivation and subsequent p27(kip1) downregulation, which is clearly shown in the incapacity of cEpo to induce erythroid cell growth.
Copyright © 2013 Elsevier B.V. All rights reserved.

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Year:  2013        PMID: 23602701     DOI: 10.1016/j.bbamcr.2013.04.006

Source DB:  PubMed          Journal:  Biochim Biophys Acta        ISSN: 0006-3002


  19 in total

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Authors:  Vijayeta Rangarajan; Sandra E Juul
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Authors:  Kenneth Maiese
Journal:  World J Diabetes       Date:  2015-10-25

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4.  Charting a course for erythropoietin in traumatic brain injury.

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5.  CEPO (carbamylated erythropoietin)-Fc protects hippocampal cells in culture against beta amyloid-induced apoptosis: considering Akt/GSK-3β and ERK signaling pathways.

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Review 6.  Novel Treatment Strategies for the Nervous System: Circadian Clock Genes, Non-coding RNAs, and Forkhead Transcription Factors.

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Review 7.  FoxO Transcription Factors and Regenerative Pathways in Diabetes Mellitus.

Authors:  Kenneth Maiese
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Journal:  Ann Med       Date:  2014-08-08       Impact factor: 4.709

10.  Carbamoylated erythropoietin induces a neurotrophic gene profile in neuronal cells.

Authors:  Neeraj K Tiwari; Monica Sathyanesan; William Schweinle; Samuel S Newton
Journal:  Prog Neuropsychopharmacol Biol Psychiatry       Date:  2018-07-11       Impact factor: 5.067

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