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01.04.2016 | Original Article

Beneficial Effect of Erythropoietin Short Peptide on Acute Traumatic Brain Injury

verfasst von: Bo Wang, Mitchell Kang, Michelle Marchese, Esther Rodriguez, Wei Lu, Xintong Li, Yasuhiro Maeda, Peter Dowling

Erschienen in: Neurotherapeutics | Ausgabe 2/2016

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Abstract

There is currently no effective medical treatment for traumatic brain injury (TBI). Beyond the immediate physical damage caused by the initial impact, additional damage evolves due to the inflammatory response that follows brain injury. Here we show that therapy with JM4, a low molecular weight 19-amino acid nonhematopoietic erythropoietin (EPO) peptidyl fragment, containing amino acids 28–46 derived from the first loop of EPO, markedly reduces acute brain injury. Mice underwent controlled cortical injury and received either whole molecule EPO, JM4, or sham-treatment with phosphate-buffered saline. Animals treated with JM4 peptide exhibited a large decrease in number of dead neural cells and a marked reduction in lesion size at both 3 and 8 days postinjury. Therapy with JM4 also led to improved functional recovery and we observed a treatment window for JM4 peptide that remained open for at least 9 h postinjury. The full-length EPO molecule was divided into a series of 6 contiguous peptide segments; the JM4-containing segment and the adjoining downstream region contained the bulk of the death attenuating effects seen with intact EPO molecule following TBI. These findings indicate that the JM4 molecule substantially blocks cell death and brain injury following acute brain trauma and, as such, presents an excellent opportunity to explore the therapeutic potential of a small-peptide EPO derivative in the medical treatment of TBI.

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Titel: Beneficial Effect of Erythropoietin Short Peptide on Acute Traumatic Brain Injury
verfasst von: Bo Wang
Mitchell Kang
Michelle Marchese
Esther Rodriguez
Wei Lu
Xintong Li
Yasuhiro Maeda
Peter Dowling
Publikationsdatum: 01.04.2016
Verlag: Springer US
Erschienen in: Neurotherapeutics / Ausgabe 2/2016
Print ISSN: 1933-7213
Elektronische ISSN: 1878-7479
DOI: https://doi.org/10.1007/s13311-015-0418-y

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