Long-term production of BDNF and NT-3 induced by A91-immunization after spinal cord injury
- Susana Martiñónd, e, f(Autor),
- Elisa García-Vencesf(Autor),
- Diana Toscano-Tejeidaf(Autor),
- Adrian Flores-Romerof(Autor),
- Roxana Rodriguez-Barreraf(Autor),
- Manuel Ferrusquiaf(Autor)
- ,
- ,
- cUniversidad Nacional Autónoma de México,
- dInstituto Nacional de Psiquiatria Ramon de la Fuente,
- eInstituto Mexicano del Seguro Social,
- fUniversidad Anáhuac
Acceso abierto
Publication Information
Tipo de resultado
Idioma original
InglésNúmero de artículo
42Revista (Volumen, Número de Edición)
BMC Neuroscience (Volumen 17, Número 1)Hitos de publicación
- Publicada - 30/06/2016
Estado de publicación
ID de publicación externa
- Scopus: 84976430961
- PubMed: 27364353
Abstract
Background: After spinal cord (SC)-injury, a non-modulated immune response contributes to the damage of neural tissue. Protective autoimmunity (PA) is a T cell mediated, neuroprotective response induced after SC-injury. Immunization with neural-derived peptides (INDP), such as A91, has shown to promote-in vitro-the production of neurotrophic factors. However, the production of these molecules has not been studied at the site of injury. Results: In order to evaluate these issues, we performed four experiments in adult female Sprague-Dawley rats. In the first one, brain derived neurotrophic factor (BDNF) and neurotrophin-3 (NT-3) concentrations were evaluated at the site of lesion 21 days after SC-injury. BDNF and NT-3 were significantly increased in INDP-treated animals. In the second experiment, proliferation of anti-A91 T cells was assessed at chronic stages of injury. In this case, we found a significant proliferation of these cells in animals subjected to SC-injury + INDP. In the third experiment, we explored the amount of BDNF and NT3 at the site of injury in the chronic phase of rats subjected to either SC-contusion (SCC; moderate or severe) or SC-transection (SCT; complete or incomplete). The animals were treated with INDP immediately after injury. Rats subjected to moderate contusion or incomplete SCT showed significantly higher levels of BDNF and NT-3 as compared to PBS-immunized ones. In rats with severe SCC and complete SCT, BDNF and NT-3 concentrations were barely detected. Finally, in the fourth experiment we assessed motor function recovery in INDP-treated rats with moderate SC-injury. Rats immunized with A91 showed a significantly higher motor recovery from the first week and up to 4 months after SC-injury. Conclusions: The results of this study suggest that PA boosted by immunization with A91 after moderate SC-injury can exert its benefits even at chronic stages, as shown by long-term production of BDNF and NT-3 and a substantial improvement in motor recovery.