RESUMEN
Barium oxynitridosilicates, Ba3Si6O12N2 and Ba3Si6O9N4, were obtained from a mixture of BaCN2 and SiO2 at 800 °C, which is several hundred degrees lower than the temperature required in solid state reactions using BaCO3, SiO2 and Si3N4. The low-temperature formation mechanism was investigated by thermogravimetry analysis in conjunction with gas chromatography and mass spectroscopy. The phase ratio between the oxynitridosilicates was controlled by tuning the reaction temperature, duration, and atmosphere. Almost single-phase Ba3Si6O12N2 was obtained by reaction at 800 °C for 15 h under a N2 atmosphere, but the product changed to Ba3Si6O9N4 after 50 h at 800 °C or by heating at 950 °C for 15 h. The photoluminescence properties of Eu-doped products obtained at 800 °C using a mixture of BaCN2 : Eu and SiO2 were investigated.
RESUMEN
Brain injury causes serious motor, sensory, and cognitive disabilities. Accumulating evidence has demonstrated that histone deacetylase (HDAC) inhibitors exert neuroprotective effects against various insults to the central nervous system (CNS). In this study, we investigated the effects of the HDAC inhibition on the expression of brain-derived neurotrophic factor (BDNF) and functional recovery after traumatic brain injury (TBI) in mice. Administration of class I HDAC inhibitor increased the number of synaptic boutons in rewiring corticospinal fibers and improved the recovery of motor functions after TBI. Immunohistochemistry results showed that HDAC2 is mainly expressed in the neurons of the mouse spinal cord under normal conditions. After TBI, HDAC2 expression was increased in the spinal cord after 35 days, whereas BDNF expression was decreased after 42 days. Administration of CI-994 increased BDNF expression after TBI. Knockdown of HDAC2 elevated H4K5ac enrichment at the BDNF promoter, which was decreased following TBI. Together, our findings suggest that HDAC inhibition increases expression of neurotrophic factors, and promote neuronal rewiring and functional recovery following TBI.