RESUMO
The supported palladium catalysts perform well in the oxidative removal of hazardous aromatic hydrocarbons. However, water vapor can seriously deactivate the catalysts especially in the low-temperature regime. Hence, improving moisture resistance of the Pd-based catalysts is full of challenge in the removal of aromatics. Herein, we report a new type of Pd@NC/BN catalysts featured with nitrogen-doped carbon layers modified Pd supported on hexagonal boron nitride (h-BN), and the relationship between structure and water resistance of the catalysts. The results show that in the presence of 10 vol% H2O in the feedstock, the Pd@NC/BN catalyst could effectively oxidize o-xylene (with an almost 87% removal efficiency), whereas o-xylene conversion declined from 69% to 20% over the conventional Pd/Al2O3 at a reaction temperature of 210 °C and a space velocity of 40,000 mL/(g h). The adsorption of H2O was significantly inhibited on the nitrogen-doped carbon layers due to the hydrophobic nature. Meanwhile, the oxygen species active for o-xylene oxidation were not only from the adsorbed gas-phase oxygen but also from the new active oxygen (*OOH and *OH) species that were generated via the interaction of O2 and H2O in the presence of water in the feedstock. It is concluded that the reactive oxygen species that accelerated the activation and cleavage of C-H bonds significantly facilitated the conversion of key intermediate species (from benzaldehyde to benzoic acid), thus playing a decisive role in o-xylene oxidation. The present work provides a direction for developing the superior water resistance catalysts with hydrophobic nature and good water activation ability in the oxidative removal of volatile organic compounds.
RESUMO
Mitochondrial dysfunction and oxidative stress occur in neurodegenerative diseases. Other results show that bombesin-releasable calcium stores (BRCS) from the endoplasmic reticulum (ER) are exaggerated in fibroblasts from patients with Alzheimer's disease (AD) compared with controls and in fibroblasts from a young control treated with H(2)O(2). We hypothesize that alterations in oxidative stress underlie the exaggeration in BRCS in AD, and that appropriate antioxidants may be useful in treating this abnormality. Two indicators of different oxidant species were used to determine the effects of select oxidants on cellular oxidation status: carboxydichlorofluorescein (c-DCF) to detect reactive oxygen species (ROS), and 4-amino-5-methylamino-2',7'-difluorofluorescein (DAF) to detect nitric oxide (NO(.-)). Various conditions that induce ROS, including H(2)O(2), oxygen/glucose deprivation, and 3-morpholinosyndnonimine (SIN-1), were used to test the ability of alpha-keto-ss-methyl-n-valeric acid (KMV) to scavenge ROS. KMV diminished c-DCF-detectable ROS that were induced by H(2)O(2), oxygen/glucose deprivation, or SIN-1 in PC12 cells, primary neuronal cultures, or fibroblasts. Furthermore, KMV reduced the H(2)O(2)-induced increase in BRCS and diminished the elevation in BRCS in cells from AD patients to control levels. On the other hand, DAF-detectable NO(.-) induced by SIN-1 was not scavenged by KMV and did not exaggerate BRCS. The results indicate that KMV is an effective antioxidant of c-DCF-detectable ROS. The effects of KMV are not cell type specific, but are ROS specific. The same H(2)O(2)-induced ROS that reacts with KMV may also underlie the changes in BRCS related to AD. Thus, KMV ameliorates the effects of ROS on calcium homeostasis related to oxidative stress and to AD.