RESUMO
The effect of TiCl4 hydrolysis temperature on the structural, textural and morphological properties of the resulting rutile and on the changes of these properties upon calcination was studied. The XRD, Raman spectroscopy, mercury porosimetry, BET, SEM and TEM studies have revealed that TiO2 rutile has a hierarchical 3D-architecture. The obtained nanostructured rutile had a cauliflowerlike/ spherical morphology composed of fan-shaped nanofibers. Rutile samples were shown to have a heterogeneous pore structure including micro-, meso- and macropores with a BET surface area of 110-140 m2/g. According to the mercury porosimetry, among mesopores and macropores the latter dominate in the samples. Elevation of the synthesis temperature from 50-70 to 80-90 °C decreased the fraction of macropores from 95 to 70%. The BET method showed that the samples synthesized at low temperatures (50-70 °C) contain 30-44% of micropores in the total amount of mesopores and micropores. The fraction of micropores decreases to 25-18% with a subsequent increase in the fraction of mesopores as the synthesis temperature is raised to 80-90 °C. As shown by a study of the samples upon calcination in the temperature range of 100-1000 °C, temperature is the key factor that produces changes in the crystallites size, nanofiber length and packing density, and 3D particle shape at different levels of the hierarchical system and determines features of the porous structure and morphological properties of nanostructured rutile. The assessment of photocatalytic activity in the oxidation of acetone vapor demonstrated that, regardless of the hydrolysis temperature, the synthesized samples of nanostructured rutile are able to oxidize acetone vapor to carbon dioxide and water. In the process, activity of the samples is comparable with that of commercial photocatalysts under UV light and is superior to the activity of commercial photocatalysts P25 (2-4 times) and TiO2 KRONOS vlp 7000 (1.2-2 times) under visible light in dependence on the synthesis temperature.
RESUMO
Background: The development of new antiviral drugs based on nucleic acids is under scrutiny. An important problem in this aspect is to find the most vulnerable conservative regions in the viral genome as targets for the action of these agents. Another challenge is the development of an efficient system for their delivery into cells. To solve this problem, we proposed a TiO2·PL-DNA nanocomposite consisting of titanium dioxide nanoparticles and polylysine (PL)-containing oligonucleotides. Results: The TiO2·PL-DNA nanocomposites bearing the DNA fragments targeted to different conservative regions of (-)RNA and (+)RNA of segment 5 of influenza A virus (IAV) were studied for their antiviral activity in MDCK cells infected with the H1N1, H5N1, and H3N2 virus subtypes. Within the negative strand of each of the studied strains, the efficiency of DNA fragments increased in the direction of its 3'-end. Thus, the DNA fragment aimed at the 3'-noncoding region of (-)RNA was the most efficient and inhibited the reproduction of different IAV subtypes by 3-4 orders of magnitude. Although to a lesser extent, the DNA fragments targeted at the AUG region of (+)RNA and the corresponding region of (-)RNA were also active. For all studied viral subtypes, the nanocomposites bearing the DNA fragments targeted to (-)RNA appeared to be more efficient than those containing fragments aimed at the corresponding (+)RNA regions. Conclusion: The proposed TiO2·PL-DNA nanocomposites can be successfully used for highly efficient and site-specific inhibition of influenza A virus of different subtypes. Some patterns of localization of the most vulnerable regions in IAV segment 5 for the action of DNA-based drugs were found. The (-)RNA strand of IAV segment 5 appeared to be more sensitive as compared to (+)RNA.
