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Many engineered nanomaterials (NMs) are being synthesized and explored for potential use in consumer and medical products. Already, nanoparticles (NPs) of titanium dioxide (TiO(2)), zinc oxide (ZnO), silver (Ag) and other metals or their oxides are present in commercial products such as sunscreens, cosmetics, wound dressings, surgical tools, detergents, automotive paints and tires. More recent and advanced FDA-approved use of NMs includes quantum dots (QDs) in live cell imaging, zirconium oxides in bone replacement and prosthetic devices and nanocarriers in drug delivery. The benefits from nanotechnology are aplenty, comprising antimicrobial activities, scratch- and water-resistance, long-lasting shine, improved processor speeds and better display resolution, to name a few. While developers of these products often focus on the exciting beneficial aspects of their products, safety and toxicity issues are often not discussed in detail. Long-term effects such as chronic exposure and environmental pollution are even less documented. Along with widespread manufacture and use of NMs, concerns for occupational hazards, proper handling, disposal, storage, shipping and clean up are expected to rise. This review focus on the possible biological impact of engineered NPs, serving as a reminder that nanomaterials can become a double-edged sword if not properly handled.  相似文献   
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Zika virus (ZIKV) represents a re-emerging threat to global health due to its association with congenital birth defects. ZIKV NS2B-NS3 protease is crucial for virus replication by cleaving viral polyprotein at various junctions to release viral proteins and cause cytotoxic effects in ZIKV-infected cells. This study characterized the inhibitory effects of doxycycline against ZIKV NS2B-NS3 protease and viral replication in human skin cells. The in silico data showed that doxycycline binds to the active site of ZIKV protease at a low docking energy (−7.8 Kcal/mol) via four hydrogen bonds with the protease residues TYR1130, SER1135, GLY1151, and ASP83. Doxycycline efficiently inhibited viral NS2B-NS3 protease at average human temperature (37 °C) and human temperature with a high fever during virus infection (40 °C). Interestingly, doxycycline showed a higher inhibitory effect at 40 °C (IC50 = 5.3 µM) compared to 37 °C (9.9 µM). The virus replication was considerably reduced by increasing the concentration of doxycycline. An approximately 50% reduction in virus replication was observed at 20 µM of doxycycline. Treatment with 20 µM of doxycycline reduced the cytopathic effects (CPE), and the 40 µM of doxycycline almost eliminated the CPE of human skin cells. This study showed that doxycycline binds to the ZIKV protease and inhibits its catalytic activity at a low micro-molecular concentration range. Treatment of human skin fibroblast with doxycycline eliminated ZIKV infection and protected the cells against the cytopathic effects of the infection.  相似文献   
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Research on Chemical Intermediates - Magnetite nanoparticles (Fe3O4 NPs) have received considerable attention in various biomedical applications due to their fascinating properties and multiple...  相似文献   
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