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Selecting the perfect sleeve ironing board replacement cover can be a game-changer for keeping cloth...
sleeve ironing board replacement covers
2025-08-14 05:08
Transforming your ironing experience begins with the right accessory, and the 42 ironing board cover...
42 ironing board cover
2025-08-14 04:14
The Importance of a Good Ironing Board Cover A Step Towards Efficient Ironing Ironing is often viewe...
54 ironing board cover
2025-08-14 04:10
For homeowners seeking an efficient, space-saving solution to their ironing woes, the over-the-door...
funda y almohadilla para tabla de planchar sobre la puerta
2025-08-14 04:05
When stepping into the dynamic world of home essential accessories, ironing board covers often go un...
venta de fundas para tablas de planchar
2025-08-14 03:55
Leopard ironing board covers have become a popular choice for those who want to add a touch of style...
leopard ironing board cover
2025-08-14 03:36
Beautiful ironing board covers are not just functional; they are an essential part of maintaining a...
beautiful ironing board covers
2025-08-14 03:36
An ironing board cover is a vital household accessory that ensures smooth and efficient ironing. Ove...
How to Clean and Maintain Your Ironing Board Cover for Longevity
2025-08-14 03:32
In the modern household, the ironing board can often be overlooked, seen as a mundane utility rather...
110 x 33 ironing board cover
2025-08-14 03:08
Black table covers, often underappreciated in their role, have emerged as essential components in bo...
black table cover
2025-08-14 02:48
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    Different dermal cell types have been reported to differ in their sensitivity to nano-sized TiO2 . Kiss et al. exposed human keratinocytes (HaCaT), human dermal fibroblast cells, sebaceous gland cells (SZ95) and primary human melanocytes to 9 nm-sized TiO2 particles at concentrations from 0.15 to 15 μg/cm2 for up to 4 days. The particles were detected in the cytoplasm and perinuclear region in fibroblasts and melanocytes, but not in kerati-nocytes or sebaceous cells. The uptake was associated with an increase in the intracellular Ca2+ concentration. A dose- and time-dependent decrease in cell proliferation was evident in all cell types, whereas in fibroblasts an increase in cell death via apoptosis has also been observed. Anatase TiO2 in 20–100 nm-sized form has been shown to be cytotoxic in mouse L929 fibroblasts. The decrease in cell viability was associated with an increase in the production of ROS and the depletion of glutathione. The particles were internalized and detected within lysosomes. In human keratinocytes exposed for 24 h to non-illuminated, 7 nm-sized anatase TiO2, a cluster analysis of the gene expression revealed that genes involved in the “inflammatory response” and “cell adhesion”, but not those involved in “oxidative stress” and “apoptosis”, were up-regulated. The results suggest that non-illuminated TiO2 particles have no significant impact on ROS-associated oxidative damage, but affect the cell-matrix adhesion in keratinocytes in extracellular matrix remodelling. In human keratinocytes, Kocbek et al. investigated the adverse effects of 25 nm-sized anatase TiO2 (5 and 10 μg/ml) after 3 months of exposure and found no changes in the cell growth and morphology, mitochondrial function and cell cycle distribution. The only change was a larger number of nanotubular intracellular connections in TiO2-exposed cells compared to non-exposed cells. Although the authors proposed that this change may indicate a cellular transformation, the significance of this finding is not clear. On the other hand, Dunford et al. studied the genotoxicity of UV-irradiated TiO2 extracted from sunscreen lotions, and reported severe damage to plasmid and nuclear DNA in human fibroblasts. Manitol (antioxidant) prevented DNA damage, implying that the genotoxicity was mediated by ROS.