16 research outputs found
Protection from ultraviolet damage and photocarcinogenesis by vitamin d compounds
Get PDF© Springer Nature Switzerland AG 2020. Exposure of skin cells to UV radiation results in DNA damage, which if inadequately repaired, may cause mutations. UV-induced DNA damage and reactive oxygen and nitrogen species also cause local and systemic suppression of the adaptive immune system. Together, these changes underpin the development of skin tumours. The hormone derived from vitamin D, calcitriol (1,25-dihydroxyvitamin D3) and other related compounds, working via the vitamin D receptor and at least in part through endoplasmic reticulum protein 57 (ERp57), reduce cyclobutane pyrimidine dimers and oxidative DNA damage in keratinocytes and other skin cell types after UV. Calcitriol and related compounds enhance DNA repair in keratinocytes, in part through decreased reactive oxygen species, increased p53 expression and/or activation, increased repair proteins and increased energy availability in the cell when calcitriol is present after UV exposure. There is mitochondrial damage in keratinocytes after UV. In the presence of calcitriol, but not vehicle, glycolysis is increased after UV, along with increased energy-conserving autophagy and changes consistent with enhanced mitophagy. Reduced DNA damage and reduced ROS/RNS should help reduce UV-induced immune suppression. Reduced UV immune suppression is observed after topical treatment with calcitriol and related compounds in hairless mice. These protective effects of calcitriol and related compounds presumably contribute to the observed reduction in skin tumour formation in mice after chronic exposure to UV followed by topical post-irradiation treatment with calcitriol and some, though not all, related compounds
Demonstration of calcium transport markers in the ceca of owls (Aves: Strigiformes), with remarks on basic ceca structure
No full textImproved Survival of Patients with Warfarin-Associated Intracerebral Haemorrhage: A Retrospective Longitudinal Population-Based Study
No full text1α,25-Dihydroxycholecalciferol Induces Nitric Oxide Production in Cultured Endothelial Cells
No full textNuclear lipid microdomains regulate nuclear vitamin D3 uptake and influence embryonic hippocampal cell differentiation
No full textIn the cell nucleus, the 1,25-(OH)2 vitamin D3 (1,25-(OH)2D3) receptor (VDR) is localized in specialized microdomains enriched in sphingomyelin and cholesterol. The integrity of these microdomains is necessary for 1,25-(OH)2D3–induced differentiation of embryonic hippocampal cells. Serum deprivation alters nuclear microdomains, which lose the VDR
The Vitamin D Receptor Inhibits the Respiratory Chain, Contributing to the Metabolic Switch that Is Essential for Cancer Cell Proliferation
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Vitamin D receptor is present on the neuronal plasma membrane and is co-localized with amyloid precursor protein, ADAM10 or Nicastrin
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