首页> 美国卫生研究院文献>Cancer Control : Journal of the Moffitt Cancer Center >Artificial Light at Night of Different Spectral CompositionsDifferentially Affects Tumor Growth in Mice: Interaction With Melatonin andEpigenetic Pathways
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Artificial Light at Night of Different Spectral CompositionsDifferentially Affects Tumor Growth in Mice: Interaction With Melatonin andEpigenetic Pathways

机译:夜间不同光谱成分的人造光差异影响小鼠肿瘤的生长:与褪黑激素和表观遗传途径

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摘要

Lighting technology is rapidly advancing toward shorter wavelength illuminations that offer energy-efficient properties. Along with this advantage, the increased use of such illuminations also poses some health challenges, particularly breast cancer progression. Here, we evaluated the effects of artificial light at night (ALAN) of 4 different spectral compositions (500-595 nm) at 350 Lux on melatonin suppression by measuring its urine metabolite 6-sulfatoxymelatonin, global DNA methylation, tumor growth, metastases formation, and urinary corticosterone levels in 4T1 breast cancer cell-inoculated female BALB/c mice. The results revealed an inverse dose-dependent relationship between wavelength and melatonin suppression. Short wavelength increased tumor growth, promoted lung metastases formation, and advanced DNA hypomethylation, while long wavelength lessened these effects. Melatonin treatment counteracted these effects and resulted in reduced cancer burden. The wavelength suppression threshold for melatonin-induced tumor growth was 500 nm. These results suggest that short wavelength increases cancer burden by inducing aberrant DNA methylation mediated by the suppression of melatonin. Additionally, melatonin suppression and global DNA methylation are suggested as promising biomarkers for early diagnosis andtherapy of breast cancer. Finally, ALAN may manifest other physiologicalresponses such as stress responses that may challenge the survival fitness ofthe animal under natural environments.
机译:照明技术正迅速向提供节能特性的更短波长的照明发展。伴随着这种优势,增加使用这种照明也带来了一些健康挑战,特别是乳腺癌的发展。在这里,我们通过测量尿液代谢物6-磺酰氧基褪黑素,总体DNA甲基化,肿瘤生长,转移灶的形成,评估了350勒克斯下4种不同光谱成分(500-595 nm)的夜间人工光(ALAN)对褪黑素抑制的影响,和接种4T1乳腺癌细胞的雌性BALB / c小鼠的尿皮质酮水平。结果显示波长与褪黑激素抑制之间呈反剂量依赖性关系。短波长增加了肿瘤的生长,促进了肺转移的形成,并促进了DNA低甲基化,而长波长则减少了这些影响。褪黑素治疗抵消了这些影响,并减少了癌症负担。褪黑素诱导的肿瘤生长的波长抑制阈值为500 nm。这些结果表明,短波长通过诱导由褪黑激素抑制介导的异常DNA甲基化而增加了癌症负担。此外,褪黑激素抑制和整体DNA甲基化被建议作为早期诊断和治疗的有前途的生物标志物。乳腺癌的治疗。最后,ALAN可能表现出其他生理可能会挑战生存能力的压力反应等压力反应自然环境下的动物。

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