UVR

UVR
  • 文章类型: Journal Article
    皮肤-脑轴已被认为在几种病理生理状况中起作用,包括阿片类药物成瘾,帕金森病和许多其他疾病。最近的证据表明,调节皮肤色素沉着的途径可能直接和间接地调节行为。相反,中枢神经系统驱动的神经和激素反应已被证明可以调节色素沉着,例如,在压力下。此外,由于中枢神经系统中黑素细胞和神经元的共同神经外胚层起源,某些中枢神经系统疾病可能与色素沉着相关的变化有关,例如,MC1R变体。此外,皮肤的HPA类似物将皮肤色素沉着与内分泌系统联系起来,从而允许皮肤索引可能的荷尔蒙异常明显。在这次审查中,提供了对大脑中皮肤色素产生和神经黑色素合成的洞察力,并总结了最近的发现,特别关注色素沉着,与中枢神经系统相连。因此,这篇综述可能有助于更好地理解几种皮肤-大脑关联在健康和疾病中的作用机制.
    The skin-brain axis has been suggested to play a role in several pathophysiological conditions, including opioid addiction, Parkinson\'s disease and many others. Recent evidence suggests that pathways regulating skin pigmentation may directly and indirectly regulate behaviour. Conversely, CNS-driven neural and hormonal responses have been demonstrated to regulate pigmentation, e.g., under stress. Additionally, due to the shared neuroectodermal origins of the melanocytes and neurons in the CNS, certain CNS diseases may be linked to pigmentation-related changes due to common regulators, e.g., MC1R variations. Furthermore, the HPA analogue of the skin connects skin pigmentation to the endocrine system, thereby allowing the skin to index possible hormonal abnormalities visibly. In this review, insight is provided into skin pigment production and neuromelanin synthesis in the brain and recent findings are summarised on how signalling pathways in the skin, with a particular focus on pigmentation, are interconnected with the central nervous system. Thus, this review may supply a better understanding of the mechanism of several skin-brain associations in health and disease.
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  • 文章类型: Journal Article
    由于长期和过度暴露于UVR导致的累积皮肤损伤,户外工人患角质形成细胞癌的风险增加。这项研究旨在确定潜在的非侵入性生物标志物来评估慢性UVR暴露。我们分析了从2个皮肤位置和2个职业组收集的角质层生物标志物,并对比了太阳能UVR暴露:户外工人和室内工人的额头和耳后皮肤。使用线性混合模型调整年龄和皮肤照型,我们比较了室内和室外工作人员皮肤部位的生物标志物.我们测量了免疫反应和皮肤屏障的标志物,包括细胞因子,GFs,15-羟基二十碳四烯酸,顺式和反式尿酸,和角质细胞地形图,由圆形纳米物体表示。2个皮肤部位之间的差异被发现为顺式尿路酸,总尿路酸,IL-1α,IL-1RA,IL-1RA/IL-1α,IL-18,15-羟基二十碳四烯酸,CCL4和圆形纳米物体。室内和室外工人的顺式尿酸和CCL4的水平也不同。这些发现强调了UVR诱导的免疫应答和皮肤屏障的变化。它们表明角质层生物标志物在检测职业环境中的慢性UVR暴露和帮助制定预防措施方面的潜在效用。
    Outdoor workers have increased risk of developing keratinocyte cancer due to accumulated skin damage resulting from chronic and excessive exposure to UVR. This study aims to identify potential noninvasive biomarkers to assess chronic UVR exposure. We analyzed stratum corneum biomarkers collected from 2 skin locations and 2 occupational groups with contrasting solar UVR exposure: the forehead and retroauricular skin among outdoor workers and indoor workers. Using a linear mixed model adjusting for age and skin phototype, we compared biomarkers between both skin sites in indoor and outdoor workers. We measured markers of the immune response and skin barrier, including cytokines, GFs, 15-hydroxyeicosatetraenoic acid, cis- and trans-urocanic acid, and corneocyte topography, indicated by circular nano objects. Differences between the 2 skin sites were found for cis-urocanic acid, total urocanic acid, IL-1α, IL-1RA, IL-1RA/IL-1α, IL-18, 15-hydroxyeicosatetraenoic acid, CCL4, and circular nano objects. The levels of cis-urocanic acid and CCL4 also differed between indoor and outdoor workers. These findings underscore changes in both immune response and skin barrier induced by UVR. They indicate the potential utility of stratum corneum biomarkers in detecting both chronic UVR exposure in occupational setting and aiding in the development of preventive measures.
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  • 文章类型: Journal Article
    线粒体是在能量代谢中起作用的真核细胞细胞器,ROS生产,和程序性细胞死亡。皮肤上皮和毛囊毛乳头细胞是能量丰富的细胞,因此可能受到线粒体功能障碍和DNA突变积累的影响。在这次审查中,我们旨在总结评估与线粒体功能障碍相关的皮肤病和结局的医学文献.对PubMed和Embase进行搜索,随后进行手工搜索以检索其他相关文章。线粒体DNA(mtDNA)缺失,突变积累,损伤与皮肤老化的表型迹象有关,脱发,伤口愈合受损。此外,几种皮肤病与线粒体活性异常有关,比如系统性红斑狼疮,牛皮癣,白癜风,和特应性皮炎。小鼠模型研究在线粒体损伤和皮肤病学结果之间建立了更好的因果关系,其中一些描绘了线粒体功能恢复后的可逆性。线粒体功能介导各种皮肤病,和线粒体成分可能是治疗策略的有希望的靶标。
    Mitochondria are eukaryotic cellular organelles that function in energy metabolism, ROS production, and programmed cell death. Cutaneous epithelial and hair follicle dermal papilla cells are energy-rich cells that thereby may be affected by mitochondrial dysfunction and DNA mutation accumulation. In this review, we aimed to summarize the medical literature assessing dermatologic conditions and outcomes associated with mitochondrial dysfunction. A search of PubMed and Embase was performed with subsequent handsearching to retrieve additional relevant articles. Mitochondrial DNA (mtDNA) deletions, mutation accumulation, and damage are associated with phenotypic signs of cutaneous aging, hair loss, and impaired wound healing. In addition, several dermatologic conditions are associated with aberrant mitochondrial activity, such as systemic lupus erythematosus, psoriasis, vitiligo, and atopic dermatitis. Mouse model studies have better established causality between mitochondrial damage and dermatologic outcomes, with some depicting reversibility upon restoration of mitochondrial function. Mitochondrial function mediates a variety of dermatologic conditions, and mitochondrial components may be a promising target for therapeutic strategies.
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  • 文章类型: Journal Article
    维生素D3的激素形式,1,25(OH)2D3,减少紫外线诱导的DNA损伤。紫外线照射会引发皮肤中维生素D3的产生,和持续的紫外线曝光光异构化前维生素D3产生“过度辐射产品”,如lumisterol3(L3)。皮肤中的细胞色素P450侧链裂解酶(CYP11A1)催化L3的转化产生三种主要衍生物:24-羟基-L3[24(OH)L3],22-羟基-L3[22(OH)L3],和20,22-二羟基-L3[20,22(OH)L3]。当前的研究调查了主要的过度辐射代谢产物的光保护特性,24(OH)L3,在人原代角质形成细胞和人皮肤外植体中。结果表明,用24(OH)L3或1,25(OH)2D3进行紫外线处理后立即减少了紫外线诱导的环丁烷嘧啶二聚体和氧化DNA损伤,在角质形成细胞中具有相似的浓度响应曲线,虽然在皮肤外植体中,1,25(OH)2D3更有效。两种化合物对DNA损伤的减少,至少在某种程度上,通过增加糖酵解增加能量可用性来增加DNA修复的结果,以及核苷酸切除修复途径中增加的DNA损伤识别蛋白。在存在较低活性氧的情况下,两种化合物都会减少紫外线诱导的DNA光致氧化。结果表明,在体外和离体条件下,24(OH)L3提供类似于1,25(OH)2D3的抗UV损伤的光保护。
    The hormonal form of vitamin D3, 1,25(OH)2D3, reduces UV-induced DNA damage. UV exposure initiates pre-vitamin D3 production in the skin, and continued UV exposure photoisomerizes pre-vitamin D3 to produce \"over-irradiation products\" such as lumisterol3 (L3). Cytochrome P450 side-chain cleavage enzyme (CYP11A1) in skin catalyzes the conversion of L3 to produce three main derivatives: 24-hydroxy-L3 [24(OH)L3], 22-hydroxy-L3 [22(OH)L3], and 20,22-dihydroxy-L3 [20,22(OH)L3]. The current study investigated the photoprotective properties of the major over-irradiation metabolite, 24(OH)L3, in human primary keratinocytes and human skin explants. The results indicated that treatment immediately after UV with either 24(OH)L3 or 1,25(OH)2D3 reduced UV-induced cyclobutane pyrimidine dimers and oxidative DNA damage, with similar concentration response curves in keratinocytes, although in skin explants, 1,25(OH)2D3 was more potent. The reductions in DNA damage by both compounds were, at least in part, the result of increased DNA repair through increased energy availability via increased glycolysis, as well as increased DNA damage recognition proteins in the nucleotide excision repair pathway. Reductions in UV-induced DNA photolesions by either compound occurred in the presence of lower reactive oxygen species. The results indicated that under in vitro and ex vivo conditions, 24(OH)L3 provided photoprotection against UV damage similar to that of 1,25(OH)2D3.
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  • 文章类型: Journal Article
    皮肤是形成身体的天然外皮系统的薄层组织,其充当屏障以保护其免受在体内诱导不期望的生物反应的外源和内源因素的影响。在这些风险因素中,由太阳紫外线辐射(UVR)引起的皮肤损伤是皮肤病学中不断升级的问题,急性和慢性皮肤反应的发生率增加。几项流行病学研究为阳光的有益和有害影响提供了证据,特别是人类的太阳能紫外线照射。由于过度暴露于地球表面的太阳UVR,户外专业人士,如农民,农村工人,建筑商和道路工人最容易患上职业性皮肤病。室内晒黑也与各种皮肤病的风险增加有关。晒伤被描述为除了黑色素增加和角质形成细胞凋亡以预防皮肤癌之外的红体急性皮肤反应。分子的变化,色素和形态学特征导致皮肤恶性肿瘤的致癌进展和皮肤的过早老化。阳光紫外线损伤导致免疫抑制性皮肤病,如光毒性和光过敏反应。紫外线诱导的色素沉着持续较长时间,叫做持久的色素沉着。防晒霜是提到最多的皮肤保护行为,它是太阳智能信息中最受欢迎的部分,以及其他有效的皮肤保护策略,如服装,也就是说,长袖,帽子和太阳镜。
    Skin is the thin layer of tissue forming the natural integumentary system of the body that acts as a barrier to protect it from exogenous and endogenous factors that induce undesirable biological responses in the body. Among these risk factors, skin damage triggered by solar ultraviolet radiation (UVR) is an escalating problem in dermatology with an increased incidence of acute and chronic cutaneous reactions. Several epidemiological studies have provided evidence for both beneficial and harmful effects of sunlight, particularly the solar UVR exposure of human beings. Due to overexposure to solar UVR on the earth\'s surface, outdoor professionals such as farmers, rural workers, builders and road workers are most vulnerable to developing occupational skin diseases. Indoor tanning is also associated with increased risks for various dermatological diseases. Sunburn is described as the erythematic acute cutaneous response in addition to increased melanin and apoptosis of keratinocytes to prevent skin carcinoma. Alterations in molecular, pigmentary and morphological characteristics cause carcinogenic progression in skin malignancies and premature ageing of the skin. Solar UV damage leads to immunosuppressive skin diseases such as phototoxic and photoallergic reactions. UV-induced pigmentation persists for a longer time, called long-lasting pigmentation. Sunscreen is the most mentioned skin protective behaviour and it is the most promoted part of the sun smart message along with other effective skin protection strategies such as clothing, that is, long sleeves, hats and sunglasses.
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  • 文章类型: Journal Article
    拉曼光谱是一种新兴的皮肤病学技术,具有以无标记和非侵入性方式在细胞类型之间进行生物化学区分的潜力。这里,我们使用活的单细胞拉曼光谱和主成分分析(PCA)对小鼠黑素细胞进行指纹,黑素细胞,角质形成细胞和黑色素瘤细胞。我们显示了它们光谱的差异可归因于黑色素生物合成途径中的生物标志物,并且黑色素瘤细胞是异质群体,位于未分化的黑素细胞和分化的黑素细胞之间的轨迹上。我们证明了拉曼光谱作为一种高度敏感的工具来探测黑色素生物合成途径及其对紫外线(UV)辐射的即时反应的实用性,揭示了黑素细胞对UVA和UVB辐射的先前未描述的相反反应。最后,我们确定了β-胡萝卜素的黑素细胞特异性积累与脂质和蛋白质中UVR反应的稳定相关,这与β-胡萝卜素介导的光保护机制一致。总之,我们的数据表明,拉曼光谱可用于确定黑素细胞谱系细胞的分化状态,并描述与紫外线照射相关的即时和时间生化变化,这些变化取决于细胞类型,黑色素的分化状态和合成能力。我们的工作独特地应用拉曼光谱来通过细胞在培养中生长时的生物学功能和分化状态来区分细胞类型。在这样做的时候,我们首次证明了它作为探测黑色素生物合成途径的工具的实用性。
    Raman spectroscopy is an emerging dermatological technique with the potential to discriminate biochemically between cell types in a label-free and non-invasive manner. Here, we use live single-cell Raman spectroscopy and principal component analysis (PCA) to fingerprint mouse melanoblasts, melanocytes, keratinocytes and melanoma cells. We show the differences in their spectra are attributable to biomarkers in the melanin biosynthesis pathway and that melanoma cells are a heterogeneous population that sit on a trajectory between undifferentiated melanoblasts and differentiated melanocytes. We demonstrate the utility of Raman spectroscopy as a highly sensitive tool to probe the melanin biosynthesis pathway and its immediate response to ultraviolet (UV) irradiation revealing previously undescribed opposing responses to UVA and UVB irradiation in melanocytes. Finally, we identify melanocyte-specific accumulation of β-carotene correlated with a stabilisation of the UVR response in lipids and proteins consistent with a β-carotene-mediated photoprotective mechanism. In summary, our data show that Raman spectroscopy can be used to determine the differentiation status of cells of the melanocyte lineage and describe the immediate and temporal biochemical changes associated with UV exposure which differ depending on cell type, differentiation status and competence to synthesise melanin. Our work uniquely applies Raman spectroscopy to discriminate between cell types by biological function and differentiation status while they are growing in culture. In doing so, we demonstrate for the first time its utility as a tool with which to probe the melanin biosynthesis pathway.
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  • 文章类型: Journal Article
    自然种群的性状表达通常共同取决于普遍存在的非生物环境条件和捕食风险。co足类动物,例如,可以改变它们对紫外线辐射(UVR)的保护作用的化合物的表达,如虾青素和霉菌素样氨基酸(MAAs),与捕食风险有关。尽管有充分的证据表明co足类动物在存在捕食者的情况下积累的虾青素较少,关于浮游鱼类的群落组成如何影响光保护化合物的整体表达知之甚少。这里,我们研究了格陵兰岛南部湖泊生态系统中北极炭(Salvelinusalpinus)和三叶草刺背鱼(Gasterosteusaculeatus)的(共同)发生如何影响co足类Leptodiaptomusminutus的光保护表型。我们发现,虾青素和MAA的平均含量在有stickleback的湖泊中最低,但是我们没有发现证据表明这些光保护化合物受到了charr的影响。此外,在存在stickleback的情况下,单个co足类动物中虾青素的变化最大,并且co足类动物的虾青素含量与增加的stickleback密度呈负相关。总的来说,我们表明,stickleback的存在和密度共同影响co足类的光保护化合物的含量,说明了生态系统中捕食者的群落组成如何确定猎物特征的表达,这些特征也受到非生物胁迫的影响。
    Trait expression of natural populations often jointly depends on prevailing abiotic environmental conditions and predation risk. Copepods, for example, can vary their expression of compounds that confer protection against ultraviolet radiation (UVR), such as astaxanthin and mycosporine-like amino acids (MAAs), in relation to predation risk. Despite ample evidence that copepods accumulate less astaxanthin in the presence of predators, little is known about how the community composition of planktivorous fish can affect the overall expression of photoprotective compounds. Here, we investigate how the (co-)occurrence of Arctic charr (Salvelinus alpinus) and threespine stickleback (Gasterosteus aculeatus) affects the photoprotective phenotype of the copepod Leptodiaptomus minutus in lake ecosystems in southern Greenland. We found that average astaxanthin and MAA contents were lowest in lakes with stickleback, but we found no evidence that these photoprotective compounds were affected by the presence of charr. Furthermore, variance in astaxanthin among individual copepods was greatest in the presence of stickleback and the astaxanthin content of copepods was negatively correlated with increasing stickleback density. Overall, we show that the presence and density of stickleback jointly affect the content of photoprotective compounds by copepods, illustrating how the community composition of predators in an ecosystem can determine the expression of prey traits that are also influenced by abiotic stressors.
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  • 文章类型: Journal Article
    先前的研究将高水平暴露于紫外线辐射与皮肤恶性黑色素瘤(CMM)的更大风险相关联。这项研究的重点是CMM随时间的变化(从1990年到2017年)在意大利东北部的威尼托地区,及其阿尔卑斯山地区(贝卢诺省)。还考虑了按居住地划分的CMM的临床病理特征。进行了连接点回归分析,以确定按性别和年龄划分的CMM年发病率的显着变化。对于每个趋势,还计算了年平均百分比变化(AAPC)。在2017年CMM队列中,该研究包括对该疾病分类临床病理变量的描述性分析。在被调查的人群中,在过去的30年中,CMM的发病率显着增加。在0-49岁的高山居民中,CMM发病率的AAPC明显高于该地区其他人群(男性:6.9对2.4;女性分别为7.7对2.7)。在阿尔卑斯山的居民中,0-49岁女性的AAPC是50岁以上女性的3.35倍。CMM的临床病理特征与居住地显着相关。三十多年来,威尼托人群观察到CMM的发病率显着增加,和它的AAPC。这两种趋势在高山居民中明显更为明显,尤其是年轻女性。虽然流行病学和临床病理特征支持紫外线辐射在CMM中的作用,受CMM影响的女性人群年龄较小,这表明其他可能与宿主相关的病因.这些发现也证实了一级和二级预防策略的重要性。
    Previous studies associated high-level exposure to ultraviolet radiation with a greater risk of cutaneous malignant melanoma (CMM). This study focuses on the changing incidence of CMM over time (from 1990 to 2017) in the Veneto region of Northeast Italy, and its Alpine area (the province of Belluno). The clinicopathological profile of CMM by residence is also considered. A joinpoint regression analysis was performed to identify significant changes in the yearly incidence of CMM by sex and age. For each trend, the average annual percent change (AAPC) was also calculated. In the 2017 CMM cohort, the study includes a descriptive analysis of the disease\'s categorical clinicopathological variables. In the population investigated, the incidence of CMM has increased significantly over the last 30 years. The AAPC in the incidence of CMM was significantly higher among Alpine residents aged 0-49 than for the rest of the region\'s population (males: 6.9 versus 2.4; females 7.7 versus 2.7, respectively). Among the Alpine residents, the AAPC was 3.35 times greater for females aged 0-49 than for people aged 50+. The clinicopathological profile of CMM was significantly associated with the place of residence. Over three decades, the Veneto population has observed a significant increase in the incidence of CMM, and its AAPC. Both trends have been markedly more pronounced among Alpine residents, particularly younger females. While epidemiology and clinicopathological profiles support the role of UV radiation in CMM, the young age of this CMM-affected female population points to other possible host-related etiological factors. These findings also confirm the importance of primary and secondary prevention strategies.
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  • 文章类型: Journal Article
    背景:大汗腺癌(ASGC)是狗和人类罕见的恶性皮肤肿瘤。迄今为止发表的文献主要集中在这些肿瘤的临床流行病学方面,但是对它们的发病机理知之甚少。在这项研究中,我们旨在确定p53基因是否参与狗的大汗腺癌变以及紫外线辐射(UV)是否与之相关。
    方法:40只犬ASGC接受激光捕获显微切割分离肿瘤细胞,随后从其中提取DNA。然后进行p53外显子2-8的PCR扩增和测序,然后对获得的序列进行计算机分析。
    结果:在13个肿瘤中发现了p53基因中的16个突变。突变涉及C→T,T→C,G→A,和CC→TT转换,C→G变性和腺嘌呤缺失,这是已知与人类皮肤癌发生过程中紫外线辐射相关的基因改变类型。13例肿瘤病例中有6例在外显子4的同一位置显示C→T转变,13例病例中有3例在外显子5的同一位置显示T→C。
    结论:本研究的结果表明p53基因的参与和紫外线辐射对狗ASGC形成的影响。
    BACKGROUND: Apocrine sweat gland carcinomas (ASGCs) are rare malignant skin tumours in dogs and humans. The literature published so far focuses mostly on the clinico-epidemiological aspect of these tumours, but little is known about their pathogenesis. In this study we aimed to determine whether the p53 gene is involved in the carcinogenesis of the apocrine sweat gland in dogs and whether ultraviolet radiation (UV) is related to it.
    METHODS: Forty canine ASGCs were submitted to laser capture microdissection to isolate neoplastic cells, from which DNA was subsequently extracted. PCR amplification and sequencing of p53 exons 2-8 was then performed, followed by computer analysis of the obtained sequences.
    RESULTS: Sixteen mutations within the p53 gene were found in 13 tumours. The mutations involved C → T, T → C, G → A, and CC → TT transitions, C → G transversion and adenine deletion, which are gene alteration types known to be related to UV radiation in the process of skin carcinogenesis in humans. Six of the thirteen tumour cases displayed the C → T transitions in the same location in exon 4 and three of the thirteen cases displayed T → C in the same location in exon 5.
    CONCLUSIONS: The results of the present study indicate both the participation of the p53 gene and the influence of UV radiation in the formation of ASGCs in dogs.
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  • 文章类型: Journal Article
    Action spectra are important biological weighting functions for risk/benefit analyses of ultraviolet (UV) radiation (UVR) exposure. One important human benefit of exposure to terrestrial solar UVB radiation (∼295 to 315 nm) is the cutaneous synthesis of vitamin D3 that is initiated by the photoconversion of 7-dehydrocholesterol to previtamin D3 An action spectrum for this process that is followed by other nonphotochemical steps to achieve biologically active vitamin D3 has been established from ex vivo data and is widely used, although its validity has been questioned. We tested this action spectrum in vivo by full- or partial-body suberythemal irradiation of 75 healthy young volunteers with five different polychromatic UVR spectra on five serial occasions. Serum 25-hydroxyvitamin D3 [25(OH)D3] levels, as the most accurate measure of vitamin D3 status, were assessed before, during, and after the exposures. These were then used to generate linear dose-response curves that were different for each UVR spectrum. It was established that the previtamin D3 action spectrum was not valid when related to the serum 25(OH)D3 levels, as weighting the UVR doses with this action spectrum did not result in a common regression line unless it was adjusted by a blue shift, with 5 nm giving the best fit. Such a blue shift is in accord with the published in vitro action spectra for vitamin D3 synthesis. Thus, calculations regarding the risk (typically erythema) versus the benefit of exposure to solar UVR based on the ex vivo previtamin D3 action spectrum require revision.
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