Revisiting the role of melatonin in human melanocyte physiology: A skin context perspective

IF 8.3 1区 医学 Q1 ENDOCRINOLOGY & METABOLISM
Alec Sevilla, Jérémy Chéret, Radomir M. Slominski, Andrzej T. Slominski, Ralf Paus
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引用次数: 22

Abstract

The evolutionarily ancient methoxyindoleamine, melatonin, has long perplexed investigators by its versatility of functions and mechanisms of action, which include the regulation of vertebrate pigmentation. Although first discovered through its potent skin-lightening effects in amphibians, melatonin's role in human skin and hair follicle pigmentation and its impact on melanocyte physiology remain unclear. Synthesizing our limited current understanding of this role, we specifically examine its impact on melanogenesis, oxidative biology, mitochondrial function, melanocyte senescence, and pigmentation-related clock gene activity, with emphasis on human skin, yet without ignoring instructive pointers from nonhuman species. Given the strict dependence of melanocyte functions on the epithelial microenvironment, we underscore that melanocyte responses to melatonin are best interrogated in a physiological tissue context. Current evidence suggests that melatonin and some of its metabolites inhibit both, melanogenesis (via reducing tyrosinase activity) and melanocyte proliferation by stimulating melatonin membrane receptors (MT1, MT2). We discuss whether putative melanogenesis-inhibitory effects of melatonin may occur via activation of Nrf2-mediated PI3K/AKT signaling, estrogen receptor-mediated and/or melanocortin-1 receptor- and cAMP-dependent signaling, and/or via melatonin-regulated changes in peripheral clock genes that regulate human melanogenesis, namely Bmal1 and Per1. Melatonin and its metabolites also accumulate in melanocytes where they exert net cyto- and senescence-protective as well as antioxidative effects by operating as free radical scavengers, stimulating the synthesis and activity of ROS scavenging enzymes and other antioxidants, promoting DNA repair, and enhancing mitochondrial function. We argue that it is clinically and biologically important to definitively clarify whether melanocyte cell culture-based observations translate into melatonin-induced pigmentary changes in a physiological tissue context, that is, in human epidermis and hair follicles ex vivo, and are confirmed by clinical trial results. After defining major open questions in this field, we close by suggesting how to begin answering them in clinically relevant, currently available preclinical in situ research models.

重新审视褪黑素在人类黑素细胞生理学中的作用:皮肤背景的观点
进化上古老的甲氧基吲哚胺,褪黑素,由于其功能和作用机制的多样性,包括对脊椎动物色素沉着的调节,长期以来一直困扰着研究人员。虽然首次发现褪黑素是在两栖动物身上发现的,但褪黑素在人类皮肤和毛囊色素沉着中的作用及其对黑素细胞生理的影响尚不清楚。综合我们目前对这一作用的有限理解,我们特别研究了它对黑素形成、氧化生物学、线粒体功能、黑素细胞衰老和色素相关时钟基因活性的影响,重点是人类皮肤,但不忽视非人类物种的指导指标。鉴于黑素细胞功能对上皮微环境的严格依赖,我们强调黑素细胞对褪黑激素的反应最好在生理组织背景下进行研究。目前的证据表明,褪黑激素及其一些代谢物通过刺激褪黑激素膜受体(MT1, MT2)抑制黑素生成(通过降低酪氨酸酶活性)和黑素细胞增殖。我们讨论了褪黑激素是否可能通过激活nrf2介导的PI3K/AKT信号、雌激素受体介导的和/或黑素皮质素-1受体和camp依赖的信号,以及/或通过褪黑激素调节的调节人类黑色素形成的外周时钟基因(即Bmal1和Per1)的变化来抑制黑色素形成。褪黑素及其代谢物也在黑素细胞中积累,通过作为自由基清除剂,刺激活性氧清除酶和其他抗氧化剂的合成和活性,促进DNA修复,增强线粒体功能,发挥净细胞和衰老保护以及抗氧化作用。我们认为,明确阐明基于黑素细胞培养的观察结果是否转化为褪黑素诱导的生理组织(即体外的人类表皮和毛囊)色素变化,并得到临床试验结果的证实,在临床上和生物学上都是重要的。在定义了该领域的主要开放问题之后,我们建议如何开始在临床相关的,目前可用的临床前原位研究模型中回答这些问题。
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来源期刊
Journal of Pineal Research
Journal of Pineal Research 医学-内分泌学与代谢
CiteScore
17.70
自引率
4.90%
发文量
66
审稿时长
1 months
期刊介绍: The Journal of Pineal Research welcomes original scientific research on the pineal gland and melatonin in vertebrates, as well as the biological functions of melatonin in non-vertebrates, plants, and microorganisms. Criteria for publication include scientific importance, novelty, timeliness, and clarity of presentation. The journal considers experimental data that challenge current thinking and welcomes case reports contributing to understanding the pineal gland and melatonin research. Its aim is to serve researchers in all disciplines related to the pineal gland and melatonin.
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