Melanin processing by keratinocytes: A non‐microbial type of host‐pathogen interaction?

Moreiras, Hugo; Silva, Mafalda Lopes da; Seabra, Miguel C.; Barral, Duarte C.

doi:10.1111/tra.12638

Cited by 9 publications

(9 citation statements)

References 32 publications

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“…Low molecular weight components such as dimeric compounds were appreciably internalized after 1 h incubation. These data provide further confirmation to biological studies indicating that keratinocytes are able to internalize melanins as the result of a cross-talk with melanocytes, mediated by the protease-activated receptor 2 (PAR-2) and the Ras-related protein Rab11 [59,60]. Overall, our findings demonstrate that MeDHICA-melanin is able to enter the cells and activate the antioxidant system to protect skin cells from UVA-induced damage, encouraging its use as an effective component in dermo-cosmetic formulations for the treatment of skin damage, photoaging and skin cancers.…”

Section: Discussionsupporting

confidence: 79%

A Melanin-Related Phenolic Polymer with Potent Photoprotective and Antioxidant Activities for Dermo-Cosmetic Applications

Liberti¹,

Alfieri²,

Monti³

et al. 2020

Antioxidants

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Eumelanins, the dark variant of skin pigments, are endowed with a remarkable antioxidant activity and well-recognized photoprotective properties that have been ascribed to pigment components derived from the biosynthetic precursor 5,6-dihydroxyindole-2-carboxylic acid (DHICA). Herein, we report the protective effect of a polymer obtained starting from the methyl ester of DHICA (MeDHICA-melanin) against Ultraviolet A (UVA)-induced oxidative stress in immortalized human keratinocytes (HaCaT). MeDHICA-melanin was prepared by aerial oxidation of MeDHICA. At concentrations as low as 10 µg/mL, MeDHICA-melanin prevented reactive oxygen species accumulation and partially reduced glutathione oxidation in UVA-irradiated keratinocytes. Western blot experiments revealed that the polymer is able to induce the translocation of nuclear factor erythroid 2–related factor 2 (Nrf-2) to the nucleus with the activation of the transcription of antioxidant enzymes, such as heme-oxygenase 1. Spectrophotometric and HPLC analysis of cell lysate allowed to conclude that a significant fraction (ca. 7%), consisting mainly of the 4,4′-dimer of MeDHICA (ca. 2 μM), was internalized in the cells. Overall these data point to the potential use of MeDHICA-melanin as an antioxidant for the treatment of skin damage, photoaging and skin cancers.

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Section: Discussionsupporting

confidence: 79%

A Melanin-Related Phenolic Polymer with Potent Photoprotective and Antioxidant Activities for Dermo-Cosmetic Applications

Liberti¹,

Alfieri²,

Monti³

et al. 2020

Antioxidants

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“…Hence, the first task where this approach can find application is the investigation of melanin fate and its redistribution in the epidermis upon stress conditions such as UV exposure 2,68 , oxidative and mechanical stress 11 , etc. Although this task is seemingly simple, the fact is that a number of questions about the melanin fate (such as the presence of "melanin dust" in the stratum corneum 13,14 ), kinetics and mechanisms of its transfer in normal and stress conditions and the degradation pathways 7,[11][12][13][14] require additional studies, in which the suggested method could be useful.…”

Section: Discussionmentioning

confidence: 99%

“…However, in later works, autophagy was demonstrated not to have a substantial effect on skin pigmentation 9 , and melanosomes were shown to be non-degradative 10 . Other mechanisms like inherent asymmetric localization of melanosomes between dividing keratinocytes could be potentially involved in a complex inhomogeneous distribution of melanin in the epidermis [11][12][13] . Hence, precise assessment of melanin distribution in different epidermal layers is required to study fundamental processes and identify melanin-related abnormalities in norm and pathology.…”

mentioning

confidence: 99%

Melanin distribution from the dermal–epidermal junction to the stratum corneum: non-invasive in vivo assessment by fluorescence and Raman microspectroscopy

Yakimov

Shirshin

Schleusener

et al. 2020

Sci Rep

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the fate of melanin in the epidermis is of great interest due to its involvement in numerous physiological and pathological processes in the skin. Melanin localization can be assessed ex vivo and in vivo using its distinctive optical properties. Melanin exhibits a characteristic Raman spectrum band shape and discernible near-infrared excited (NIR) fluorescence. However, a detailed analysis of the capabilities of depth-resolved confocal Raman and fluorescence microspectroscopy in the evaluation of melanin distribution in the human skin is lacking. Here we demonstrate how the fraction of melanin at different depths in the human skin in vivo can be estimated from its Raman spectra (bands at 1,380 and 1,570 cm −1) using several procedures including a simple ratiometric approach, spectral decomposition and non-negative matrix factorization. The depth profiles of matrix factorization components specific to melanin, collagen and natural moisturizing factor provide information about their localization in the skin. The depth profile of the collagen-related matrix factorization component allows for precise determination of the dermal-epidermal junction, i.e. the epidermal thickness. Spectral features of fluorescence background originating from melanin were found to correlate with relative intensities of the melanin Raman bands. We also hypothesized that NIR fluorescence in the skin is not originated solely from melanin, and the possible impact of oxidized species should be taken into account. The ratio of melanin-related Raman bands at 1,380 and 1,570 cm −1 could be related to melanin molecular organization. the proposed combined analysis of the Raman scattering signal and NIR fluorescence could be a useful tool for rapid non-invasive in vivo diagnostics of melanin-related processes in the human skin.

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“…Skin melanocytes and RPE cells are two mammalian cell types in which melanosomes move from the cell body to the cell periphery. In melanocytes, melanosome biogenesis is active (Raposo and Marks, 2007) and the melanosomes do not return to the cell body; they are delivered to keratinocytes from the melanocyte dendrites (Hume et al, 2001;Wasmeier et al, 2008;Fukuda, 2013;Wu and Hammer, 2014;Moreiras et al, 2019). By contrast, melanosome biogenesis is very low in the postnatal RPE (Lopes et al, 2007b).…”

Section: Discussionmentioning

confidence: 99%

“…In mammalian skin, melanosome biogenesis occurs in melanocytes (Raposo and Marks, 2007). The melanosomes then pass from the dendrites of the melanocytes to neighboring keratinocytes (Hume et al, 2001;Wasmeier et al, 2008;Fukuda, 2013;Wu and Hammer, 2014;Moreiras et al, 2019). Preceding the intercellular transfer, melanosomes must be transported and retained in the melanocyte dendrites.…”

Section: Introductionmentioning

confidence: 99%

Microtubule motor transport in the delivery of melanosomes to the actin-rich apical domain of the retinal pigment epithelium

Jiang

Paniagua

Volland

et al. 2020

Journal of Cell Science

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Melanosomes are motile, light-absorbing organelles that are present in pigment cells of the skin and eye. It has been proposed that melanosome localization, in both skin melanocytes and the retinal pigment epithelium (RPE), involves melanosome capture from microtubule motors by an unconventional myosin, which dynamically tethers the melanosomes to actin filaments. Recent studies with melanocytes have questioned this cooperative capture model. Here, we test the model in RPE cells by imaging melanosomes associated with labeled actin filaments and microtubules, and by investigating the roles of different motor proteins. We found that a deficiency in cytoplasmic dynein phenocopies the lack of myosin-7a, in that melanosomes undergo fewer of the slow myosin-7a-dependent movements and are absent from the RPE apical domain. These results indicate that microtubule-based motility is required for the delivery of melanosomes to the actin-rich apical domain and support a capture mechanism that involves both microtubule and actin motors.

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Melanin processing by keratinocytes: A non‐microbial type of host‐pathogen interaction?

Cited by 9 publications

References 32 publications

A Melanin-Related Phenolic Polymer with Potent Photoprotective and Antioxidant Activities for Dermo-Cosmetic Applications

A Melanin-Related Phenolic Polymer with Potent Photoprotective and Antioxidant Activities for Dermo-Cosmetic Applications

Melanin distribution from the dermal–epidermal junction to the stratum corneum: non-invasive in vivo assessment by fluorescence and Raman microspectroscopy

Microtubule motor transport in the delivery of melanosomes to the actin-rich apical domain of the retinal pigment epithelium

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