IL-17 and TNF Synergistically Modulate Cytokine Expression while Suppressing Melanogenesis: Potential Relevance to Psoriasis

Wang, Claire Q.F.; Akalu, Yemsratch T; Suárez‐Fariñas, Mayte; Gonzalez, Juana; Mitsui, Hiroshi; Lowes, Michelle A.; Orlow, Seth J.; Manga, Prashiela; Krueger, James G.

doi:10.1038/jid.2013.237

Cited by 167 publications

(161 citation statements)

References 54 publications

(59 reference statements)

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“…There is evidence of melanocyte activation, such as increase in their size, intense labelling and marked elongation and increase in the number of their dendrites with all used MoAbs, similar to findings previously reported with Melan A. These features have been attributed to an influence by the cytokines interleukin 17 and tumour necrosis factor α [10]. In our study, the activation marker HMB45 revealed a 3-fold increase in melanocytes of the psoriatic lesions, thus confirming the aforementioned morphological cell activation signs.…”

Section: Discussionsupporting

confidence: 72%

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Increased Activity and Number of Epidermal Melanocytes in Lesional Psoriatic Skin

Abdel-Naser¹,

Liakou²,

Elewa³

et al. 2016

Dermatology

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Background: Psoriatic lesions may resolve with hypo- or hyperpigmentation. The involvement of melanocytes in this dichotomous clinical outcome is not fully investigated. Objectives: Qualitative and quantitative assessment of melanocytes in untreated lesional and non-lesional psoriatic skin (n = 15) and healthy controls (n = 10). Methods: Skin biopsies were labelled immunohistochemically (APAAP technique) with the antimelanocyte monoclonal antibodies (MoAbs) HMB45, Melan A, tyrosinase and microphthalmia-associated transcription factor (MITF). The labelled melanocytes were evaluated by an independent investigator with a digital image analyser. Results: Lesional melanocytes, in contrast to those in non-lesional and healthy skin, exhibited features of activation in the form of dilatation, prominent and long dendrites and intense labelling. The number of melanocytes was significantly increased in psoriatic lesions in comparison with non-lesional psoriatic and healthy skin as shown by counts of cells labelled with the MoAbs HMB45 (3-fold; p < 0.001), Melan A (1.6-fold; p < 0.01) and tyrosinase (1.5-fold; p < 0.01). In contrast, labelling with MITF revealed no significant difference (1.2-fold increase; p > 0.05). Likewise, no significant difference between non-lesional psoriatic and healthy skin control was found (p > 0.05). Furthermore, no positively labelled dermal cells were detected, apart from few only detected with Melan A. Conclusions: Epidermal melanocyte activity and numbers are increased in the epidermal compartment of psoriatic lesions providing an explanation for postinflammatory hyperpigmentation.

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Section: Discussionsupporting

confidence: 72%

“…Circulating mediators known to contribute to inflammation in psoriatic skin are likely to affect the neighbouring epidermal and dermal cells, such as melanocytes and papillary blood vessels [10]. …”

Section: Discussionmentioning

confidence: 99%

Increased Activity and Number of Epidermal Melanocytes in Lesional Psoriatic Skin

Abdel-Naser¹,

Liakou²,

Elewa³

et al. 2016

Dermatology

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“…For example, TNF was shown to induce the reversible dedifferentiation of melanoma cells [35] and an increased melanocyte number while inhibiting their differentiation-related pigmentation [68]. Similarly, TNF promotes neural stem (NSC) cell proliferation but inhibits their differentiation [69] and maintains osteosarcomas in their undifferentiated state [70].…”

Section: Discussionmentioning

confidence: 99%

Transient TNF regulates the self-renewing capacity of stem-like label-retaining cells in sphere and skin equivalent models of melanoma

Ostyn

Machhour

Bégard

et al. 2014

Cell Communication and Signaling

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Background: It is well established that inflammation promotes cancer, including melanoma, although the exact mechanisms involved are less known. In this study, we tested the hypothesis that inflammatory factors affect the cancer stem cell (CSC) compartment responsible for tumor development and relapse. Results: Using an inducible histone 2B-GFP fusion protein as a tracer of cell divisional history, we determined that tumor necrosis factor (TNF), which is a classical pro-inflammatory cytokine, enlarged the CSC pool of GFP-positive label-retaining cells (LRCs) in tumor-like melanospheres. Although these cells acquired melanoma stem cell markers, including ABCB5 and CD271, and self-renewal ability, they lost their capacity to differentiate, as evidenced by the diminished MelanA expression in melanosphere cells and the loss of pigmentation in a skin equivalent model of human melanoma. The undifferentiated cell phenotype could be reversed by LY294002, which is an inhibitor of the PI3K/AKT signaling pathway, and this reversal was accompanied by a significant reduction in CSC phenotypic markers and functional properties. Importantly, the changes induced by a transient exposure to TNF were long-lasting and observed for many generations after TNF withdrawal.

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“…Most of these acquired hypopigmentation disorders are associated with inflammation and a recent study shows that TNF-a and IL-17 synergistically suppress pigmentation-related signaling and melanin production partly via MC1R (Wang et al 2013). Hypopigmentation is also related with other syndromes (such as ataxia telangiectasia, Alezzandrini syndrome, Preus syndrome, Tietz syndrome, tuberous sclerosis, Rothmund-Thomson syndrome, and Werner syndrome) and infections (such as HIV, Hansen's disease, Malassezia furfur, and syphilis).…”

Section: Acquired Hypopigmentation Disordersmentioning

confidence: 99%

Melanocytes and Their Diseases

Yamaguchi

Hearing

2014

Cold Spring Harbor Perspectives in Medicine

168

118

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Human melanocytes are distributed not only in the epidermis and in hair follicles but also in mucosa, cochlea (ear), iris (eye), and mesencephalon (brain) among other tissues. Melanocytes, which are derived from the neural crest, are unique in that they produce eu-/pheomelanin pigments in unique membrane-bound organelles termed melanosomes, which can be divided into four stages depending on their degree of maturation. Pigmentation production is determined by three distinct elements: enzymes involved in melanin synthesis, proteins required for melanosome structure, and proteins required for their trafficking and distribution. Many genes are involved in regulating pigmentation at various levels, and mutations in many of them cause pigmentary disorders, which can be classified into three types: hyperpigmentation (including melasma), hypopigmentation (including oculocutaneous albinism [OCA]), and mixed hyper-/hypopigmentation (including dyschromatosis symmetrica hereditaria). We briefly review vitiligo as a representative of an acquired hypopigmentation disorder.

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IL-17 and TNF Synergistically Modulate Cytokine Expression while Suppressing Melanogenesis: Potential Relevance to Psoriasis

Cited by 167 publications

References 54 publications

Increased Activity and Number of Epidermal Melanocytes in Lesional Psoriatic Skin

Increased Activity and Number of Epidermal Melanocytes in Lesional Psoriatic Skin

Transient TNF regulates the self-renewing capacity of stem-like label-retaining cells in sphere and skin equivalent models of melanoma

Melanocytes and Their Diseases

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