The Essential Role of p53 in Hyperpigmentation of the Skin via Regulation of Paracrine Melanogenic Cytokine Receptor Signaling

Murase, Daiki; Hachiya, Akira; Amano, Y.; Ohuchi, Atsushi; Kitahara, Takashi; Takema, Yoshinori

doi:10.1074/jbc.m805570200

Cited by 90 publications

(83 citation statements)

References 76 publications

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“…Additionally, it was also confirmed that cell viability was not changed by the application of this extract to HSSs (data not shown). This inhibitory effect on melanin synthesis in HSSs was shown to be equal to that of pifithrin-α, the inhibitor of SCF-inducing phosphorylation of MAPK, as we previously reported [8]. Additionally, our clinical study revealed that application of this extract significantly depresses UVB-induced pigmentation even at 1 week after irradiation in a dose-dependent manner (Fig.…”

Section: Resultssupporting

confidence: 84%

The inhibitory effect of a Platycodon root extract on ultraviolet B-induced pigmentation due to a decrease in Kit expression

et al. 2014

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The signaling of stem cell factor (SCF) through its receptor Kit is known to play an important role in regulating cutaneous melanogenesis. In the course of UVB-induced pigmentation, the expression of membrane-bound SCF by epidermal keratinocytes is upregulated at an early phase and subsequently activates neighboring melanocytes via their Kit receptors. In order to identify effective skin-lightening materials, we screened botanical extracts to determine their abilities to diminish Kit expression in melanocytes. A Platycodon root extract was consequently found to have a remarkable inhibitory activity on Kit expression. When the extract was applied to three-dimensional human skin substitutes in vitro and to human skin in vivo after UVB irradiation, their pigmentation was significantly reduced, confirming the substantial contribution of the suppression of SCF/Kit signaling to preventing or inhibiting melanin synthesis. These data demonstrate that a Platycodon root extract is a promising material for a skin-lightening product to improve pigmentation-related diseases.

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Section: Resultssupporting

confidence: 84%

The inhibitory effect of a Platycodon root extract on ultraviolet B-induced pigmentation due to a decrease in Kit expression

et al. 2014

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“…The transcriptional activation of KITLG upon p53 activation has been clearly demonstrated in multiple studies utilizing different cell types, different p53-activating stimuli and different measurement techniques (McGowan et al, 2008; Murase et al, 2009; Smeenk et al, 2011; Terzian et al, 2010; Wei et al, 2006). Consistent with this, we observed significant p53 binding to KITLG in the region that harbors the KITLG p53-RE SNP, in 10 out of 11 different cell line and treatment combinations (Figure 3A).…”

Section: Resultsmentioning

confidence: 99%

“…Specifically, KITLG and its receptor C-KIT are a part of a pathway that is known to be central in regulating proliferation, survival and migration of primordial germ cells, melanoblasts and hematopoietic stem cells (Lennartsson and Rönnstrand, 2012). In the pigmentary system, ultraviolet radiation induces p53-Kitlg signaling in keratinocytes, which in turn affects melanocytes that express the c-Kit receptor in order to mount a cutaneous UV response such as tanning (Murase et al, 2009). Interestingly, when we compared this response in mice either wild-type (WT) or null for p53 ( p53 null ), we noted dramatic differences.…”

Section: Resultsmentioning

confidence: 99%

A Polymorphic p53 Response Element in KIT Ligand Influences Cancer Risk and Has Undergone Natural Selection

Zerón-Medina

Wang

Repapi

et al. 2013

Cell

112

101

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SUMMARY The ability of p53 to regulate transcription is crucial for tumor suppression and implies that inherited polymorphisms in functional p53-binding sites could influence cancer. Here, we identify a polymorphic p53 responsive element and demonstrate its influence on cancer risk using genome-wide data sets of cancer susceptibility loci, genetic variation, p53 occupancy, and p53-binding sites. We uncover a single-nucleotide polymorphism (SNP) in a functional p53-binding site and establish its influence on the ability of p53 to bind to and regulate transcription of the KITLG gene. The SNP resides in KITLG and associates with one of the largest risks identified among cancer genome-wide association studies. We establish that the SNP has undergone positive selection throughout evolution, signifying a selective benefit, but go on to show that similar SNPs are rare in the genome due to negative selection, indicating that polymorphisms in p53-binding sites are primarily detrimental to humans.

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“…Our results unraveled a mechanism involving a-MSH and p53 in the adaptive response of melanocytes to UVR. Others have shown that p53 increases the expression of the melanogenic enzymes tyrosinase and tyrosine-related protein 1 (TYRP-1), suggesting its role in regulating melanogenesis (20,21). In mouse skin, p53 stimulates the expression of proopiomelanocortin (POMC), the precursor of a-MSH and adrenocorticotropic hormone (ACTH; refs.…”

Section: Introductionmentioning

confidence: 99%

Alpha-Melanocyte–Stimulating Hormone Suppresses Oxidative Stress through a p53-Mediated Signaling Pathway in Human Melanocytes

Kadekaro

Chen

Yang

et al. 2012

Molecular Cancer Research

107

133

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Epidermal melanocytes are skin cells specialized in melanin production. Activation of the melanocortin 1 receptor (MC1R) on melanocytes by a-melanocyte-stimulating hormone (a-MSH) induces synthesis of the brown/black pigment eumelanin that confers photoprotection from solar UV radiation (UVR). Contrary to keratinocytes, melanocytes are slow proliferating cells that persist in the skin for decades, in an environment with high levels of UVR-induced reactive oxygen species (ROS). We previously reported that in addition to its role in pigmentation, a-MSH also reduces oxidative stress and enhances the repair of DNA photoproducts in melanocytes, independent of melanin synthesis. Given the significance of ROS in carcinogenesis, here we investigated the mechanisms by which a-MSH exerts antioxidant effects in melanocytes. We show that activation of the MC1R by a-MSH contributes to phosphorylation of p53 on serine 15, a known requirement for stabilization and activation of p53, a major sensor of DNA damage. This effect is mediated by the cAMP/PKA pathway and by the activation of phosphoinositide 3-kinase (PI3K) ATR and DNA protein kinase (DNA-PK). a-MSH increases the levels of 8-oxoguanine DNA glycosylase (OGG1) and apurinic apyrimidinic endonuclease 1 (APE-1/Ref-1), enzymes essential for base excision repair. Nutlin-3, an HDM2 inhibitor, mimicked the effects of a-MSH resulting in reduced phosphorylation of H2AX (g-H2AX), a marker of DNA damage. Conversely, the p53 inhibitor pifithrin-a or silencing of p53 abolished the effects of a-MSH and augmented oxidative stress. These results show that p53 is an important target of the downstream MC1R signaling that reduces oxidative stress and possibly malignant transformation of melanocytes. Mol Cancer Res; 10(6); 778-86. Ó2012 AACR. IntroductionThe melanocortin 1 receptor (MC1R) is best known for its role in stimulating eumelanin synthesis in melanocytes (MC). In the skin, presence of eumelanin is considered the major photoprotective factor against UV radiation (UVR)-induced DNA damage and carcinogenesis. Eumelanin creates not only a physical barrier against the deep penetration of UVR into the epidermal and dermal layers (1) but also reduces oxidative stress by scavenging free radicals (2-4).

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The Essential Role of p53 in Hyperpigmentation of the Skin via Regulation of Paracrine Melanogenic Cytokine Receptor Signaling

Cited by 90 publications

References 76 publications

The inhibitory effect of a Platycodon root extract on ultraviolet B-induced pigmentation due to a decrease in Kit expression

The inhibitory effect of a Platycodon root extract on ultraviolet B-induced pigmentation due to a decrease in Kit expression

A Polymorphic p53 Response Element in KIT Ligand Influences Cancer Risk and Has Undergone Natural Selection

Alpha-Melanocyte–Stimulating Hormone Suppresses Oxidative Stress through a p53-Mediated Signaling Pathway in Human Melanocytes

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