Langerhans Cells Facilitate Epithelial DNA Damage and Squamous Cell Carcinoma

Modi, Badri; Neustadter, Jason; Binda, Elisa; Lewis, Julia M.; Filler, Renata; Roberts, Scott; Kwong, Bernice Y.; Reddy, Swapna; Overton, John D.; Galan, Anjela; Tigelaar, Robert E.; Cai, Lining; Fu, Peter P.; Shlomchik, Mark J.; Kaplan, Daniel H.; Hayday, Adrian; Girardi, Michael

doi:10.1126/science.1211600

Cited by 132 publications

(122 citation statements)

References 33 publications

(43 reference statements)

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“…This finding is in line with previous reports that demonstrate that activin A induces the differentiation of Langerhans cells from circulating and skinresident precursor cells , and that transgenic mice overexpressing follistatin in keratinocytes have a strongly reduced number of Langerhans cells (Stoitzner et al, 2005). As these cells promote skin carcinogenesis that is induced by DMBA and TPA, by metabolizing DMBA into a more mutagenic compound and thereby increasing DNA damage (Modi et al, 2012), their accumulation in the epidermis of activin-overexpressing mice could further contribute to the pro-tumorigenic phenotype.…”

Section: A Functional Role Of Activin In Skin Cancersupporting

confidence: 92%

The bright and the dark sides of activin in wound healing and cancer

Antsiferova

Werner

2012

Journal of Cell Science

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SummaryActivin was initially described as a protein that stimulates release of follicle stimulating hormone from the pituitary, and it is well known for its important roles in different reproductive functions. In recent years, this multifunctional factor has attracted the attention of researchers in other fields, as new functions of activin in angiogenesis, inflammation, immunity, fibrosis and cancer have been discovered. Studies from our laboratory have identified activin as a crucial regulator of wound healing and skin carcinogenesis. On the one hand, it strongly accelerates the healing process of skin wounds but, on the other hand, it enhances scar formation and the susceptibility to skin tumorigenesis. Finally, results from several laboratories have revealed that activin enhances tumour formation and/ or progression in some other organs, in particular through its effect on the tumour microenvironment, and that it also promotes cancerinduced bone disruption and muscle wasting. These findings provide the basis for the use of activin or its downstream targets for the improvement of impaired wound healing, and of activin antagonists for the prevention and treatment of fibrosis and of malignant tumours that overexpress activin. Here, we summarize the previously described roles of activin in wound healing and scar formation and discuss functional studies that revealed different functions of activin in the pathogenesis of cancer. The relevance of these findings for clinical applications will be highlighted.

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Section: A Functional Role Of Activin In Skin Cancersupporting

confidence: 92%

The bright and the dark sides of activin in wound healing and cancer

Antsiferova

Werner

2012

Journal of Cell Science

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“…When LCs are absent, metabolic activation of chemical carcinogens (e.g., DMBA) that induce tumor initiation was impaired (37). Moreover, although DETC-depleted mice manifest higher susceptibility to DMBA/TPA tumorigenesis by themselves (27), combined depletion of DETCs and LCs retained the robust LCdeficient tumor-resistant phenotype (47).…”

Section: Discussionmentioning

confidence: 99%

“…These results suggested that although Runx3-expressing DCs were essential, they were not sufficient to furnish Runx3-null full tumor resistance. Modi and colleagues (37) showed that absence of epidermal LCs confers complete resistance to DMBA/TPAinduced tumorigenesis. Therefore, we evaluated the involvement of LCs in Runx3-null tumor resistance by immunostaining of epidermal sheets from na€ ve DC Runx3À/À ear skin and flow cytometry (Fig.…”

Section: Runx3 Ablation Decreases Tpa-induced Epidermal Proliferationmentioning

confidence: 99%

Carcinogen-Induced Skin Tumor Development Requires Leukocytic Expression of the Transcription Factor Runx3

Bauer

Hantisteanu

Lotem

et al. 2014

Cancer Prevention Research

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Carcinogen-induced skin tumorigenesis depends heavily on proinflammatory tumor-promoting processes. Here, we show that leukocytic Runx3 expression is central to the two-stage DMBA/TPA-induced skin tumorigenesis. Runx3-null mice were highly resistant to this process and concomitant ablation of Runx3 in dendritic and T cells fully recapitulated this resistance. Mechanistically, this resistance was associated with a shift in the skin cytokine milieu toward a tumor nonpermissive microenvironment. Specifically, leukocytic Runx3 loss substantially increased the antitumorigenic cytokine thymic stromal lymphopoietin (TSLP) and profoundly decreased two protumorigenic cytokines, interleukin-17a and osteopontin. Therefore, inflammation-mediated tumor promotion requires leukocytic Runx3 expression, as its loss creates a unique cytokine composition that polarizes the tumor microenvironment to a potent antitumorigenic state. Cancer Prev Res; 7(9); 913-26. Ó2014 AACR.

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“…It is important to recognise that the presence of foreign compounds in the skin can lead to localised effects e.g. Langerhan cells may increase the likelihood of carcinogenesis due to the metabolisation of dermally absorbed PAH (Modi et al, 2012); similar observations of the genotoxicity of benzo[a]pyrene have also been made for metablolisation by kerotinocytes (e.g. Brinkmann et al 2013).…”

Section: Dermal Absorptionmentioning

confidence: 93%

A review of the current state of the art of physiologically-based tests for measuring human dermal in vitro bioavailability of polycyclic aromatic hydrocarbons (PAH) in soil

Beriro

Cave

Wragg

et al. 2016

Journal of Hazardous Materials

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Polycyclic Aromatic Hydrocarbons are classed as Persistent Organic Pollutants, a large group of compounds that share similar characteristics. They are lipophilic, resistant to degradation in the environment and harmful to human and environmental health. Soil has been identified as the primary reservoir for Polycyclic Aromatic Hydrocarbons in the United Kingdom. This study reviews the literature associated with, or is relevant to, the measurement and modelling of dermal absorption of Polycyclic Aromatic Hydrocarbons from soils. The literature illustrates the use of in vivo, in vitro and in silico methods from a wide variety of scientific disciplines including occupational and environmental exposure, medical, pharmaceutical and cosmetic research and associated mathematical modelling. The review identifies a number of practical shortcomings which must be addressed if they are to be applied to high throughput laboratory analysis of contaminated soils for human health risk assessment.

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Langerhans Cells Facilitate Epithelial DNA Damage and Squamous Cell Carcinoma

Cited by 132 publications

References 33 publications

The bright and the dark sides of activin in wound healing and cancer

The bright and the dark sides of activin in wound healing and cancer

Carcinogen-Induced Skin Tumor Development Requires Leukocytic Expression of the Transcription Factor Runx3

A review of the current state of the art of physiologically-based tests for measuring human dermal in vitro bioavailability of polycyclic aromatic hydrocarbons (PAH) in soil

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