Interferon Gamma Induces Steroid Sulfatase Expression in Human Keratinocytes

Hattori, Kenji; Yamaguchi, Naohito; Umezawa, Kazuo; Tamura, Hiroomi

doi:10.1248/bpb.b12-00028

Cited by 4 publications

(3 citation statements)

References 38 publications

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“…It is located proximal to the portion of the gene that encodes enzyme expression, but the promoter sequence varies in a tissue-specific fashion [54]. While cytokines such as TNFα and IL-6 upregulate enzyme activity, IL-1β instead reportedly downregulates SSase activity [55], although IL-1β (as well as interferon γ) reportedly down-regulate SSase expression by inhibiting NFkB, while activating the glucocorticoidreceptor [55]. Finally, both retinoids and 1,25(OH) 2 vitamin D3 induce both SSase activity and expression [56].…”

Section: Molecular Biology and Regulation Of Ssasementioning

confidence: 99%

Role of cholesterol sulfate in epidermal structure and function: Lessons from X-linked ichthyosis

Elias

Williams

Choi

et al. 2014

Biochimica et Biophysica Acta (BBA) - Molecular and Cell Biolog

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X-linked ichthyosis is a relatively common syndromic form of ichthyosis most often due to deletions in the gene encoding the microsomal enzyme, steroid sulfatase, located on the short area of the X chromosome. Syndromic features are mild or unapparent unless contiguous genes are affected. In normal epidermis, cholesterol sulfate is generated by cholesterol sulfotransferase (SULT2B1b), but desulfated in the outer epidermis, together forming a ‘cholesterol sulfate cycle’ that potently regulates epidermal differentiation, barrier function and desquamation. In XLI, cholesterol sulfate levels my exceed 10% of total lipid mass (≈1% of total weight). Multiple cellular and biochemical processes contribute to the pathogenesis of the barrier abnormality and scaling phenotype in XLI. This article is part of a Special Issue entitled The Important Role of Lipids in the Epidermis and their Role in the Formation and Maintenance of the Cutaneous Barrier. Guest Editors: Kenneth R. Feingold and Peter Elias.

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Section: Molecular Biology and Regulation Of Ssasementioning

confidence: 99%

Role of cholesterol sulfate in epidermal structure and function: Lessons from X-linked ichthyosis

Elias

Williams

Choi

et al. 2014

Biochimica et Biophysica Acta (BBA) - Molecular and Cell Biolog

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“…These properties, as well as the relative long life of a keratinocyte compared with other inflammatory cells such as the neutrophil or eosinophil, make the keratinocyte a potentially important player in the amplification and persistence of inflammatory and immune responses in AD. Several groups have reported that GC exhibits anti-inflammatory eff ;ects in keratinocytes treated with TNFα [32,33], hapten [34], UV-B irradiation [35], IFNg [36], and induces keratinocyte terminal differentiation [37]. However, few investigations have been conducted to determine whether SEB contributes to the resistance to GCs through keratinocytes.…”

Section: Discussionmentioning

confidence: 99%

Glucocorticoid insensitivity by staphylococcal enterotoxin B in keratinocytes of allergic dermatitis is associated with impaired nuclear translocation of the Glucocorticoid Receptor α

Huang

Ran

Wang

et al. 2018

Journal of Dermatological Science

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Background: staphylococcal enterotoxin plays an important role in patients with glucocorticoid (GC)resistant atopic dermatitis (AD), but the exact mechanism is not fully understood. Objective: The aim of this study was to investigate the mechanisms underlying the ability of staphylococcal enterotoxin B (SEB) to induce steroid insensitivity through impaired nuclear translocation of GRα in keratinocytes. Methods: The steroid-resistant AD induced by SEB was assessed by analyzing dermatitis score, dermal thickness, scratching behavior, infiltrating cells/HPF, levels of SEB-specific IgE and IgG2a antibody. In addition, dexamethasone (DEX)-induced GRα nuclear translocation and keratinocyte-derived cytokines and chemokines were analyzed in the lesional keratinocytes of AD and in HaCaT cells. Furthermore, the expressions of immunophilins FKBP51, FKBP52 and HSP90 responsive to GC in HaCaT cells were determined in the presence of SEB. Results: SEB dose-dependently diminished the inhibitory effect of DEX on dermatitis score, dermal thickness, scratching behavior, infiltrating cells/HPF, keratinocyte-derived cytokines and chemokines such as RANTES, MCP-1, TSLP and GM-CSF. In vivo and in vitro data showed that in the presence of DEX, SEB dose-dependently caused a marked decrease of GRα nuclear translocation in lesional keratinocytes of AD and in HaCaT cells. Importantly, in the presence of DEX, SEB increased the expression of FKBP51 and the product of keratinocyte-derived cytokines and chemokines in HaCaT cells. Conclusion: These results demonstrate that GC insensitivity by SEB in keratinocytes of AD is associated with impaired nuclear translocation of the GRα. Increased DEX-induced FKBP51 by SEB may contribute to accumulation of the GRα in cytoplasm of keratinocytes.

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“…G6PD E:S then acts as a sink for DHEA, stimulating OATP2B1, the transport protein responsible for importing DHEAS into the cell. Inactivation of TP53 also hyperactivates NFKB ( Weisz et al 2007 , Kawauchi et al 2008 , Cooks et al 2013 ), triggering steroid sulfatase ( Hattori et al 2012 , Dias & Selcer 2016 ), which potentiates the importation of DHEAS and its intracellular activation to DHEA. OATP2B1 is also stimulated by the intracellular presence of de-sulfated androgens ( Grube et al 2006 ), such that as the intracellular concentration of DHEA rises, DHEAS is imported into the p53-affected cell at an ever-accelerating rate.…”

Section: Introductionmentioning

confidence: 99%

Detection of a novel, primate-specific ‘kill switch’ tumor suppression mechanism that may fundamentally control cancer risk in humans: an unexpected twist in the basic biology of TP53

Nyce¹

2018

Endocrine-Related Cancer

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The activation of TP53 is well known to exert tumor suppressive effects. We have detected a primate-specific adrenal androgen-mediated tumor suppression system in which circulating DHEAS is converted to DHEA specifically in cells in which TP53 has been inactivated. DHEA is an uncompetitive inhibitor of glucose-6-phosphate dehydrogenase (G6PD), an enzyme indispensable for maintaining reactive oxygen species within limits survivable by the cell. Uncompetitive inhibition is otherwise unknown in natural systems because it becomes irreversible in the presence of high concentrations of substrate and inhibitor. In addition to primate-specific circulating DHEAS, a unique, primate-specific sequence motif that disables an activating regulatory site in the glucose-6-phosphatase (G6PC) promoter was also required to enable function of this previously unrecognized tumor suppression system. In human somatic cells, loss of TP53 thus triggers activation of DHEAS transport proteins and steroid sulfatase, which converts circulating DHEAS into intracellular DHEA, and hexokinase which increases glucose-6-phosphate substrate concentration. The triggering of these enzymes in the TP53-affected cell combines with the primate-specific G6PC promoter sequence motif that enables G6P substrate accumulation, driving uncompetitive inhibition of G6PD to irreversibility and ROS-mediated cell death. By this catastrophic ‘kill switch’ mechanism, TP53 mutations are effectively prevented from initiating tumorigenesis in the somatic cells of humans, the primate with the highest peak levels of circulating DHEAS. TP53 mutations in human tumors therefore represent fossils of kill switch failure resulting from an age-related decline in circulating DHEAS, a potentially reversible artifact of hominid evolution.

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Interferon Gamma Induces Steroid Sulfatase Expression in Human Keratinocytes

Cited by 4 publications

References 38 publications

Role of cholesterol sulfate in epidermal structure and function: Lessons from X-linked ichthyosis

Role of cholesterol sulfate in epidermal structure and function: Lessons from X-linked ichthyosis

Glucocorticoid insensitivity by staphylococcal enterotoxin B in keratinocytes of allergic dermatitis is associated with impaired nuclear translocation of the Glucocorticoid Receptor α

Detection of a novel, primate-specific ‘kill switch’ tumor suppression mechanism that may fundamentally control cancer risk in humans: an unexpected twist in the basic biology of TP53

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