Expression of the tumor necrosis factor gene by dermal fibroblasts in response to ultraviolet irradiation or lipopolysaccharide

S. De Kossodo; Ponciano D Cruz; I. Dougherty; P. Thompson; M. Silva-Valdez; Bruce A Beutler

doi:10.1111/1523-1747.ep12665361

Expression of the tumor necrosis factor gene by dermal fibroblasts in response to ultraviolet irradiation or lipopolysaccharide

S. De Kossodo, Ponciano D Cruz, I. Dougherty, P. Thompson, M. Silva-Valdez, Bruce A Beutler

Research output: Contribution to journal › Article › peer-review

40 Scopus citations

Abstract

To examine the effects of different wavelengths of ultraviolet (UV) radiation on tumor necrosis factor (TNF) production, we took advantage of mice carrying a chloramphenicol acetyl transferase (CAT) reporter transgene bearing the entire TNF promoter and 3'-untranslated region. Aside from constitutive expression in the thymus, CAT activity was detected only in locally UVB- or UVC-irradiated skin. After UVB irradiation, markedly greater amounts of CAT activity were traced to the dermis rather than the epidermis; by contrast, almost all CAT activity was localized to the epidermis after UVC irradiation. Fibroblasts have not been shown previously to express the TNF gene, i.e., the TNF gene is highly methylated and inaccessible to exogenous modulation in 3T3 fibroblasts. However, the present report reveals that cultured dermal fibroblasts are capable of producing both CAT and TNF in response to treatment in vitro with either UVB irradiation, UVC irradiation, or lipopolysaccharide. These findings indicate that dermal fibroblasts may serve not only as a target for but also as a source of TNF.

Original language	English (US)
Pages (from-to)	318-322
Number of pages	5
Journal	Journal of Investigative Dermatology
Volume	104
Issue number	3
DOIs	https://doi.org/10.1111/1523-1747.ep12665361
State	Published - 1995

ASJC Scopus subject areas

Biochemistry
Molecular Biology
Dermatology
Cell Biology

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title = "Expression of the tumor necrosis factor gene by dermal fibroblasts in response to ultraviolet irradiation or lipopolysaccharide",

abstract = "To examine the effects of different wavelengths of ultraviolet (UV) radiation on tumor necrosis factor (TNF) production, we took advantage of mice carrying a chloramphenicol acetyl transferase (CAT) reporter transgene bearing the entire TNF promoter and 3'-untranslated region. Aside from constitutive expression in the thymus, CAT activity was detected only in locally UVB- or UVC-irradiated skin. After UVB irradiation, markedly greater amounts of CAT activity were traced to the dermis rather than the epidermis; by contrast, almost all CAT activity was localized to the epidermis after UVC irradiation. Fibroblasts have not been shown previously to express the TNF gene, i.e., the TNF gene is highly methylated and inaccessible to exogenous modulation in 3T3 fibroblasts. However, the present report reveals that cultured dermal fibroblasts are capable of producing both CAT and TNF in response to treatment in vitro with either UVB irradiation, UVC irradiation, or lipopolysaccharide. These findings indicate that dermal fibroblasts may serve not only as a target for but also as a source of TNF.",

author = "{De Kossodo}, S. and Cruz, {Ponciano D} and I. Dougherty and P. Thompson and M. Silva-Valdez and Beutler, {Bruce A}",

note = "Funding Information: S. de K. is supported by a grant from the Fonds National pour la Recherche Suisse (Switzerland). These studies used the resources of the University of Texas Southwestern Medical Center Skin Disease Research Core Center (NIH-AR-4-1940) and the University of Texas Southwestern. Diabetes Center (5-POIDK42582). We wish to thank Ms. Lesa Ellinger for expert technical assistance.",

year = "1995",

doi = "10.1111/1523-1747.ep12665361",

language = "English (US)",

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AU - De Kossodo, S.

AU - Cruz, Ponciano D

AU - Dougherty, I.

AU - Thompson, P.

AU - Silva-Valdez, M.

AU - Beutler, Bruce A

N1 - Funding Information: S. de K. is supported by a grant from the Fonds National pour la Recherche Suisse (Switzerland). These studies used the resources of the University of Texas Southwestern Medical Center Skin Disease Research Core Center (NIH-AR-4-1940) and the University of Texas Southwestern. Diabetes Center (5-POIDK42582). We wish to thank Ms. Lesa Ellinger for expert technical assistance.

PY - 1995

Y1 - 1995

N2 - To examine the effects of different wavelengths of ultraviolet (UV) radiation on tumor necrosis factor (TNF) production, we took advantage of mice carrying a chloramphenicol acetyl transferase (CAT) reporter transgene bearing the entire TNF promoter and 3'-untranslated region. Aside from constitutive expression in the thymus, CAT activity was detected only in locally UVB- or UVC-irradiated skin. After UVB irradiation, markedly greater amounts of CAT activity were traced to the dermis rather than the epidermis; by contrast, almost all CAT activity was localized to the epidermis after UVC irradiation. Fibroblasts have not been shown previously to express the TNF gene, i.e., the TNF gene is highly methylated and inaccessible to exogenous modulation in 3T3 fibroblasts. However, the present report reveals that cultured dermal fibroblasts are capable of producing both CAT and TNF in response to treatment in vitro with either UVB irradiation, UVC irradiation, or lipopolysaccharide. These findings indicate that dermal fibroblasts may serve not only as a target for but also as a source of TNF.

AB - To examine the effects of different wavelengths of ultraviolet (UV) radiation on tumor necrosis factor (TNF) production, we took advantage of mice carrying a chloramphenicol acetyl transferase (CAT) reporter transgene bearing the entire TNF promoter and 3'-untranslated region. Aside from constitutive expression in the thymus, CAT activity was detected only in locally UVB- or UVC-irradiated skin. After UVB irradiation, markedly greater amounts of CAT activity were traced to the dermis rather than the epidermis; by contrast, almost all CAT activity was localized to the epidermis after UVC irradiation. Fibroblasts have not been shown previously to express the TNF gene, i.e., the TNF gene is highly methylated and inaccessible to exogenous modulation in 3T3 fibroblasts. However, the present report reveals that cultured dermal fibroblasts are capable of producing both CAT and TNF in response to treatment in vitro with either UVB irradiation, UVC irradiation, or lipopolysaccharide. These findings indicate that dermal fibroblasts may serve not only as a target for but also as a source of TNF.

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Expression of the tumor necrosis factor gene by dermal fibroblasts in response to ultraviolet irradiation or lipopolysaccharide

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