Photocarcinogenesis in human adult skin grafts

doi:10.1093/carcin/23.1.181

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Carcinogenesis, Vol. 23, No. 1, 181-187, January 2002
© 2002 Oxford University Press

CARCINOGENESIS

Photocarcinogenesis in human adult skin grafts

Carola Berking¹, Richelle Takemoto¹, Robert L. Binder², Scott M. Hartman², Dirk J. Ruiter¹^,4, Patricia M. Gallagher², Stuart R. Lessin³^,5 and Meenhard Herlyn¹^,6

¹ The Wistar Institute, 3601 Spruce Street, Philadelphia, PA 19104, USA,
² The Procter and Gamble Company, Miami Valley Laboratories, Cincinnati, OH 45253-8707, USA and
³ Department of Dermatology, University of Pennsylvania School of Medicine, 3400 Spruce Street, Philadelphia, PA 19104, USA

It has been demonstrated previously that the exposure to 7,12-dimethyl[a]benzanthracene(DMBA) and UVB radiation leads to the development of epidermalcysts, squamous cell carcinomas (SCC), melanocytic hyperplasiaand melanoma in human foreskins from newborns grafted to immunodeficientmice. Improved techniques in grafting full-thickness skin fromadults have enabled us to study photocarcinogenesis in humanskin from different body sites and from older donors. One hundredand fifty-five normal white skin specimens from the trunk andface of 53 adult individuals were grafted onto severe combinedimmunodeficient (SCID) and recombinase activating gene-1 (Rag-1)knockout mice and irradiated two to three times weekly with40 mJ/cm² UVB or solar-simulated UV (SSUV) over a period ofup to 10 months with or without one prior topical applicationof DMBA. Over an observation period of 2–22 months, histopathologicaland immunohistochemical analyses of 134 specimens revealed actinickeratoses in 30% of the DMBA- + UV-treated grafts, in 18% ofthe grafts exposed to SSUV only, and in 10% of the grafts exposedto UVB only. Actinic keratoses were absent in grafts treatedwith DMBA only. One SCC was found in an abdominal skin graft3 months after exposure to DMBA followed by UVB. Point mutationsin codon 61 of the human Ha-ras gene were detected in the SCC,five of six analyzed actinic keratoses and in non-lesional epidermisof DMBA- and UVB-treated grafts, indicating that DMBA as wellas UVB alone can induce these mutations in human skin. In contrastto the previous experience with neonatal foreskin grafts, melanocyticlesions were not found except for mild hyperplasia in few cases.The data suggest that melanocytes from young individuals aremore susceptible to the transforming effects of genotoxic agentsthan melanocytes from adults.

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