Radiation dermatitis in the hairless mouse model mimics human radiation dermatitis

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Radiation dermatitis in the hairless mouse model mimics human radiation dermatitis

Authors

Lawrence, J.; Seelig, D.; Demos-Davies, K.; Ferreira, C.; Ren, Y.; Wang, L.; Alam, S. K.; Yang, R.; Guedes, A.; Craig, A.; Hoeppner, L. H.

Abstract

Over half of all people diagnosed with cancer receive radiation therapy. Moderate to severe radiation dermatitis occurs in most human radiation patients, causing pain, aesthetic distress, and a negative impact on tumor control. No effective prevention or treatment for radiation dermatitis exists. The lack of well-characterized, clinically relevant animal models of human radiation dermatitis contributes to the absence of strategies to mitigate radiation dermatitis. Here, we establish and characterize a hairless SKH-1 mouse model of human radiation dermatitis by correlating temporal stages of clinical and pathological skin injury. We demonstrate that a single ionizing radiation treatment of 30 Gy using 6 MeV electrons induces severe clinical grade 3 peak toxicity at 12 days, defined by marked erythema, desquamation and partial ulceration, with resolution occurring by 25 days. Histopathology reveals that radiation-induced skin injury features temporally unique inflammatory changes. Upregulation of epidermal and dermal TGF-{beta}1 and COX-2 protein expression occurs at peak dermatitis, with sustained epidermal TGF-{beta}1 expression beyond resolution. Specific histopathological variables that remain substantially high at peak toxicity and early clinical resolution, including epidermal thickening, hyperkeratosis and dermal fibroplasia/fibrosis, serve as specific measurable parameters for in vivo interventional preclinical studies that seek to mitigate radiation-induced skin injury.

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