Abstract
Stimulation of epidermal growth factor (EGF) receptor by ligands such as transforming growth factor (TGF)α may be associated with cell proliferation or transformation in both nevocytes and keratinocytes. Previously, EGF receptors have been identified within a variety of pigmented lesions, suggesting a possible responsiveness to ligands such as TGFα. In the present study, we characterize the intralesional expression and distribution of immunoreactive TGFα protein by avidin-biotin immunoperoxidase localization in benign nevi, congenital nevi, dysplastic nevi, and malignant melanomas. In situ hybridization techniques with TGFα riboprobes confirmed the constitutive production of TGFα in all types of pigmented lesions. The localization of TGFα expression to nevocytes when coupled with the previous reports of expression in basal keratinocytes suggests the possibility of either an autocrine mechanism of action for TGFα or a paracrime interplay of TGFα between keratinocytes and nevocytes within melanocytic lesions. An increase in immunoreactive TGFα in nevocytes was noted in both benign and dysplastic nevi from dysplastic nevus patients, as compared to benign nevi from normal patients. Congenital nevi and malignant melanomas showed an intermediate and variable level of TGFα immunoreactivity. When coupled with previous studies the data suggest linkage of the TGFα/EGF receptor pathway in the evolution of melanocytic lesions. © 1994.
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Nanney, L. B., Coffey, R. J., & Ellis, D. L. (1994). Expression and distribution of transforming growth factor-α within melanocytic lesions. Journal of Investigative Dermatology, 103(5), 707–714. https://doi.org/10.1111/1523-1747.ep12398575
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