Abstract

Melanins are an important factor determining the vulnerability of mammalian skin to UV radiation and thus to UV-induced skin cancers. Transgenic mice overexpressing hepatocyte growth factor/scatter factor (HGF/SF) have extra-follicular dermal melanocytes, notably in the papillary upper dermis, and are susceptible to UV-induced melanoma. Pigmented HGF/SF neonatal mice are more susceptible than albino HGF/SF animals to UVA -induced melanoma, indicating an involvement of melanin in melanoma formation. This raises the question of the effect of transgenic HGF/SF on melanization. We developed a methodology to accurately quantitate both the production of melanin and the efficiency of melanogenesis in normal, and HGF/SF transgenic mice in vivo. Skin and hair shafts of 5 day old and adult (3 week old) C57BL/6-HGF/SF and corresponding C57BL/6 wild type mice were investigated by electron paramagnetic resonance spectroscopy (EPR) to quantitate melanin, by transmission electron microscopy (TEM) for the presence of melanosomes, and by standard histology and by Western blotting and zymography to determine the expression and activity of melanogenesis-related proteins. Eumelanin but no phaeomelanin was detected in transgenic C57BL/6-HGF and C57BL/6 wild type mice. Transgenic HGF/SF overexpression did not change the type of melanin produced in the skin or hair, did not affect the terminal content of melanin production in standard samples of hair and did not influence hair cycle/morphogenesis-related changes in skin thickness. No melanocytes were found in the epidermis and no melanosomes were found in epidermal keratinocytes. HGF/SF transgenic mice thus lack the epidermal melanin UV-protection found in constitutively dark human skin. We conclude that melanocytes in the HGF/SF transgenic mouse, particularly in the papillary dermis, are vulnerable to UVA which interacts with eumelanin but not phaeomelanin to induce melanoma.

Highlights

  • In contrast to humans, in the mouse trunk skin melanocytes are localized exclusively in the hair follicles [1,2,3]

  • Among animal models of melanoma, the hepatocyte growth factor/scatter factor (HGF/SF) transgenic mouse is of particular interest, as it possesses additional copies of HGF/SF gene that lead to extrafollicular localization of melanocytes [4,5]

  • These extrafollicular melanocytes are prone to UV-induced malignant transformation when the neonatal HGF/SF transgenic mouse is exposed to UV radiation [5,6]

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Summary

Introduction

In the mouse trunk skin melanocytes are localized exclusively in the hair follicles [1,2,3]. The skin of wild-type C57BL/6 and transgenic C57BL/6 HGF/SF mice contains hair follicles in this stage of morphogenesis, which can be further confirmed by a higher thickness of skin, as compared to the telogen skin.

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