Article ID Journal Published Year Pages File Type
1909098 Free Radical Biology and Medicine 2012 10 Pages PDF
Abstract

The naturally occurring skin hypoxia has emerged as a crucial host factor of the epidermal microenvironment. We wanted to systematically investigate how reduced oxygen availability of the epidermis modulates the response of keratinocytes and melanocytes to noxious ultraviolet B radiation (UVB). We report that the exposure of normal human keratinocytes (NHKs) or melanocytes (NHEMs) to mild hypoxia drastically impacts cell death responses following UVB irradiation. The hypoxic microenvironment favors survival and reduces apoptosis of UVB-irradiated NHEMs and their malignant counterparts (melanoma cells). In contrast, NHKs, but not the transformed keratinocytes, under hypoxic conditions display increased levels of reactive oxygen species (ROS) and are significantly sensitized to UVB-mediated apoptosis as compared to NHKs treated under normoxic conditions. Prolonged exposure of UVB-treated NHKs to hypoxia triggers a sustained and reactive oxygen species-dependent activation of the stress kinases p38MAPK and JNKs, which in turn, engage the activation of Noxa and Bim proapoptotic proteins. Combined silencing of Noxa and Bim significantly inhibits UVB-mediated apoptosis under hypoxic conditions, demonstrating that hypoxia results in an amplification of the intrinsic apoptotic pathway. Physiologically occurring skin hypoxia, by facilitating the specific removal of UVB-damaged keratinocytes, may represent a decisive host factor impeding important steps of the photocarcinogenesis process.

► Mild hypoxia(1,5%O2) sensitizes NHKs to UVB-induced apoptosis while it protects NHEMs; ► Mild hypoxia increases reactive oxygen species specifically in NHKs but not in NHEMs, ► UVB-induced activation of p38MAPK/JNK is more sustained under mild hypoxia in NHKs, ► JNK contributes to mitochondrial localization of Bim while Noxa is p38MAPK-dependent, ► Mild hypoxia-mediated sensitization to UVB-induced apoptosis is lost in cancer cells.

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