Abstract

IB kinase (IKK), one of the two catalytic subunits of the IKK complex involved in nuclear factor B (NF-B) activation, also functions as a molecular switch that controls epidermal differentiation. This unexpected function requires IKK nuclear translocation but does not depend on its kinase activity, and is independent of NF-B signalling. Ikk^–/– mice present with a hyperproliferative and undifferentiated epidermis characterized by complete absence of a granular layer and stratum corneum. Ikk-deficient keratinocytes do not express terminal differentiation markers and continue to proliferate even when subjected to differentiation-inducing stimuli. This antiproliferative function of IKK is also important for the suppression of squamous cell carcinogenesis. The exact mechanisms by which nuclear IKK controls keratinocyte proliferation and differentiation remained mysterious for some time. Recent studies, however, have revealed that IKK is a major cofactor in a TGF–Smad2/3 signalling pathway that is Smad4 independent. This pathway controls cell cycle withdrawal during keratinocyte terminal differentiation. Although these are not the only functions of nuclear IKK, this multifunctional protein is a key regulator of keratinocyte and epidermal differentiation and a critical suppressor of skin cancer.

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