Abstract
Nonmelanoma skin cancers (NMSC) are the most common human malignancies. IKKα is an essential protein for skin development and is also involved in the genesis and progression of NMSC, through mechanisms not fully understood. While different studies show that IKKα protects against skin cancer, others indicate that it promotes NMSC. To resolve this controversy we have generated two models of transgenic mice expressing the IKKα protein in the nucleus (N-IKKα mice) or the cytoplasm (C-IKKα mice) of keratinocytes. Chemical skin carcinogenesis experiments show that tumors developed by both types of transgenic mice exhibit histological and molecular characteristics that make them more prone to progression and invasion than those developed by Control mice. However, the mechanisms through which IKKα promotes skin tumors are different depending on its subcellular localization; while IKKα of cytoplasmic localization increases EGFR, MMP-9 and VEGF-A activities in tumors, nuclear IKKα causes tumor progression through regulation of c-Myc, Maspin and Integrin-α6 expression. Additionally, we have found that N-IKKα skin tumors mimic the characteristics associated to aggressive human skin tumors with high risk to metastasize. Our results show that IKKα has different non-overlapping roles in the nucleus or cytoplasm of keratinocytes, and provide new targets for intervention in human NMSC progression.
Highlights
The epidermis is a stratified squamous epithelium composed mainly of keratinocytes
IKKa is an essential protein for skin development and is involved in the genesis and progression of Nonmelanoma skin cancers (NMSC), through mechanisms not fully understood
While different studies show that IKKa protects against skin cancer, others indicate that it promotes NMSC
Summary
The epidermis is a stratified squamous epithelium composed mainly of keratinocytes. Basal keratinocytes proliferate and give rise to differentiated cells, which, upon full maturation, generate the squamous cornified cell layer. Alterations in the normal physiology of the skin lead to numerous pathologies such as cancer. Keratinocyte derived non-melanoma skin cancer (NMSC) comprises two different entities: basal cell carcinoma (BCC) and cutaneous squamous cell carcinoma (SCC). NMSC is the most common form of cancer in the Caucasian population, representing 90% of skin cancers [1]. 5% of SCCs metastasize; due to its high incidence, the mortality concomitant to aggressive cutaneous SCCs is reaching important numbers [2, 3]
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