Literature DB >> 21654840

Caspase-14 is required for filaggrin degradation to natural moisturizing factors in the skin.

Esther Hoste1, Patrick Kemperman, Michael Devos, Geertrui Denecker, Sanja Kezic, Nico Yau, Barbara Gilbert, Saskia Lippens, Philippe De Groote, Ria Roelandt, Petra Van Damme, Kris Gevaert, Richard B Presland, Hidenari Takahara, Gerwin Puppels, Peter Caspers, Peter Vandenabeele, Wim Declercq.   

Abstract

Caspase-14 is a protease that is mainly expressed in suprabasal epidermal layers and activated during keratinocyte cornification. Caspase-14-deficient mice display reduced epidermal barrier function and increased sensitivity to UVB radiation. In these mice, profilaggrin, a protein with a pivotal role in skin barrier function, is processed correctly to its functional filaggrin (FLG) repeat unit, but proteolytic FLG fragments accumulate in the epidermis. In wild-type stratum corneum, FLG is degraded into free amino acids, some of which contribute to generation of the natural moisturizing factors (NMFs) that maintain epidermal hydration. We found that caspase-14 cleaves the FLG repeat unit and identified two caspase-14 cleavage sites. These results indicate that accumulation of FLG fragments in caspase-14(-/-) mice is due to a defect in the terminal FLG degradation pathway. Consequently, we show that the defective FLG degradation in caspase-14-deficient skin results in substantial reduction in the amount of NMFs, such as urocanic acid and pyrrolidone carboxylic acid. Taken together, we identified caspase-14 as a crucial protease in FLG catabolism.

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Year:  2011        PMID: 21654840     DOI: 10.1038/jid.2011.153

Source DB:  PubMed          Journal:  J Invest Dermatol        ISSN: 0022-202X            Impact factor:   8.551


  54 in total

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