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First published online July 2, 2007
doi: 10.1242/10.1242/jcs.004481

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Conditional targeting of plectin in prenatal and adult mouse stratified epithelia causes keratinocyte fragility and lesional epidermal barrier defects

Reinhard Ackerl^1,*, Gernot Walko^1,*, Peter Fuchs¹, Irmgard Fischer¹, Matthias Schmuth² and Gerhard Wiche^1,

¹ Department of Molecular Cell Biology, Max F. Perutz Laboratories, University of Vienna, 1030 Vienna, Austria
² Department of Dermatology and Venereology, Medical University of Innsbruck, 6020 Innsbruck, Austria

Author for correspondence (e-mail: gerhard.wiche{at}univie.ac.at)

Accepted 15 May 2007

Plectin, a widespread intermediate filament-based cytolinker protein capable of interacting with a variety of cytoskeletal structures and plasma membrane-bound junctional complexes, serves essential functions in maintenance of cell and tissue cytoarchitecture. We have generated a mouse line bearing floxed plectin alleles and conditionally deleted plectin in stratified epithelia. This strategy enabled us to study the consequences of plectin deficiency in this particular type of tissues in the context of the whole organism without plectin loss affecting other tissues. Conditional knockout mice died early after birth, showing signs of starvation and growth retardation. Blistering was observed on their extremities and on the oral epithelium after initial nursing, impairing food uptake. Knockout epidermis was very fragile and showed focal epidermal barrier defects caused by the presence of small skin lesions. Stratification, proliferation and differentiation of knockout skin seemed unaffected by epidermis-restricted plectin deficiency. In an additionally generated mouse model, tamoxifen-induced Cre-ER^T-mediated recombination led to mice with a mosaic plectin deletion pattern in adult epidermis, combined with microblister formation and epidermal barrier defects. Our study explains the early lethality of plectin-deficient mice and provides a model to ablate plectin in adult animals which could be used for developing gene or pharmacological therapies.

Key words: Conditional gene targeting, Epidermolysis bullosa, Hemidesmosomes, Keratinocytes, Plectin, Transepidermal water loss

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