Abstract

With the discovery that mutations in fourteen different keratin genes can cause eight distinct epithelial fragility disorders, comes the realization that the keratin filament cytoskeleton is crucial to the structural integrity of epithelial tissues exposed to mechanical stress. The identification of mutations causing these disorders has improved our understanding of keratin structure and function, particularly with regard to the highly conserved regions of the central rod domain. However, two central questions in keratin biology still remain. The first question concerns the regulation of individual keratin genes, since the tightly regulated synthesis of these proteins is a pre-requisite for the normal development of the epidermis. To address this question, we will focus on two keratin genes that are expressed at different stages of epidermal development, keratins K14 and K1. K14 is one of the first genes expressed in the surface ectoderm after commitment to stratification. We have recently demonstrated that the transcription factor p63 is the molecular switch for initiation of the epidermal stratification program. This discovery has provided us with novel insights into the molecular mechanisms responsible for the induction of K14 expression during epidermal development. We have also discovered that a switch in p63 isoform expression is required to allow basal keratinocytes to withdraw from the cell cycle and commit to terminal differentiation. Since K1 is one of the first genes expressed in the epidermis after keratinocytes have committed to terminal differentiation, we will exploit this discovery to gain insight into the molecular mechanisms regulating K1 expression during maturation of the epidermis. The second question concerns the roles of the keratin N- and C-terminal end domains. These domains are distinctive for each keratin protein but are remarkably well conserved across species and presumably have functional significance. In vitro studies have suggested that these domains interact with desmosomes and/or the cell envelope, however very little is known regarding cell type-specific functions of these domains in vivo. Two transgenic approaches are proposed to address this question. Finally, epidermolytic hyperkeratosis (EHK), the dominantly inherited skin disorder caused by mutations in the post-mitotically expressed keratins, K1 or K10, presents a challenge for gene therapy. During the last funding period of this grant, we generated a mouse model that mimics EHK at both the genetic and phenotypic level. This mouse model has provided new insights into the molecular and cellular basis of EHK and we propose to use this model to test new gene therapy strategies. The results of this research will yield valuable information that can lead to novel therapeutic approaches for other diseases affecting post-mitotic keratinocytes.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
7R01AR052263-20
Application #
7480146
Study Section
Special Emphasis Panel (ZRG1-ACTS (01))
Program Officer
Baker, Carl
Project Start
1989-04-01
Project End
2009-05-31
Budget Start
2007-06-02
Budget End
2008-05-31
Support Year
20
Fiscal Year
2007
Total Cost
$283,664
Indirect Cost

  Institution

Name
University of Colorado Denver
Department
Dermatology
Type
Schools of Medicine
DUNS #
041096314
City
Aurora
State
CO
Country
United States
Zip Code
80045

  Publications

Kim, Soeun; Choi, Irene F; Quante, Jessica R et al. (2009) p63 directly induces expression of Alox12, a regulator of epidermal barrier formation. Exp Dermatol 18:1016-21
Koster, Maranke I; Marinari, Barbara; Payne, Aimee S et al. (2009) DeltaNp63 knockdown mice: A mouse model for AEC syndrome. Am J Med Genet A 149A:1942-7
Chen, Jiang; Roop, Dennis R (2008) Genetically engineered mouse models for skin research: taking the next step. J Dermatol Sci 52:1-12
Guttormsen, Jillian; Koster, Maranke I; Stevens, John R et al. (2008) Disruption of epidermal specific gene expression and delayed skin development in AP-2 gamma mutant mice. Dev Biol 317:187-95
Chen, Jiang; Jaeger, Karin; Den, Zhining et al. (2008) Mice expressing a mutant Krt75 (K6hf) allele develop hair and nail defects resembling pachyonychia congenita. J Invest Dermatol 128:270-9
Iwai, Naomi; Zhou, Zhijian; Roop, Dennis R et al. (2008) Horizontal basal cells are multipotent progenitors in normal and injured adult olfactory epithelium. Stem Cells 26:1298-306
Koster, Maranke I; Roop, Dennis R (2007) Mechanisms regulating epithelial stratification. Annu Rev Cell Dev Biol 23:93-113
Koster, Maranke I; Kim, Soeun; Huang, Jian et al. (2006) TAp63alpha induces AP-2gamma as an early event in epidermal morphogenesis. Dev Biol 289:253-61
Chen, Jiangli; Cheng, Xing; Merched-Sauvage, Maria et al. (2006) An unexpected role for keratin 10 end domains in susceptibility to skin cancer. J Cell Sci 119:5067-76
Koster, Maranke I; Lu, Shi-Long; White, Lisa D et al. (2006) Reactivation of developmentally expressed p63 isoforms predisposes to tumor development and progression. Cancer Res 66:3981-6

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