Abstract

The global objective of this research is to elucidate the mechanisms underlying growth, differentiation and development in mammalian epidermis and hair. To achieve this goal, we are focusing on understanding the regulatory controls that govern the expression of keratins, the major structural proteins of these cells. There are > 15 keratin genes that are differentially expressed at various stages of epidermal and follicle differentiation. Understanding how this complex pattern of keratin gene expression is established is therefore key to understanding how these cells develop and differentiate, and how these processes go awry in human skin diseases and cancers. The 5' keratin gene sequences are often sufficient to faithfully drive cell type and differentiation-specific expression in transgenic mice. We are particularly interested in understanding gene regulation of keratins K5 and K14, because they are the major proteins of basal keratinocytes. Due to their enormous proliferative capacity in culture, these cells have been used successfully for burn operations and are potentially powerful vehicles for drug delivery and gene therapy. Elucidating how KS and K14 promoter activity is controlled will be key in developing keratinocytes as therapeutic agents. We have already identified some important transcription factors involved in controlling KS and K14 gene expression in vitro and in vivo. The AP2 family of proteins bind to most keratinocyte-specific genes, and although they are not sufficient, they seem to be important for keratinocyte- specific gene expression. It is now essential that we explore further the functional significance of multiple AP2 genes in keratinocyte development and differentiation, and that we identify additional factors that are central to this process. A related issue is how the basal keratinocyte switches its program of gene expression when it commits to terminally differentiate. Through the use of dominant negative retinoic acid receptor mutants, we have discovered that retinoids control this switch. We are now within reach of identifying the downstream receptor target genes that are key to controlling early stages of differentiation. This knowledge is a fundamental prerequisite to understanding why retinoids are useful in treating a variety of skin diseases, and how they exert their effects on skin. Finally, we are interested in how embryonic cells choose between an epidermal vs. hair cell fate, and we have shown that a transcription factor, LEF-1, is essential for hair follicle morphogenesis and gene expression. Identifying the upstream and downstream members in the LEF-1 pathway will be important in understanding how this process is defective in congenital hair disorders, which are often severe and involve additional organs. Our laboratory has recently pioneered research that illustrates how an understanding of skin proteins can lead us to the genetic bases of human skin disorders. In the coming years, we will continue our endeavors to apply our molecular genetic research to medicine.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
Research Project (R01)
Project #
5R01AR031737-17
Application #
6029934
Study Section
General Medicine A Subcommittee 2 (GMA)
Program Officer
Moshell, Alan N
Project Start
1983-01-01
Project End
2001-06-30
Budget Start
1999-07-01
Budget End
2000-06-30
Support Year
17
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Chicago
Department
Genetics
Type
Schools of Medicine
DUNS #
225410919
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Sonobe, Yoshifumi; Ghadge, Ghanashyam; Masaki, Katsuhisa et al. (2018) Translation of dipeptide repeat proteins from the C9ORF72 expanded repeat is associated with cellular stress. Neurobiol Dis 116:155-165
Naik, Shruti; Larsen, Samantha B; Cowley, Christopher J et al. (2018) Two to Tango: Dialog between Immunity and Stem Cells in Health and Disease. Cell 175:908-920
Adam, Rene C; Yang, Hanseul; Ge, Yejing et al. (2018) Temporal Layering of Signaling Effectors Drives Chromatin Remodeling during Hair Follicle Stem Cell Lineage Progression. Cell Stem Cell 22:398-413.e7
Naik, Shruti; Larsen, Samantha B; Gomez, Nicholas C et al. (2017) Inflammatory memory sensitizes skin epithelial stem cells to tissue damage. Nature 550:475-480
Ge, Yejing; Gomez, Nicholas C; Adam, Rene C et al. (2017) Stem Cell Lineage Infidelity Drives Wound Repair and Cancer. Cell 169:636-650.e14
Gonzales, Kevin Andrew Uy; Fuchs, Elaine (2017) Skin and Its Regenerative Powers: An Alliance between Stem Cells and Their Niche. Dev Cell 43:387-401
Yang, Hanseul; Adam, Rene C; Ge, Yejing et al. (2017) Epithelial-Mesenchymal Micro-niches Govern Stem Cell Lineage Choices. Cell 169:483-496.e13
Ouspenskaia, Tamara; Matos, Irina; Mertz, Aaron F et al. (2016) WNT-SHH Antagonism Specifies and Expands Stem Cells prior to Niche Formation. Cell 164:156-169
Adam, Rene C; Fuchs, Elaine (2016) The Yin and Yang of Chromatin Dynamics In Stem Cell Fate Selection. Trends Genet 32:89-100
Fuchs, Elaine (2016) Epithelial Skin Biology: Three Decades of Developmental Biology, a Hundred Questions Answered and a Thousand New Ones to Address. Curr Top Dev Biol 116:357-74

Showing the most recent 10 out of 82 publications