Abstract

The goal objective of this research is to elucidate the mechanisms underlying the control of keratinocyte growth and gene expression in oral epithelial tissues, and to assess how these processes are altered in oral cancers. To achieve this goal, we are focusing on understanding the regulatory controls that govern the genes that encode keratins, the major structural proteins of oral epithelial cells. This understanding will not only be useful to our understanding of how malignancy leads to aberrations in gene control, but in addition, the keratin promoters will be valuable for developing keratinocytes as a vehicle for gene therapy in the treatment of premalignant and/or postoperative head and neck Cancers. The 5' sequences of K14 and K5 are sufficient to faithfully drive expression in the mitotically active keratinocytes of tongue, buccal and tooth epithelia of transgenic mice. Due to their enormous proliferative capacity in culture, keratinocytes have been used successfully for bum operations and are potentially powerful vehicles for drug delivery and gene therapy of oral cancers and other tissue abnormalities. Elucidating how K5 and K14 promoter activity is controlled will be key in developing keratinocytes for these purposes. To this end, we will identify the critical sequences and factors that are central to efficient expression of foreign genes in oral keratinocytes. We will also explore how these factors are themselves regulated, and whether these processes are altered in oral squamous cell carcinomas (SQCCs). We will also explore how retinoids control differentiation in normal and SQCC keratinocytes, and elucidate the key retinoid receptor mediated target genes involved in this process. Such work is particularly important to developing new and improved retinoids for the treatment of oral leukoplakias caused by heavy smoking. We are also interested in identifying the critical molecular differences that distinguish a mitotically active oral keratinocyte from a leukoplakia keratinocyte and from an SQCC keratinocyte. We have devised a strategy to screen for such differences, and to test their importance by examining premalignant and malignant tissues in vivo. Finally, using transgenic mouse technology, embryonic stem cell technology and conditional knockouts with oral keratinocyte promoters, we will engineer in mice the molecular aberrations that we detect in the keratinocytes of oral cancers. These studies will not only allow us to assess the functional significance of such aberrations and their role in tumor progression, but in addition will provide valuable animal models for developing new and improved tools for the-diagnosis and treatment of these cancers. Our laboratory has recently pioneered research that illustrates how an understanding of keratinocyte biology can lead us to the causes of a variety of human genetic 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 Dental & Craniofacial Research (NIDCR)
Type
Specialized Center (P50)
Project #
5P50DE011921-05
Application #
6354654
Study Section
Project Start
1996-09-30
Project End
2001-07-31
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
5
Fiscal Year
2000
Total Cost
$92,820
Indirect Cost

  Institution

Name
University of Chicago
Department
Type
DUNS #
005421136
City
Chicago
State
IL
Country
United States
Zip Code
60637

  Publications

Cohen, Ezra E W; Rosner, Marsha Rich (2009) MicroRNA-regulated feed forward loop network. Cell Cycle 8:2477-8
Cohen, Ezra E W; Zhu, Hongyan; Lingen, Mark W et al. (2009) A feed-forward loop involving protein kinase Calpha and microRNAs regulates tumor cell cycle. Cancer Res 69:65-74
Logemann, Jeri A; Pauloski, Barbara Roa; Rademaker, Alfred W et al. (2008) Swallowing disorders in the first year after radiation and chemoradiation. Head Neck 30:148-58
Huang, R Stephanie; Duan, Shiwei; Kistner, Emily O et al. (2008) Genetic variants contributing to daunorubicin-induced cytotoxicity. Cancer Res 68:3161-8
Zhang, Wei; Duan, Shiwei; Kistner, Emily O et al. (2008) Evaluation of genetic variation contributing to differences in gene expression between populations. Am J Hum Genet 82:631-40
Shukla, Sunita J; Duan, Shiwei; Badner, Judith A et al. (2008) Susceptibility loci involved in cisplatin-induced cytotoxicity and apoptosis. Pharmacogenet Genomics 18:253-62
Logemann, Jeri A; Rademaker, Alfred W; Pauloski, Barbara Roa et al. (2006) Site of disease and treatment protocol as correlates of swallowing function in patients with head and neck cancer treated with chemoradiation. Head Neck 28:64-73
Cohen, Ezra Eddy Wyssam; Lingen, Mark W; Zhu, Bangmin et al. (2006) Protein kinase C zeta mediates epidermal growth factor-induced growth of head and neck tumor cells by regulating mitogen-activated protein kinase. Cancer Res 66:6296-303
Milano, Michael T; Vokes, Everett E; Kao, Johnny et al. (2006) Intensity-modulated radiation therapy in advanced head and neck patients treated with intensive chemoradiotherapy: preliminary experience and future directions. Int J Oncol 28:1141-51
Pasche, Boris; Knobloch, Thomas J; Bian, Yansong et al. (2005) Somatic acquisition and signaling of TGFBR1*6A in cancer. JAMA 294:1634-46

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