Abstract

The mechanism governing differentiation of intestinal epithelial cells is unknown. Due to the extremely complex nature of the mammalian gastrointestinal tract, homogeneous cultured intestinal epithelial cell lines may be more suitable for the initial study of cellular and molecular events that control epithelial differentiation. The human carcinoma cell line HT29 and its clonal derivatives have been shown to exhibit biochemical and morphological characteristics of enterocyte differentiation in vitro and are therefore excellent models for the study of intestinal differentiation. The long-term goal of the proposed project is to define the molecular mechanisms controlling intestinal differentiation in the culture model system of human colon carcinoma cell lines HT29-18 and HT29- 18-C. The major objectives are: 1) to isolate and characterize differentially expressed genes in differentiating HT29-18 cells, and 2) to examine the mechanism regulating transcription of these genes in differentiating HT29-18 cells. Using the molecular technique of subtraction cDNA library screening, we have already isolated a full-length cDNA clone (A4) representing a novel gene whose expression is differentially regulated in HT29-18 and HT29-18-C cells. The A4 cDNA represents a messenger RNA of 1.0 kb in size whose abundance is dramatically induced as HT29-18 cells differentiate. Amino acid sequences deduced from A4 nucleotide sequences have a limited homology to a portion of the cytoskeletal protein, ankyrin. The expression of A4 is enriched in colonic mucosa and is transcriptionally activated during HT29 differentiation. We have also shown that the gene encoding the cystic fibrosis transmembrane conductance regulator protein (CFTR) is also transcriptionally activated during HT29 differentiation. We now plan to perform the following experiments: 1) to isolate by subtraction cloning additional cDNA clones that are transcriptionally activated, 2) to characterize the newly identified differentiation-dependent genes, and 3) to investigate the mechanisms regulating transcription of differentially expressed genes including A4, CFTR and genes obtained in (1). By performing these experiments, we hope to identify a concerted mechanism regulating transcription of a selected group of genes in a culture model of intestinal epithelial differentiation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Program Projects (P01)
Project #
5P01DK044484-05
Application #
3710306
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
5
Fiscal Year
1996
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Type
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Aihara, Eitaro; Montrose, Marshall H (2014) Importance of Ca(2+) in gastric epithelial restitution-new views revealed by real-time in vivo measurements. Curr Opin Pharmacol 19:76-83
Singh, Varsha; Yang, Jianbo; Chen, Tiane-e et al. (2014) Translating molecular physiology of intestinal transport into pharmacologic treatment of diarrhea: stimulation of Na+ absorption. Clin Gastroenterol Hepatol 12:27-31
Lin, Rong; Murtazina, Rakhilya; Cha, Boyoung et al. (2011) D-glucose acts via sodium/glucose cotransporter 1 to increase NHE3 in mouse jejunal brush border by a Na+/H+ exchange regulatory factor 2-dependent process. Gastroenterology 140:560-71
Hartley, Jane Louise; Zachos, Nicholas C; Dawood, Ban et al. (2010) Mutations in TTC37 cause trichohepatoenteric syndrome (phenotypic diarrhea of infancy). Gastroenterology 138:2388-98, 2398.e1-2
Zachos, Nicholas C; Hodson, Caleb; Kovbasnjuk, Olga et al. (2008) Elevated intracellular calcium stimulates NHE3 activity by an IKEPP (NHERF4) dependent mechanism. Cell Physiol Biochem 22:693-704
Li, Xuhang; Donowitz, Mark (2008) Fractionation of subcellular membrane vesicles of epithelial and nonepithelial cells by OptiPrep density gradient ultracentrifugation. Methods Mol Biol 440:97-110
Lee, Aven; Rayfield, Andrew; Hryciw, Deanne H et al. (2007) Na+-H+ exchanger regulatory factor 1 is a PDZ scaffold for the astroglial glutamate transporter GLAST. Glia 55:119-29
Donowitz, Mark; Singh, Siddharth; Salahuddin, Farah F et al. (2007) Proteome of murine jejunal brush border membrane vesicles. J Proteome Res 6:4068-79
Murtazina, Rakhilya; Kovbasnjuk, Olga; Zachos, Nicholas C et al. (2007) Tissue-specific regulation of sodium/proton exchanger isoform 3 activity in Na(+)/H(+) exchanger regulatory factor 1 (NHERF1) null mice. cAMP inhibition is differentially dependent on NHERF1 and exchange protein directly activated by cAMP in ileum versus J Biol Chem 282:25141-51
Donowitz, Mark; Li, Xuhang (2007) Regulatory binding partners and complexes of NHE3. Physiol Rev 87:825-72

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