Your search keyword '"C, Basbaum"' showing total 7 results

1. Sp1 is involved in the transcriptional activation of lysozyme in epithelial cells.

Author

Suico MA, Koga T, Shuto T, Hisatsune A, Lu Z, Basbaum C, Okiyoneda T, and Kai H

Subjects

5' Flanking Region, Base Sequence, Binding Sites, Cell Line, Tumor, Epithelial Cells enzymology, Humans, Muramidase biosynthesis, Plicamycin pharmacology, Promoter Regions, Genetic, Proto-Oncogene Proteins metabolism, Proto-Oncogene Proteins c-ets, Sp1 Transcription Factor antagonists & inhibitors, Transcription Factors metabolism, Muramidase genetics, Plicamycin analogs & derivatives, Sp1 Transcription Factor physiology, Transcriptional Activation drug effects

Abstract

Lysozyme protects us from the ever-present danger of bacterial infection. The expression of lysozyme is, in part, regulated by the Ets factor, myeloid elf-1-like factor (MEF). MEF binds to the ETS site of the lysozyme promoter at -46 to -40bp. Closer analysis of the promoter using a series of deletion mutants and point mutants indicated that the region around -75bp is also essential in regulating the activity of lysozyme. The sequences in this region correspond to the Sp1 consensus binding site. Sp1 is known to regulate a variety of house-keeping and tissue-specific genes by itself or with other transcription factors like AP-1 or ETS. We indicate here that Sp1 regulates the lysozyme gene by binding to the GT-core sequences of lysozyme promoter. Treatment with mithramycin A down-regulated the promoter activity and the transfection of anti-sense Sp1 induced a decrease in the endogenous expression of lysozyme.

Published

2004

2. [Novel transcription factor MEF is associated with the function of lung epithelial cells].

Author

Hisatsune A, Uto A, Koyanagi T, Chihara T, Miyata T, Basbaum C, and Kai H

Subjects

Animals, Cattle, Cells, Cultured, Consensus Sequence, Epithelial Cells physiology, Lung cytology, Promoter Regions, Genetic, Transcriptional Activation, Transfection, DNA-Binding Proteins physiology, Lung physiology, Muramidase genetics, Transcription Factors physiology

Abstract

Lysozyme is an important component of innate immunity against common pathogens at mucosal surfaces. We previously cloned and characterized the bovine lysozyme 5A (lys5A) promoter with the purpose of determining cis- and trans-acting elements controlling airway epithelial cell-specific expression. We found that such expression is controlled by protein binding to an ETS consensus sequence located approximately at -46 to -40 bp from the transcription start site. The identity of the ETS-related protein responsible for gene transactivation was unknown. In this study, we screened six ETS-related proteins by transient transfection into epithelial cells and fibroblasts. Results showed that among these factors, the myeloid Elf-I-like factor (MEF) was the most potent. Gel shift analysis of epithelial cell nuclear extracts using a lys5A probe including the ETS-binding site (-50/-31) yielded a single band with retarded mobility. This band was super-shifted by an antibody directed against MEF. Supporting the possibility that MEF is responsible for functional transactivation of lysozyme in epithelial cells, we found that antisense MEF mRNA decreased lys5A promoter activity and that MEF overexpression in stably transfected cells increased lysozyme mRNA and protein expression. We conclude that MEF is required for epithelial cell transactivation of lysozyme.

Published

1999

3. Myeloid ELF-1-like factor up-regulates lysozyme transcription in epithelial cells.

Author

Kai H, Hisatsune A, Chihara T, Uto A, Kokusho A, Miyata T, and Basbaum C

Subjects

Animals, Base Sequence, Bone Marrow metabolism, Cell Line, DNA Primers, Ephrin-A2, Epithelial Cells enzymology, Humans, Transcription Factors metabolism, Muramidase genetics, Transcription Factors physiology, Transcription, Genetic physiology, Up-Regulation physiology

Abstract

Lysozyme is an important component of innate immunity against common pathogens at mucosal surfaces. We previously cloned and characterized the bovine lysozyme 5A (lys5A) promoter with the purpose of determining cis- and trans-acting elements controlling airway epithelial cell-specific expression. We found that such expression is controlled by protein binding to an ETS consensus sequence located approximately at -46 to -40 bp from the transcription start site. The identity of the ETS-related protein responsible for gene transactivation was unknown. In this study, we screened six ETS-related proteins by transient transfection into epithelial cells and fibroblasts. Results showed that among these factors, the myeloid Elf-1-like factor (MEF) was the most potent. Gel shift analysis of epithelial cell nuclear extracts using a lys5A probe including the ETS-binding site (-50/-31) yielded a single band with retarded mobility. This band was supershifted by an antibody directed against MEF. Supporting the possibility that MEF is responsible for functional transactivation of lysozyme in epithelial cells, we found that antisense MEF mRNA decreased lys5A promoter activity and that MEF overexpression in stably transfected cells increased lysozyme mRNA and protein expression. We conclude that MEF is required for epithelial cell transactivation of lysozyme.

Published

1999

4. Transcriptional regulation of the lysozyme gene in airway gland serous cells.

Author

Kai H, Takeuchi K, Ohmori H, Li JD, Gallup M, and Basbaum C

Subjects

Amino Acid Sequence, Animals, Base Sequence, Binding Sites, Biomarkers, Cattle, Cell Differentiation, Chickens, Cloning, Molecular, Humans, Mice, Molecular Sequence Data, Plasmids, Promoter Regions, Genetic, Protein Binding, Sequence Deletion, Sequence Homology, Serous Membrane cytology, TATA Box, Trachea cytology, Transcription, Genetic, Transfection, Gene Expression Regulation, Enzymologic, Muramidase genetics, Serous Membrane enzymology, Trachea enzymology

Abstract

Lysozyme is expressed in serous, but not mucous, cells of the tracheobronchial glands and thereby constitutes a marker of the serous cell lineage in these glands. To identify DNA regulatory elements and transcription factors mediating the commitment of progenitor cells to the serous cell lineage, we have characterized the regulatory activity and DNA-protein interactions of the 5'-flanking region of the bovine lysozyme gene lys 5a. Results obtained from these studies indicate that although approximately 94 bp of 5'flanking DNA are necessary for high level expression in transient transfection assays, an evolutionarily conserved promoter within 66 bp of the transcription start site is sufficient to confer serous cell-specific expression. Farther upstream, within 6.1 kb of the 5' flanking region, are 4 silencers. Analysis of the serous cell-specific lysozyme promoter by electrophoretic mobility shift assay (EMSA) revealed the presence of binding sites for 3 serous cell nuclear proteins, designated LSF1, LSF2 and LSF3. Binding of LSF2 and LSF3 was localized to a 20-mer subdomain (-50/-30) of the cell-specific promoter using binding competition assays. More accurate identification of the protein binding site(s) was achieved through the use of mutagenesis, which implicated the motif 5' AAGGAAT 3' (-46/-40) in both protein binding and serous cell-specific transcriptional activity. This motif has previously been identified as a binding site for ets protein transcription factors, suggesting that serous cell-specific regulation of lys 5a transcription is partly controlled by the binding of ets-like protein(s) to the motif 5'AGGAAGT3'.

Published

1996

5. Distribution of lysozyme and mucin (MUC2 and MUC3) mRNA in human bronchus.

Author

Dohrman A, Tsuda T, Escudier E, Cardone M, Jany B, Gum J, Kim Y, and Basbaum C

Subjects

Blotting, Northern, Bronchi cytology, DNA, Complementary analysis, Epithelial Cells, Epithelium metabolism, Humans, In Situ Hybridization, Mucin-2, Mucin-3, Mucins biosynthesis, Muramidase biosynthesis, Neoplasm Proteins biosynthesis, RNA Probes, RNA, Messenger genetics, Bronchi metabolism, Mucins genetics, Muramidase genetics, Neoplasm Proteins genetics, RNA, Messenger analysis

Abstract

Immunocytochemical studies have shown that gel-forming glycoproteins (mucins) and the bacteriolytic protein lysozyme are selectively expressed in airway mucous and serous cells, respectively. The mechanisms mediating this selectivity are unknown. In this study, we localized mucin and lysozyme mRNA by in situ hybridization to investigate the possibility that phenotype-specific expression of these proteins is controlled at the level of mRNA. Radiolabelled sense and antisense probes were constructed from the human tracheal mucin cDNA, HAM1 (MUC2 gene), the human small intestinal mucin cDNA, SIB139 (MUC3 gene), and the bovine tracheal lysozyme cDNA, Lys 7a. Frozen sections of human bronchus were hybridized with these probes and washed under routine conditions. Autoradiography showed that although lysozyme mRNA was strictly limited to cells expressing lysozyme, mucin mRNA was present both in mucin-expressing and mucin-non-expressing epithelial cells. This suggests that the restriction of lysozyme to serous cells is controlled at the level of mRNA (synthesis and/or degradation), whereas the restriction of mucin to mucous cells is controlled at the level of translation.

Published

1994

6. Multiple cDNA sequences of bovine tracheal lysozyme.

Author

Takeuchi K, Irwin DM, Gallup M, Shinbrot E, Kai H, Stewart CB, and Basbaum C

Subjects

Amino Acid Sequence, Animals, Base Sequence, Blotting, Southern, Cattle, Cells, Cultured, DNA Primers, DNA, Complementary, Electrophoresis, Polyacrylamide Gel, Molecular Sequence Data, Polymerase Chain Reaction, Sequence Homology, Amino Acid, Sequence Homology, Nucleic Acid, Muramidase genetics, Trachea enzymology

Abstract

The principal role of lysozyme is to prevent bacterial invasion at body surfaces. We are interested in how lysozyme is regulated at the surface of the respiratory tract, where the serous gland cell is regarded as the primary cellular source of this enzyme. Since the cow genome contains at least 10 lysozyme-like genes, our objective was to determine which of them are expressed in the cow tracheal gland serous cell. By screening tracheal cDNA libraries with a probe constructed from the cDNA encoding stomach lysozyme 2, we obtained 3 lysozyme cDNAs: 5a (1023 base pairs (bp)), 7a (1060 bp), and 14d (1249 bp). cDNA 7a corresponds to a previously reported gene (showing sequence identity to the stomach 2 lysozyme gene), whereas cDNAs 5a and 14d correspond to lysozyme genes not previously reported. Northern blot analysis of cow tracheal RNA showed lysozyme mRNAs of three distinct lengths. Based on hybridization with probes specific for each cDNA, we determined that the longest transcript corresponded to cDNA 5a, the shortest to 7a, and the intermediate-length transcript to 14d. Cultured cow tracheal gland serous cell RNA, reverse transcribed and amplified by the polymerase chain reaction with primers common to all three cDNAs, yielded a product that hybridized to oligonucleotide probes specific for all three cDNAs but most strongly to that for 5a. These results indicate that multiple lysozyme mRNAs are expressed in the cow trachea and that the lysozyme encoded by cDNA 5a is the major form expressed in the tracheal gland serous cell. This serous cell lysozyme is predicted to differ importantly in structure from both 7a and 14d lysozymes, with an arginine:lysine ratio almost 10-fold higher. The sequence differences may underlie functional differences, including variable resistance to proteolysis and variable affinity for large polyanions (e.g. mucins) found in the respiratory tract lumen.

Published

1993

7. Lysozyme and mucin cDNAs as tools for the study of serous and mucous cell differentiation.

Author

Basbaum C, Tsuda T, Takeuchi K, Royce F, and Jany B

Subjects

Animals, Cattle, Cell Differentiation, Humans, Mucins metabolism, Mucous Membrane cytology, Mucous Membrane metabolism, Muramidase metabolism, Serous Membrane cytology, Serous Membrane metabolism, Trachea metabolism, DNA isolation & purification, Mucins genetics, Muramidase genetics, Trachea cytology

Published

1992