Developmental Regulation of Specific Protein Interactions with an Enhancerlike Binding Site Far Upstream from the Avian Very-Low-Density Apolipoprotein II Gene

Hoodless, Pamela A.; Roy, Rabindra; Ryan, Aimee K.; Haché, Robert J.G.; Vasa, Monika; Deeley, Roger G.

doi:10.1128/mcb.10.1.154-164.1990

Molecular and Cellular Biology

1990

DOI: 10.1128/mcb.10.1.154-164.1990

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Developmental Regulation of Specific Protein Interactions with an Enhancerlike Binding Site Far Upstream from the Avian Very-Low-Density Apolipoprotein II Gene

Pamela A. Hoodless

Rabindra Roy

Aimee K. Ryan

et al.

Abstract: Expression of the avian very-low-density apolipoprotein II (apoVLDLII) gene is completely dependent on estrogen and restricted to the liver. We have identified binding sites for nonhistone nuclear proteins located between -1.96 and -2.61 kilobases. One of these sites, located at -2.6 kilobases (designated site 1), was found to span an MspI site that becomes demethylated between days 7 and 9 of embryogenesis, the stage of development at which competence to express the apoVLDLII gene begins to be acquired. Level… Show more

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1994

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“…The sequential onset of specific gene expression during development may reflect a differential requirement of liverenriched transcription factors, some of which might themselves be developmentally regulated. This notion is supported by studies by us and by others showing developmentally regulated interactions of liver nuclear proteins with cis-regulatory elements of liver-specific genes (29,33,71).…”

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confidence: 59%

Transcriptional Regulation of the Phosphoenolpyruvate Carboxykinase Gene by Cooperation Between Hepatic Nuclear Factors

Yanuka-Kashles

Cohen

Trus

et al. 1994

Molecular and Cellular Biology

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To study the transcriptional regulation of the liver gluconeogenic phenotype, the underdifferentiated mouse Hepa-1c1c7 (Hepa) hepatoma cell line was used. These cells mimicked the fetal liver by appreciably expressing the alpha-fetoprotein and albumin genes but not the phosphoenolpyruvate carboxykinase (PEPCK) gene. Unlike the fetal liver, however, Hepa cells failed to express the early-expressed factors hepatocyte nuclear factor 1 alpha (HNF-1 alpha) and HNF-4 and the late-expressed factor C/EBP alpha, thereby providing a suitable system for examining possible cooperation between these factors in the transcriptional regulation of the PEPCK gene. Transient transfection assays of a chimeric PEPCK-chloramphenicol acetyltransferase construct showed a residual PEPCK promoter activity in the Hepa cell line, which was slightly stimulated by cotransfection with a single transcription factor from either the C/EBP family or HNF-1 alpha but not at all affected by cotransfection of HNF-4. In contrast, cotransfection of the PEPCK construct with members from the C/EBP family plus HNF-1 alpha resulted in a synergistic stimulation of the PEPCK promoter activity. This synergistic effect depended on the presence in the PEPCK promoter region of the HNF-1 recognition sequence and on the presence of two C/EBP recognition sequences. The results demonstrate a requirement for coexistence and cooperation between early and late liver-enriched transcription factors in the transcriptional regulation of the PEPCK gene. In addition, the results suggest redundancy between members of the C/EBP family of transcription factors in the regulation of PEPCK gene expression.

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supporting

confidence: 59%

Transcriptional Regulation of the Phosphoenolpyruvate Carboxykinase Gene by Cooperation Between Hepatic Nuclear Factors

Yanuka-Kashles

Cohen

Trus

et al. 1994

Molecular and Cellular Biology

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show abstract

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Developmental Regulation of Specific Protein Interactions with an Enhancerlike Binding Site Far Upstream from the Avian Very-Low-Density Apolipoprotein II Gene

Cited by 1 publication

References 44 publications

Transcriptional Regulation of the Phosphoenolpyruvate Carboxykinase Gene by Cooperation Between Hepatic Nuclear Factors

Transcriptional Regulation of the Phosphoenolpyruvate Carboxykinase Gene by Cooperation Between Hepatic Nuclear Factors

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