Your search keyword '"Lifang Shao"' showing total 3 results

1. Identification of a classic cytokine-induced enhancer upstream in the human iNOS promoter.

Author

Zhong Guo, Lifang Shao, Qiang Du, Kyung Soo Park, and Geller, David A.

Subjects

*CYTOKINES, *LUNGS, *LIVER cells, *THYMIDINE, *GENES, *PROTEIN binding, *GENETIC transcription

Abstract

The human inducible NOS (iNOS) promoter transcriptionally regulated by 5′ flanking region extending 16 kb upstream that contains cytokine-responsive DNA motifs. In this study, we further identified a classic inducible enhancer located between --5 and --6 kb in the hiNOS upstream promoter. This 1 kb promoter sequence functions as a cytokine-inducible enhancer in an orientation- and position-independent manner in human lung A549 and liver AKN1 cells. This DNA enhancer also confers cytokine inducibility to the heterologous thymidine kinase (TK) promoter. Chromatin immunoprecipitation (ChIP) analysis was applied, and confirmed cytokine-inducible in vivo DNA-protein interactions within this enhancer region. In vivo functional binding of both NF-κB (p65/p50) and Stat-lα at the --5.8 kb human iNOS promoter site was significantly increased in A549 cells after cytokine stimulation, while only Stat-1α bound at the --5.2 kb site. These results identify the --5 to --6 kb promoter region as a classic transcriptional enhancer for the human iNOS gene and provide definitive in vivo evidence of specific NF-κB and Stat-1 nuclear protein binding that mediates transcription of the hiNOS gene under cytokine stimulation. [ABSTRACT FROM AUTHOR]

Published

2007

2. A critical role for C/EBPΒ binding to the AABS promoter response element in the human iNOS gene.

Author

Zhong Guo, Lifang Shao, Xuesheng Feng, Reid, Kaye, Marderstein, Eric, Nakao, Atsunori, and Geller, David A.

Subjects

*NITRIC oxide, *OXIDES, *NITROGEN compounds, *GENES, *MOLECULAR genetics, *HEREDITY

Abstract

Discusses a study which identified the molecular mechanisms accounting for the liver-specific human inducible nitric oxide synthase (hiNOS) gene transcription. Description of the gene; Effort taken to further determine a putative role for AABS element in hiNOS transcription; Fields where LAP overexpression and cotransfection with the hiNOS promoter were examined.

Published

2003

3. Up-regulation of human iNOS transcription by coactivator p300.

Author

Zhong Guo, Lifang Shao, Qiang Du, Kyung Soo Park, and Geller, David A

Subjects

*GENETIC transcription, *INOSINE, *GENE expression, *CYTOKINES, *GENE transfection, *LUNGS, *CELLS

Abstract

Served as one of general transcription coactivators, p300 plays an important role in mediating gene transcriptional activation. Our previous work demonstrated that human iNOS expression can be highly induced with the cytokine mixture (CM) of TNFα + IL-1β + IFNγ. In this study, we explored the potential function of p300 in the regulation of human iNOS gene expression. Our initial results showed that overexpression of p300 by transient transfection in human A549 lung cells significantly increased the basal and cytokine induced human iNOS promoter activities. Interestingly, p300 activated cytokine induced human iNOS transcription which was completely abrogated by the deletion of an enhancer region between -5 kb and -6 kb in the hiNOS upstream promoter. However, the enhanced basal promoter activity by p300 overexpression still remained high even with the enhancer deletion. Our data suggest that coactivator p300 is capable of up-regulating human iNOS transcription. The transcription machinery responsible for p300 interaction with necessary transcription factors is being further investigated. [ABSTRACT FROM AUTHOR]

Published

2007