Identification of AHR and hypoxia co-regulated immune target genes as potential factors of inflammation-driven oncogenesis
The transcription factors AHR and HIFs dimerize with the common co-activator ARNT during adaptive responses to xenobiotic exposure and oxygen tension. This cross-talk may subsequently modulate inflammation and/or physiological adaptation via immune cellular survival and maturation. Dysregulation of...
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sg-ntu-dr.10356-653002023-02-28T18:36:48Z Identification of AHR and hypoxia co-regulated immune target genes as potential factors of inflammation-driven oncogenesis Zaiden, Norazean Lee Kian Leong Lorenz Poellinger School of Biological Sciences Cancer Science Institute of Singapore DRNTU::Science::Biological sciences::Molecular biology The transcription factors AHR and HIFs dimerize with the common co-activator ARNT during adaptive responses to xenobiotic exposure and oxygen tension. This cross-talk may subsequently modulate inflammation and/or physiological adaptation via immune cellular survival and maturation. Dysregulation of AHR and HIF pathways can cause chronic inflammation leading to oncogenesis, thus we hypothesized that AHR and hypoxia signaling co-operate in potentiating inflammation-driven oncogenesis. To address this, we analyzed AHR-mediated transcriptional responses in three frequently xenobiotic-exposed study models (murine liver, human keratinocytes, human intestinal epithelial cells), especially in the intestine, where AHR and hypoxia signaling constantly co-exist. Although AHR signaling is evolutionary conserved, we find that the AHR mediates diverse responses in a cell type- and species-dependent manner. Concurrent activation with hypoxia signaling in intestinal cells indicate a promotion of chronic inflammation through down-regulation of numerous anti-inflammatory target genes, and up-regulation of pro-inflammatory genes such as PTGS2, GZMB, and MMP1. Master of Science 2015-07-10T07:51:31Z 2015-07-10T07:51:31Z 2015 2015 Thesis Zaiden, N. (2015). Identification of AHR and hypoxia co-regulated immune target genes as potential factors of inflammation-driven oncogenesis. Master's thesis, Nanyang Technological University, Singapore. http://hdl.handle.net/10356/65300 en 133 p. application/pdf |
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DRNTU::Science::Biological sciences::Molecular biology Zaiden, Norazean Identification of AHR and hypoxia co-regulated immune target genes as potential factors of inflammation-driven oncogenesis |
| description |
The transcription factors AHR and HIFs dimerize with the common co-activator ARNT during adaptive responses to xenobiotic exposure and oxygen tension. This cross-talk may subsequently modulate inflammation and/or physiological adaptation via immune cellular survival and maturation. Dysregulation of AHR and HIF pathways can cause chronic inflammation leading to oncogenesis, thus we hypothesized that AHR and hypoxia signaling co-operate in potentiating inflammation-driven oncogenesis. To address this, we analyzed AHR-mediated transcriptional responses in three frequently xenobiotic-exposed study models (murine liver, human keratinocytes, human intestinal epithelial cells), especially in the intestine, where AHR and hypoxia signaling constantly co-exist. Although AHR signaling is evolutionary conserved, we find that the AHR mediates diverse responses in a cell type- and species-dependent manner. Concurrent activation with hypoxia signaling in intestinal cells indicate a promotion of chronic inflammation through down-regulation of numerous anti-inflammatory target genes, and up-regulation of pro-inflammatory genes such as PTGS2, GZMB, and MMP1. |
| author2 |
Lee Kian Leong |
| author_facet |
Lee Kian Leong Zaiden, Norazean |
| format |
Theses and Dissertations |
| author |
Zaiden, Norazean |
| author_sort |
Zaiden, Norazean |
| title |
Identification of AHR and hypoxia co-regulated immune target genes as potential factors of inflammation-driven oncogenesis |
| title_short |
Identification of AHR and hypoxia co-regulated immune target genes as potential factors of inflammation-driven oncogenesis |
| title_full |
Identification of AHR and hypoxia co-regulated immune target genes as potential factors of inflammation-driven oncogenesis |
| title_fullStr |
Identification of AHR and hypoxia co-regulated immune target genes as potential factors of inflammation-driven oncogenesis |
| title_full_unstemmed |
Identification of AHR and hypoxia co-regulated immune target genes as potential factors of inflammation-driven oncogenesis |
| title_sort |
identification of ahr and hypoxia co-regulated immune target genes as potential factors of inflammation-driven oncogenesis |
| publishDate |
2015 |
| url |
http://hdl.handle.net/10356/65300 |
| _version_ |
1759854500135305216 |