期刊
BIOSCIENCE REPORTS
卷 33, 期 -, 页码 57-U78出版社
PORTLAND PRESS LTD
DOI: 10.1042/BSR20120095
关键词
androgen; cholesterol; 3 beta-hydroxysterol Delta(24)-reductase (DHCR24); Kruppel-like factor 5 (KLF5); promoter analysis; sterol-regulatory-element-binding protein (SREBP)
资金
- Ministerio de Ciencia y Tecnologia [BMC2002-01262, SAF2011-29951]
- Fondo de Investigacion Sanitaria [PI081063]
- Comunidad Autonoma de Madrid
DHCR24 (3 beta-hydroxysterol Delta(24)-reductase) catalyses the reduction of the C-24 double bond of sterol intermediates during cholesterol biosynthesis. DHCR24 has also been involved in cell growth, senescence and cellular response to oncogenic and oxidative stress. Despite its important roles, little is known about the transcriptional mechanisms controlling DHCR24 gene expression. We analysed the proximal promoter region and the cholesterol-mediated regulation of DHCR24. A putative SRE (sterol-regulatory element) at -98/-90 bp of the transcription start site was identified. Other putative regulatory elements commonly found in SREBP (SRE-binding protein)-targeted genes were also identified. Sterol responsiveness was analysed by luciferase reporter assays of approximately 1 kb 5'-flanking region of the human DHCR24 gene in HepG2 and SK-N-MC cells. EMSAs (electrophoretic mobility-shift assays) and ChIP (chromatin immunoprecipitation) assays demonstrated cholesterol-dependent recruitment and binding of SREBPs to the putative SRE. Given the presence of several CACCC-boxes in the DHCR24 proximal promoter, we assessed the role of KLF5 (Kruppel-like factor 5) in androgen-regulated DHCR24 expression. DHT (dihydrotestosterone) increased DHCR24 expression synergistically with lovastatin. However, DHT was unable to activate the DHCR24 proximal promoter, whereas KLF5 did, indicating that this mechanism is not involved in the androgen-induced stimulation of DHCR24 expression. The results of the present study allow the elucidation of the mechanism of regulation of the DHCR24 gene by cholesterol availability and identification of other putative cis-acting elements which may be relevant for the regulation of DHCR24 expression.
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