Phenobarbital Response Elements of Cytochrome P450 Genes and Nuclear Receptors

Revisão Revisado por pares

Phenobarbital Response Elements of Cytochrome P450 Genes and Nuclear Receptors

2001; Annual Reviews; Volume: 41; Issue: 1 Linguagem: Inglês

10.1146/annurev.pharmtox.41.1.123

ISSN

1545-4304

Autores

Tatsuya Sueyoshi, Masahiko Negishi,

Tópico(s)

Drug Transport and Resistance Mechanisms

Resumo

Phenobarbital (PB) response elements are composed of various nuclear receptor (NR)-binding sites. A 51-bp distal element PB-responsive enhancer module (PBREM) conserved in the PB-inducible CYP2B genes contains two NR-binding direct repeat (DR)-4 motifs. Responding to PB exposure in liver, the NR constitutive active receptor (CAR) translocates to the nucleus, forms a dimer with the retinoid X receptor (RXR), and activates PBREM via binding to DR-4 motifs. For CYP3A genes, a common NR site [DR-3 or everted repeat (ER)-6] is present in proximal promoter regions. In addition, the distal element called the xenobiotic responsive module (XREM) is found in human CYP3A4 genes, which contain both DR-3 and ER-6 motifs. Pregnane X receptor (PXR) could bind to all of these sites and, upon PB induction, a PXR:RXR heterodimer could transactivate XREM. These response elements and NRs are functionally versatile, and capable of responding to distinct but overlapping groups of xenochemicals.

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Phenobarbital Response Elements of Cytochrome P450 Genes and Nuclear Receptors