Genome-wide approaches for identification of nuclear receptor target genes | Zendy

Luz E. Tavera-Mendoza | Zendy; Sylvie Mader | Zendy; John H. White | Zendy

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Genome-wide approaches for identification of nuclear receptor target genes

Author(s) -

Luz E. Tavera-Mendoza,

Sylvie Mader,

John H. White

Publication year - 2006

Publication title -

nuclear receptor signaling

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.434

H-Index - 33

ISSN - 1550-7629

DOI - 10.1621/nrs.04018

Subject(s) - computational biology , nuclear receptor , dna microarray , biology , chromatin immunoprecipitation , genomics , in silico , genome , chromatin , gene , genetics , gene expression , transcription factor , promoter

Large-scale genomics analyses have grown by leaps and bounds with the rapid advances in high throughput DNA sequencing and synthesis techniques. Nuclear receptor signaling is ideally suited to genomics studies because receptors function as ligand-regulated gene switches. This review will survey the strengths and limitations of three major classes of high throughput techniques widely used in the nuclear receptor field to characterize ligand-dependent gene regulation: expression profiling studies (microarrays, SAGE and related techniques), chromatin immunoprecipitation followed by microarray (ChIP-on-chip), and genome-wide in silico hormone response element screens. We will discuss each technique, and how each has contributed to our understanding of nuclear receptor signaling.

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