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首页> 外文期刊>dna and cell biology >Thyroid Hormone and Retinoic Acid Receptors Form Heterodimers with Retinoid X Receptors on Direct Repeats, Palindromes, and Inverted Palindromes
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Thyroid Hormone and Retinoic Acid Receptors Form Heterodimers with Retinoid X Receptors on Direct Repeats, Palindromes, and Inverted Palindromes

机译:Thyroid Hormone and Retinoic Acid Receptors Form Heterodimers with Retinoid X Receptors on Direct Repeats, Palindromes, and Inverted Palindromes

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ABSTRACTThyroid hormone 3,5,3′-triodothyronine (T3) and retinoic acid (RA) receptors (T3Rs and RARs) are liganddependent transcription factors that regulate the transcription of T3- and RA-responsive genes, respectively, by binding to specific DNA sequences as homodimers or as heterodimers with retinoid X receptors (RXRs). These T3and RA response elements are composed of two copies of the consensus half-site motif PuGGTCA. However, the specificity of the receptor complexes for response elements is dictated by their discrimination of the distance and the relative orientation of the half-sites. We found that both T3R–RXR and RAR–RXR heterodimers act functionally on all three response element configurations: direct repeats, palindromes, and inverted palindromes. On direct repeats, T3R–RXR and RAR–RXR heterodimers showed maximaltrans-activation andin vitroDNA binding affinity when the core binding motifs were spaced by 4, 2, or 1 and 5 or 2 nucleotides, respectively, whereas both heterodimer types were mostly active on palindromes with no spacing. The binding of andtrans-activation by T3R–RXR and RAR–RXR heterodimers on inverted palindromes was maximal with a half-site spacing of 5 or 6 and 7 or 8 nucleotides, respectively. Inverted palindromes, however, were the most specific response elements, because they were the only ones on which the activities of homodimeric and heterodimeric receptor complexes could be discriminated. We developed a model that suggests a sterical link between the optimal spacings observed with direct repeats and inverted palindromes. Taken together, the experimental data and the model provide further understanding of the regulation of T3-and retinoid-res

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