Genetic Dissection of Functional Domains within the Avian Erythroblastosis Virus v-<i>erbA</i> Oncogene

The v-erbA oncoprotein (P75 gag-v-erbA ) can repress thyroid hormone receptor induced transcriptional activation of target genes. A central question is how hormone responsive elements in a target gene determine the transcriptional regulation mediated by P75 gag-v-erbA . We addressed this with receptors chimeric between P75 gag-v-erbA and thyroid hormone receptor (TR) by testing their regulatory activities on thyroid hormone response elements (TREs) diering in the sequence of the consensus core recognition motif AGGTCA. We report here that enhances, TR dependent transcriptional activation is conferred by P75 gag-v-erbA when the thymidine in the half site recognition motif is exchanged for an adenosine. The enhancement was independent of the DNA binding region of P75 gag-v-erbA , whereas increased expression of corepressor abolished the enhancing eect. The data indicate that the enhancement results from an impaired DNA binding by the oncoprotein combined with an eective scavenging of corepressors. Our data thus suggest the P75 gag-v-erbA indirectly can contribute to enhancement of thyroid hormone induced gene expression.

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A choice between transcriptional enhancement and repression by the v-erbA oncoprotein governed by one nucleotide in a thyroid hormone responsive half site

Andersson

Vennström

2000

Oncogene

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Genetic Dissection of Functional Domains within the Avian Erythroblastosis Virus v-erbA Oncogene

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References 35 publications

A choice between transcriptional enhancement and repression by the v-erbA oncoprotein governed by one nucleotide in a thyroid hormone responsive half site

A choice between transcriptional enhancement and repression by the v-erbA oncoprotein governed by one nucleotide in a thyroid hormone responsive half site

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