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Transcriptional Regulation

GATA Elements Are Necessary for the Activity and Tissue Specificity of the T-Cell Receptor Beta-Chain Transcriptional Enhancer

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Pages 4286-4294 | Received 29 Dec 1993, Accepted 08 Mar 1994, Published online: 30 Mar 2023
 

Abstract

Three high-affinity binding sites for the GATA family of transcriptional regulators have been identified within the T-cell receptor beta-chain (TCRp) transcriptional enhancer, and their functional significance has been determined in an effort to understand the T-cell specificity of the enhancer more fully. One site, TE4, is important for activity of the enhancer in T cells. Neither site TE1 nor site TE2 can functionally replace a mutated TE4 site in T cells; however, the same protein, probably GATA-3, binds all three sites, as judged by electrophoretic mobility shift, oligonucleotide competition, and proteolytic clipping assays. These data suggest that additional proteins are critical for the ability of GATA-3 to activate the TCRp enhancer. In fibroblasts, the GATA sequence at site TE1 appears to bind a negative regulator. Since this is not true in B cells, B cells and fibroblasts appear to have different mechanisms for negative regulation of the TCRP enhancer.

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