Indistinguishable Nuclear Factor Binding to Functional Core Sites of the T-Cell Receptor δ and Murine Leukemia Virus Enhancers
We have previously shown that the δE3 site is an essential element for transcriptional activation by the human T-cell receptor (TCR) δ enhancer and identified two factors, NF-8E3A and NF-δE3C, that bound to overlapping core (TGTGGTTT) and E-box motifs within δE3. In this study, we show that protein...
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Published in | Molecular and cellular biology Vol. 12; no. 11; pp. 4817 - 4823 |
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Main Authors | , , , , , |
Format | Journal Article |
Language | English |
Published |
Taylor & Francis
01.11.1992
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Abstract | We have previously shown that the δE3 site is an essential element for transcriptional activation by the human T-cell receptor (TCR) δ enhancer and identified two factors, NF-8E3A and NF-δE3C, that bound to overlapping core (TGTGGTTT) and E-box motifs within δE3. In this study, we show that protein binding to the core motif is necessary but not sufficient for transcriptional activation by the δE3 element. In contrast, protein binding to the E-box motif does not contribute significantly to enhancer activity. A similar core motif present within the enhancers of T-cell-tropic murine retroviruses has been shown to contribute to transcriptional activity of the viral long terminal repeat in T lymphocytes and to viral T-cell tropism. We therefore determined the relationship between the nuclear factors that bind to the TCR δ and Moloney murine leukemia virus core motifs. On the basis of electrophoretic mobility shift binding and competition studies, biochemical analysis of affinity-labeled DNA-binding proteins, and the binding of a purified core binding factor, the proteins that bound to the TCR δ core site were indistinguishable from those that bound to the murine leukemia virus core site. These data argue that DNA-binding proteins that interact with the core site of murine leukemia virus long terminal repeats and contribute to viral T-cell tropism also play an essential role in the T-cell-specific expression of cellular genes. |
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AbstractList | We have previously shown that the δE3 site is an essential element for transcriptional activation by the human T-cell receptor (TCR) δ enhancer and identified two factors, NF-8E3A and NF-δE3C, that bound to overlapping core (TGTGGTTT) and E-box motifs within δE3. In this study, we show that protein binding to the core motif is necessary but not sufficient for transcriptional activation by the δE3 element. In contrast, protein binding to the E-box motif does not contribute significantly to enhancer activity. A similar core motif present within the enhancers of T-cell-tropic murine retroviruses has been shown to contribute to transcriptional activity of the viral long terminal repeat in T lymphocytes and to viral T-cell tropism. We therefore determined the relationship between the nuclear factors that bind to the TCR δ and Moloney murine leukemia virus core motifs. On the basis of electrophoretic mobility shift binding and competition studies, biochemical analysis of affinity-labeled DNA-binding proteins, and the binding of a purified core binding factor, the proteins that bound to the TCR δ core site were indistinguishable from those that bound to the murine leukemia virus core site. These data argue that DNA-binding proteins that interact with the core site of murine leukemia virus long terminal repeats and contribute to viral T-cell tropism also play an essential role in the T-cell-specific expression of cellular genes. |
Author | Miguel Redondo, Juan Pfohl, Jeffrey L. Wang, Shuwen Hernandez-Munain, Cristina Speck, Nancy A. Krangel, Michael S. |
Author_xml | – sequence: 1 givenname: Juan surname: Miguel Redondo fullname: Miguel Redondo, Juan organization: Department of Immunology, P.O. Box 3010, Duke University Medical Center – sequence: 2 givenname: Jeffrey L. surname: Pfohl fullname: Pfohl, Jeffrey L. organization: Department of Immunology, P.O. Box 3010, Duke University Medical Center – sequence: 3 givenname: Cristina surname: Hernandez-Munain fullname: Hernandez-Munain, Cristina organization: Department of Immunology, P.O. Box 3010, Duke University Medical Center – sequence: 4 givenname: Shuwen surname: Wang fullname: Wang, Shuwen organization: Department of Biochemistry, Dartmouth Medical School – sequence: 5 givenname: Nancy A. surname: Speck fullname: Speck, Nancy A. organization: Department of Biochemistry, Dartmouth Medical School – sequence: 6 givenname: Michael S. surname: Krangel fullname: Krangel, Michael S. organization: Department of Immunology, P.O. Box 3010, Duke University Medical Center |
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CitedBy_id | crossref_primary_10_4049_jimmunol_174_7_4144 crossref_primary_10_1073_pnas_94_16_8646 crossref_primary_10_1038_sj_onc_1203588 crossref_primary_10_1038_sj_onc_1205315 crossref_primary_10_1038_sj_onc_1205447 crossref_primary_10_1128_JVI_73_7_5535_5547_1999 crossref_primary_10_1128_JVI_00299_10 crossref_primary_10_1038_sj_onc_1206141 crossref_primary_10_1128_JVI_72_7_5579_5588_1998 |
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References | B20 B21 Wang S. (B28) 1992; 12 B22 B23 B24 B25 B27 B3a Redondo J. M. (B18) 1991; 11 B10 B11 B12 B13 B14 B15 B16 B17 B19 B1 B2 B3 B4 B5 B6 B7 B8 Thornell A. (B26) 1988; 8 B9 |
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Title | Indistinguishable Nuclear Factor Binding to Functional Core Sites of the T-Cell Receptor δ and Murine Leukemia Virus Enhancers |
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