Assembly and function of a TCR alpha enhancer complex is dependent on LEF-1-induced DNA bending and multiple protein-protein interactions.

Giese, Klaus; Kingsley, Chris; Kirshner, Jessica R.; Grosschedl, Rudolf

doi:10.1101/gad.9.8.995

Cited by 522 publications

(535 citation statements)

References 69 publications

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“…Among the ets family, ETS1 mRNA was known to be localized in the bone tissue (Kola et al, 1993). The signi®cance of the interaction between runt family and ets family has been reported (Giese et al, 1995;Wotton et al, 1994). PEBP2aA, ETS1 and DNA were reported to form a ternary complex and have a synergistic e ect on transactivation of the T cell receptor b gene, in which runt and ets binding sites are juxtaposed.…”

Section: Discussionmentioning

confidence: 99%

“…PEBP2a speci®cally recognizes a consensus sequence, PuACCPuCA and has been reported to control polyoma virus enhancer (Kamachi et al, 1990), murine leukemia virus enhancers , T cell-speci®c genes (Giese et al, 1995;Hallberg et al, 1992;Hsiang et al, 1993;Prosser et al, 1992;Redondo et al, 1992), enzymes (myeloperoxidase, neutrophil elastase, granzyme B serine protease) (Nuchprayoon et al, 1994;Wargnier et al, 1995) and cytokines and their receptors (GM-CSF, IL3, CSF-1) (Cameron et al, 1994;Frank et al, 1995;Zhang et al, 1994). PEBP2aA and ETS1 have been shown to bind together and interact synergistically on the promoter of the T cell receptor a gene (Giese et al, 1995) and T cell receptor b gene (Wotton et al, 1994).…”

Section: Introductionmentioning

confidence: 99%

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Transcriptional regulation of osteopontin gene in vivo by PEBP2αA/CBFA1 and ETS1 in the skeletal tissues

et al. 1998

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Transcriptional regulation of osteopontin gene in vivo by PEBP2αA/CBFA1 and ETS1 in the skeletal tissues

et al. 1998

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“…Thus this observation taking together with the mapping of the Erg domains responsible for the homodimerization shows that the ETS domain serves a key dual function, DNA-binding and in protein ± protein interactions. It is also the case for other transcriptional factors, for example, the Runt family proteins are able to physically interact with other factors via their RUNT domain, also responsible of DNA-binding properties (Ogawa et al, 1993;Giese et al, 1995).…”

Section: Negative In¯uence Of the Central Domain (Cd) Of Erg Proteinsmentioning

confidence: 99%

Erg proteins, transcription factors of the Ets family, form homo, heterodimers and ternary complexes via two distinct domains

et al. 1998

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The ets genes family encodes a group of proteins which function as transcription factors under physiological conditions. We report here that the Erg proteins, members of the Ets family, form homo and heterodimeric complexes in vitro. We demonstrate that the Ergp55 protein isoform forms dimers with itself and with the two other isoforms, Ergp49 and Ergp38. Using a set of Erg protein deletion mutants, we de®ne two distinct domains independently involved in dimerization. The ®rst one is located in the amino-terminal part of the protein containing the pointed domain (PNT), conserved in a subset of Ets proteins. The second one resides within the ETS domain, the DNA-binding domain. We also show that the Erg protein central region behaves as an inhibitory domain of dimerization and its removal enhances the Ergp55 transactivation properties. Furthermore, Ergp55 forms heterodimers with some other Ets proteins. Among the latter, we show that Fli-1, Ets-2, Er81 and Pu-1 physically interact with Erg. Finally, we show that the formation of the previously described ternary complex Ergp55/Fos/jun is mediated by ETS domain and Jun protein, while the ternary complex Ergp49/Fos/Jun is mediated by Fos protein.

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“…Several Ets factors interact with other regulators of gene expression and cell cycle progression. Ets-1 binds various transcription factors, including Sp1 (Gegonne et al, 1993), PEBP2a/AML-1 (Giese et al, 1995), GHF-1/Pit-1 (Bradford et al, 1995), MafB (Sieweke et al, 1996), NF-kB, AP-1 (Thomas et al, 1997), and USF-1 (Sieweke et al, 1998). Despite its high degree of structural similarity with Ets-1, only one protein-protein interaction between Ets-2 and p300/CBP (Jayaraman et al, 1999) and two transcriptional cooperations with GATA3 (Blumenthal et al, 1999) or ATF/Jun family members (Cirillo et al, 1999) have been reported.…”

Section: Introductionmentioning

confidence: 99%

IL-2 and long-term T cell activation induce physical and functional interaction between STAT5 and ETS transcription factors in human T cells

et al. 2000

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Activation of Stat5 by many cytokines implies that it cannot alone insure the speci®city of the regulation of its target genes. We have evidenced a physical and functional interaction between members of two unrelated transcription factor families, Ets-1, Ets-2 and Stat5, which could contribute to the proliferative response to interleukin 2. Competition with GAS-and EBS-speci®c oligonucleotides and immunoassays with a set of antiStat and anti-Ets families revealed that the IL-2-induced Stat5-Ets complex recognizes several GAS motifs identi®ed as target sites for activated Stat5 dimers. Coimmunoprecipitation experiments evidenced that a Stat5/Ets-1/2 complex is formed in vivo in absence of DNA. GST-pull down experiments demonstrated that the C-terminal domain of Ets-1 is su cient for this interaction in vitro. Cotransfection experiments in Kit225 T cells resulted in cooperative transcriptional activity between both transcription factors in response to a combination of IL-2, PMA and ionomycin. A Stat5-Ets protein complex was the major inducible DNAbinding complex bound to the human IL-2rE GASd/ EBSd motif in long-term proliferating normal human T cells activated by CD2 and CD28. These results suggest that the inducible Stat5-Ets protein interaction plays a role in the regulation of gene expression in response to IL-2 in human T lymphocytes.

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Assembly and function of a TCR alpha enhancer complex is dependent on LEF-1-induced DNA bending and multiple protein-protein interactions.

Cited by 522 publications

References 69 publications

Transcriptional regulation of osteopontin gene in vivo by PEBP2αA/CBFA1 and ETS1 in the skeletal tissues

Transcriptional regulation of osteopontin gene in vivo by PEBP2αA/CBFA1 and ETS1 in the skeletal tissues

Erg proteins, transcription factors of the Ets family, form homo, heterodimers and ternary complexes via two distinct domains

IL-2 and long-term T cell activation induce physical and functional interaction between STAT5 and ETS transcription factors in human T cells

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