A complex regulatory DNA element associated with a major histocompatibility complex class I gene consists of both a silencer and an enhancer.

Weissman, Jocelyn D.; Singer, Dinah S.

doi:10.1128/mcb.11.8.4217

Cited by 65 publications

(78 citation statements)

References 31 publications

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“…Tissue-specific expression is achieved through the combined effects of a promoter distal complex regulatory element and a series of promoter proximal elements. The promoter distal element, located between Ϫ700 and Ϫ800 bp, consists of overlapping enhancer and silencer elements (7). Silencer activity varies inversely with the level of class I expression in a given cell type.…”

mentioning

confidence: 99%

A T Lymphocyte-Specific Transcription Complex Containing RUNX1 Activates MHC Class I Expression

Howcroft

Weissman

Gégonne

et al. 2005

The Journal of Immunology

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MHC class I expression is subject to both tissue-specific and hormonal regulatory mechanisms. Consequently, levels of expression vary widely among tissues, with the highest levels of class I occurring in the lymphoid compartment, in T cells and B cells. Although the high class I expression in B cells is known to involve the B cell enhanceosome, the molecular basis for high constitutive class I expression in T cells has not been explored. T cell-specific genes, such as TCR genes, are regulated by a T cell enhanceosome consisting of RUNX1, CBFβ, LEF1, and Aly. In this report, we demonstrate that MHC class I gene expression is enhanced by the T cell enhanceosome and results from a direct interaction of the RUNX1-containing complex with the class I gene in vivo. T cell enhanceosome activation of class I transcription is synergistic with CIITA-mediated activation and targets response elements distinct from those targeted by CIITA. These findings provide a molecular basis for the high levels of MHC class I in T cells.

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confidence: 99%

A T Lymphocyte-Specific Transcription Complex Containing RUNX1 Activates MHC Class I Expression

Howcroft

Weissman

Gégonne

et al. 2005

The Journal of Immunology

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“…Also the PD1 silencer tends to act in an orientation-dependent manner [40]. Hence, it is not surprising that the CD46 silencer described in this report acts even on the heterologous SV40 promoter position-independently, but orientation-dependently.…”

Section: Discussionmentioning

confidence: 55%

“…The expression of these two genes are regulated tissue-specifically ; i.e. PD1 is highly expressed in the spleen, but not in the kidney [40], and TNFR2 is expressed primarily on the myeloid and lymphoid cells [41]. Interestingly, these three molecules are also expressed on macrophages and dendritic cells, and have important roles in the innate immune system.…”

Section: Discussionmentioning

confidence: 99%

“…The silencer element seems to consist of two parts, according to previous reports [40,41]. Two mutated CDPSEs (5hmut CDPSE and 3hmut CDPSE) containing nucleotide substitutions in the 5h and 3h parts were constructed (Figure 7d).…”

Section: Emsamentioning

confidence: 96%

“…A motif search revealed the presence of a silencer-binding site 2 (TATTAAAA), which is the 3h-part of the PD1 silencer (silencer sequence of the pig MHC class-I gene) in this 0.2-kb region (Figure 3). The PD1 silencer consists of two relevant sites, one 5h and one 3h [40]. The 3h site is called silencerbinding site 2 and is identical to the putative silencer of murine CD46 (Figure 6a).…”

Section: Characterization and Identification Of Putative Silencer Seqmentioning

confidence: 99%

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Identification and characterization of a silencer regulatory element in the 3′-flanking region of the murine CD46 gene

Nomura

Tsujimura

Begum

et al. 2000

Biochemical Journal

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The murine membrane cofactor protein (CD46) gene is expressed exclusively in testis, in contrast to human CD46, which is expressed ubiquitously. To elucidate the mechanism of differential CD46 gene expression among species, we cloned entire murine CD46 genomic DNA and possible regulatory regions were placed in the flanking region of the luciferase reporter gene. The reporter gene assay revealed a silencing activity not in the promoter, but in the 3´-flanking region of the gene and the silencer-like element was identified within a 0.2-kb region between 0.6 and 0.8kb downstream of the stop codon. This silencer-like element was highly similar to that of the pig MHC class-I gene. The introduction of a mutation into this putative silencer element of murine CD46 resulted in an abrogation of the silencing effect. Electrophoretic mobility-shift assay indicated the presence of the binding molecule(s) for this silencer sequence in murine cell lines and tissues. A size difference of the protein–silencer-element complex was observed depending upon the solubilizers used for preparation of the nuclear extracts. A mutated silencer sequence failed to interact with the binding molecules. The level of the binding factor was lower in the testicular germ cells compared with other organs. Thus the silencer element and its binding factor may play a role in transcriptional regulation of murine CD46 gene expression. These results imply that the effects of the CD46 silencer element encompass the innate immune and reproductive systems, and in mice may determine the testicular germ-cell-dominant expression of CD46.

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The 3′-UT of the ubiquitous mRNA of human CD46 confers selective suppression of protein production in murine cells

et al. 1999

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A complex regulatory DNA element associated with a major histocompatibility complex class I gene consists of both a silencer and an enhancer.

Cited by 65 publications

References 31 publications

A T Lymphocyte-Specific Transcription Complex Containing RUNX1 Activates MHC Class I Expression

A T Lymphocyte-Specific Transcription Complex Containing RUNX1 Activates MHC Class I Expression

Identification and characterization of a silencer regulatory element in the 3′-flanking region of the murine CD46 gene

The 3′-UT of the ubiquitous mRNA of human CD46 confers selective suppression of protein production in murine cells

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