The Interferon-Inducible p202 Protein as a Modulator of Transcription: Inhibition of NF-κB, c-Fos, and c-Jun Activities

Wang, Min; Ghosh, Sankar; Lengyel, Péter

doi:10.1128/mcb.16.1.359

Cited by 147 publications

(159 citation statements)

References 75 publications

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“…In this model, pRB would be required to antagonize the inhibitor. One protein that could ful®ll this role is p202; it is induced by IFNs, acts as a transcriptional repressor, and interacts directly with pRB (Choubey and Lengyel, 1995;Choubey et al, 1996;Min et al, 1996). The inhibitor could also be a protein like PU.1, which speci®cally represses Ab expression by binding an element next to the Y box, and also interacts with pRB (Borras et al, 1995;Hagemeier et al, 1993).…”

Section: Discussionmentioning

confidence: 99%

pRB is required for interferon-γ-induction of the MHC class II Aβ gene

Zhu¹,

Pattenden

Bremner

1999

Oncogene

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pRB is required for IFN-g-induction of MHC class II in human tumor cell lines, providing a potential link between tumor suppressors and the immune system. However, other genes, such as cyclin D1, show pRBdependency only in tumor cells, so by analogy, pRB may not be necessary for cII-regulation in normal cells. Here, we demonstrate that induction of the mouse MHC class II I-A heterodimer is normal in RB +/+ mouse embryonic ®broblasts (MEFs), but de®cient in RB 7/7 MEFs. Inducibility is restored in RB 7/7 MEFs stably transfected with wild type RB cDNA or infected with an adenovirus expressing pRB. Thus, involvement of pRB in MHC class II expression is conserved in the mouse and is not an aberrant feature of tumorigenic, aneuploid, human tumor cells. Although cII genes are generally induced in a coordinate fashion, suggesting a common mechanism, we found that pRB was speci®cally required for induction of the Ab, but not Aa or other MHC cII genes including Eb, Ii and H2-Ma. Finally, IFN-ginduction of class II transactivator (CIITA), was pRBindependent, suggesting that pRB works downstream of this master-regulator of MHC class II expression.

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Section: Discussionmentioning

confidence: 99%

pRB is required for interferon-γ-induction of the MHC class II Aβ gene

Zhu¹,

Pattenden

Bremner

1999

Oncogene

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“…The expression of these molecules is limited to a few tissues, including subsets of hematopoietic cells and fibroblasts [40], and each is expressed in the nucleus either constitutively or inducibly after addition of IFN-␣ or -␥ [40]. The binding of p202 to cell growth regulatory proteins pRb [21] and p53 [22], and its ability to inhibit transcriptional activation through E2F [23], NF-B, c-Jun, and c-Fos [24] are clear evidence of a role in modulation of a number of generic transcriptional systems. We now have ample evidence that IFI 16 has similar properties in that it can act as a powerful transcriptional repressor in certain model systems in vitro, can bind to pRb, p53, c-Fos but not c-Jun both in vitro and in vivo, and can regulate the cell cycle [unpublished results].…”

Section: Discussionmentioning

confidence: 99%

“…The effect of p202 on transcription mediated by pRb remains to be elucidated, however, p202 can modulate E2F-mediated transcriptional activation by inhibiting sequencespecific DNA binding by E2F [23]. p202 can also associate with other growth regulatory proteins such as nuclear factor B (NF-B), c-Jun, and c-Fos both in vitro and in vivo, and can inhibit the transcriptional activity of these proteins by inhibiting their binding to DNA [24].…”

Section: Introductionmentioning

confidence: 99%

The IFN-inducible nucleoprotein IFI 16 is expressed in cells of the monocyte lineage, but is rapidly and markedly down-regulated in other myeloid precursor populations

Dawson

Elwood

Johnstone

et al. 1998

Journal of Leukocyte Biology

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“…47 IFI202 is a transcription factor that influences proliferation, survival and differentiation of B cells and induced by both IFNa and IFNg. 48 Such an example indicates the need to investigate human IFN-inducible genes as well as genes in its signaling pathway as candidates for susceptibility genes to human SLE.…”

Section: Type I Ifn In Mouse Lupus Modelsmentioning

confidence: 99%

A compass that points to lupus: genetic studies on type I interferon pathway

Kyogoku

Tsuchiya

2007

Genes Immun

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It was more than 20 years ago that patients with systemic lupus erythematosus (SLE) were first reported to display elevated serum levels of type I interferon (IFN). Since then, extensive studies revealed a crucial role for type I IFN in SLE pathogenesis. The current model proposes that small increase of type I IFN production by plasmacytoid dendritic cells (pDCs) is sufficient to induce unabated activation of immature peripheral DCs. IFN-matured DCs select and activate autoreactive T cells and B cells, rather than deleting them, resulting in peripheral tolerance breakdown, a characteristic feature of SLE. Furthermore, immune complexes provide an amplification loop to pDCs for further IFN production. In the past 5 years, high-throughput technologies such as expression profiling and single-nucleotide polymorphism (SNP) typing established the role of altered type I IFN system in SLE, and a detailed picture of its molecular mechanisms is beginning to emerge. In this review, we discuss two major lines of genetics studies on type I IFN pathway related to human SLE: (1) expression profiling of IFN-responsive genes and (2) disease-associated SNPs of IFN-related genes, especially IRF5 (IFN-regulatory factor 5). Lastly, we discuss how such genetic alterations in type I IFN pathway fit in the current model of SLE pathogenesis.

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The Interferon-Inducible p202 Protein as a Modulator of Transcription: Inhibition of NF-κB, c-Fos, and c-Jun Activities

Cited by 147 publications

References 75 publications

pRB is required for interferon-γ-induction of the MHC class II Aβ gene

pRB is required for interferon-γ-induction of the MHC class II Aβ gene

The IFN-inducible nucleoprotein IFI 16 is expressed in cells of the monocyte lineage, but is rapidly and markedly down-regulated in other myeloid precursor populations

A compass that points to lupus: genetic studies on type I interferon pathway

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