Novel Transcription Coactivator Complex Containing Activating Signal Cointegrator 1

Jung, Dong Ju; Sung, Hee Sook; Goo, Young Wha; Lee, Hyun Mi; Park, Ok Ku; Jung, Sung Yun; Lim, Janghoo; Kim, Han Jong; Lee, Soo Kyung; Kim, Tae Sung; Lee, Jae Woon; Lee, Young Chul

doi:10.1128/mcb.22.14.5203-5211.2002

Cited by 106 publications

(114 citation statements)

References 28 publications

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“…The asc-1 gene (Y53F4B.15), a homolog of human activating signal cointegrator-1 (Jung et al, 2002), showed an average 28-fold increase in tags (p < 0.001). The non-coding transcribed telomeric sequence (tts-1) transcript (F09E10.11, reported in Jones et al, 2001) was also found at higher levels (average 57 fold increase) in both daf-2 adults and dauer larvae (p < 0.001).…”

Section: Correlation Of the Sage Data With Differences In Longevitymentioning

confidence: 99%

Genes that may modulate longevity in C. elegans in both dauer larvae and long-lived daf-2 adults

Ruzanov

Riddle

Marra

et al. 2007

Experimental Gerontology

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SummaryWe used Serial Analysis of Gene Expression (SAGE) to compare the global transcription profiles of long-lived mutant daf-2 adults and dauer larvae, aiming to identify aging-related genes based on similarity of expression patterns. Genes that are expressed similarly in both long-lived types potentially define a common life-extending program. Comparison of eight SAGE libraries yielded a set of 120 genes, the expression of which was significantly different in long-lived worms versus normal adults. The gene annotations indicate a strong link between oxidative stress and life span, further supporting the hypothesis that metabolic activity is a major determinant in longevity. The SAGE data show changes in mRNA levels for electron transport chain components, elevated expression of glyoxylate shunt enzymes and significantly reduced expression for components of the TCA cycle in longer-lived nematodes. We propose a model for enhanced longevity through a cytochrome c oxidase-mediated reduction in reactive oxygen species commonly held to be a major contributor to aging.

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Section: Correlation Of the Sage Data With Differences In Longevitymentioning

confidence: 99%

Genes that may modulate longevity in C. elegans in both dauer larvae and long-lived daf-2 adults

Ruzanov

Riddle

Marra

et al. 2007

Experimental Gerontology

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“…Trip4, also called activating signal cointegrator 1 (Asc1), is a transcription coactivator of nuclear receptors that plays a pivotal role in the transactivation of NFB and AP1 (44). Trip4 also regulates androgen receptor transactivation and testicular function (45,46).…”

Section: Snail1 Induces Il-17 Expression To Inhibit Adipogenesismentioning

confidence: 99%

A Proteomic Analysis Reveals That Snail Regulates the Expression of the Nuclear Orphan Receptor Nuclear Receptor Subfamily 2 Group F Member 6 (Nr2f6) and Interleukin 17 (IL-17) to Inhibit Adipocyte Differentiation *

Peláez‐García

Barderas

Batlle

et al. 2015

Molecular & Cellular Proteomics

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Adipogenic differentiation is driven by a complex cascade of transcription factors (TFs) 1 and cell signaling molecules that lead to the expression of the master regulators CCAAT/enhancer-binding protein (C/EBP) (1) and peroxisome proliferator-activated receptor (PPAR) (2) family proteins. In a sequential process, C/EBP␦ and C/EBP␤ are initially induced and followed by C/EBP␣ and PPAR␥ expression. These two master TFs induce the final program of gene expression for adipocyte differentiation.The transcription factor Snail1 is a major inducer of the epithelial-mesenchymal transition (EMT) during embryonic development and cancer progression (3, 4). Snail1 expression is very restricted in adult individuals (5), but reappears to drive the EMT process that confers promigratory, invasive, and stem cell properties to cancer epithelial cells (4). During this process, Snail represses the expression of E-cadherin and promotes the expression of mesenchymal genes like vimenFrom the ‡Department

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“…Nowadays, ASCC1 protein is considered to establish a cross talk with Jun and NF-kB that links inflammatory to tumor suppressive/oncogenic pathways (18). However, very little is known about ASCC1 function and its role in the NF-kB pathway.…”

Section: Discussionmentioning

confidence: 99%

“…TRIP4 contains a transactivation domain with a putative zinc finger motif, which serves as a binding site for TATA-binding protein, TFIIA, SRC1, CBP/p300, and nuclear receptors (19). It also interacts with a wide range of transcription factors including serum response factor, NF-kB, and AP1, and has been shown to be part of a coactivator complex that links these factors to the transcriptional machinery (18). Overexpressed TRIP4 has been normally local- ized in the nucleus but accumulates in the cytoplasm under serumdeprived conditions (19).…”

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confidence: 99%

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A Truncated Variant of ASCC1, a Novel Inhibitor of NF-κB, Is Associated with Disease Severity in Patients with Rheumatoid Arthritis

Torices

Álvarez-Rodríguez

Grande

et al. 2015

The Journal of Immunology

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Loss of the regulatory mechanisms that avoid excessive or constitutive activation of NF-κB may be associated with chronic inflammatory disorders, including rheumatoid arthritis (RA). After massive sequencing of 158 regulators of the NF-κB pathway in RA patients, we focused on a scarcely known gene, ASCC1, and showed that it potently inhibits the expression of NF-κB target genes (TRAIL, TNF-α, cIAP-1, IL8) and blocks activation of a NF-κB–luciferase reporter construct in five different human cell lines. Therefore, ASCC1 may contribute to avoiding a pathologic activation of this transcription factor. A truncated variant of ASCC1 (p.S78*) was found in RA patients and control individuals. Functional in vitro studies revealed that truncation abrogated the NF-κB inhibition capacity of ASCC1. In contrast with full-length protein, truncated ASCC1 did not reduce the transcriptional activation of NF-κB and the secretion of TNF-α in response to inflammatory stimuli. We analyzed the clinical impact of p.S78* variant in 433 patients with RA and found that heterozygous carriers of this variant needed more disease-modifying antirheumatic drugs, and more patients with this genotype needed treatment with corticoids and biologic agents. Moreover, the truncated allele-carrier group had lower rates of remission compared with the full-length variant carriers. Overall, our findings show for the first time, to our knowledge, that ASCC1 inhibits NF-κB activation and that a truncated and inactive variant of ASCC1 is associated with a more severe disease, which could have clinical value for assessing the progression and prognosis of RA.

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Novel Transcription Coactivator Complex Containing Activating Signal Cointegrator 1

Cited by 106 publications

References 28 publications

Genes that may modulate longevity in C. elegans in both dauer larvae and long-lived daf-2 adults

Genes that may modulate longevity in C. elegans in both dauer larvae and long-lived daf-2 adults

A Proteomic Analysis Reveals That Snail Regulates the Expression of the Nuclear Orphan Receptor Nuclear Receptor Subfamily 2 Group F Member 6 (Nr2f6) and Interleukin 17 (IL-17) to Inhibit Adipocyte Differentiation *

A Truncated Variant of ASCC1, a Novel Inhibitor of NF-κB, Is Associated with Disease Severity in Patients with Rheumatoid Arthritis

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