Cited2 controls left-right patterning and heart development through a Nodal-Pitx2c pathway

Bamforth, Simon D.; Bragança, José; Farthing, Cassandra R.; Schneider, Jürgen; Broadbent, C; Michell, Anna C.; Clarke, Kieran; Neubauer, Stefan; Norris, Dominic P.; Brown, Nigel A.; Anderson, Robert H.; Bhattacharya, Shoumo

doi:10.1038/ng1446

Cited by 190 publications

(202 citation statements)

References 44 publications

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“…Cited2 acts upstream of Nodal, a member of the TGF-␤ superfamily, and is required for normal establishment of the left-right axis (14,15). Overexpression of Cited2 in Rat1 cells results in loss of cell contact inhibition, anchorage-independent growth in soft agar, and tumor formation in nude mice, suggesting that Cited2 is a transforming gene (1).…”

Section: Cited2 (Camp-responsive Element-binding Protein-binding Protmentioning

confidence: 99%

Post-transcriptional Control of Cited2 by Transforming Growth Factor β

Chou

2006

Journal of Biological Chemistry

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Cited2 is a transcription factor without typical DNA binding domains. Cited2 interacts with cAMP-responsive element-binding protein-binding protein (CBP)/p300, TFAP2, Lhx2, and nuclear receptors, such as peroxisome proliferator-activated receptor and estrogen receptor to function as a transcriptional modulator. Overexpression of Cited2 in Rat1 cells leads to tumor formation in nude mice, suggesting that Cited2 is a transforming gene. Through microarray analysis, Cited2 was found to be down-regulated by transforming growth factor ␤1 (TGF-␤) in various cell lines. In this study, we confirmed that both mRNA and protein levels of Cited2 are down-regulated in MDA-MB-231 breast cancer cells. Overexpression of Smad7 or knockdown of Smad4 in MDA-MB-231 cells showed that the Smad pathway is involved in the down-regulation of Cited2. Based on nuclear run-on analysis and Cited2 promoter/reporter assay, Cited2 transcription was not affected by TGF-␤, supporting that down-regulation of Cited2 by TGF-␤ is most likely through post-transcriptional regulation. By using transcriptional inhibitors, we demonstrated that the turnover of Cited2 transcripts appears to be accelerated during TGF-␤ stimulation. Pharmacologic inhibition of translation with cycloheximide attenuated Cited2 down-regulation by TGF-␤. We examined the expression of recombinant Cited2 gene introduced into MDA-MB-231 cells by stable transfection, and we found that mRNA containing the Cited2 protein-coding region controlled by a heterologous promoter indeed responds to TGF-␤-mediated down-regulation. Study from Cited2 deletion mutants showed that the C-terminal conserved region of Cited2 coding sequence is essential for the down-regulation. This is the first demonstration that TGF-␤-mediated down-regulation of Cited2 is post-transcriptional, through the Smad pathway, and requires the presence of its coding sequence. Cited2 (cAMP-responsive element-binding protein-binding protein (CBP)2 /p300-interacting transactivators with glutamic acid and aspartic acid-rich tail) is one of the founding members of transcriptional activators, previously named melanocyte-specific gene-related gene (MRG)1/p35srj (1-4). The members in this family function as transcriptional modulators through interaction with the p300/CBP complex (5-7). Cited2 interacts with Lhx2 to enhance the recruitment of CBP/ p300 and the TATA-binding protein leading to transcription of glycoprotein hormone ␣ subunit genes (5). On the other hand, Cited2 competes with HIF-1␣ for binding to the CH1 domain of p300, and functions as a negative modulator in the hypoxia signaling pathway (2). In addition, Cited2 interacts with TFAP2 (8) and nuclear receptors such as estrogen receptor (9) and peroxisome proliferator-activated receptor (10) to function as a transcriptional coactivator. Cited2 Ϫ/Ϫ mouse embryos die during mid-gestation with profound developmental abnormalities, including cardiac malformations, exencephaly, and adrenal agenesis (11-13). Cited2 acts upstream of Nodal, a member of the TGF-␤ superfamily, an...

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Section: Cited2 (Camp-responsive Element-binding Protein-binding Protmentioning

confidence: 99%

Post-transcriptional Control of Cited2 by Transforming Growth Factor β

Chou

2006

Journal of Biological Chemistry

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“…Further studies revealed left-right patterning defects in these embryos, especially in co-isogenic C57BL/6J backgrounds (26). Moreover, CITED2 could selectively maintain adult hemopoietic stem cell functions, at least in part via Ink4a/Arf and Trp53 (27).…”

mentioning

confidence: 92%

Negative Feedback Regulation of NF-κB Action by CITED2 in the Nucleus

Lou

Sun

Chen

et al. 2011

The Journal of Immunology

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NF-κB is a family of important transcription factors that modulate immunity, development, inflammation, and cancer. The biological activity of NF-κB is subjected to various spatial and temporal regulations. Bioinformatics analysis predicts that CITED2 is topologically close to NF-κB in the protein interaction networks. In this study, we show that ectopic expression or knockdown of CITED2 attenuates or potentiates, respectively, the expression of NF-κB–responsive genes. Mechanistically, CITED2 constitutively localizes inside the nucleus and interacts specifically with the coactivator p300. This prevents p65 from binding to p300, impairs p65 acetylation, and attenuates p65 binding to its cognate promoters. Furthermore, LPS induces CITED2 expression via NF-κB in macrophages. CITED2 sensitizes cells to TNF-α–induced apoptosis. Collectively, this study identifies CITED2 as a novel regulator of NF-κB in the nucleus, which reveals a negative feedback mechanism for NF-κB signaling.

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“…2 These initial in vitro studies underscore the potential roles of Cited2 in different biologic processes. Deletion of Cited2 gene results in embryonic lethality in the mid to late gestation with embryos displaying cardiac malformations, neural tube defects, 7 adrenal agenesis, [8][9][10] left-right patterning defects, 9,11 and placental defects. 12 Further mechanistic studies have provided evidence that Cited2 plays pivotal roles in these processes through its transcriptional modulator functions for HIF-1 8,13 or AP-2␣ signaling.…”

Section: Introductionmentioning

confidence: 99%

“…12 Further mechanistic studies have provided evidence that Cited2 plays pivotal roles in these processes through its transcriptional modulator functions for HIF-1 8,13 or AP-2␣ signaling. [9][10][11] Accumulated evidence has implicated the role of Cited2 in hematopoiesis because Bmi-1, which is essential for adult hematopoietic stem cell self-renewal, 14 is induced by Cited2 in mouse embryonic fibroblast (MEF) cells. 15 CBP and p300 are fate decision factors for HSCs, responsible for HSC self-renewal and hematopoietic differentiation, respectively.…”

Section: Introductionmentioning

confidence: 99%