Bmi1 Functions as an Oncogene Independent of Ink4A/Arf Repression in Hepatic Carcinogenesis

Xu, Cenke; Lee, Susie; Ho, Coral; Bommi, Prashant V.; Huang, Shiang; Cheung, Siu Tim; Dimri, Goberdhan P.; Chen, Xin

doi:10.1158/1541-7786.mcr-09-0333

Cited by 65 publications

(56 citation statements)

References 50 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…As a member of the polycomb group (PcG) family, Bmi-1 has an essential role in embryogenesis and regulation of cell cycle. Moreover, it serves as a pro-oncogene in tumorigenicity [39] and also contributes to the maintenance of the cancer stem cells [29,40].…”

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Hotair mediates hepatocarcinogenesis through suppressing miRNA-218 expression and activating P14 and P16 signaling

Zhu

Wang

et al. 2015

Journal of Hepatology

164

153

View full text Add to dashboard Cite

Section: Discussionmentioning

confidence: 99%

“…The two tumor suppressors play important roles in regulating cell cycle arrest and carcinogenesis. P14 ARF binds and inhibits the P53 antagonist Mdm2, leading to the accumulation of P53 [29,40]. Furthermore, P16 Ink4a is frequently inactivated in tumors and activation of P16 Ink4a -Rb signaling results in senescence [41].…”

Section: Discussionmentioning

confidence: 99%

Hotair mediates hepatocarcinogenesis through suppressing miRNA-218 expression and activating P14 and P16 signaling

Zhu

Wang

et al. 2015

Journal of Hepatology

164

153

View full text Add to dashboard Cite

“…Primary human MDMs were transfected with 100 nM scrambled or ON-TARGETplus SMARTpool siRNA against Twist1, Twist2, c-Maf, Bmi1, ATF4, C/EBPα, Runx1, Runx2, (Dharmacon, Lafayette, CO) (4 pooled siRNAs for each gene), or with 2 μg pT3-EF1a-Bmi1 (Addgene plasmid 31783 kindly deposited by X. Chen (23)), c-Maf (GeneCopoeia, Rockville, MD) or empty vector using Amaxa nucleofector technology (Amaxa, San Diego, CA).…”

Section: Methodsmentioning

confidence: 99%

Twist1 and Twist2 Contribute to Cytokine Downregulation following Chronic NOD2 Stimulation of Human Macrophages through the Coordinated Regulation of Transcriptional Repressors and Activators

Zheng

Hedl

Abraham

2015

The Journal of Immunology

View full text Add to dashboard Cite

Proper regulation of microbial-induced cytokines is critical to intestinal immune homeostasis. Acute stimulation of nucleotide-binding oligomerization domain 2 (NOD2), the Crohn’s disease–associated sensor of bacterial peptidoglycan, induces cytokines. However, chronic NOD2 stimulation in macrophages decreases cytokines upon pattern recognition receptor (PRR) restimulation; cytokine attenuation to PRR stimulation is similarly observed in intestinal macrophages. The role for the transcriptional repressors Twist1 and Twist2 in regulating PRR-induced cytokine outcomes is poorly understood and has not been reported for NOD2. We found that Twist1 and Twist2 were required for optimal cytokine downregulation during acute and, particularly, chronic NOD2 stimulation of human macrophages. Consistently, Twist1 and Twist2 expression was increased after chronic NOD2 stimulation; this increased expression was IL-10 and TGF-β dependent. Although Twist1 and Twist2 did not coregulate each other’s expression, they cooperated to enhance binding to cytokine promoters after chronic NOD2 stimulation. Moreover, Twist1 and Twist2 contributed to enhance expression and promoter binding of the proinflammatory inhibitor c-Maf and the transcriptional repressor Bmi1. Restoring c-Maf and Bmi1 expression in Twist-deficient macrophages restored NOD2-induced cytokine downregulation. Furthermore, with chronic NOD2 stimulation, Twist1 and Twist2 contributed to the decreased expression and cytokine promoter binding of the transcriptional activators activating transcription factor 4, C/EBPα, Runx1, and Runx2. Knockdown of these transcriptional activators in Twist-deficient macrophages restored cytokine downregulation after chronic NOD2 stimulation. Finally, NOD2 synergized with additional PRRs to increase Twist1 and Twist2 expression and Twist-dependent pathways. Therefore, after chronic NOD2 stimulation Twist1 and Twist2 coordinate the regulation of both transcriptional activators and repressors, thereby mediating optimal cytokine downregulation.

show abstract

“…Co-immunoprecipitation Assays-HEK293 cells were transfected with expression plasmids pCR3.1-HNF4␣ and either FLAG-MED25 or siRNA (Thermo Fisher, L-014689-01) against MED25 using Lipofectamine 2000 (Invitrogen); cells were also co-transfected with pCMVHA-EED, pCMVHAhEZH2 (26), pCMVHA-SUZ12 (27), or pT3-EF1a-BMI1 (28). Nuclear extracts were prepared as described previously (29) and immunoprecipitated with 2 g of HNF4␣ (rabbit, sc-8987, Santa Cruz Biotechnology), hemagglutinin (HA) (rat, catalog No.…”

Section: Methodsmentioning

confidence: 99%

Epigenetic Modification of Histone 3 Lysine 27

Englert

Luo

Goldstein

et al. 2015

Journal of Biological Chemistry

View full text Add to dashboard Cite

Background: Mediator subunit MED25 associates with hepatocyte nuclear factor 4␣ to initiate activation of select genes. Results: CYP2C9 activation by MED25 involves preinitiation complex formation, H3K27 acetylation, and chromatin conformation changes, and the absence of MED25 results in H3K27 trimethylation and Polycomb group recruitment. Conclusion: MED25 is a key regulator of epigenetic mechanisms. Significance: MED25 regulates human drug metabolism gene CYP2C9 by epigenetic modification.

show abstract

Bmi1 Functions as an Oncogene Independent of Ink4A/Arf Repression in Hepatic Carcinogenesis

Cited by 65 publications

References 50 publications

Hotair mediates hepatocarcinogenesis through suppressing miRNA-218 expression and activating P14 and P16 signaling

Hotair mediates hepatocarcinogenesis through suppressing miRNA-218 expression and activating P14 and P16 signaling

Twist1 and Twist2 Contribute to Cytokine Downregulation following Chronic NOD2 Stimulation of Human Macrophages through the Coordinated Regulation of Transcriptional Repressors and Activators

Epigenetic Modification of Histone 3 Lysine 27

Contact Info

Product

Resources

About