Zinc finger transcription factor 191, directly binding to β-catenin promoter, promotes cell proliferation of hepatocellular carcinoma

Liu, Guoyuan; Jiang, Songmin; Wang, Chenji; Jiang, Wei; Liu, Zulong; Liu, Chao; Saiyin, Hexige; Yang, Xiaosong; Shen, Suqin; Jiang, Deke; Zhou, Ping; Han, Dingding; Hu, Xiaohui; Yi, Qing; Liu, Yu

doi:10.1002/hep.25564

Cited by 51 publications

(72 citation statements)

References 69 publications

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“…Promoter luciferase assay indicated that the wild-type ZNF24 can increase transcription activity of CTNNB1 promoter by about 2.7 fold compared with transfecting control vector (Figure 7). This is consistent with previous reports that ZNF24 can activate β-Catenin in hepatocellular carcinoma cell lines[9]. In contrast, when the ZF region was missing, the ZNF24 mutants failed to activate the CTNNB1 promoter (Figure 7, compare dZF1-2 or p1-250 with WT).…”

Section: Discussionsupporting

confidence: 92%

“…Allelic variations of HUMTH01 are known to have a quantitative silencing effect on TH gene expression and to correlate with quantitative and qualitative changes in the binding by ZNF24[8]. ZNF24 also can directly bind to CTNNB1 promoter, and activates the expression of β-Catenin and promotes cell proliferation of hepatocellular carcinoma[9]. ZNF24 shows 94% identity to its mouse homologue Zfp191, which is the most highly conserved among the human-mouse SCAN family member orthologues pairs[10].…”

Section: Introductionmentioning

confidence: 99%

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Identification of a Functional Nuclear Localization Signal Mediating Nuclear Import of the Zinc Finger Transcription Factor ZNF24

Xia

Gong

et al. 2013

PLoS ONE

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ZNF24 is a member of the SCAN domain family of Krüppel-like zinc finger (ZF) transcription factors, which plays a critical role in cell proliferation and differentiation. However, how ZNF24 enters the nucleus in order to exert its function remains unclear since its nuclear localization signal(s) (NLS) has not been identified. Here, we generated a series of GFP-tagged deletion and point mutants and assessed their subcellular localization. Our results delimit the NLS to ZF1-2. Deletion of ZF1-2 caused cytoplasmic accumulation of ZNF24. Fusion of the ZF1-2 to green fluorescent protein (GFP) targeted GFP to the nucleus, demonstrating that the ZF1-2 is both necessary and sufficient for nuclear localization. ZNF24 containing histidine to leucine mutations that disrupt the structure of ZF1 or/and ZF2 retains appropriate nuclear localization, indicating that neither the tertiary structure of the zinc fingers nor specific DNA binding are necessary for nuclear localization. K286A and R290A mutation led to partial cytoplasmic accumulation. Co-immunoprecipitation demonstrated that ZNF24 interacted with importin-β and this interaction required the ZF motifs. The β-Catenin (CTNNB1) luciferase assays showed that the ZNF24 mutants defective in nuclear localization could not promote CTNNB1promoter activation as the wild-type ZNF24 did. Taken together, these results suggest that consecutive ZF1-2 is critical for the regulation of ZNF24 nuclear localization and its transactivation function.

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Section: Discussionsupporting

confidence: 92%

Section: Introductionmentioning

confidence: 99%

Identification of a Functional Nuclear Localization Signal Mediating Nuclear Import of the Zinc Finger Transcription Factor ZNF24

Xia

Gong

et al. 2013

PLoS ONE

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“…In fact, only a few previous studies have provided evidence for a transcriptional mechanism of β -catenin regulation. 24, 25 Here our study provides solid evidence for a transcriptional mechanism of β -catenin regulation in CRC carcinogenesis. The ChIP, EMSA and luciferase assays revealed that Elf3 could bind to the promoter of β -catenin and transactivate its transcription.…”

Section: Discussionmentioning

confidence: 55%

Elf3 drives β-catenin transactivation and associates with poor prognosis in colorectal cancer

et al. 2014

Cell Death Dis

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Aberrant regulation of the Wnt/β-catenin pathway plays important roles in colorectal carcinogenesis, with over 90% of cases of sporadic colon cancer featuring β-catenin accumulation. While ubiquitination-mediated degradation is widely accepted as a major route for β-catenin protein turnover, little is known about the regulation of β-catenin in transcriptional level. Here we show that Elf3, a member of the E-twenty-six family of transcription factors, drives β-catenin transactivation and associates with poor survival of colorectal cancer (CRC) patients. We first found recurrent amplification and upregulation of Elf3 in CRC tissues, and further Gene Set Enrichment Analysis identified significant association between Elf3 expression and activity of WNT/β-catenin pathway. Chromatin immunoprecipitation and electrophoretic mobility shift assay consistently revealed that Elf3 binds to and transactivates β-catenin promoter. Ectopic expression of Elf3 induces accumulation of β-catenin in both nucleus and cytoplasm, causing subsequent upregulation of several effector genes including c-Myc, VEGF, CCND1, MMP-7 and c-Jun. Suppressing Elf3 in CRC cells attenuates β-catenin signaling and decreases cell proliferation, migration and survival. Targeting Elf3 in xenograft tumors suppressed tumor progression in vivo. Taken together, our data identify Elf3 as a pivotal driver for β-catenin signaling in CRC, and highlight potential prognostic and therapeutic significance of Elf3 in CRC.

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“…ZNF 191 may activate the expression of β-catenin and its downstream target genes (Liu et al, 2012). β-catenin has been implicated in depression (Dias et al, 2014), glucose metabolism (Elghazi et al, 2012), and idiopathic pulmonary fibrosis (Chilosi et al, 2003).…”

Section: Discussionmentioning

confidence: 99%

Comorbidities Among Persons With Incident Psychiatric Condition

Fluegge

2016

Gerontology and Geriatric Medicine

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Objective I sought to determine how medical comorbidities co-exist with incident psychiatric condition. Method I used data from all 11 available waves (1992-2012) of the Health and Retirement Study (HRS). I identified 4,358 index participants with self-reported incident psychiatric condition. I collected comorbidity data from participants preceding, including, and succeeding that incident wave. Comorbidities assessed included high blood pressure (HBP), diabetes mellitus, cancer, lung disease, heart disease, stroke, and arthritis. Modified Poisson regression combined with log-linked binomial regression was used to estimate relative risks (RRs) of reporting a comorbidity preceding and following the incident wave. Multiple comparison testing dictated significance of RRs with p < .007. Results For the waves preceding the index wave, the RRs of reporting all comorbidities except HBP and cancer were significantly (p < .007) increased. For the waves following incident psychiatric condition, the risks of reporting heart disease, diabetes, and lung disease were significantly (p < .007) increased. These results were adjusted for participant age, race, gender, other comorbidities listed, and the wave in which a comorbidity was reported. Conclusion The bidirectional association between a psychiatric condition and medical illnesses could only be statistically confirmed for lung disease, diabetes, and heart disease. It is of interest to determine how reporting a psychiatric condition may affect the sequelae of health care use and treatment outcomes for patients with either of these comorbidities or a combination of them.

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Zinc finger transcription factor 191, directly binding to β-catenin promoter, promotes cell proliferation of hepatocellular carcinoma

Cited by 51 publications

References 69 publications

Identification of a Functional Nuclear Localization Signal Mediating Nuclear Import of the Zinc Finger Transcription Factor ZNF24

Identification of a Functional Nuclear Localization Signal Mediating Nuclear Import of the Zinc Finger Transcription Factor ZNF24

Elf3 drives β-catenin transactivation and associates with poor prognosis in colorectal cancer

Comorbidities Among Persons With Incident Psychiatric Condition

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