Your search keyword '"E2F4"' showing total 33 results

1. Uncovering Novel Roles of miR-122 in the Pathophysiology of the Liver: Potential Interaction with NRF1 and E2F4 Signaling.

Author

Paluschinski, Martha, Schira-Heinen, Jessica, Pellegrino, Rossella, Heij, Lara R., Bednarsch, Jan, Neumann, Ulf P., Longerich, Thomas, Stuehler, Kai, Luedde, Tom, and Castoldi, Mirco

Subjects

*HEPATITIS B, *LIVER, *MICRORNA, *LIVER diseases, *CELLULAR signal transduction, *PROTEOMICS, *GENE expression, *GENE expression profiling, *TRANSCRIPTION factors, *CELL lines, *OXIDOREDUCTASES, *HEPATOCELLULAR carcinoma, *DISEASE complications

Abstract

Simple Summary: The microRNA miR-122 plays a crucial role in liver function, but its full impact on gene regulation and disease mechanisms remains unclear. To better understand miR-122, two different methods were used: studying its effects on translation through ribosome occupancy analysis and at the protein level. We found that miR-122 could potentially antagonize the activity of disease-related transcription factors and influence the expression of malignancy-associated proteins. Many of these proteins have been validated as novel targets of miR-122 and linked to liver disease biogenesis. In summary, this study sheds new light on the role of miR-122 by proposing a novel molecular mechanism on how disruption of this miRNA may contribute to the development of liver disease. MicroRNA miR-122 plays a pivotal role in liver function. Despite numerous studies investigating this miRNA, the global network of genes regulated by miR-122 and its contribution to the underlying pathophysiological mechanisms remain largely unknown. To gain a deeper understanding of miR-122 activity, we employed two complementary approaches. Firstly, through transcriptome analysis of polyribosome-bound RNAs, we discovered that miR-122 exhibits potential antagonistic effects on specific transcription factors known to be dysregulated in liver disease, including nuclear respiratory factor-1 (NRF1) and the E2F transcription factor 4 (E2F4). Secondly, through proteome analysis of hepatoma cells transfected with either miR-122 mimic or antagomir, we discovered changes in several proteins associated with increased malignancy. Interestingly, many of these proteins were reported to be transcriptionally regulated by NRF1 and E2F4, six of which we validated as miR-122 targets. Among these, a negative correlation was observed between miR-122 and glucose-6-phosphate dehydrogenase levels in the livers of patients with hepatitis B virus-associated hepatocellular carcinoma. This study provides novel insights into potential alterations of molecular pathway occurring at the early stages of liver disease, driven by the dysregulation of miR-122 and its associated genes. [ABSTRACT FROM AUTHOR]

Published

2023

2. Enhancer-driven transcription of MCM8 by E2F4 promotes ATR pathway activation and glioma stem cell characteristics.

Author

Sun, Yu-meng, Zhang, Yi-meng, Shi, Hai-liang, Yang, Song, Zhao, Yin-long, Liu, Hong-jiang, Li, Chen, Liu, Hong-lei, Yang, Ji-peng, Song, Jian, Sun, Guo-zhu, and Yang, Jian-kai

Subjects

*STEM cells, *GLIOMAS, *GENE expression, *GENE enhancers, *TRANSCRIPTION factors

Abstract

Background: Glioma stem cells (GSCs) are responsible for glioma recurrence and drug resistance, yet the mechanisms underlying their maintenance remains unclear. This study aimed to identify enhancer-controlled genes involved in GSCs maintenance and elucidate the mechanisms underlying their regulation. Methods: We analyzed RNA-seq data and H3K27ac ChIP-seq data from GSE119776 to identify differentially expressed genes and enhancers, respectively. Gene Ontology analysis was performed for functional enrichment. Transcription factors were predicted using the Toolkit for Cistrome Data Browser. Prognostic analysis and gene expression correlation was conducted using the Chinese Glioma Genome Atlas (CGGA) data. Two GSC cell lines, GSC-A172 and GSC-U138MG, were isolated from A172 and U138MG cell lines. qRT-PCR was used to detect gene transcription levels. ChIP-qPCR was used to detect H3K27ac of enhancers, and binding of E2F4 to target gene enhancers. Western blot was used to analyze protein levels of p-ATR and γH2AX. Sphere formation, limiting dilution and cell growth assays were used to analyze GSCs growth and self-renewal. Results: We found that upregulated genes in GSCs were associated with ataxia-telangiectasia-mutated-and-Rad3-related kinase (ATR) pathway activation, and that seven enhancer-controlled genes related to ATR pathway activation (LIN9, MCM8, CEP72, POLA1, DBF4, NDE1, and CDKN2C) were identified. Expression of these genes corresponded to poor prognosis in glioma patients. E2F4 was identified as a transcription factor that regulates enhancer-controlled genes related to the ATR pathway activation, with MCM8 having the highest hazard ratio among genes positively correlated with E2F4 expression. E2F4 bound to MCM8 enhancers to promote its transcription. Overexpression of MCM8 partially restored the inhibition of GSCs self-renewal, cell growth, and the ATR pathway activation caused by E2F4 knockdown. Conclusion: Our study demonstrated that E2F4-mediated enhancer activation of MCM8 promotes the ATR pathway activation and GSCs characteristics. These findings offer promising targets for the development of new therapies for gliomas. [ABSTRACT FROM AUTHOR]

Published

2023

3. E2F4 regulates the cell cycle and DNA replication in the silkworm, Bombyx mori.

Author

Chen, Peng, Wang, Ling, Long, Yan‐Bi, Liang, Guang‐Yan, Yang, Xiu, Dong, Zhan‐Qi, Jiang, Xia, Zhu, Yan, Pan, Min‐Hui, and Lu, Cheng

Subjects

*SILKWORMS, *DNA replication, *CELL cycle, *DNA synthesis, *GENETIC overexpression, *TRANSCRIPTION factors

Abstract

The E2F family of transcription factors is crucial for cell cycle progression and cell fate decisions. Although E2Fs have been widely studied in mammals, there have been few studies performed in insects. Here, we determined the function of E2F4 in the silkworm, Bombyx mori. We demonstrate that E2F proteins are highly conserved among species from lower animals to higher mammals. Overexpression of the BmE2F4 gene led to cell cycle arrest in the G1 phase, whereas interfering with the BmE2F4 mRNA led to accumulation of cells in the S phase. These results indicate that BmE2F4 is important in cell cycle regulation. We also demonstrate that the BmE2F4 gene is involved in DNA replication of BmN‐SWU1 cells and DNA synthesis in the silk gland. Furthermore, we identified a protein called Bm14‐3‐3ζ that can interact with BmE2F4 and allow it to localize in the nucleus. Overexpression of the Bm14‐3‐3ζ gene led to cell cycle arrest in the G1 phase, while knocking down the gene increased the proportion of cells in S phase. These findings provide important insights into the function of E2F transcription factors and increase our understanding of their involvement in cell cycle regulation. [ABSTRACT FROM AUTHOR]

Published

2022

4. E2f4 is required for intestinal and otolith development in zebrafish.

Author

Jin, Xiaolin, Liu, Junjun, Wang, Shuo, Shi, Jiale, Zhao, Chengtian, Xie, Haibo, and Kang, Yunsi

Subjects

*OTOLITHS, *BRACHYDANIO, *CILIA & ciliary motion, *INTESTINES, *GROWTH disorders, *EMBRYOLOGY, *CELL cycle

Abstract

E2f4 is a multifunctional transcription factor that is essential for many cellular processes. Although the role of E2f4 during cell cycle progression has been investigated in great detail, less is known about E2f4 during embryonic development. Here, we investigated the role of E2f4 during zebrafish development. Zebrafish e2f4 mutants displayed ectopic otolith formation due to abnormal ciliary beating in the otic vesicle. The beating defects of motile cilia were caused by abnormal expression of ciliary motility genes. The expression of two genes, lrrc23 and ccdc151, were significantly decreased in the absence of E2f4. In addition to that, e2f4 mutants also displayed growth retardation both in the body length and body weight and mostly died at around 6 months old. Although food intake was normal in the mutants, we found that the microvilli of the intestinal epithelia were significantly affected in the mutants. Finally, the intestinal epithelia of e2f4 mutants also displayed reduced cell proliferation, together with an increased level of cell apoptosis. Our data suggested a tissue‐specific role of E2f4 during zebrafish development, which is distinct from the traditional views of this protein as a transcription repressor. [ABSTRACT FROM AUTHOR]

Published

2022

5. Transcriptional regulation of multiciliated cell differentiation.

Author

Lewis, Michael and Stracker, Travis H.

Subjects

*CELLULAR control mechanisms, *CELL differentiation, *CELL cycle, *CENTRIOLES, *FLUID flow

Abstract

• GEMC1 and MCIDAS control multiciliated cell differentiation in a stepwise manner. • p73 plays a major role in multiciliogenesis. • Multiciliated cells activate a cell cycle program to regulate centriole amplification. • PLK4, mother centrioles and deuterosomes are not strictly required for multiciliogenesis. • Centriole numbers scale to cell surface area. Multiciliated cells (MCC) project dozens to hundreds of motile cilia from the cell surface to generate fluid flow across epithelial surfaces or turbulence to promote the transport of gametes. The MCC differentiation program is initiated by GEMC1 and MCIDAS, members of the geminin family, that activate key transcription factors, including p73 and FOXJ1, to control the multiciliogenesis program. To support the generation of multiple motile cilia, MCCs must undergo massive centriole amplification to generate a sufficient number of basal bodies (modified centrioles). This transcriptional program involves the generation of deuterosomes, unique structures that act as platforms to regulate centriole amplification, the reactivation of cell cycle programs to control centriole amplification and release, and extensive remodeling of the cytoskeleton. This review will focus on providing an overview of the transcriptional regulation of MCCs and its connection to key processes, in addition to highlighting exciting recent developments and open questions in the field. [ABSTRACT FROM AUTHOR]

Published

2021

6. Long non‐coding RNA LINC00337 induces autophagy and chemoresistance to cisplatin in esophageal squamous cell carcinoma cells via upregulation of TPX2 by recruiting E2F4.

Author

Yang, Chengliang, Shen, Sining, Zheng, Xiaoli, Ye, Ke, Ge, Hong, Sun, Yanan, and Lu, Yufei

Abstract

Esophageal cancer represents the eighth most frequently occurring cancer, as well as the sixth most widespread cause of cancer‐related deaths. In recent years, accumulating evidence has implicated long non‐coding RNAs in the progression of esophageal squamous cell carcinoma (ESCC). The aim of the present study was to investigate the potential involvement and underlying mechanisms of LINC00337 in ESCC. Expression patterns of LINC00337 and targeting protein for Xenopus kinesin‐like protein 2 (TPX2) in ESCC tissues and cells were detected using RT‐qPCR and immunohistochemical staining. Next, the interactions among LINC00337, E2F4, and TPX2 were identified using chromatin immunoprecipitation, dual‐luciferase reporter, and RNA‐binding protein immunoprecipitation assays, suggesting that LINC00337 could recruit E2F4 to enhance the transcription of TPX2. Thereafter, the regulatory roles of LINC00337 and TPX2 in ESCC were analyzed by altering the expression of LINC00337 or TPX2 in ESCC cells following treatment with cisplatin (DDP). The levels of autophagy‐related proteins Beclin1 and LC3II/LC3I, viability, autophagy, apoptosis, and chemoresistance of ESCC cells to DDP were measured following transfection treatment with different plasmids. Additionally, the role of the LINC00337/E2F4/TPX2 axis was assessed in vivo by measuring tumor formation in nude mice. The results demonstrated that LINC00337 upregulated TPX2, consequently leading to elevated levels of Beclin1 and LC3II/LC3I, promoted cell viability and autophagy, while inhibiting apoptosis and chemosensitivity to DDP in ESCC. In sum, the current study evidenced that the overexpression of LINC00337 could potentially enhance ESCC cell autophagy and chemoresistance to DDP via the upregulation of TPX2 by recruiting E2F4. Thus, LINC00337 may serve as a potential candidate for the treatment of ESCC. [ABSTRACT FROM AUTHOR]

Published

2020

7. Transcription factor E2F4 is a positive regulator of milk biosynthesis and proliferation of bovine mammary epithelial cells.

Author

Zhen, Zhen, Zhang, Minghui, Yuan, Xiaohan, and Li, Meng

Subjects

*PROLACTIN, *TRANSCRIPTION factors, *EPITHELIAL cells, *BIOSYNTHESIS, *SMALL interfering RNA, *MESSENGER RNA

Abstract

The transcription factor E2F4 is a key determinant of cell differentiation and cell‐cycle progression, but its function and regulatory mechanism are not completely understood. Here, we report that E2F4 acts as a positive regulator of the biosynthesis of milk components and proliferation of bovine mammary epithelial cells (BMECs). Overexpression of E2F4 in BMECs resulted in the upregulation of β‐casein, triglyceride, and lactose levels and increased cell proliferation, whereas E2F4 knockdown by small interfering RNA had the opposite effects. We further detected that overexpression of E2F4 significantly increased the messenger RNA expression of mTOR, SREBP‐1c, and Cyclin D1, and increased protein levels of SREBP‐1c, and Cyclin D1, and the ratio of p‐mTOR/mTOR, whereas E2F4 knockdown had the opposite effects. E2F4 was almost entirely located in the nucleus, and we further identified, via ChIP‐qPCR analysis, that mTOR, SREBP‐1c, and Cyclin D1 were E2F4 target genes, and exogenous administration of methionine, leucine, β‐estradiol, and prolactin markedly increased the protein levels of E2F4 and its binding to the promoters of these three genes. In summary, our data reveal that E2F4 responds to extracellular stimuli and regulates the expression of mTOR, SREBP‐1c, and Cyclin D1 for milk biosynthesis and proliferation of BMECs. [ABSTRACT FROM AUTHOR]

Published

2020

8. Association of overexpressed MYC gene with altered PHACTR3 and E2F4 genes contributes to non-small cell lung carcinoma pathogenesis.

Author

Dragoj, Miodrag, Bankovic, Jasna, Podolski-Renic, Ana, Buric, Sonja Stojkovic, Pesic, Milica, Tanic, Nikola, and Stankovic, Tijana

Subjects

*GENE amplification, *MYC oncogenes, *GENES

Abstract

C-Myc is one of the major cellular oncogenes overexpressed in non-small cell lung carcinoma (NSCLC). Its deregulated expression is necessary but not sufficient for malignant transformation. We evaluated expression of MYC gene in NSCLC patients and its association with alterations in the genes previously identified to be related to NSCLC pathogenesis, PHACTR3 and E2F4. We analyzed MYC gene expression by qRT-PCR in 30 NSCLC patients' samples and paired normal lung tissue. MYC expression was further statistically evaluated in relation to histopathological parameters, PHACTR3 and E2F4 gene alterations and survival. Alterations in aforementioned genes were previously detected and identified based on AP-PCR profiles of paired normal and tumor DNA samples, selection of DNA bands with altered mobility in tumor samples and their characterization by the reamplification, cloning and sequencing. MYC expression was significantly increased in NSCLC samples and its overexpression significantly associated with squamous cell carcinoma subtype. Most importantly, MYC overexpression significantly coincided with mutations in PHACTR3 and E2F4 genes, in group of all patients and in squamous cell carcinoma subtype. Moreover, patients with jointly overexpressed MYC and altered PHACTR3 or E2F4 showed trend of shorter survival. Overall, MYC is frequently overexpressed in NSCLC and it is associated with mutated PHACTR3 gene, as well as mutated E2F4 gene. These joint gene alterations could be considered as potential molecular markers of NSCLC and its specific subtypes. [ABSTRACT FROM AUTHOR]

Published

2019

9. Competitive regulation by transcription factors and DNA methylation in the bovine SIRT5 promoter: Roles of E2F4 and KLF6.

Author

Hong, Jieyun, Wang, Xiaoyu, Mei, Chugang, and Zan, Linsen

Subjects

*DNA methylation, *TRANSCRIPTION factors, *NICOTINAMIDE, *DINUCLEOTIDES, *LUCIFERASES, *IMMUNOPRECIPITATION

Abstract

Abstract Sirtuin 5 (SIRT5) belongs to the mitochondrial sirtuin family, which constitutes a highly conserved family of nicotinamide adenine dinucleotide NAD+-dependent deacetylases and ADP-ribosyltransferases that play important regulatory roles in stress resistance and metabolic homeostasis. SIRT5 was shown to have deacetylase, desuccinylase, and demalonylase activities. However, the mechanisms regulating SIRT5 transcription remain unclear. To explore the molecular regulation of bovine SIRT5 expression, we obtained a 500-base pair fragment of the 5′-regulatory region of bovine SIRT5 by molecular cloning, which contained a region with 3 CpG islands. Electrophoretic mobility shift assays and luciferase reporter assays revealed the E2F transcription factor 4 (E2F4) and Kruppel-like factor 6 (KLF6) binding sites as transcriptional activators or repressors in the promoter region of SIRT5. We further verified that E2F4 and KLF6 bind to the SIRT5 promoter by chromatin immunoprecipitation assays. Additionally, methylation and luciferase report assays showed that SIRT5 promoter activity was enhanced by demethylation, and transcriptional activation by E2F4 and transcriptional inhibition by KLF6 of SIRT5 expression was strengthened by demethylation during adipocytes differentiation. This study focused on the mechanism underlying the methylation and transcriptional regulation of SIRT5 expression in bovine adipocytes. Highlights • SIRT5 plays important regulatory roles in stress resistance and metabolic homeostasis. • The transcription factor binding sites of E2F4 and KLF6 contain two methylation sites. • E2F4 is transcriptional activator of SIRT5 promoter activity. • KLF6 is transcriptional inhibitor of SIRT5 promoter activity. • Demethylation significantly enhanced the binding of E2F4 and KLF6 to SIRT5 promoter. [ABSTRACT FROM AUTHOR]

Published

2019

10. Stable overexpression of p130/E2F4 affects the multipotential abilities of bone‐marrow‐derived mesenchymal stem cells.

Author

Zhang, Xiwen, Chen, Jianxiao, Liu, Airan, Xu, Xiuping, Xue, Ming, Xu, Jingyuan, Yang, Yi, Qiu, Haibo, and Guo, Fengmei

Subjects

*MESENCHYMAL stem cells, *CELL cycle, *STEM cells, *CELL differentiation, *CELL proliferation, *GENE expression

Abstract

Bone‐marrow‐derived mesenchymal stem cells (MSCs) have great potential in transplantation medicine due to their multiple advantages. However, the controlled differentiation of MSCs is one of the key aspects of effective clinical transplantation. Growing evidence suggests that the cell cycle plays an important role in regulating differentiation, while p130 and E2F4 are key to cell cycle checkpoints. The aim of the study is to evaluate the effects and mechanism of p130/E2F4 on the multidifferentiation of MSCs. Our data showed that the transduction efficiencies of p130 or E2F4 mediated by lentiviral vectors were 80.3%–84.4%. p130 and E2F4 mRNA expression was significantly higher in MSC‐p130 and MSC‐E2F4 cells than in MSC normal control (NC) cells. Similar results were also observed for p130 and E2F4 protein expression. After osteogenic or adipogenic differentiation, the G1 phase was significantly delayed in the MSC‐p130 and MSC‐E2F4 groups compared with that in the MSC‐NC group. However, the G1 phase in the MSC‐p130 and MSC‐E2F4 groups did the opposite after chondrogenic differentiation. Moreover, overexpressing p130 or E2F4 significantly improved osteogenic differentiation while inhibiting adipogenic and chondrogenic differentiation of mouse MSCs (mMSCs). Moreover, overexpressing p130 or E2F4 significantly improved migration but not proliferation of mMSCs. Our data suggest that cell cycle regulation may be involved in p130/E2F4‐mediated changes in the multipotential abilities of bone‐marrow‐derived mMSCs. The controlled differentiation of mesenchymal stem cells (MSCs) is one of the key aspects of effective clinical transplantation. Growing evidence suggests that the cell cycle plays an important role in regulating differentiation, while p130 and E2F4 are key to cell cycle checkpoints. Our data suggest that cell cycle regulation may be involved in p130/E2F4‐mediated changes in the multipotential abilities of bone‐marrow‐derived mouse MSCs (mMSCs). [ABSTRACT FROM AUTHOR]

Published

2018

11. Distinct requirements of E2f4 versus E2f5 activity for multiciliated cell development in the zebrafish embryo.

Author

Chong, Yan Ling, Zhang, Yiliu, Zhou, Feng, and Roy, Sudipto

Subjects

*LOGPERCH, *DNA-binding proteins, *KIDNEY tubules, *PLACODES, *NUCLEAR proteins

Abstract

Abstract Multiciliated cells (MCCs) differentiate arrays of motile cilia that beat to drive fluid flow over epithelia. Recent studies have established two Geminin family coiled-coil containing nuclear regulatory proteins, Gmnc and Multicilin (Mci), in the specification and differentiation of the MCCs. Both Gmnc and Mci are devoid of a DNA binding domain: they regulate transcription by associating with E2f family transcription factors, notably E2f4 and E2f5. Here, we have studied the relative contribution of these two E2f factors in MCC development using the zebrafish embryo, which differentiates MCCs within kidney tubules and the nose. We found that while E2f4 is fully dispensable, E2f5 is essential for MCCs to form in the kidney tubules. Moreover, using a variety of double mutant combinations we show that E2f5 has a more prominent role in MCC development in the zebrafish than E2f4. This contrasts with current evidence from the mouse, where E2f4 seems to be more important. Thus, distinct combinatorial activities of the E2f4 and E2f5 proteins regulate the specification and differentiation of MCCs in zebrafish and mice. Highlights • Both E2f4 and E2f5 contribute to multiciliated cell (MCC) formation in zebrafish. • In contrast to mice, E2f5 has a more important role in zebrafish MCC development. • Relative contribution of the E2fs is distinct between pronephros and nasal placode. • The master regulator for MCC development, Gmnc, interacts with both E2f4 and E2f5. [ABSTRACT FROM AUTHOR]

Published

2018

12. Interfering with Dusp2 alleviates high glucose-induced vascular endothelial cell dysfunction by promoting p38 MAPK pathway activation.

Author

Jiang, Xinmiao, Yan, Qiong, He, Jiaqi, Zheng, Zeqi, Peng, Xiaoping, Cao, Xiaoyan, Zhou, Fangbin, Nie, Jungang, and Kang, Ting

Subjects

*VASCULAR endothelial cells, *ENDOTHELIUM diseases, *MITOGEN-activated protein kinases, *ENDOTHELIAL cells, *PERFUSION imaging, *BLOOD flow, *HYPERGLYCEMIA, *VASCULAR cell adhesion molecule-1

Abstract

Hyperglycemia-induced vascular endothelial cell dysfunction is a major factor contributing to diabetic lower extremity ischemia. We intend to investigate the role of Dusp2 in hyperglycemia-induced vascular endothelial cell dysfunction and related mechanisms. The human umbilical vein endothelial cells (HUVECs) were treated with high glucose (HG) as the cell model. Streptozotocin injection was performed to induce diabetes and femoral artery ligation was to induce hind limb ischemia in mice. The levels of Dusp2, p-p38 MAPK, E2F4, and p38 MAPK were evaluated by Western blot or quantitative real-time PCR. The laser Doppler perfusion imaging was conducted to measure blood flow recovery. The cell counting kit-8, transwell, and tube formation assay were performed to evaluate cell proliferation, migration, and angiogenesis, respectively. CD31 immunohistochemical staining was carried out to detect the capillary density of gastrocnemius. The dual-luciferase reporter gene assay and Chromatin immunoprecipitation assay were executed to explore the interaction between E2F4 and Dusp2. Dusp2 was highly expressed in HG-induced HUVECs and diabetic lower extremity ischemia model mice. Interference with Dusp2 promoted cell proliferation, migration, and angiogenesis, as well as alleviated mouse diabetic hindlimb ischemia. Dusp2 knockdown up-regulated p-p38 MAPK levels. We verified the binding between E2F4 and Dusp2. Overexpressing E2F4 suppressed Dusp2 levels and promoted cell proliferation, migration, and angiogenesis, co-overexpression of Dusp2 reversed the results. Overexpressing E2F4 promotes endothelial cell proliferation, migration, and angiogenesis by inhibiting Dusp2 expression and activating p38 MAPK to alleviate vascular endothelial cell dysfunction under HG stimulation. HG down-regulates the expression of E2F4 and up-regulates DUSP2, thereby inhibiting the activation of the p38 MAPK pathway, resulting in the inhibition of endothelial cell proliferation, migration, and angiogenesis. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

13. Interplay between NRF1, E2F4 and MYC transcription factors regulating common target genes contributes to cancer development and progression.

Author

Bhawe, Kaumudi and Roy, Deodutta

Subjects

*TRANSCRIPTION factors, *CANCER invasiveness, *MITOCHONDRIA, *APOPTOSIS, *CANCER cell proliferation

Abstract

Background: Nuclear respiratory factor 1 (NRF1), historically perceived as a protein regulating genes controlling mitochondrial biogenesis, is now widely recognized as a multifunctional protein and as a key player in the transcriptional modulation of genes implicated in various cellular functions. Here, we present emerging data supporting novel roles of NRF1 in cancer development and progression through its interplay with the transcription factors E2F4 and MYC. To identify common human NRF1, E2F4 and MYC target genes, we analyzed the Encyclopedia of DNA Elements (ENCODE) NRF1 ChIP-Seq data. By doing so, we identified 9253 common target genes with NRF1, E2F4 and MYC binding motifs. NRF1 binding motifs were found to be present in genes operating in signaling pathways governing all hallmarks of malignant transformation and progression, including proliferation, invasion, self-renewal and apoptosis.Conclusions: In addition to controlling mitochondrial biogenesis NRF1, in conjunction with E2F4 and MYC, may play a critical role in the acquisition of human cancer characteristics. Additionally, NRF1 may orchestrate both MYC and E2F4 to regulate common target genes linked to multiple networks in the development and progression of cancer. A comprehensive understanding of this dynamic interplay will set the stage, not only for the design of novel treatment strategies, but also for the discovery of pan-cellular transcription factor regulatory strategies to predict cancer risk, therapy response and patient prognosis. [ABSTRACT FROM AUTHOR]

Published

2018

14. The von Hippel Lindau tumour suppressor gene is a novel target of E2F4-mediated transcriptional repression in preeclampsia.

Author

Garcia, Julia, Alahari, Sruthi, Caniggia, Isabella, and Post, Martin

Subjects

*TUMOR suppressor proteins, *DNA methylation, *PREECLAMPSIA, *TRANSFORMING growth factors, *RENAL cell carcinoma

Abstract

The von Hippel Lindau tumour suppressor (VHL) protein is essential for proper placental development and is downregulated in preeclampsia (PE), a devastating disorder of pregnancy typified by chronic hypoxia. To date, knowledge on VHL genetic and epigenetic regulation is restricted to inactivating mutations and loss-of-heterozygosity in renal cell carcinomas. Herein, we sought to examine whether VHL DNA is subject to differential methylation, and if so, whether it is altered in early-onset PE ( E -PE). Sodium bisulfite modification and methylation-specific PCR analysis revealed that VHL is subject to extensive methylation in a CpG-rich region within its promoter in the human placenta. Notably, we detected significant differences in methylation in E -PE placentae relative to normotensive age-matched controls at key transcription factor binding sites, including that of the transcriptional repressor E2F4. Treatment of JEG3 cells with 5-Aza-2′-deoxycytidine, revealed that loss of DNA methylation promoted VHL transcription by attenuating VHL association with E2F4. RNAi knockdown of E2F4 in vitro confirmed its function on VHL repression. Exposure of JEG3 cells to transforming growth factor beta (TGFβ) downregulated VHL mRNA. In line with elevated levels of TGFβ3 in E -PE, chromatin immunoprecipitation assays revealed that E2F4- VHL association was enhanced upon TGFβ3 treatment, indicative of VHL transcriptional inhibition. In line with decreased VHL expression in E -PE, augmented E2F4- VHL association was also observed in E -PE placental tissue relative to controls. In conclusion, we demonstrate for the first time that hypomethylation of VHL DNA at a key transcription factor binding site has significant consequences for its transcriptional repression in early-onset preeclampsia. [ABSTRACT FROM AUTHOR]

Published

2018

15. MiR-17-5p enhances pancreatic cancer proliferation by altering cell cycle profiles via disruption of RBL2/E2F4-repressing complexes.

Author

Zhu, Youwei, Gu, Jiangning, Li, Ying, Peng, Chenghong, Shi, Minmin, Wang, Xuelong, Wei, Gang, Ge, Ouyang, Wang, Di, Zhang, Bosen, Wu, Jian, Zhong, Yiming, Shen, Baiyong, and Chen, Hao

Subjects

*PANCREATIC cancer, *CELL proliferation, *CELL cycle, *RETINOBLASTOMA protein, *MICRORNA, *RNA physiology, *ADENOCARCINOMA, *CELL lines, *CELL physiology, *PANCREATIC tumors, *PROTEINS, *DUCTAL carcinoma

Abstract

The members of the miR-17-92 cluster are upregulated in various cancers and function as a cluster of oncogenic miRNA. Our study characterized a new function of miR-17-5p, a member of the miR-17-92 cluster, in regulating cell proliferation in pancreatic cancer. Our results indicate that miR-17-5p was up-regulated in pancreatic adenocarcinoma and directly targeted the retinoblastoma-like protein 2 (RBL2), a tumor suppressor belonging to the Rb family. High levels of miR-17-5p and low levels of RBL2 were associated with poor prognosis. RBL2 interacted with the transcription factor E2F4 and bound to the promoter regions of the E2F target genes. Disruption of the RBL2/E2F4 complex by miR-17-5p overexpression shifted the activity of E2F from gene repressing to gene activating, which induced cell cycle entry and proliferation. These results suggest that miR-17-5p promoted proliferation in pancreatic ductal adenocarcinoma cells (PDAC), and altered cell cycle profiles in vivo and in vitro, by disrupting the RBL2/E2F4-associated gene repressing complexes via direct targeting of RBL2. The new regulatory network, involving miR-17-5p and RBL2, emerges as a new target of PDAC treatment. [ABSTRACT FROM AUTHOR]

Published

2018

16. The E2F4 prognostic signature predicts pathological response to neoadjuvant chemotherapy in breast cancer patients.

Author

Mark, Kenneth M. K., Varn, Frederick S., Ung, Matthew H., Feng Qian, Chao Cheng, Qian, Feng, and Cheng, Chao

Subjects

*BREAST cancer patients, *ADJUVANT treatment of cancer, *CANCER chemotherapy, *BREAST cancer treatment, *GENE expression profiling, *ONCOLOGY, *ESTROGEN receptors, *PROTEIN analysis, *PROTEIN metabolism, *BREAST tumors, *COMBINED modality therapy, *DATABASES, *PROGNOSIS, *PROTEINS, *RESEARCH funding, *RECEIVER operating characteristic curves

Abstract

Background: Neoadjuvant chemotherapy is a key component of breast cancer treatment regimens and pathologic complete response to this therapy varies among patients. This is presumably due to differences in the molecular mechanisms that underlie each tumor's disease pathology. Developing genomic clinical assays that accurately categorize responders from non-responders can provide patients with the most effective therapy for their individual disease.Methods: We applied our previously developed E2F4 genomic signature to predict neoadjuvant chemotherapy response in breast cancer. E2F4 individual regulatory activity scores were calculated for 1129 patient samples across 5 independent breast cancer neoadjuvant chemotherapy datasets. Accuracy of the E2F4 signature in predicting neoadjuvant chemotherapy response was compared to that of the Oncotype DX and MammaPrint predictive signatures.Results: In all datasets, E2F4 activity level was an accurate predictor of neoadjuvant chemotherapy response, with high E2F4 scores predictive of achieving pathologic complete response and low scores predictive of residual disease. These results remained significant even after stratifying patients by estrogen receptor (ER) status, tumor stage, and breast cancer molecular subtypes. Compared to the Oncotype DX and MammaPrint signatures, our E2F4 signature achieved similar performance in predicting neoadjuvant chemotherapy response, though all signatures performed better in ER+ tumors compared to ER- ones. The accuracy of our signature was reproducible across datasets and was maintained when refined from a 199-gene signature down to a clinic-friendly 33-gene panel.Conclusion: Overall, we show that our E2F4 signature is accurate in predicting patient response to neoadjuvant chemotherapy. As this signature is more refined and comparable in performance to other clinically available gene expression assays in the prediction of neoadjuvant chemotherapy response, it should be considered when evaluating potential treatment options. [ABSTRACT FROM AUTHOR]

Published

2017

17. Dietary myo-inositol modulates immunity through antioxidant activity and the Nrf2 and E2F4/cyclin signalling factors in the head kidney and spleen following infection of juvenile fish with Aeromonas hydrophila.

Author

Jiang, Wei-Dan, Hu, Kai, Liu, Yang, Jiang, Jun, Wu, Pei, Zhao, Juan, Zhang, Yong-An, Zhou, Xiao-Qiu, and Feng, Lin

Subjects

*ANTIOXIDANTS, *INOSITOL, *AEROMONAS hydrophila, *INFECTION, *MALONDIALDEHYDE

Abstract

This study was conducted to investigate the effects of the dietary vitamin myo -inositol (MI), on the immunity and structural integrity of the head kidney and spleen following infection of fish with the major freshwater pathogen bacterial Aeromonas hydrophila . The results demonstrated for the first time that MI deficiency depressed the lysozyme and acid phosphatase (ACP) activities and the complement 3 (C3) and C4 contents in the head kidney and spleen compared with the optimal MI levels, indicating that MI deficiency decreased the immunity of these important fish immune organs. The depression in immunity due to MI deficiency was partially related to oxidative damage [indicated by increases in the malondialdehyde (MDA) and protein carbonyl (PC) contents] that was in turn partially due to the decreased glutathione (GSH) content and the disturbances in antioxidant enzyme activities [total superoxide dismutase (T-SOD), CuZnSOD, MnSOD, catalase (CAT), glutathione peroxidase (GPx) and glutathione reductase (GR)]. MI deficiency inhibited the antioxidant-related gene transcription [CuZnSOD, MnSOD, CAT, GPx1a, GR and NF-E2-related factor 2 (Nrf2)] in the head kidney and spleen following infection of the fish with A. hydrophila . The oxidative damage due to MI deficiency also resulted in the inhibition of proliferation-associated signalling (cyclin D1, cyclin A, cyclin E and E2F4). Thus, MI deficiency partially inhibited damage repair. Excessive MI exhibited negative effects that were similar to MI deficiency, whereas the optimal MI content reversed those indicators. These observations indicated that an MI deficiency or excess could cause depression of the immune system that might be partially related to oxidative damage, antioxidant disturbances, and the inhibition of the proliferation-associated signalling in the head kidney and spleen following infection of fish with A. hydrophila . Finally, the optimal MI levels were 660.7 (based on ACP) and 736.8 mg kg −1 diet (based on MDA) in the head kidney and 770.5 (based on ACP) and 766.9 mg kg −1 diet (based on MDA) in the spleen of juvenile Jian carp. [ABSTRACT FROM AUTHOR]

Published

2016

18. Anti-apoptotic function of the E2F transcription factor 4 (E2F4)/p130, a member of retinoblastoma gene family in cardiac myocytes

Author

Dingar, Dharmendra, Konecny, Filip, Zou, Jian, Sun, Xuetao, and von Harsdorf, Rüdiger

Subjects

*APOPTOSIS inhibition, *TRANSCRIPTION factors, *RETINOBLASTOMA, *CELL cycle regulation, *HEART cells, *HYPOXEMIA, *HISTONE deacetylase

Abstract

Abstract: The E2F4–p130 transcriptional repressor complex is a cell-cycle inhibitor in mitotic cells. However, the role of E2F4/p130 in differentiated cells is largely unknown. We investigated the role of E2F4/p130 in the regulation of apoptosis in postmitotic cardiomyocytes. Here we demonstrate that E2F4 can inhibit hypoxia-induced cell death in isolated ventricular cardiomyocytes. As analyzed by chromatin immunoprecipitation, the E2F4–p130-repressor directly blocks transcription of essential apoptosis-related genes, E2F1, Apaf-1, and p73α through recruitment of histone deacetylase 1 (HDAC1). In contrast, diminution of the E2F4–p130–HDAC1-repressor and recruitment of E2F1 and histone acetylase activity to these E2F-regulated promoters is required for the execution of cell death. Expression of kinase-dead HDAC1.H141A or HDAC-binding deficient p130ΔHDAC1 abolishes the antiapoptotic effect of E2F4. Moreover, histological examination of E2F4−/− hearts revealed a markedly enhanced degree of cardiomyocyte apoptosis. Taken together, our genetic and biochemical data delineate an essential negative function of E2F4 in cardiac myocyte apoptosis. [Copyright &y& Elsevier]

Published

2012

19. E2F4 is required for cardiomyocyte proliferation.

Author

Van Amerongen, Machteld J., Diehl, Florian, Novoyatleva, Tatyana, Patra, Chinmoy, and Engel, Felix B.

Subjects

*HEART cells, *CELL proliferation, *TRANSCRIPTION factors, *CELL cycle, *CELL culture

Abstract

Aims: Although the fundamental role of the E2F transcription factor family in cell proliferation is well established, the specific function of E2F4 is unclear. On the basis of findings from cell culture experiments, E2F4 is generally considered as an inhibitor of cell proliferation. Accumulating evidence suggests, however, that E2F4 acts as an activator of cell proliferation in certain contexts. Here, we have investigated the role of E2F4 during heart development and in proliferating cardiomyocytes. Methods and results: Nuclear E2F4 expression in cardiomyocytes declined during mouse heart development, which correlates with the loss of proliferative capacity of cardiomyocytes. Re-induction of proliferation in postnatal cardiomyocytes increased nuclear E2F4 expression. E2F4 accumulated in the nucleus at the end of the S phase, remained nuclear during mitosis, and disappeared at the end of cytokinesis. siRNA-mediated inhibition of E2F4 in proliferating postnatal cardiomyocytes resulted in a significant reduction in mitosis, but not in DNA synthesis. Co-staining of E2F4 and Crest revealed that E2F4 co-localizes with kinetochores. Moreover, chromatin immunoprecipitation showed that E2F4 binds to centromeric α-satellite DNA during mitosis. Conclusion: Our data indicate that E2F4 is required for cardiomyocyte proliferation and suggest a function for E2F4 in mitosis. [ABSTRACT FROM PUBLISHER]

Published

2010

20. A structural pocket mutation of pRb increases its affinity for E2F4, which is coupled with activation of muscle differentiation.

Author

Popov, B. V., Watt, S. M., Rosanov, J. M., and Chang, L.-S.

Subjects

*NEUROBLASTOMA, *NERVOUS system tumors, *CANCER cells, *RETINOBLASTOMA, *TRANSCRIPTION factors

Abstract

Coordination of proliferation and differentiation in cells committed to muscle fate requires the interaction of the retinoblastoma gene product (pRb) with transcription factors of the E2F family, pRb having different affinities for distinct E2Fs. It was found that pRb carrying a small deletion at the end of the T antigen-binding region (ΔS/N) and unable to interact with the SV40 large T antigen could induce an acute cell cycle block, stable prolongation of the cell cycle in G0/G1 and G2/M phases, and suppression of the growth of tumor cells. ΔS/N showed increased affinity for E2F4, bound hyperphosphorylated forms of E2F4, and induced its nuclear compartmentalization. The ability of ΔS/N to form complexes with E2F4 on DNA was associated with an increased formation of “free” E2F4 and trans-suppression of a specific reporter through preferential binding to E2F4, but not to E2F1. Stable expression of ΔS/N in multipotent fibroblasts promoted early muscle commitment. It was assumed that a mutation in the T antigen-binding region increases pRb affinity for E2F4 combined with activation of muscle differentiation. [ABSTRACT FROM AUTHOR]

Published

2010

21. E2F4 cooperates with pRB in the development of extra-embryonic tissues

Author

Lee, Eunice Y., Yuan, Tina L., Danielian, Paul S., West, Julie C., and Lees, Jacqueline A.

Subjects

*TRANSCRIPTION factors, *DEVELOPMENTAL biology, *RETINOBLASTOMA, *TUMOR suppressor genes, *APOPTOSIS, *TISSUES, *EMBRYOLOGY, *LABORATORY mice

Abstract

Abstract: The retinoblastoma gene, RB-1, was the first identified tumor suppressor. Rb−/− mice die in mid-gestation with defects in proliferation, differentiation and apoptosis. The activating E2F transcription factors, E2F1–3, contribute to these embryonic defects, indicating that they are key downstream targets of the retinoblastoma protein, pRB. E2F4 is the major pRB-associated E2F in vivo, yet its role in Rb−/− embryos is unknown. Here we establish that E2f4 deficiency reduced the lifespan of Rb−/− embryos by exacerbating the Rb mutant placental defect. We further show that this reflects the accumulation of trophectoderm-like cells in both Rb and Rb;E2f4 mutant placentas. Thus, Rb and E2f4 play cooperative roles in placental development. We used a conditional mouse model to allow Rb−/−;E2f4−/− embryos to develop in the presence of Rb wild-type placentas. Under these conditions, Rb−/−;E2f4−/− mutants survived to birth. These Rb−/−;E2f4−/− embryos exhibited all of the defects characteristic of the Rb and E2f4 single mutants and had no novel defects. Taken together, our data show that pRB and E2F4 cooperate in placental development, but play largely non-overlapping roles in the development of many embryonic tissues. [Copyright &y& Elsevier]

Published

2009

22. Dysfunctional memory CD8+ T cells after priming in the absence of the cell cycle regulator E2F4

Author

Bancos, Simona, Cao, QingYu, Bowers, William J., and Crispe, Ian Nicholas

Subjects

*T cells, *LYMPHOCYTES, *EPITHELIAL cells, *VIRUS diseases

Abstract

Abstract: The transcriptional repressor E2F4 is important for cell cycle exit and terminal differentiation in epithelial cells, neuronal cells and adipocytes but its role in T lymphocytes proliferation and memory formation is not known. Herein, we investigated the function of E2F4 protein for the formation of functional murine memory T cells. Murine transgenic CD8+ T cells were infected in vitro with lentivirus vector expressing a shRNA targeted against E2F4 followed by in vitro stimulation with SIINFEKL antigenic peptide. For in vivo assays, transduced cells were injected into congenic mice which were then infected with HSV-OVA. The primary response, memory formation and secondary stimulation were determined for CD8+ lentivirus transduced cells. In the absence of E2F4 cell cycle repressor, activated CD8+ T cells underwent intensive proliferation in vitro and in vivo. These cells had the ability to differentiate into memory cells in vivo, but they were defective in recall proliferation. We show that transient suppression of E2F4 during CD8+ T cell priming enhances primary proliferation and has a negative effect on secondary stimulation. These findings demonstrate that the cell cycle repressor E2F4 is essential for the formation of functional memory T cells. A decrease in CD8+ T-lymphocyte compartment would diminish our capacity to control viral infections. [Copyright &y& Elsevier]

Published

2009

23. Inhibition of pituitary tumors in Rb mutant chimeras through E2f4 loss reveals a key suppressive role for the pRB/E2F pathway in urothelium and ganglionic carcinogenesis.

Author

Parisi, T., Bronson, R. T., and Lees, J. A.

Subjects

*GENETIC toxicology, *CELL proliferation, *RETINOBLASTOMA, *PSEUDOGLIOMA, *CELL populations

Abstract

The retinoblastoma protein pRB suppresses tumorigenesis largely through regulation of the E2F transcription factors. E2F4, the most abundant E2F protein, is thought to act in cooperation with pRB to restrain cell proliferation. In this study, we analyse how loss of E2f4 affects the tumorigenicity of pRB-deficient tissues. As Rb−/−;E2f4−/− germline mice die in utero, we generated Rb−/−;E2f4−/− chimeric animals to allow examination of adult tumor phenotypes. We found that loss of E2f4 had a differential effect on known Rb-associated neuroendocrine tumors. It did not affect thyroid and adrenal glands tumors but partially suppressed lung neuroendocrine hyperplasia. The most striking effect was in the pituitary where E2F4 loss delayed the development, and reduced the incidence, of Rb mutant tumors. This tumor suppression increased the longevity of the Rb−/−;E2f4−/− chimeric animals allowing us to identify novel tumor types. We observed ganglionic neuroendocrine neoplasms, lesions not associated earlier with mutation of either Rb or E2f4. Moreover, a subset of the Rb−/−;E2f4−/− chimeras developed either low- or high-grade carcinomas in the urothelium transitional epithelium supporting a key role for Rb in bladder cancer.Oncogene (2009) 28, 500–508; doi:10.1038/onc.2008.406; published online 10 November 2008 [ABSTRACT FROM AUTHOR]

Published

2009

24. Cell Cycle Regulator E2F4 Is Essential for the Development of the Ventral Telencephalon.

Author

Ruzhynsky, Vladimir A., McClellan, Kelly A., Vanderluit, Jacqueline L., Yongsu Jeong, Furimsky, Marosh, Park, David S., Epstein, Douglas J., Wallace, Valerie A., and Slack, Ruth S.

Subjects

*CELL cycle regulation, *TELENCEPHALON, *PROSENCEPHALON, *STEM cells, *CELL proliferation

Abstract

Early forebrain development is characterized by extensive proliferation of neural precursors coupled with complex structural transformations; however, little is known regarding the mechanisms by which these processes are integrated. Here, we show that deficiency of the cell cycle regulatory protein, E2F4, results in the loss of ventral telencephalic structures and impaired self-renewal of neural precursor cells. The mechanism underlying aberrant ventral patterning lies in a dramatic loss of Sonic hedgehog (Shh) expression specifically in this region. The E2F4-deficient phenotype can be recapitulated by interbreeding mice heterozygous for E2F4 with those lacking one allele of Shh, suggesting a genetic interaction between these pathways. Treatment of E2F4-deficient cells with a Hh agonist rescues stem cell self-renewal and cells expressing the homeodomain proteins that specify the ventral telencephalic structures. Finally, we show that E2F4 deficiency results in impaired activity of Shh forebrain-specific enhancers. In conclusion, these studies establish a novel requirement for the cell cycle regulatory protein, E2F4, in the development of the ventral telencephalon. [ABSTRACT FROM AUTHOR]

Published

2007

25. E2f4 is required for normal development of the airway epithelium

Author

Danielian, Paul S., Bender Kim, Carla F., Caron, Alicia M., Vasile, Eliza, Bronson, Roderick T., and Lees, Jacqueline A.

Subjects

*LUNGS, *EPITHELIUM, *PARANASAL sinuses, *MUCINS, *EMBRYOLOGY, *CELL proliferation, *TRANSCRIPTION factors, *RHINITIS

Abstract

Abstract: The airway epithelium is comprised of specialized cell types that play key roles in protecting the lungs from environmental insults. The cellular composition of the murine respiratory epithelium is established during development and different cell types populate specific regions along the airway. Here we show that E2f4-deficiency leads to an absence of ciliated cells from the entire airway epithelium and the epithelium of the submucosal glands in the paranasal sinuses. This defect is particularly striking in the nasal epithelium of E2f4−/− mice where ciliated cells are replaced by columnar secretory cells that produce mucin-like substances. In addition, in the proximal lung, E2f4 loss causes a reduction in Clara cell marker expression indicating that Clara cell development is also affected. These defects arise during embryogenesis and, in the nasal epithelium, appear to be independent of any changes in cell proliferation, the principal process regulated by members of the E2f family of transcription factors. We therefore conclude that E2f4 is required to determine the appropriate development of the airway epithelium. Importantly, the combination of no ciliated cells and excess mucous cells can account for the chronic rhinitis and increased susceptibility to opportunistic infections that causes the postnatal lethality of E2f4 mutant mice. [Copyright &y& Elsevier]

Published

2007

26. Cell cycle-related transformation of the E2F4-p130 repressor complex

Author

Popov, Boris, Chang, Long-Sheng, and Serikov, Vladimir

Subjects

*CYTOPLASM, *TUMORS, *CLONE cells, *CANCER cells

Abstract

Abstract: During G0 phase the p130, member of the pRb tumor suppressor protein family, forms a repressor complex with E2F4 which is inactivated in G1/S by hyperphosphorylation of the p130. The role of p130 after G1/S remains poorly investigated. We found that in nuclear extracts of T98G cells, the p130-E2F4-DNA (pp-E2F4) complex does not dissociate at G1/S transition, but instead reverts to the p130-E2F4-cyclin E/A-cdk2 (cyc/cdk-pp-E2F4) complex, which is detected in S and G2/M phases of the cell cycle. Hyperphosphorylation of the p130 at G1/S transition is associated with a decrease of its total amount; however, this protein is still detected during the rest of the cell cycle, and it is increasingly hyperphosphorylated in the cytosol, but continuously dephosphorylated in the nucleus. Both nuclear and cytosol cell fractions in T98G cells contain a hyperphosphorylated form of p130 in complex with E2F4 at S and G2/M cell cycle phases. In contrast to T98G cells, transformation of the p130 containing cyc/cdk-pp-E2F4 complex into the p130-pp-E2F4 repressor does not occur in HeLa cells under growth restriction conditions. [Copyright &y& Elsevier]

Published

2005

27. Regulation of neuron survival and death by p130 and associated chromatin modifiers.

Author

Liu, David X., Nath, Niharika, Chellappan, Srikumar P., and Greene, Lloyd A.

Subjects

*GENES, *NEURONS, *CELLS, *DEATH, *MOLECULES, *APOPTOSIS

Abstract

E2F-mediated gene repression plays a key role in regulation of neuron survival and death. However, the key molecules involved in such regulation and the mechanisms by which they respond to apoptotic stimuli are largely unknown. Here we show that p130 is the predominant Rb family member associated with E2F in neurons, that its major partner for repression of pro-apoptotic genes is E2F4, and that the p130-E2F4 complex recruits the chromatin modifiers HDAC1 and Suv39H1 to promote gene silencing and neuron survival. Apoptotic stimuli induce neuron death by sequentially causing p130 hyperphosphorylation, dissociation of p130-E2F4-Suv39H1-HDAC complexes, altered modification of H3 histone and gene derepression. Experimental suppression of such events blocks neuron death while interference with the synthesis of E2F4 or p130, or with the interaction of E2F4-p130 with chromatin modifiers, induces neuron death. Thus, neuron survival and death are dependent on the integrity of E2F4-p130-HDAC/Suv39H1 complexes. [ABSTRACT FROM AUTHOR]

Published

2005

28. Opposing Roles of E2Fs in Cell Proliferation and Death.

Published

2004

29. Phosphorylation-dependent and -independent functions of p130 cooperate to evoke a sustained G1 block.

Author

Hansen, Klaus, Farkas, Thomas, Lukas, Jiri, Holm, Karin, Rönnstrand, Lars, and Bartek, Jiri

Subjects

*PHOSPHORYLATION, *CYCLINS, *RETINOBLASTOMA, *GROWTH factors, *PROTEIN kinases, *CELLULAR control mechanisms

Abstract

The retinoblastoma (pRb)-retated p130 pocket protein is a regulator of cell growth and differentiation, and a candidate tumour suppressor. Both pRb and p130 operate through interactions with cellular proteins, including the E2F transcription factors. White such interactions are controlled by phosphorylation of multiple sites of pRb, regulation of p130 remains poorly understood. We now identify 22 in vivo phosphorylation sites of p130, targeted by diverse kinases, and present evidence for three cyclin-dependent kinase 4(6) [Cdk4(6)] specific phosphorylations, which appear critical for controlling the growth-restraining activity of p130. When expressed in U2OS cells, the phosphorylation-deficient mutant p130ΔCdk4, in which the Cdk4 specific sites were mutated to alanine residues, imposed a more sustained G1 arrest than a constitutively active pRbΔCdk, known to repress all cellular E2F activity. Experiments using p130ΔCdk4 and another phosphorylation-deficient mutant, p130PM19A, with 19 phosphorylation sites mutated, revealed that the p130-imposed G1 block reflects cooperative growth-suppressive effects of phosphorylation-regulated E2F binding and phosphorylation-independent sequestration of cyclin E(A)-Cdk2 through the N-terminal cyclin binding motif of p130. [ABSTRACT FROM AUTHOR]

Published

2001

30. ZBTB7A, a potential biomarker for prognosis and immune infiltrates, inhibits progression of endometrial cancer based on bioinformatics analysis and experiments.

Author

Geng, Rong, Zheng, Yuhua, zhou, Donghua, Li, Qingdong, Li, Ruiman, and Guo, Xiaoling

Subjects

*BIOMARKERS, *ENDOMETRIAL cancer, *PROGNOSIS, *ZINC-finger proteins, *CANCER invasiveness, *ENDOMETRIAL tumors

Abstract

Backgroud: ZBTB protein is an important member of the C2H2 zinc finger protein family. As a transcription factor, it is widely involved in the transcriptional regulation of genes, cell proliferation, differentiation, and apoptosis. The ZBTB7A has been largely linked to different kinds of tumors due to its diverse function. However, the value for ZBTB7A in uterine corpus endometrial carcinoma (UCEC) is unclear. Methods: In our work, we assessed the importance of ZBTB7A in UCEC. Firstly, Using Oncomine and Tumor Immunoassay Resource (TIMER) databases to evaluate the expression of ZBTB7A. Secondly, we explored the co-expression network of ZBTB7A through the cBioPortal online tool, Metascape, and LinkedOmics. TIMER was also used to explore the relationship between ZBTB7A and tumor immune invasion, and to detect the correlation between the ZBTB7A and the marker genes related to immune infiltration. Finally, CCK8, migration, ChIP assays were introduced to partly validate ZBTB7A function in endometrial cancer cells. Results: We found the ZBTB7A expression in TIMER was associated with various cancers, especially UCEC. The decreased expression of ZBTB7A was markedly related to the stage and prognosis of UCEC. Furthermore, ZBTB7A was also related to the expression of various immune markers such as Neutrophils, Dendritic cell, T cell (general), Th1, Th2, and Treg. Finally, we verified that ZBTB7A repressed E2F4 transcription and inhibited cells proliferation and migration. These results indicate that ZBTB7A may play a vital role in regulating immune cell infiltration in UCEC, and is a valuable prognostic marker. Conclusions: In summary, we demonstrate that ZBTB7A is notably downregulated in UCEC, plays a vital role in regulating immune cell infiltration, possesses diagnostic and prognostic values and attenuates E2F4 transcription and cell proliferation, migration in vitro. [ABSTRACT FROM AUTHOR]

Published

2020

31. Long non-coding RNA GAS5 inhibits DDP-resistance and tumor progression of epithelial ovarian cancer via GAS5-E2F4-PARP1-MAPK axis.

Author

Long, Xiaoran, Song, Keqi, Hu, Hao, Tian, Qi, Wang, Wenjing, Dong, Qian, Yin, Xia, and Di, Wen

Subjects

*NON-coding RNA, *OVARIAN epithelial cancer, *CANCER invasiveness, *OVARIAN cancer, *CISPLATIN, *EPITHELIAL tumors, *DRUG tolerance, *RAPAMYCIN, *GENITALIA

Abstract

Background: Epithelial ovarian cancer (EOC) is the malignant tumor of the female reproductive system with the highest fatality rate. Tolerance of chemotherapeutic drugs like cisplatin (DDP) occurring in very early stage is one of the important factors of the poor prognosis of epithelial ovarian cancer. Here we aim to study the dysregulation of a particular long noncoding RNA, lncRNA GAS5, and its role in EOC progression. Methods: The low expression of lncRNA GAS5 in EOC tissues and OC cell lines was determined by microarray analyses and Real-Time qPCR. Flow cytometer assays were used to detect cell cycle and apoptosis of OC cells. CCK8 assay were performed to investigate the DDP sensitivity of OC cells. Western blot was carried out to detect cell growth markers, apoptotic markers, PARP1, E2F4, MAPK pathway protein expression and other protein expression in OC cell lines. The binding of GAS5 and E2F4 were proved by RNA pull-down and RIP assay. The effect of E2F4 on PARP1 were determined by CHIP-qPCR assay and luciferase reporter assay. The effect of lncRNA GAS5 on OC cells was assessed in vitro and in vivo. Results: By microarray (3 EOC tissues νs. 3 normal ovary tissues) and RT- qPCR (53 EOC tissues νs. 10 normal ovary tissues) we identified lncRNA GAS5 to be dramatically low expressed in EOC samples and correlated with prognosis. Compared with sensitive cell lines, GAS5 was also low expressed in DDP resistant OC cell lines, and over-expression of GAS5 significantly enhanced the sensitivity of OC cells to DDP in vivo and in vitro. Meanwhile the over-expression of GAS5 also caused OC cells G0/G1 arrest and apoptosis increase. Mechanistically, GAS5 might regulate PARP1 expression by recruiting the transcription factor E2F4 to its promoter, and then affect the MAPK pathway activity. Due to the 5'TOP structure, GAS5 could be regulated by transcription inhibitor rapamycin in OC cells. Conclusion: Here we explored the specific mechanisms of EOC cisplatin resistance and tumor progress due to lncRNA-GAS5, presented the GAS5-E2F4-PARP1-MAPK axis and its role in OC drug-sensitivity and progression for the first time, and the results may provide experimental basis for clinical application. [ABSTRACT FROM AUTHOR]

Published

2019

32. Overexpressing p130/E2F4 in mesenchymal stem cells facilitates the repair of injured alveolar epithelial cells in LPS-induced ARDS mice.

Author

Zhang, Xiwen, Chen, Jianxiao, Xue, Ming, Tang, Yuying, Xu, Jingyuan, Liu, Ling, Huang, Yingzi, Yang, Yi, Qiu, Haibo, and Guo, Fengmei

Subjects

*MESENCHYMAL stem cells, *ALVEOLAR process, *ADULT respiratory distress syndrome, *EPITHELIAL cells, *LIPOPOLYSACCHARIDES, *EOSIN, *LUNG injuries

Abstract

Background: Low differentiation rates of mesenchymal stem cells (MSCs) limit their therapeutic effects on patients in clinical studies. Our previous study demonstrated that overexpressing p130 or E2F4 affected the multipotential differentiation of MSCs, and the underlying mechanism was attributed to the regulation of the G1 phase. Improving the efficiency of MSC differentiation into epithelial cells is considered to be a new method. Therefore, this study was conducted to evaluate the effects of overexpressing p130 or E2F4 in MSCs on improving re-epithelization in lipopolysaccharide (LPS)-induced ARDS animals. Methods: Mouse MSCs (mMSCs) stably transfected with p130 and E2F4 were transplanted intratracheally into LPS-induced ARDS mice. After 7 and 14 days, the mice were sacrificed, and the histopathology of the lungs was assessed by haematoxylin-eosin staining and lung injury scoring. Homing and differentiation of mMSCs were analysed by labelling and tracking mMSCs with NIR815 dye and immunofluorescent staining. Surfactant proteins A and C and occludin in the lungs were assessed by western blot. Permeability was evaluated by analysing the protein concentration of BALF using ELISA. Alveolar fluid clearance was assessed by absorbance measurements of BALF. Lung fibrosis was assessed by Masson's trichrome staining and Ashcroft scoring. Results: The engraftment of mMSCs overexpressing p130 or E2F4 led to attenuated histopathological impairment of the lung tissue, and the lung injury scores of the LPS+mBM-MSC-p130 and LPS+mBM-MSC-E2F4 groups were also decreased (p < 0.05). Overexpression of p130 or E2F4 also increased the retention of mMSCs in the lung (p < 0.05), increased differentiation into type II alveolar epithelial cells (p < 0.05), and improved alveolar epithelial permeability (p < 0.05). Additionally, mMSCs overexpressing p130 or E2F4 inhibited lung fibrosis according to the deposition of collagen and the fibrosis score in the lungs (p < 0.05). Conclusion: Overexpressing p130 or E2F4 in mMSCs could further improve the injured structure and function of epithelial cells in the lungs of ARDS mice as a result of improved differentiation of mMSCs into epithelial cells. [ABSTRACT FROM AUTHOR]

Published

2019

33. Multicilin drives centriole biogenesis via E2f proteins.

Author

Ma, Lina, Quigley, Ian, Omran, Heymut, and Kintner, Chris

Subjects

*CENTRIOLES, *CELL cycle, *CILIA & ciliary motion, *CELL motility, *CELL membrane formation

Abstract

Multiciliate cells employ hundreds of motile cilia to produce fluid flow, which they nucleate and extend by first assembling hundreds of centrioles. In most cells, entry into the cell cycle allows centrioles to undergo a single round of duplication, but in differentiating multiciliate cells, massive centriole assembly occurs in G0 by a process initiated by a small coiled-coil protein, Multicilin. Here we show that Multicilin acts by forming a ternary complex with E2f4 or E2f5 and Dp1 that binds and activates most of the genes required for centriole biogenesis, while other cell cycle genes remain off. This complex also promotes the deuterosome pathway of centriole biogenesis by activating the expression of deup1 but not its paralog, cep63. Finally, we show that this complex is disabled by mutations in human Multicilin that cause a severe congenital mucociliary clearance disorder due to reduced generation of multiple cilia. By coopting the E2f regulation of cell cycle genes, Multicilin drives massive centriole assembly in epithelial progenitors in a manner required for multiciliate cell differentiation. [ABSTRACT FROM AUTHOR]

Published

2014