Your search keyword '"BET protein"' showing total 41 results

1. Bromodomain and extraterminal domain (BET) promote autophagy in buffalo sertoli cells.

Author

Yang Y, Zhang J, Zhang Y, Sun Q, Liu R, Xu C, Xu P, Lu Y, and Fu Q

Abstract

Sertoli cells (SCs) play a pivotal role in spermatogenesis, with autophagy modulation being an evolutionarily conserved mechanism for maintaining cellular homeostasis and protecting spermatogenic cells against apoptosis. The bromodomain and extraterminal domain (BET) family are transcriptional regulators of autophagy. This study investigated the relationship between BET inhibition and autophagy in buffalo SCs. Our findings reveal that BET inhibition suppresses cell proliferation and alters the biological characteristics of SCs. RNA-seq analysis demonstrated significant downregulation of autophagy-related genes upon BET inhibition. Moreover, our bioinformatics analysis suggested the involvement of the PI3K-AKT signaling pathway in autophagy regulation within buffalo SCs. Immunofluorescence and Transmission electron microscopy observations indicated that BET inhibition results in autophagosome accumulation and impedes autophagosome-lysosome degradation, thereby compromising autophagy activity and flux. In summary, this study sheds light on the indispensable role of BET proteins in autophagy and paves the way for further investigations into the mechanisms governing BET protein-mediated autophagy regulation and its implications for male reproduction., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

2. In silico DOCKING STUDIES FOR THE FUNGAL METABOLITES TOWARDS THE BROMODOMAIN AND EXTRATERMINAL PROTEIN.

Author

DEVI, A., KUMARI, K., PRATHAPAN, S., ROMAULD, S. I., and DEVI, P. B.

Subjects

*FUNGAL metabolites, *MOLECULAR docking, *PROTEIN-ligand interactions, *STRUCTURE-activity relationships, *MYCOSES

Abstract

Fungal infections are the most common infection among humans. In this study, in silico activities have been carried out to analyse the fungal infection caused by Candida albicans. Candida albicans are the natural gut organisms which does not cause any infection but intake the antibiotics for a longer period of time. Humans who have weaker immune system have high risk in developing the infection. The target selected is the First bromodomain (BDF1) from BET protein is responsible for Candida albicans multiplication and viability. Inhibition of BDF1 from BET protein will block the multiplication and viability of Candida albicans. The nutmeg metabolites are used against many fungal infections since ages, and they are showing good results in inhibiting the fungal infections. By performing the in-silico activity studies the protein-ligand interactions are predicted. The selected nutmeg compounds from the Pubmed have been docked with the co-crystalised protein by keeping the compound Fluconazole as a reference ligand. All the compounds selected for docking studies possessed good docking score when compared with Fluconazole. Further the compounds were studied for its structure activity relationship with the co-crystallised protein and the drug likeliness was studied and the Lipinski rule of 5 has been studied. [ABSTRACT FROM AUTHOR]

Published

2022

3. The Short Isoform of BRD4 Promotes HIV-1 Latency by Engaging Repressive SWI/SNF Chromatin-Remodeling Complexes

Author

Conrad, Ryan J, Fozouni, Parinaz, Thomas, Sean, Sy, Hendrik, Zhang, Qiang, Zhou, Ming-Ming, and Ott, Melanie

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Biological Sciences, Human Genome, Infectious Diseases, HIV/AIDS, Genetics, Sexually Transmitted Infections, 2.1 Biological and endogenous factors, Aetiology, Infection, Azepines, Cell Cycle Proteins, Chromatin, Chromatin Assembly and Disassembly, Chromatin Immunoprecipitation, Chromosomal Proteins, Non-Histone, DNA Helicases, DNA, Viral, Dose-Response Relationship, Drug, Down-Regulation, Gene Expression Regulation, Viral, HEK293 Cells, HIV-1, High-Throughput Nucleotide Sequencing, Host-Pathogen Interactions, Humans, Jurkat Cells, Nuclear Proteins, Promoter Regions, Genetic, Protein Binding, Protein Isoforms, RNA Interference, Retroelements, T-Lymphocytes, Time Factors, Transcription Factors, Transcription, Genetic, Transfection, Triazoles, Virus Latency, BET protein, BRD4, BRG1, HIV, JQ1, LTR, SWI/SNF, bromodomain, chromatin, latency, Medical and Health Sciences, Developmental Biology, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

BET proteins commonly activate cellular gene expression, yet inhibiting their recruitment paradoxically reactivates latent HIV-1 transcription. Here we identify the short isoform of BET family member BRD4 (BRD4S) as a corepressor of HIV-1 transcription. We found that BRD4S was enriched in chromatin fractions of latently infected T cells, and it was more rapidly displaced from chromatin upon BET inhibition than the long isoform. BET inhibition induced marked nucleosome remodeling at the latent HIV-1 promoter, which was dependent on the activity of BRG1-associated factors (BAF), an SWI/SNF chromatin-remodeling complex with known repressive functions in HIV-1 transcription. BRD4S directly bound BRG1, a catalytic subunit of BAF, via its bromodomain and extraterminal (ET) domain, and this isoform was necessary for BRG1 recruitment to latent HIV-1 chromatin. Using chromatin immunoprecipitation sequencing (ChIP-seq) combined with assay for transposase-accessible chromatin coupled to high-throughput sequencing (ATAC-seq) data, we found that the latent HIV-1 promoter phenotypically resembles endogenous long terminal repeat (LTR) sequences, pointing to a select role of BRD4S-BRG1 complexes in genomic silencing of invasive retroelements.

Published

2017

4. Inhibition of the bromodomain and extra-terminal family of epigenetic regulators as a promising therapeutic approach for gastric cancer.

Author

Kang, Sun Kyoung, Bae, Hyun Joo, Kwon, Woo Sun, Kim, Tae Soo, Kim, Kyoo Hyun, Park, Sejung, Yu, Seo Young, Hwang, Jihyun, Park, Juin, Chung, Hyun Cheol, and Rha, Sun Young

Subjects

*THERAPEUTICS, *STOMACH cancer, *LABORATORY mice, *RESPONSE inhibition, *CARCINOGENESIS, *ONE-way analysis of variance

Abstract

Purpose: Epigenetic dysregulation is a common characteristic of cancers, including gastric cancer (GC), and contributes to cancer development and progression. Although the efficacy of BET (an epigenetic regulator) inhibition has been demonstrated in various cancer types, predictive genetic markers of its efficacy in GC are currently lacking. Therefore, we aimed to identify markers that predict the response of BET inhibition in GC and, suggest an effective treatment regimen through combined therapy. Methods: The effect of BET inhibition was evaluated using iBET-151, a small-molecule inhibitor of BET proteins, in a large panel (n = 49) of GC cell lines and xenograft mouse models. Comprehensive genetic information was used to identify cell lines sensitive to iBET-151. Flow cytometry, Western blotting, and colony-formation and migration assays were used to evaluate the effects of iBET-151 and/or paclitaxel. The synergistic effect of iBET-151 and paclitaxel was evaluated using an organoid model. Results: We found that iBET-151 showed a modest growth-inhibitory effect in GC cells (73%, 36/49). iBET-151 inhibited tumorigenicity in vitro and significantly promoted cell cycle arrest and apoptosis. Based on comprehensive genetic information analysis in relation to BET family expression, we found that BRD4 was highly expressed in the iBET-151-sensitive cell lines. We also identified WNT5B and IRS2 as potential biomarkers that are predictive for sensitivity to iBET-151. In GC xenograft model mice, iBET-151 significantly decreased tumor volumes and Ki-67 and BRD4 expression. Combination treatment showed that iBET-151 increased the sensitivity of GC cells to paclitaxel in approximately 70% of the cell lines (34/49) tested. iBET-151 plus paclitaxel significantly promoted cell cycle arrest and apoptosis and suppressed c-Myc, Bcl-2 and Bcl-xL expression. In GC organoids, iBET-151 and paclitaxel showed a synergistic effect. Conclusions: Collectively, our data suggest that iBET-151 is a potential therapeutic agent for GC, especially in combination with paclitaxel, and that WNT5B and IRS2 may predict iBET-151 sensitivity. [ABSTRACT FROM AUTHOR]

Published

2021

5. BET protein inhibition regulates cytokine production and promotes neuroprotection after spinal cord injury

Author

Judith Sánchez-Ventura, Jesús Amo-Aparicio, Xavier Navarro, and Clara Penas

Subjects

BET protein, Inflammation, Cytokine, Neuroprotection, Spinal cord injury, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Background Spinal cord injury (SCI) usually causes a devastating lifelong disability for patients. After a traumatic lesion, disruption of the blood-spinal cord barrier induces the infiltration of macrophages into the lesion site and the activation of resident glial cells, which release cytokines and chemokines. These events result in a persistent inflammation, which has both detrimental and beneficial effects, but eventually limits functional recovery and contributes to the appearance of neuropathic pain. Bromodomain and extra-terminal domain (BET) proteins are epigenetic readers that regulate the expression of inflammatory genes by interacting with acetylated lysine residues. While BET inhibitors are a promising therapeutic strategy for cancer, little is known about their implication after SCI. Thus, the current study was aimed to investigate the anti-inflammatory role of BET inhibitors in this pathologic condition. Methods We evaluated the effectiveness of the BET inhibitor JQ1 to modify macrophage reactivity in vitro and to modulate inflammation in a SCI mice model. We analyzed the effects of BET inhibition in pro-inflammatory and anti-inflammatory cytokine production in vitro and in vivo. We determined the effectiveness of BET inhibition in tissue sparing, inflammation, neuronal protection, and behavioral outcome after SCI. Results We have found that the BET inhibitor JQ1 reduced the levels of pro-inflammatory mediators and increased the expression of anti-inflammatory cytokines. A prolonged treatment with JQ1 also decreased reactivity of microglia/macrophages, enhanced neuroprotection and functional recovery, and acutely reduced neuropathic pain after SCI. Conclusions BET protein inhibition is an effective treatment to regulate cytokine production and promote neuroprotection after SCI. These novel results demonstrate for the first time that targeting BET proteins is an encouraging approach for SCI repair and a potential strategy to treat other inflammatory pathologies.

Published

2019

6. BRD4 regulates self‐renewal ability and tumorigenicity of glioma‐initiating cells by enrichment in the Notch1 promoter region

Author

Zhennan Tao, Xuetao Li, Hao Wang, Guangliang Chen, Zibin Feng, Yue Wu, Haoran Yin, Guozheng Zhao, Zhitong Deng, Chaohui Zhao, Yanyan Li, Ting Sun, and Youxin Zhou

Subjects

BET protein, BRD4, glioma‐initiating cells, notch1, self‐renewal, tumorigenicity, Medicine (General), R5-920

Abstract

Abstract Bromodomain and extraterminal domain (BET) family proteins are considered to be epigenetic readers that regulate gene expression by recognizing acetyl lysine residues on histones and nonhistone chromatin factors and have been classified as curative targets for a variety of cancers. Glioma‐initiating cells (GICs), which commit self‐renewal, perpetual proliferation, multidirectional differentiation, and vigorous tumorigenicity, sustain the peculiar genetic and epigenetic diversification in the GBM patients, thus, GICs result in tumor recurrence. Abundant evidence demonstrates that BET proteins regulate differentiation of stem cells. However, it endures ambiguous how individual BET proteins take part in GIC advancement, and how do small molecule inhibitors like I‐BET151 target functional autonomous BET proteins. Here, we validated that BRD4, not BRD2 or BRD3, has value in targeted glioma therapy. We announce a signaling pathway concerning BRD4 and Notch1 that sustains the self‐renewal of GICs. Moreover, in‐depth mechanistic research showed that BRD4 was concentrated at the promoter region of Notch1 and may be involved in the process of tumor metabolism. Furthermore, in intracranial models, I‐BET151 eliminated U87 GICs’ tumorigenicity. The outcomes of this research could be conducive to design clinical trials for treatment of glioma based on BRD4.

Published

2020

7. Bromo‐ and extraterminal domain protein inhibition improves immunotherapy efficacy in hepatocellular carcinoma.

Author

Liu, Chen, Miao, Xiaolong, Wang, Yao, Wen, Liang, Cheng, Xiawei, Kong, Deqiang, Zhao, Pengwei, Song, Dandan, Wang, Xinyi, Ding, Xianfeng, Xia, Hongguang, Wang, Weilin, Sun, Qiming, and Gong, Weihua

Abstract

Hepatocellular carcinoma (HCC) represents the majority of liver cancer and is the fourth most common cause of cancer‐related death. Although advances in molecular targeted therapy have shown promise, none of these agents has yet demonstrated significant clinical benefit. Bromo‐ and extraterminal domain (BET) protein inhibitors have been considered potential therapeutic drugs for HCC but the biological activity remains unclear. This study found that BET protein inhibition did not effectively suppress the progression of HCC, using a transgenic HCC mouse model. Mechanistically, the BET protein inhibitor JQ1 upregulated the expression of programmed cell death‐ligand 1 (PD‐L1) on the plasma membrane in vivo and in vitro. Moreover, JQ1 enhanced the expression of Rab8A, which upregulated the expression of PD‐L1 on the plasma membrane. This study also showed that JQ1 combined with anti‐PD‐L1 Ab effectively suppressed HCC progression, and this benefit was obtained by enhancing the activation and cytotoxic capabilities of CD8 T cells. These results revealed the crucial role and regulation of BET protein inhibition on the expression of PD‐L1 in HCC. Thus, combining BET protein inhibition with immune checkpoint blockade offers an efficient therapeutic approach for HCC. [ABSTRACT FROM AUTHOR]

Published

2020

8. Effect of TNIK upregulation on JQ1-resistant human colorectal cancer HCT116 cells.

Author

Takahashi, Chihiro, Kondo, Shingo, Sadaoka, Kensuke, Ishizuka, Shuhei, Noguchi, Kohji, Kato, Yu, and Sugimoto, Yoshikazu

Subjects

*CANCER cells, *COLORECTAL cancer, *WNT proteins, *PROTEIN kinases, *CLONE cells, *CELL proliferation

Abstract

JQ1 disrupts the binding of bromodomain and extra-terminal (BET) family of proteins to acetylated histones, modulates the expression of various genes, and inhibits the proliferation of cancer cells. We established two JQ1-resistant sublines from human colorectal cancer HCT116 cells. These resistant cells showed an 8- to 9-fold higher resistance to JQ1, and a 2- to 4-fold higher resistance to various anti-cancer agents, such as doxorubicin, etoposide, mitoxantrone, SN-38, cisplatin, and methotrexate than the parental HCT116 cells. The JQ1-resistant cells expressed higher levels of TRAF2 and NCK-interacting protein kinase (TNIK), cyclin D1 (CCND1), cyclin E1 (CCNE1), and their corresponding mRNAs than the parental cells. TNIK is a regulator of Wnt/β-catenin signaling and is known to transactivate CCND1. Transient transfection of HCT116 cells with a TNIK expression plasmid resulted in the upregulation of cyclin D1, cyclin E1, and their corresponding mRNAs, as well as an increase in CCNE1 promoter activity. Furthermore, luciferase assay revealed that the JQ1-resistant cells showed high CCNE1 promoter activity. These results suggest that TNIK also transactivates CCNE1. Three stable TNIK transfectant clones of HEK293 cells expressed 1.5- to 2-fold higher levels of TNIK, cyclin D1, and cyclin E1 than the parental cells. The 293/TNIK-6 cells, which expressed the highest level of TNIK among the transfectants, showed a 2.3-fold higher resistance to JQ1 than the parental cells. These results suggest the possible involvement of TNIK in cellular resistance to JQ1. • Cross-resistance of JQ1-resistant cells to DNA-damaging agents. • Upregulation of TNIK, cyclin D1, and cyclin E1 in JQ1-resistant cells. • Upregulation of cyclin D1 and cyclin E1 in TNIK -transfected cells. • Increased CCNE1 promoter activity in JQ1-resistant cells and TNIK -transfected cells. • JQ1 resistance of stable TNIK -transfected cells. [ABSTRACT FROM AUTHOR]

Published

2020

9. De Novo Variants in SPOP Cause Two Clinically Distinct Neurodevelopmental Disorders.

Author

Nabais Sá, Maria J., El Tekle, Geniver, de Brouwer, Arjan P.M., Sawyer, Sarah L., del Gaudio, Daniela, Parker, Michael J., Kanani, Farah, van den Boogaard, Marie-José H., van Gassen, Koen, Van Allen, Margot I., Wierenga, Klaas, Purcarin, Gabriela, Elias, Ellen Roy, Begtrup, Amber, Keller-Ramey, Jennifer, Bernasocchi, Tiziano, van de Wiel, Laurens, Gilissen, Christian, Venselaar, Hanka, and Pfundt, Rolph

Subjects

*ENDOMETRIAL cancer, *CONGENITAL disorders, *DEVELOPMENTAL delay, *DISEASES, *INTELLECTUAL disabilities

Abstract

Recurrent somatic variants in SPOP are cancer specific; endometrial and prostate cancers result from gain-of-function and dominant-negative effects toward BET proteins, respectively. By using clinical exome sequencing, we identified six de novo pathogenic missense variants in SPOP in seven individuals with developmental delay and/or intellectual disability, facial dysmorphisms, and congenital anomalies. Two individuals shared craniofacial dysmorphisms, including congenital microcephaly, that were strikingly different from those of the other five individuals, who had (relative) macrocephaly and hypertelorism. We measured the effect of SPOP variants on BET protein amounts in human Ishikawa endometrial cancer cells and patient-derived cell lines because we hypothesized that variants would lead to functional divergent effects on BET proteins. The de novo variants c.362G>A (p.Arg121Gln) and c. 430G>A (p.Asp144Asn), identified in the first two individuals, resulted in a gain of function, and conversely, the c.73A>G (p.Thr25Ala), c.248A>G (p.Tyr83Cys), c.395G>T (p.Gly132Val), and c.412C>T (p.Arg138Cys) variants resulted in a dominant-negative effect. Our findings suggest that these opposite functional effects caused by the variants in SPOP result in two distinct and clinically recognizable syndromic forms of intellectual disability with contrasting craniofacial dysmorphisms. [ABSTRACT FROM AUTHOR]

Published

2020

10. Are BET Inhibitors yet Promising Latency-Reversing Agents for HIV-1 Reactivation in AIDS Therapy?

Author

Thanarat Salahong, Christian Schwartz, and Rungroch Sungthong

Subjects

HIV-1, latently HIV-1-infected cell, latency-reversing agent, BET protein, BRD2, BRD4, Microbiology, QR1-502

Abstract

AIDS first emerged decades ago; however, its cure, i.e., eliminating all virus sources, is still unachievable. A critical burden of AIDS therapy is the evasive nature of HIV-1 in face of host immune responses, the so-called “latency.” Recently, a promising approach, the “Shock and Kill” strategy, was proposed to eliminate latently HIV-1-infected cell reservoirs. The “Shock and Kill” concept involves two crucial steps: HIV-1 reactivation from its latency stage using a latency-reversing agent (LRA) followed by host immune responses to destroy HIV-1-infected cells in combination with reinforced antiretroviral therapy to kill the progeny virus. Hence, a key challenge is to search for optimal LRAs. Looking at epigenetics of HIV-1 infection, researchers proved that some bromodomains and extra-terminal motif protein inhibitors (BETis) are able to reactivate HIV-1 from latency. However, to date, only a few BETis have shown HIV-1-reactivating functions, and none of them have yet been approved for clinical trial. In this review, we aim to demonstrate the epigenetic roles of BETis in HIV-1 infection and HIV-1-related immune responses. Possible future applications of BETis and their HIV-1-reactivating properties are summarized and discussed.

Published

2021

11. Structural Insights into BET Client Recognition of Endometrial and Prostate Cancer-Associated SPOP Mutants.

Author

Ostertag, Michael Sebastian, Hutwelker, Wiebke, Plettenburg, Oliver, Sattler, Michael, and Popowicz, Grzegorz Maria

Subjects

*ENDOMETRIAL cancer, *PROSTATE cancer, *INDIVIDUALIZED medicine, *ANTINEOPLASTIC agents, *BROMODOMAINS, *CRYSTALLIZATION, *PROTEIN binding, *GENETIC mutation

Abstract

BET proteins such as BRD3 are oncogenic transcriptional coactivators. SPOP binding triggers their proteasomal degradation. In both endometrial and prostate cancers, SPOP mutations occur in the MATH domain, but with opposed influence on drug susceptibility. In prostate cancer, SPOP mutations presumably cause increased BET levels, decreasing BET inhibitor drug susceptibility. As opposed, in endometrial cancer, decreased BET levels concomitant with higher BET inhibitor drug susceptibility were observed. Here, we present the to our knowledge first co-crystal structure of SPOP and a bromodomain containing protein (BRD3). Our structural and biophysical data confirm the suggested loss-of-function in prostate cancer-associated SPOP mutants and provide mechanistic explanation. As opposed to previous literature, our data on endometrial cancer-associated SPOP mutants do not show altered binding behavior compared to wild-type SPOP, indicating a more complex regulatory mechanism. SPOP mutation screening may thus be considered a valuable personalized medicine tool for effective antitumor therapy. Unlabelled Image • BET proteins are anticancer drug targets which are ubiquitination clients of SPOP. • Our structures explain the SPOP–BET loss-of-binding mechanism in prostate cancer. • SPOP–BET binding influences drug susceptibility in prostate and endometrial cancer. • SPOP mutation screens may improve personalized cancer treatment in human patients. [ABSTRACT FROM AUTHOR]

Published

2019

12. Current Understanding of the Role of the Brd4 Protein in the Papillomavirus Lifecycle

Author

Moon Kyoo Jang and Alison A. McBride

Subjects

Brd4, BET protein, HPV, papillomavirus, transcription, chromatin, replication, tethering, partitioning, bromodomain, Microbiology, QR1-502

Abstract

The Brd4 protein is an epigenetic reader that is central to regulation of cellular transcription and mitotic bookmarking. The transcription and replication proteins of many viruses interact with Brd4. We describe the multiple roles of Brd4 in the papillomavirus lifecycle.

Published

2013

13. The Molecular Regulation of Dendritic Arbor Shape During Development and Disease

Author

Bagley, Joshua Adam

Subjects

Neurosciences, Cellular biology, Genetics, aging, BET protein, bromodomain, dendrite morphology, epigenetics, polyQ

Abstract

The brain is composed of a network of neural cells which have elaborate cellular structures, especially their dendritic arbors. The correct function of neural networks requires the development of specific dendritic arbor shapes, and altered shapes leads to neural dysfunction. Therefore, understanding the molecules which specify dendritic arbor shapes during development is paramount to understanding how dendritic arbors are misshapen during disease. A complex array of genetic factors regulates dendritic arbor morphology. Therefore, using the Drosophila dendritic arborization (da) neurons, we performed a candidate-based genetic screen to identify molecules associated with neurodegenerative disease and brain aging which can regulate dendritic arbor morphology. Among the many screen hits, we discovered a role of the double-bromodomain and extra terminal (BET) family proteins in regulating dendrite arbor complexity and mechanosensory function. Our results identify a novel role for BET family proteins in regulating dendrite morphology, and a possible separation of developmental pathways specifying neural cell morphology and ion channel expression. Since the BET proteins are known to bind acetylated histone tails, these results also suggest a role of epigenetic histone modifications, and the `histone code,' in regulating dendrite morphology. Finally, we developed a system to study how the expression of disease related molecules can impact mature, already formed, dendritic arbors. Our results indicate that expression of pathogenetic polyglutamine proteins cause a progressive retraction of dendritic branches. This system can be used to study how dendritic arbors are maintained throughout life, and how this maintenance is disrupted during disease.

Published

2015

14. CXCL8 histone H3 acetylation is dysfunctional in airway smooth muscle in asthma: regulation by BET.

Author

Clifford, Rachel L., Patel, Jamie K., John, Alison E., Tatler, Amanda L., Mazengarb, Lisa, Brightling, Christopher E., and Knox, Alan J.

Subjects

*ASTHMA treatment, *CHEMOKINES, *HISTONE acetylation, *DNA methylation, *AIRWAY (Anatomy), *BROMODOMAIN-containing proteins, *RNA polymerase II, *INFLAMMATION treatment

Abstract

Asthma is characterized by airway inflammation and remodeling and CXCL8 is a CXC chemokine that drives steroid-resistant neutrophilic airway inflammation. We have shown that airway smooth muscle (ASM) cells isolated from asthmatic individuals secrete more CXCL8 than cells from nonasthmatic individuals. Here we investigated chromatin modifications at the CXCL8 promoter in ASM cells from nonasthmatic and asthmatic donors to further understand how CXCL8 is dysregulated in asthma. ASM cells from asthmatic donors had increased histone H3 acetylation, specifically histone H3K18 acetylation, and increased binding of histone acetyltransferase p300 compared with nonasthmatic donors but no differences in CXCL8 DNA methylation. The acetylation reader proteins Brd3 and Brd4 were bound to the CXCL8 promoter and Brd inhibitors inhibited CXCL8 secretion from ASM cells by disrupting Brd4 and RNA polymerase II binding to the CXCL8 promoter. Our results show a novel dysregulation of CXCL8 transcriptional regulation in asthma characterized by a promoter complex that is abnormal in ASM cells isolated from asthmatic donors and can be modulated by Brd inhibitors. Brd inhibitors may provide a new therapeutic strategy for steroid-resistant inflammation. [ABSTRACT FROM AUTHOR]

Published

2015

15. BET protein inhibition regulates cytokine production and promotes neuroprotection after spinal cord injury

Author

Sánchez-Ventura, Judith, Amo-Aparicio, Jesús, Navarro, Xavier, and Penas, Clara

Published

2019

16. BRD4 regulates self‐renewal ability and tumorigenicity of glioma‐initiating cells by enrichment in the Notch1 promoter region

Author

Chaohui Zhao, Youxin Zhou, Zhennan Tao, Guozheng Zhao, Yanyan Li, Haoran Yin, Hao Wang, Zibin Feng, Zhitong Deng, Xuetao Li, Guangliang Chen, Ting Sun, and Yue Wu

Subjects

0301 basic medicine, BRD4, Medicine (miscellaneous), BET protein, 03 medical and health sciences, 0302 clinical medicine, Glioma, medicine, Epigenetics, self‐renewal, notch1, Research Articles, lcsh:R5-920, glioma‐initiating cells, biology, medicine.disease, Chromatin, Bromodomain, 030104 developmental biology, Histone, 030220 oncology & carcinogenesis, Cancer research, biology.protein, tumorigenicity, Molecular Medicine, Signal transduction, Stem cell, lcsh:Medicine (General), Research Article

Abstract

Bromodomain and extraterminal domain (BET) family proteins are considered to be epigenetic readers that regulate gene expression by recognizing acetyl lysine residues on histones and nonhistone chromatin factors and have been classified as curative targets for a variety of cancers. Glioma‐initiating cells (GICs), which commit self‐renewal, perpetual proliferation, multidirectional differentiation, and vigorous tumorigenicity, sustain the peculiar genetic and epigenetic diversification in the GBM patients, thus, GICs result in tumor recurrence. Abundant evidence demonstrates that BET proteins regulate differentiation of stem cells. However, it endures ambiguous how individual BET proteins take part in GIC advancement, and how do small molecule inhibitors like I‐BET151 target functional autonomous BET proteins. Here, we validated that BRD4, not BRD2 or BRD3, has value in targeted glioma therapy. We announce a signaling pathway concerning BRD4 and Notch1 that sustains the self‐renewal of GICs. Moreover, in‐depth mechanistic research showed that BRD4 was concentrated at the promoter region of Notch1 and may be involved in the process of tumor metabolism. Furthermore, in intracranial models, I‐BET151 eliminated U87 GICs’ tumorigenicity. The outcomes of this research could be conducive to design clinical trials for treatment of glioma based on BRD4., 1. We evaluated BRD4, not BRD2 or BRD3, has value in targeted glioma therapy. 2. A signaling pathway involving BRD4 and Notch1 sustains GICs’ self‐renewal. 3. BRD4 was enriched at Notch1 promoter region and may be involved in the process of tumor metabolism. 4. BRD4 abolished the tumorigenicity of GICs in intracranial model after I‐BET151 (BET inhibitor) treatment.

Published

2020

17. Bromo- and extraterminal domain protein inhibition improves immunotherapy efficacy in hepatocellular carcinoma

Author

Deqiang Kong, Xianfeng Ding, Liang Wen, Qiming Sun, Weihua Gong, Yao Wang, Weilin Wang, Xiaolong Miao, Pengwei Zhao, Xinyi Wang, Chen Liu, Hongguang Xia, Xiawei Cheng, and Dandan Song

Subjects

0301 basic medicine, Male, Cancer Research, Carcinoma, Hepatocellular, medicine.medical_treatment, JQ1, Cell, Antineoplastic Agents, CD8-Positive T-Lymphocytes, BET protein, B7-H1 Antigen, Targeted therapy, 03 medical and health sciences, Mice, 0302 clinical medicine, Basic and Clinical Immunology, PD-L1, Cell Line, Tumor, medicine, Cytotoxic T cell, Animals, Humans, Molecular Targeted Therapy, biology, Chemistry, Liver Neoplasms, Proteins, General Medicine, Immunotherapy, Hep G2 Cells, hepatocellular carcinoma, medicine.disease, Immune checkpoint, digestive system diseases, Up-Regulation, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, Oncology, PD‐L1, 030220 oncology & carcinogenesis, Hepatocellular carcinoma, Cancer research, biology.protein, Disease Progression, Original Article, immunotherapy, Liver cancer

Abstract

Hepatocellular carcinoma (HCC) represents the majority of liver cancer and is the fourth most common cause of cancer‐related death. Although advances in molecular targeted therapy have shown promise, none of these agents has yet demonstrated significant clinical benefit. Bromo‐ and extraterminal domain (BET) protein inhibitors have been considered potential therapeutic drugs for HCC but the biological activity remains unclear. This study found that BET protein inhibition did not effectively suppress the progression of HCC, using a transgenic HCC mouse model. Mechanistically, the BET protein inhibitor JQ1 upregulated the expression of programmed cell death‐ligand 1 (PD‐L1) on the plasma membrane in vivo and in vitro. Moreover, JQ1 enhanced the expression of Rab8A, which upregulated the expression of PD‐L1 on the plasma membrane. This study also showed that JQ1 combined with anti‐PD‐L1 Ab effectively suppressed HCC progression, and this benefit was obtained by enhancing the activation and cytotoxic capabilities of CD8 T cells. These results revealed the crucial role and regulation of BET protein inhibition on the expression of PD‐L1 in HCC. Thus, combining BET protein inhibition with immune checkpoint blockade offers an efficient therapeutic approach for HCC., Treatment with JQ1 enhanced the expression of Rab8A, subsequently inducing programmed cell death‐ligand 1 (PD‐L1) expression on the plasma membrane of hepatocellular carcinoma (HCC), which sensitized the liver response to anti‐PD‐L1 blockade. Thus, a combined treatment of JQ1 and anti‐PD‐L1 Ab was an effective combination immunotherapy for HCC.

Published

2020

18. BET acetyl-lysine binding proteins control pathological cardiac hypertrophy.

Author

Spiltoir, Jessica I., Stratton, Matthew S., Cavasin, Maria A., Demos-Davies, Kim, Reid, Brian G., Qi, Jun, Bradner, James E., and McKinsey, Timothy A.

Subjects

*BROMODOMAIN-containing proteins, *LYSINE, *CARRIER proteins, *PATHOLOGY, *CARDIAC hypertrophy, *HEALTH outcome assessment, *HEART failure patients

Abstract

Abstract: Cardiac hypertrophy is an independent predictor of adverse outcomes in patients with heart failure, and thus represents an attractive target for novel therapeutic intervention. JQ1, a small molecule inhibitor of bromodomain and extraterminal (BET) acetyl-lysine reader proteins, was identified in a high throughput screen designed to discover novel small molecule regulators of cardiomyocyte hypertrophy. JQ1 dose-dependently blocked agonist-dependent hypertrophy of cultured neonatal rat ventricular myocytes (NRVMs) and reversed the prototypical gene program associated with pathological cardiac hypertrophy. JQ1 also blocked left ventricular hypertrophy (LVH) and improved cardiac function in adult mice subjected to transverse aortic constriction (TAC). The BET family consists of BRD2, BRD3, BRD4 and BRDT. BRD4 protein expression was increased during cardiac hypertrophy, and hypertrophic stimuli promoted recruitment of BRD4 to the transcriptional start site (TSS) of the gene encoding atrial natriuretic factor (ANF). Binding of BRD4 to the ANF TSS was associated with increased phosphorylation of local RNA polymerase II. These findings define a novel function for BET proteins as signal-responsive regulators of cardiac hypertrophy, and suggest that small molecule inhibitors of these epigenetic reader proteins have potential as therapeutics for heart failure. [Copyright &y& Elsevier]

Published

2013

19. Identification of the feline foamy virus Bet domain essential for APOBEC3 counteraction.

Author

Lukic, Dragana Slavkovic, Hotz-Wagenblatt, Agnes, Lei, Janet, Räthe, Ann-Mareen, Mühle, Michael, Denner, Joachim, Münk, Carsten, and Löchelt, Martin

Subjects

*FOAMY viruses, *CYTIDINE deaminase, *LENTIVIRUSES, *VIRAL replication, *BIOINFORMATICS, *PROTEIN stability

Abstract

Background: APOBEC3 (A3) proteins restrict viral replication by cytidine deamination of viral DNA genomes and impairing reverse transcription and integration. To escape this restriction, lentiviruses have evolved the viral infectivity factor (Vif), which binds A3 proteins and targets them for proteolytic degradation. In contrast, foamy viruses (FVs) encode Bet proteins that allow replication in the presence of A3, apparently by A3 binding and/or sequestration, thus preventing A3 packaging into virions and subsequent restriction. Due to a long-lasting FV-host coevolution, Bet proteins mainly counteract restriction by A3s from their cognate or highly related host species. Results: Through bioinformatics, we identified conserved motifs in Bet, all localized in the bel2 exon. In line with the localization of these conserved motifs within bel2, this part of feline FV (FFV) Bet has been shown to be essential for feline A3 (feA3) inactivation and feA3 protein binding. To study the function of the Bet motifs in detail, we analyzed the ability of targeted deletion, substitution, and chimeric FFV-PFV (prototype FV) Bet mutants to physically bind and/or inactivate feA3. Binding of Bet to feA3Z2b is sensitive to mutations in the first three conserved motifs and N- and C-terminal deletions and substitutions across almost the complete bel2 coding sequence. In contrast, the Bel1 (also designated Tas) domain of Bet is dispensable for basal feA3Z2b inactivation and binding but mainly increases the steady state level of Bet. Studies with PFV Bel1 and full-length FFV Bel2 chimeras confirmed the importance of Bel2 for A3 inactivation indicating that Bel1 is dispensable for basal feA3Z2b inactivation and binding but increases Bet stability. Moreover, the bel1/tas exon may be required for expression of a fully functional Bet protein from a spliced transcript. Conclusions: We show that the Bel2 domain of FV Bet is essential for the inactivation of APOBEC3 cytidine deaminase restriction factors. The Bel1/Tas domain increases protein stability and can be exchanged by related sequence. Since feA3 binding and inactivation by Bet are highly correlated, the data support the view that FV Bet prevents A3-mediated restriction of viral replication by creating strong complexes with these proteins. [ABSTRACT FROM AUTHOR]

Published

2013

20. Current Understanding of the Role of the Brd4 Protein in the Papillomavirus Lifecycle.

Author

McBride, Alison A. and Moon Kyoo Jang

Subjects

*EPIGENETICS, *CELL cycle, *REPLICATION protein A, *REPLICATION factors (Biochemistry), *PAPILLOMAVIRUS diseases

Abstract

The Brd4 protein is an epigenetic reader that is central to regulation of cellular transcription and mitotic bookmarking. The transcription and replication proteins of many viruses interact with Brd4. We describe the multiple roles of Brd4 in the papillomavirus lifecycle. [ABSTRACT FROM AUTHOR]

Published

2013

21. Immunisation with foamy virus Bet fusion proteins as novel strategy for HIV-1 epitope delivery.

Author

Mühle, Michael, Hoffmann, Kerstin, Löchelt, Martin, and Denner, Joachim

Abstract

The induction of 2F5- and 4E10-like antibodies broadly neutralising HIV-1 and targeting the membrane external proximal region (MPER) of the transmembrane envelope protein gp41 would be a major advancement for the development of a preventive HIV-1 vaccine, but successful attempts remain rare. Recent studies demonstrated that broadly reactive antibodies develop relatively late during infection and after intensive affinity maturation. Therefore, a prolonged antigen delivery might be beneficial to induce them. Replicating foamy viruses which are characterised by apathogenic but persistent infection could represent suitable carrier viruses for this purpose. In order to develop such a system, we modified the accessory foamy virus Bet protein to contain the MPER of gp41, or the MPER linked to the stabilising fusion peptide proximal region of gp41 and analysed here the antigenic and immunogenic properties of such hybrid proteins. The antigens, expressed and purified to homogeneity, were recognised by the monoclonal antibodies 2F5 and 4E10 with nanomolar affinities and induced high levels of antibodies specific to gp41 after immunisation of rats. The antisera also bound to virus particles attached to infected cells, and peptide-based epitope mapping showed that they recognised the 2F5 epitope. Although no HIV-1 neutralising activity was observed, the presented data demonstrate that using the foamy virus Bet for HIV-1 epitope delivery is successfully applicable. Together with the attractive potential for sustained antigen expression after transfer to replicating virus, these results should therefore provide a first basis for the development of chimeric foamy viruses as novel HIV-1 vaccine vectors. [ABSTRACT FROM AUTHOR]

Published

2013

22. Two faces of BRD4.

Author

Devaiah, Ballachanda N. and Singer, Dinah S.

Subjects

*BROMODOMAIN-containing proteins, *CELL cycle, *RNA polymerases, *MITOSIS, *TRANSCRIPTION factors

Abstract

The bromodomain protein BRD4 links cell cycle and transcription, bookmarking active genes during mitosis and serving as a scaffold for transcription factors. Our recent discovery that BRD4 is a RNA Polymerase II CTD kinase identifies a novel transcriptional function. Here we discuss our model in the context of current knowledge. [ABSTRACT FROM AUTHOR]

Published

2013

23. Molecular and functional interactions of cat APOBEC3 and feline foamy and immunodeficiency virus proteins: Different ways to counteract host-encoded restriction

Author

Chareza, Sarah, Slavkovic Lukic, Dragana, Liu, Yang, Räthe, Ann-Mareen, Münk, Carsten, Zabogli, Elisa, Pistello, Mauro, and Löchelt, Martin

Subjects

*FELINE immunodeficiency virus, *FOAMY viruses, *VIRAL proteins, *CYTIDINE deaminase, *PROTEIN-protein interactions, *VIRAL replication

Abstract

Abstract: Defined host-encoded feline APOBEC3 (feA3) cytidine deaminases efficiently restrict the replication and spread of exogenous retroviruses like Feline Immunodeficiency Virus (FIV) and Feline Foamy Virus (FFV) which developed different feA3 counter-acting strategies. Here we characterize the molecular interaction of FFV proteins with the diverse feA3 proteins. The FFV accessory protein Bet is the virus-encoded defense factor which is shown here to bind all feA3 proteins independent of whether they restrict FFV, a feature shared with FIV Vif that induces degradation of all feA3s including those that do not inactivate FIV. In contrast, only some feA3 proteins bind to FFV Gag, a pattern that in part reflects the restriction pattern detected. Additionally, one-domain feA3 proteins can homo- and hetero-dimerize in vitro, but a trans-dominant phenotype of any of the low-activity feA3 forms on FFV restriction by one of the highly-active feA3Z2 proteins was not detectable. [Copyright &y& Elsevier]

Published

2012

24. Inhibition of BET Proteins and Histone Deacetylase (HDACs): Crossing Roads in Cancer Therapy

Author

Alessia Ciarrocchi, Valentina Sancisi, and Gloria Manzotti

Subjects

0301 basic medicine, Cancer Research, Review, BET protein, lcsh:RC254-282, combination therapy, 03 medical and health sciences, 0302 clinical medicine, HDAC, medicine, cancer, Gene, biology, Chemistry, histone modifications, epigenetic drugs, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Chromatin, Cell biology, Bromodomain, 030104 developmental biology, Histone, Oncology, Mechanism of action, Acetylation, 030220 oncology & carcinogenesis, biology.protein, Histone deacetylase, medicine.symptom, Function (biology)

Abstract

Histone DeACetylases (HDACs) are enzymes that remove acetyl groups from histones and other proteins, regulating the expression of target genes. Pharmacological inhibition of these enzymes re-shapes chromatin acetylation status, confusing boundaries between transcriptionally active and quiescent chromatin. This results in reinducing expression of silent genes while repressing highly transcribed genes. Bromodomain and Extraterminal domain (BET) proteins are readers of acetylated chromatin status and accumulate on transcriptionally active regulatory elements where they serve as scaffold for the building of transcription-promoting complexes. The expression of many well-known oncogenes relies on BET proteins function, indicating BET inhibition as a strategy to counteract their activity. BETi and HDACi share many common targets and affect similar cellular processes to the point that combined inhibition of both these classes of proteins is regarded as a strategy to improve the effectiveness of these drugs in cancer. In this work, we aim to discuss the molecular basis of the interplay between HDAC and BET proteins, pointing at chromatin acetylation as a crucial node of their functional interaction. We will also describe the state of the art of their dual inhibition in cancer therapy. Finally, starting from their mechanism of action we will provide a speculative perspective on how these drugs may be employed in combination with standard therapies to improve effectiveness and/or overcome resistance.

Published

2019

25. Bromodomain and extra-terminal motif inhibitors: a review of preclinical and clinical advances in cancer therapy

Author

John Nemunaitis, Abdurahman Ahmad S Alloghbi, Neil Senzer, Ali Alqahtani, Danae M. Hammouda, Talal Khan, Mushtaq Ashraf, and Khalil Choucair

Subjects

0301 basic medicine, medicine.medical_treatment, chemical and pharmacologic phenomena, Review, BET protein, combination therapy, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, Transcription (biology), Gene expression, medicine, cancer, hematological malignancies, BET inhibitors, Transcription factor, clinical trials, biology, hemic and immune systems, Promoter, solid tumors, targeted therapy, Bromodomain, 030104 developmental biology, Histone, Acetylation, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Biotechnology

Abstract

Histone lysine acetylation is critical in regulating transcription. Dysregulation of this process results in aberrant gene expression in various diseases, including cancer. The bromodomain, present in several proteins, recognizes promotor lysine acetylation and recruits other transcription factors. The bromodomain extra-terminal (BET) family of proteins consists of four conserved mammalian members that regulate transcription of oncogenes such as MYC and the NUT fusion oncoprotein. Targeting the acetyl-lysine-binding property of BET proteins is a potential therapeutic approach of cancer. Consequently, following the demonstration that thienotriazolodiazepine small molecules effectively inhibit BET, clinical trials were initiated. We thus discuss the mechanisms of action of various BET inhibitors and the prospects for their clinical use as cancer therapeutics., Lay abstract Addition of acetyl groups to histone proteins that are present in DNA is critical for proper copying of genetic information into producing proteins. This process is dysregulated in various diseases including cancer, resulting in continuous production of oncogenes – genes responsible for promoting cancer – such as NUT and MYC. Bromodomain extra-terminal (BET) proteins mediate acetyl addition, and as a result, transcription. BET inhibitors are small molecules that block the action of BET proteins and the transcription of oncogenes. In this review, we discuss the different available BET inhibitors, the way they act, and their potential use in clinical settings for cancer treatment.

Published

2019

26. Are BET Inhibitors yet Promising Latency-Reversing Agents for HIV-1 Reactivation in AIDS Therapy?

Author

Salahong, Thanarat, Schwartz, Christian, and Sungthong, Rungroch

Subjects

*HIV, *AIDS, *ANTIRETROVIRAL agents, *IMMUNE response, *HIV infections

Abstract

AIDS first emerged decades ago; however, its cure, i.e., eliminating all virus sources, is still unachievable. A critical burden of AIDS therapy is the evasive nature of HIV-1 in face of host immune responses, the so-called "latency." Recently, a promising approach, the "Shock and Kill" strategy, was proposed to eliminate latently HIV-1-infected cell reservoirs. The "Shock and Kill" concept involves two crucial steps: HIV-1 reactivation from its latency stage using a latency-reversing agent (LRA) followed by host immune responses to destroy HIV-1-infected cells in combination with reinforced antiretroviral therapy to kill the progeny virus. Hence, a key challenge is to search for optimal LRAs. Looking at epigenetics of HIV-1 infection, researchers proved that some bromodomains and extra-terminal motif protein inhibitors (BETis) are able to reactivate HIV-1 from latency. However, to date, only a few BETis have shown HIV-1-reactivating functions, and none of them have yet been approved for clinical trial. In this review, we aim to demonstrate the epigenetic roles of BETis in HIV-1 infection and HIV-1-related immune responses. Possible future applications of BETis and their HIV-1-reactivating properties are summarized and discussed. [ABSTRACT FROM AUTHOR]

Published

2021

27. Inhibition of Bromodomain and Extraterminal Domain (BET) Proteins by JQ1 Unravels a Novel Epigenetic Modulation to Control Lipid Homeostasis

Author

Valentina Pallottini, Francesco Berardinelli, Giuseppina Caretti, Marco Segatto, Sabrina Di Bartolomeo, Claudia Tonini, Mayra Colardo, Barbara Colella, Tonini, C., Colardo, M., Colella, B., Di Bartolomeo, S., Berardinelli, F., Caretti, G., Pallottini, V., and Segatto, M.

Subjects

BET protein, Epigenesis, Genetic, lcsh:Chemistry, LDLr, lipid metabolism, BET proteins, Phosphorylation, lcsh:QH301-705.5, Cell proliferation, Spectroscopy, Sterol Regulatory Element Binding Proteins, Chemistry, Epigenetic, Azepines, Hep G2 Cells, General Medicine, Computer Science Applications, Cell biology, Cholesterol, Intracellular, Epigenetics, HMGCR, JQ1, Lipid metabolism, SREBP, TMEM97, Article, Catalysis, Inorganic Chemistry, BET inhibitor, Lipid biosynthesis, Humans, Physical and Theoretical Chemistry, Molecular Biology, epigenetics, Organic Chemistry, Membrane Proteins, Proteins, cholesterol, Triazoles, Sterol regulatory element-binding protein, Bromodomain, cell proliferation, Receptors, LDL, lcsh:Biology (General), lcsh:QD1-999, Hydroxymethylglutaryl CoA Reductases, Homeostasis

Abstract

The homeostatic control of lipid metabolism is essential for many fundamental physiological processes. A deep understanding of its regulatory mechanisms is pivotal to unravel prospective physiopathological factors and to identify novel molecular targets that could be employed to design promising therapies in the management of lipid disorders. Here, we investigated the role of bromodomain and extraterminal domain (BET) proteins in the regulation of lipid metabolism. To reach this aim, we used a loss-of-function approach by treating HepG2 cells with JQ1, a powerful and selective BET inhibitor. The main results demonstrated that BET inhibition by JQ1 efficiently decreases intracellular lipid content, determining a significant modulation of proteins involved in lipid biosynthesis, uptake and intracellular trafficking. Importantly, the capability of BET inhibition to slow down cell proliferation is dependent on the modulation of cholesterol metabolism. Taken together, these data highlight a novel epigenetic mechanism involved in the regulation of lipid homeostasis.

Published

2020

28. CXCL8 histone H3 acetylation is dysfunctional in airway smooth muscle in asthma: regulation by BET

Author

Alison E. John, Alan J. Knox, Rachel L. Clifford, Lisa Mazengarb, Jamie K. Patel, Christopher E. Brightling, and Amanda L. Tatler

Subjects

Transcription, Genetic, Physiology, Cell Cycle Proteins, BET protein, Histones, bromodomain, Transcriptional regulation, p300-CBP Transcription Factors, Promoter Regions, Genetic, Cells, Cultured, Histone Acetyltransferase p300, biology, histone acetylation, Nuclear Proteins, RNA-Binding Proteins, Acetylation, Articles, respiratory system, airway smooth muscle, 3. Good health, Chromatin, DNA-Binding Proteins, Histone, DNA methylation, Airway Remodeling, RNA Polymerase II, Protein Binding, musculoskeletal diseases, Pulmonary and Respiratory Medicine, Myocytes, Smooth Muscle, Primary Cell Culture, Nerve Tissue Proteins, Physiology (medical), CXCl8, Humans, Interleukin 8, Histone H3 acetylation, Inflammation, CCAAT-Enhancer-Binding Protein-beta, Interleukin-8, Transcription Factor RelA, Muscle, Smooth, Cell Biology, asthma, DNA Methylation, respiratory tract diseases, Cancer research, biology.protein, Transcription Factors

Abstract

Asthma is characterized by airway inflammation and remodeling and CXCL8 is a CXC chemokine that drives steroid-resistant neutrophilic airway inflammation. We have shown that airway smooth muscle (ASM) cells isolated from asthmatic individuals secrete more CXCL8 than cells from nonasthmatic individuals. Here we investigated chromatin modifications at the CXCL8 promoter in ASM cells from nonasthmatic and asthmatic donors to further understand how CXCL8 is dysregulated in asthma. ASM cells from asthmatic donors had increased histone H3 acetylation, specifically histone H3K18 acetylation, and increased binding of histone acetyltransferase p300 compared with nonasthmatic donors but no differences in CXCL8 DNA methylation. The acetylation reader proteins Brd3 and Brd4 were bound to the CXCL8 promoter and Brd inhibitors inhibited CXCL8 secretion from ASM cells by disrupting Brd4 and RNA polymerase II binding to the CXCL8 promoter. Our results show a novel dysregulation of CXCL8 transcriptional regulation in asthma characterized by a promoter complex that is abnormal in ASM cells isolated from asthmatic donors and can be modulated by Brd inhibitors. Brd inhibitors may provide a new therapeutic strategy for steroid-resistant inflammation.

Published

2015

29. The Short Isoform of BRD4 Promotes HIV-1 Latency by Engaging Repressive SWI/SNF Chromatin-Remodeling Complexes

Author

Ryan J. Conrad, Sean Thomas, Qiang Zhang, Ming-Ming Zhou, Parinaz Fozouni, Hendrik Sy, and Melanie Ott

Subjects

0301 basic medicine, Time Factors, Transcription, Genetic, Chromosomal Proteins, Non-Histone, T-Lymphocytes, Cell Cycle Proteins, BET protein, Medical and Health Sciences, Jurkat Cells, BRG1, bromodomain, 2.1 Biological and endogenous factors, Protein Isoforms, Viral, Chromatin structure remodeling (RSC) complex, Aetiology, Promoter Regions, Genetic, biology, High-Throughput Nucleotide Sequencing, Nuclear Proteins, Azepines, Biological Sciences, SWI/SNF, Chromatin, Virus Latency, Chromosomal Proteins, Infectious Diseases, Host-Pathogen Interactions, BRD4, HIV/AIDS, RNA Interference, Drug, Infection, Transcription, Protein Binding, Gene isoform, Gene Expression Regulation, Viral, Chromatin Immunoprecipitation, Retroelements, JQ1, LTR, Down-Regulation, Transfection, Chromatin remodeling, Article, Dose-Response Relationship, Promoter Regions, 03 medical and health sciences, Genetic, Genetics, Nucleosome, Humans, Molecular Biology, latency, Dose-Response Relationship, Drug, Human Genome, DNA Helicases, HIV, Non-Histone, DNA, Cell Biology, Triazoles, Chromatin Assembly and Disassembly, Molecular biology, Bromodomain, 030104 developmental biology, HEK293 Cells, Gene Expression Regulation, DNA, Viral, biology.protein, HIV-1, Corepressor, Developmental Biology, Transcription Factors

Abstract

BET proteins commonly activate cellular gene expression, yet inhibiting their recruitment paradoxically reactivates latent HIV-1 transcription. Here weidentify the short isoform of BET family member BRD4 (BRD4S) as a corepressor of HIV-1 transcription. We found that BRD4S was enriched in chromatin fractions of latently infected Tcells, and it was more rapidly displaced from chromatin upon BET inhibition than the long isoform. BET inhibition induced marked nucleosome remodeling at the latent HIV-1 promoter, which was dependent on the activity of BRG1-associated factors (BAF), an SWI/SNF chromatin-remodeling complex with known repressive functions in HIV-1 transcription. BRD4S directly bound BRG1, a catalytic subunit of BAF, via its bromodomain and extraterminal (ET) domain, and this isoform was necessary for BRG1 recruitment to latent HIV-1 chromatin. Using chromatin immunoprecipitation sequencing (ChIP-seq) combined with assay fortransposase-accessible chromatin coupled to high-throughput sequencing (ATAC-seq) data, we found that the latent HIV-1 promoter phenotypically resembles endogenous long terminal repeat (LTR) sequences, pointing to a selectrole of BRD4S-BRG1 complexes in genomic silencing of invasive retroelements.

Published

2016

30. PCNA Unloading Is Negatively Regulated by BET Proteins.

Author

Kang, Mi-Sun, Kim, Jinwoo, Ryu, Eunjin, Ha, Na Young, Hwang, Sunyoung, Kim, Byung-Gyu, Ra, Jae Sun, Kim, Yeong Jae, Hwang, Jung Me, Myung, Kyungjae, and Kang, Sukhyun

Abstract

Proliferating cell nuclear antigen (PCNA) is a DNA clamp essential for DNA replication. During DNA synthesis, PCNA is continuously loaded onto and unloaded from DNA. PCNA recruits various proteins to nascent DNA to facilitate chromosome duplication. Therefore, timely PCNA unloading is crucial for high-fidelity DNA replication. The ATAD5-RFC-like complex (ATAD5-RLC) unloads PCNA from replicated DNA. It is unclear how ATAD5-RLC activity is regulated to prevent premature PCNA unloading. Here, we find that BRD4, an acetyl-histone-binding chromatin reader, inhibits the PCNA-unloading activity of ATAD5-RLC. The BRD4 ET domain interacts with a region upstream of the ATAD5 PCNA-unloading domain. BRD4-ATAD5 binds to acetyl-histones in nascent chromatin. BRD4 release from chromatin correlates with PCNA unloading. Disruption of the interaction between BRD4 and acetyl-histones or between BRD4 and ATAD5 reduces the PCNA amount on chromatin. In contrast, the overexpression of BRD4 increases the amount of chromatin-bound PCNA. Thus, acetyl-histone-bound BRD4 fine-tunes PCNA unloading from nascent DNA. • ATAD5 and BRD4 are enriched on nascent DNA • A conserved region upstream of ATAD5 PCNA-unloading domain binds to BRD4 ET domain • Acetyl-histone-bound BRD4 inhibits PCNA unloading by ATAD5-RLC on nascent DNA Kang et al. demonstrate how PCNA unloading is regulated on nascent chromatin. Timely PCNA unloading from replicated DNA is crucial for faithful DNA replication. BRD4 binds to ATAD5, a subunit of PCNA-unloading complex. Acetyl-histone-bound BRD4 inhibits the activity of ATAD5 complex on nascent chromatin to prevent premature PCNA unloading. [ABSTRACT FROM AUTHOR]

Published

2019

31. Current Understanding of the Role of the Brd4 Protein in the Papillomavirus Lifecycle

Author

Alison A. McBride and Moon Kyoo Jang

Subjects

HPV, replication, BRD4, Transcription, Genetic, viruses, lcsh:QR1-502, Cell Cycle Proteins, Review, Computational biology, Biology, Virus Replication, Models, Biological, BET protein, papillomavirus, lcsh:Microbiology, Viral Proteins, partitioning, Virology, bromodomain, Humans, Epigenetics, Nuclear protein, Cell Cycle Protein, Papillomaviridae, Transcription factor, Genetics, Bookmarking, Nuclear Proteins, Chromatin, Infectious Diseases, Viral replication, Protein Biosynthesis, Host-Pathogen Interactions, Brd4, chromatin, tethering, transcription, Transcription Factors

Abstract

The Brd4 protein is an epigenetic reader that is central to regulation of cellular transcription and mitotic bookmarking. The transcription and replication proteins of many viruses interact with Brd4. We describe the multiple roles of Brd4 in the papillomavirus lifecycle.

Published

2013

32. Epigenetic reader BRD4 inhibition as a therapeutic strategy to suppress E2F2-cell cycle regulation circuit in liver cancer

Author

Jueng Soo You, Jeung Whan Han, Jung Woo Eun, Wahn Soo Choi, Qingyu Shen, Suk Woo Nam, Sung Kyung Choi, and Seong Hwi Hong

Subjects

0301 basic medicine, Cell cycle checkpoint, Carcinoma, Hepatocellular, JQ1, Cell Cycle Proteins, Bioinformatics, epigenetic components, BET protein, Epigenesis, Genetic, 03 medical and health sciences, hepatocellular carcinoma (HCC), E2F2 Transcription Factor, E2F, Cell Line, Tumor, medicine, Humans, Epigenetics, Cell Proliferation, Cell growth, business.industry, Liver Neoplasms, Cancer, Nuclear Proteins, Epigenome, Azepines, Cell Cycle Checkpoints, Hep G2 Cells, Cell cycle, Triazoles, medicine.disease, 030104 developmental biology, Oncology, Cancer research, Liver cancer, business, Transcription Factors, Research Paper

Abstract

Deregulation of the epigenome component affects multiple pathways in the cancer phenotype since the epigenome acts at the pinnacle of the hierarchy of gene expression. Pioneering work over the past decades has highlighted that targeting enzymes or proteins involved in the epigenetic regulation is a valuable approach to cancer therapy. Very recent results demonstrated that inhibiting the epigenetic reader BRD4 has notable efficacy in diverse cancer types. We investigated the potential of BRD4 as a therapeutic target in liver malignancy. BRD4 was overexpressed in three different large cohort of hepatocellular carcinoma (HCC) patients as well as in liver cancer cell lines. BRD4 inhibition by JQ1 induced anti-tumorigenic effects including cell cycle arrest, cellular senescence, reduced wound healing capacity and soft agar colony formation in liver cancer cell lines. Notably, BRD4 inhibition caused MYC-independent large-scale gene expression changes in liver cancer cells. Serial gene expression analyses with SK-Hep1 liver cancer cells treated with JQ1 to delineate the key player of BRD4 inhibition identified E2F2 as the first line of downstream direct target of BRD4. Further experiments including chromatin immunoprecipitation (ChIP) assay and loss of function study confirmed E2F2 as key player of BRD4 inhibition. Overexpressed E2F2 is a crucial center of cell cycle regulation and high expression of E2F2 is significantly associated with poor prognosis of HCC patients. Our findings reveal BRD4-E2F2-cell cycle regulation as a novel molecular circuit in liver cancer and provide a therapeutic strategy and innovative insights for liver cancer therapies.

Published

2016

33. BRD4 regulates self-renewal ability and tumorigenicity of glioma-initiating cells by enrichment in the Notch1 promoter region.

Author

Tao Z, Li X, Wang H, Chen G, Feng Z, Wu Y, Yin H, Zhao G, Deng Z, Zhao C, Li Y, Sun T, and Zhou Y

Abstract

Bromodomain and extraterminal domain (BET) family proteins are considered to be epigenetic readers that regulate gene expression by recognizing acetyl lysine residues on histones and nonhistone chromatin factors and have been classified as curative targets for a variety of cancers. Glioma-initiating cells (GICs), which commit self-renewal, perpetual proliferation, multidirectional differentiation, and vigorous tumorigenicity, sustain the peculiar genetic and epigenetic diversification in the GBM patients, thus, GICs result in tumor recurrence. Abundant evidence demonstrates that BET proteins regulate differentiation of stem cells. However, it endures ambiguous how individual BET proteins take part in GIC advancement, and how do small molecule inhibitors like I-BET151 target functional autonomous BET proteins. Here, we validated that BRD4, not BRD2 or BRD3, has value in targeted glioma therapy. We announce a signaling pathway concerning BRD4 and Notch1 that sustains the self-renewal of GICs. Moreover, in-depth mechanistic research showed that BRD4 was concentrated at the promoter region of Notch1 and may be involved in the process of tumor metabolism. Furthermore, in intracranial models, I-BET151 eliminated U87 GICs' tumorigenicity. The outcomes of this research could be conducive to design clinical trials for treatment of glioma based on BRD4., (© 2020 The Authors. Clinical and Translational Medicine published by John Wiley & Sons Australia, Ltd on behalf of Shanghai Institute of Clinical Bioinformatics.)

Published

2020

34. Discovery, structural insight, and bioactivities of BY27 as a selective inhibitor of the second bromodomains of BET proteins.

Author

Chen, Deheng, Lu, Tian, Yan, Ziqin, Lu, Wenchao, Zhou, Feilong, Lyu, Xilin, Xu, Biling, Jiang, Hualiang, Chen, Kaixian, Luo, Cheng, and Zhao, Yujun

Subjects

*DNA analysis, *TUMOR growth, *GAMBLING, *GENE expression, *CELL analysis, *IMIDAZOPYRIDINES

Abstract

Recently, selective inhibition of BET BD2 is emerging as a promising strategy for drug discovery. Despite significant progress in this area, systematic studies of selective BET BD2 inhibitors are still few. In this study, we report the discovery of a potent and selective BET BD2 inhibitor BY27 (47). Our high resolution co-crystal structures of 47 /BRD2 BD1 and BD2 showed that the triazole group of 47 , water molecules, H433 and N429 in BRD2 BD2 established a water-bridged H-bonding network, which is responsible for the observed selectivities. DNA microarray analysis of HepG2 cells treated with 47 or OTX015 demonstrated the transcriptome impact differences between a BET BD2 selective inhibitor and a pan BET inhibitor. In a MV4-11 mouse xenograft model, 47 caused 67% of tumor growth inhibition and was less toxic than a pan BET inhibitor 1 at high doses. We conclude that the improved safety profile of selective BET BD2 inhibitors warrant future studies in BET associated diseases. Image 1 • A potent and selectively inhibitor of BET BD2, BY27 , has been synthesized. • Two co-crystal structures of BY27 /BRD2 BD1 and BY27 /BRD2 BD2 have been obtained. • DNA microarray analysis shows gene expression alteration features of BY27. • BY27 is efficacious in MV4-11 mouse tumor xenograft model. • In vivo data suggested BY27 has better safety profile in mice. [ABSTRACT FROM AUTHOR]

Published

2019

35. Inhibition of BET Proteins and Histone Deacetylase (HDACs): Crossing Roads in Cancer Therapy.

Author

Manzotti, Gloria, Ciarrocchi, Alessia, and Sancisi, Valentina

Subjects

*CHROMOSOMES, *DRUG resistance, *GENE expression, *HYDROLASES, *ONCOGENES, *TRANSCRIPTION factors, *TUMORS, *TREATMENT effectiveness, *DNA methylation

Abstract

Histone DeACetylases (HDACs) are enzymes that remove acetyl groups from histones and other proteins, regulating the expression of target genes. Pharmacological inhibition of these enzymes re-shapes chromatin acetylation status, confusing boundaries between transcriptionally active and quiescent chromatin. This results in reinducing expression of silent genes while repressing highly transcribed genes. Bromodomain and Extraterminal domain (BET) proteins are readers of acetylated chromatin status and accumulate on transcriptionally active regulatory elements where they serve as scaffold for the building of transcription-promoting complexes. The expression of many well-known oncogenes relies on BET proteins function, indicating BET inhibition as a strategy to counteract their activity. BETi and HDACi share many common targets and affect similar cellular processes to the point that combined inhibition of both these classes of proteins is regarded as a strategy to improve the effectiveness of these drugs in cancer. In this work, we aim to discuss the molecular basis of the interplay between HDAC and BET proteins, pointing at chromatin acetylation as a crucial node of their functional interaction. We will also describe the state of the art of their dual inhibition in cancer therapy. Finally, starting from their mechanism of action we will provide a speculative perspective on how these drugs may be employed in combination with standard therapies to improve effectiveness and/or overcome resistance. [ABSTRACT FROM AUTHOR]

Published

2019

36. Bromodomain and extra-terminal motif inhibitors: a review of preclinical and clinical advances in cancer therapy.

Author

Alqahtani A, Choucair K, Ashraf M, Hammouda DM, Alloghbi A, Khan T, Senzer N, and Nemunaitis J

Abstract

Histone lysine acetylation is critical in regulating transcription. Dysregulation of this process results in aberrant gene expression in various diseases, including cancer. The bromodomain, present in several proteins, recognizes promotor lysine acetylation and recruits other transcription factors. The bromodomain extra-terminal (BET) family of proteins consists of four conserved mammalian members that regulate transcription of oncogenes such as MYC and the NUT fusion oncoprotein. Targeting the acetyl-lysine-binding property of BET proteins is a potential therapeutic approach of cancer. Consequently, following the demonstration that thienotriazolodiazepine small molecules effectively inhibit BET, clinical trials were initiated. We thus discuss the mechanisms of action of various BET inhibitors and the prospects for their clinical use as cancer therapeutics., Competing Interests: Financial & competing interests disclosure The authors have no relevant affiliations or financial involvement with any organization or entity with a financial interest in or financial conflict with the subject matter or materials discussed in the manuscript. This includes employment, consultancies, honoraria, stock ownership or options, expert testimony, grants or patents received or pending, or royalties. No writing assistance was utilized in the production of this manuscript.

Published

2019

37. Defining the Mechanism of Action of Bromodomain and Extraterminal Inhibitors in Triple-Negative Breast Cancers

Author

Brancato, Jennifer M.

Subjects

Pharmacology, Oncology, Biomedical Research, Breast cancer, BET protein, BET inhibitor, LIN9, Aurora kinase, apoptosis, senescence, mitotic catastrophe

Abstract

Inhibitors of the Bromodomain and Extraterminal (BET) family of epigenetic readers have been extensively studied in a wide range of cancers, and several are being assessed in clinical trials for their safety and efficacy in both hematologic and solid tumors. However, we have a very limited understanding of the mechanism(s) of action of these drugs in cancer. It is important to determine how BET inhibitors (BETi) elicit their effects in order to identify patients who will benefit most from the therapy and to develop effective combination treatments that will provide durable responses and prevent resistance. Our studies centered on identifying the mechanism of action of BETi in triple-negative breast cancer (TNBC), an aggressive disease that lacks effective targeted therapies. We found that BETi induced multinucleation in TNBC due in part to the suppression of the critical mitosis regulators Aurora kinases A/B, and this was followed by apoptosis and senescence. The appearance of multinucleated cells coincided with the suppression of mitosis genes, increased mitotic timing, and the induction of apoptosis during mitosis or immediately following mitotic exit, all of which indicate that BETi induce mitotic catastrophe. We further discovered that LIN9, a member of the MuvB transcriptional regulatory complex, is a key mediator of BETi activity in TNBC. BETi disrupt binding of the BET protein BRD4 to the promoter of LIN9, leading to LIN9 downregulation, which in turn suppresses expression of mitosis genes and induces multinucleation. While the selectivity of BETi for cancer cells has been attributed to the dismantling of super-enhancers (SE) by BETi, our studies revealed that LIN9 and four other critical mitosis regulators lacked SEs, indicating BETi-induced mitotic catastrophe does not rely on the disruption of SEs. Finally, we discovered TNBCs may be particularly dependent on LIN9 expression. LIN9 is amplified/overexpressed in two-thirds of TNBCs, and high LIN9 expression is associated with poor survival. Together, these data reveal that tumors with amplified/overexpressed LIN9 such as TNBCs may be particularly responsive to BETi. They further suggest that an effective therapy to treat TNBC could be the combination of BETi and drugs that increase sensitivity to mitotic catastrophe.

Published

2018

38. Recurrent mutations, including NPM1c, activate a BRD4-dependent core transcriptional program in acute myeloid leukemia

Author

M A, Dawson, E J, Gudgin, S J, Horton, G, Giotopoulos, E, Meduri, S, Robson, E, Cannizzaro, H, Osaki, M, Wiese, S, Putwain, C Y, Fong, C, Grove, J, Craig, A, Dittmann, D, Lugo, P, Jeffrey, G, Drewes, K, Lee, L, Bullinger, R K, Prinjha, T, Kouzarides, G S, Vassiliou, and B J P, Huntly

Subjects

Transcriptional Activation, Transcription, Genetic, Gene Expression Regulation, Leukemic, Gene Expression Profiling, Drug Evaluation, Preclinical, Nuclear Proteins, epigenetic therapy, Cell Cycle Proteins, acute myeloid leukemia, Xenograft Model Antitumor Assays, BET protein, Benzodiazepines, Disease Models, Animal, Leukemia, Myeloid, Acute, Mice, hemic and lymphatic diseases, Cell Line, Tumor, nucleophosmin mutation, Animals, Humans, biomarker, Original Article, Nucleophosmin, Transcription Factors

Abstract

Recent evidence suggests that inhibition of bromodomain and extra-terminal (BET) epigenetic readers may have clinical utility against acute myeloid leukemia (AML). Here we validate this hypothesis, demonstrating the efficacy of the BET inhibitor I-BET151 across a variety of AML subtypes driven by disparate mutations. We demonstrate that a common ‘core' transcriptional program, which is HOX gene independent, is downregulated in AML and underlies sensitivity to I-BET treatment. This program is enriched for genes that contain ‘super-enhancers', recently described regulatory elements postulated to control key oncogenic driver genes. Moreover, our program can independently classify AML patients into distinct cytogenetic and molecular subgroups, suggesting that it contains biomarkers of sensitivity and response. We focus AML with mutations of the Nucleophosmin gene (NPM1) and show evidence to suggest that wild-type NPM1 has an inhibitory influence on BRD4 that is relieved upon NPM1c mutation and cytosplasmic dislocation. This leads to the upregulation of the core transcriptional program facilitating leukemia development. This program is abrogated by I-BET therapy and by nuclear restoration of NPM1. Finally, we demonstrate the efficacy of I-BET151 in a unique murine model and in primary patient samples of NPM1c AML. Taken together, our data support the use of BET inhibitors in clinical trials in AML.

Published

2013

39. Identification of the feline foamy virus Bet domain essential for APOBEC3 counteraction

Author

Ann-Mareen Räthe, Michael Mühle, Martin Löchelt, Carsten Münk, Dragana Slavkovic Lukic, Joachim Denner, Agnes Hotz-Wagenblatt, and Janet Lei

Subjects

Retroviridae Proteins, chemical and pharmacologic phenomena, Bet protein, Plasma protein binding, Host-virus interaction, Cell Line, Cytosine Deaminase, Protein structure, Retrovirus, Cytidine deamination, Virology, Animals, Protein Interaction Domains and Motifs, Spumavirus, Virus defence protein, biology, Research, hemic and immune systems, APOBEC3, Cytidine deaminase, biology.organism_classification, Molecular biology, Viral infectivity factor, Infectious Diseases, Viral replication, Cats, Foamy virus, Antiviral restriction factors, Protein Binding

Abstract

Background APOBEC3 (A3) proteins restrict viral replication by cytidine deamination of viral DNA genomes and impairing reverse transcription and integration. To escape this restriction, lentiviruses have evolved the viral infectivity factor (Vif), which binds A3 proteins and targets them for proteolytic degradation. In contrast, foamy viruses (FVs) encode Bet proteins that allow replication in the presence of A3, apparently by A3 binding and/or sequestration, thus preventing A3 packaging into virions and subsequent restriction. Due to a long-lasting FV-host coevolution, Bet proteins mainly counteract restriction by A3s from their cognate or highly related host species. Results Through bioinformatics, we identified conserved motifs in Bet, all localized in the bel2 exon. In line with the localization of these conserved motifs within bel2, this part of feline FV (FFV) Bet has been shown to be essential for feline A3 (feA3) inactivation and feA3 protein binding. To study the function of the Bet motifs in detail, we analyzed the ability of targeted deletion, substitution, and chimeric FFV-PFV (prototype FV) Bet mutants to physically bind and/or inactivate feA3. Binding of Bet to feA3Z2b is sensitive to mutations in the first three conserved motifs and N- and C-terminal deletions and substitutions across almost the complete bel2 coding sequence. In contrast, the Bel1 (also designated Tas) domain of Bet is dispensable for basal feA3Z2b inactivation and binding but mainly increases the steady state level of Bet. Studies with PFV Bel1 and full-length FFV Bel2 chimeras confirmed the importance of Bel2 for A3 inactivation indicating that Bel1 is dispensable for basal feA3Z2b inactivation and binding but increases Bet stability. Moreover, the bel1/tas exon may be required for expression of a fully functional Bet protein from a spliced transcript. Conclusions We show that the Bel2 domain of FV Bet is essential for the inactivation of APOBEC3 cytidine deaminase restriction factors. The Bel1/Tas domain increases protein stability and can be exchanged by related sequence. Since feA3 binding and inactivation by Bet are highly correlated, the data support the view that FV Bet prevents A3-mediated restriction of viral replication by creating strong complexes with these proteins.

Published

2013

40. Molecular and functional interactions of cat APOBEC3 and feline foamy and immunodeficiency virus proteins: different ways to counteract host-encoded restriction

Author

Ann-Mareen Räthe, Dragana Slavkovic Lukic, Elisa Zabogli, Mauro Pistello, Carsten Münk, Sarah Chareza, Martin Löchelt, and Yang Liu

Subjects

APOBEC3 cytidine deaminase, APOBEC, Feline immunodeficiency virus, Vif protein, viruses, Feline foamy virus, Bet protein, Biology, Immunodeficiency Virus, Feline, Cat Diseases, Immunodeficiency virus, Cell Line, chemistry.chemical_compound, Viral Proteins, Virology, Cytidine Deaminase, Feline Acquired Immunodeficiency Syndrome, Animals, Anti-viral restriction, FIV, Restriction factors, Host (biology), Cytidine, biology.organism_classification, Phenotype, In vitro, chemistry, Host-Pathogen Interactions, Cats, Spumavirus, Foamy virus, Protein Binding, Retroviridae Infections

Abstract

Defined host-encoded feline APOBEC3 (feA3) cytidine deaminases efficiently restrict the replication and spread of exogenous retroviruses like Feline Immunodeficiency Virus (FIV) and Feline Foamy Virus (FFV) which developed different feA3 counter-acting strategies. Here we characterize the molecular interaction of FFV proteins with the diverse feA3 proteins. The FFV accessory protein Bet is the virus-encoded defense factor which is shown here to bind all feA3 proteins independent of whether they restrict FFV, a feature shared with FIV Vif that induces degradation of all feA3s including those that do not inactivate FIV. In contrast, only some feA3 proteins bind to FFV Gag, a pattern that in part reflects the restriction pattern detected. Additionally, one-domain feA3 proteins can homo- and hetero-dimerize in vitro, but a trans-dominant phenotype of any of the low-activity feA3 forms on FFV restriction by one of the highly-active feA3Z2 proteins was not detectable.

Published

2011

41. Epigenetic reader BRD4 inhibition as a therapeutic strategy to suppress E2F2-cell cycle regulation circuit in liver cancer.

Author

Hong SH, Eun JW, Choi SK, Shen Q, Choi WS, Han JW, Nam SW, and You JS

Subjects

Carcinoma, Hepatocellular pathology, Cell Cycle Checkpoints drug effects, Cell Cycle Checkpoints genetics, Cell Cycle Proteins, Cell Line, Tumor, Cell Proliferation drug effects, Cell Proliferation genetics, E2F2 Transcription Factor genetics, Epigenesis, Genetic, Hep G2 Cells, Humans, Liver Neoplasms pathology, Nuclear Proteins biosynthesis, Nuclear Proteins genetics, Transcription Factors biosynthesis, Transcription Factors genetics, Azepines pharmacology, Carcinoma, Hepatocellular drug therapy, Carcinoma, Hepatocellular genetics, E2F2 Transcription Factor antagonists & inhibitors, Liver Neoplasms drug therapy, Liver Neoplasms genetics, Nuclear Proteins antagonists & inhibitors, Transcription Factors antagonists & inhibitors, Triazoles pharmacology

Abstract

Deregulation of the epigenome component affects multiple pathways in the cancer phenotype since the epigenome acts at the pinnacle of the hierarchy of gene expression. Pioneering work over the past decades has highlighted that targeting enzymes or proteins involved in the epigenetic regulation is a valuable approach to cancer therapy. Very recent results demonstrated that inhibiting the epigenetic reader BRD4 has notable efficacy in diverse cancer types. We investigated the potential of BRD4 as a therapeutic target in liver malignancy. BRD4 was overexpressed in three different large cohort of hepatocellular carcinoma (HCC) patients as well as in liver cancer cell lines. BRD4 inhibition by JQ1 induced anti-tumorigenic effects including cell cycle arrest, cellular senescence, reduced wound healing capacity and soft agar colony formation in liver cancer cell lines. Notably, BRD4 inhibition caused MYC-independent large-scale gene expression changes in liver cancer cells. Serial gene expression analyses with SK-Hep1 liver cancer cells treated with JQ1 to delineate the key player of BRD4 inhibition identified E2F2 as the first line of downstream direct target of BRD4. Further experiments including chromatin immunoprecipitation (ChIP) assay and loss of function study confirmed E2F2 as key player of BRD4 inhibition. Overexpressed E2F2 is a crucial center of cell cycle regulation and high expression of E2F2 is significantly associated with poor prognosis of HCC patients. Our findings reveal BRD4-E2F2-cell cycle regulation as a novel molecular circuit in liver cancer and provide a therapeutic strategy and innovative insights for liver cancer therapies., Competing Interests: The authors have declared that no competing interests exist.

Published

2016