Your search keyword '"Kung, Andrew L."' showing total 24 results

1. BET bromodomain proteins regulate enhancer function during adipogenesis.

Author

Brown JD, Feldman ZB, Doherty SP, Reyes JM, Rahl PB, Lin CY, Sheng Q, Duan Q, Federation AJ, Kung AL, Haldar SM, Young RA, Plutzky J, and Bradner JE

Subjects

Adipogenesis, Adipose Tissue physiology, Animals, Cell Differentiation, Male, Mice, Adipocytes physiology, Adipose Tissue cytology, Gene Expression Regulation physiology, Nuclear Proteins metabolism, Transcription Factors metabolism

Abstract

Developmental transitions are guided by master regulatory transcription factors. During adipogenesis, a transcriptional cascade culminates in the expression of PPARγ and C/EBPα, which orchestrate activation of the adipocyte gene expression program. However, the coactivators controlling PPARγ and C/EBPα expression are less well characterized. Here, we show the bromodomain-containing protein, BRD4, regulates transcription of PPARγ and C/EBPα. Analysis of BRD4 chromatin occupancy reveals that induction of adipogenesis in 3T3L1 fibroblasts provokes dynamic redistribution of BRD4 to de novo super-enhancers proximal to genes controlling adipocyte differentiation. Inhibition of the bromodomain and extraterminal domain (BET) family of bromodomain-containing proteins impedes BRD4 occupancy at these de novo enhancers and disrupts transcription of Pparg and Cebpa , thereby blocking adipogenesis. Furthermore, silencing of these BRD4-occupied distal regulatory elements at the Pparg locus by CRISPRi demonstrates a critical role for these enhancers in the control of Pparg gene expression and adipogenesis in 3T3L1s. Together, these data establish BET bromodomain proteins as time- and context-dependent coactivators of the adipocyte cell state transition., Competing Interests: Conflict of interest statement: J.D.B., J.P., and J.E.B. have a patent filed on Compositions and Methods for Modulating Metabolism (application no. PCT/US2011/036647) in which BET bromodomain inhibition is used to modulate metabolic diseases including obesity and fatty liver. J.E.B. is now an executive and shareholder of Novartis AG., (Copyright © 2018 the Author(s). Published by PNAS.)

Published

2018

2. An in-tumor genetic screen reveals that the BET bromodomain protein, BRD4, is a potential therapeutic target in ovarian carcinoma.

Author

Baratta MG, Schinzel AC, Zwang Y, Bandopadhayay P, Bowman-Colin C, Kutt J, Curtis J, Piao H, Wong LC, Kung AL, Beroukhim R, Bradner JE, Drapkin R, Hahn WC, Liu JF, and Livingston DM

Subjects

Animals, Carcinoma, Ovarian Epithelial, Cell Cycle Proteins, Cell Line, Tumor, Cell Proliferation, Female, Genetic Association Studies, Humans, Mice, Proto-Oncogene Proteins c-myc metabolism, RNA, Small Interfering metabolism, Xenograft Model Antitumor Assays, Genetic Testing, Molecular Targeted Therapy, Neoplasms, Glandular and Epithelial genetics, Neoplasms, Glandular and Epithelial therapy, Nuclear Proteins metabolism, Ovarian Neoplasms genetics, Ovarian Neoplasms therapy, Transcription Factors metabolism

Abstract

High-grade serous ovarian carcinoma (HGSOC) is the most common and aggressive form of epithelial ovarian cancer, for which few targeted therapies exist. To search for new therapeutic target proteins, we performed an in vivo shRNA screen using an established human HGSOC cell line growing either subcutaneously or intraperitoneally in immunocompromised mice. We identified genes previously implicated in ovarian cancer such as AURKA1, ERBB3, CDK2, and mTOR, as well as several novel candidates including BRD4, VRK1, and GALK2. We confirmed, using both genetic and pharmacologic approaches, that the activity of BRD4, an epigenetic transcription modulator, is necessary for proliferation/survival of both an established human ovarian cancer cell line (OVCAR8) and a subset of primary serous ovarian cancer cell strains (DFs). Among the DFs tested, the strains sensitive to BRD4 inhibition revealed elevated expression of either MYCN or c-MYC, with MYCN expression correlating closely with JQ1 sensitivity. Accordingly, primary human xenografts derived from high-MYCN or c-MYC strains exhibited sensitivity to BRD4 inhibition. These data suggest that BRD4 inhibition represents a new therapeutic approach for MYC-overexpressing HGSOCs.

Published

2015

3. An epigenetic mechanism of resistance to targeted therapy in T cell acute lymphoblastic leukemia.

Author

Knoechel B, Roderick JE, Williamson KE, Zhu J, Lohr JG, Cotton MJ, Gillespie SM, Fernandez D, Ku M, Wang H, Piccioni F, Silver SJ, Jain M, Pearson D, Kluk MJ, Ott CJ, Shultz LD, Brehm MA, Greiner DL, Gutierrez A, Stegmaier K, Kung AL, Root DE, Bradner JE, Aster JC, Kelliher MA, and Bernstein BE

Subjects

Animals, Azepines pharmacology, Cell Cycle Proteins, Cell Line, Tumor, Chromatin metabolism, Chromatin Immunoprecipitation, Enzyme-Linked Immunosorbent Assay, Flow Cytometry, Gene Expression Regulation, Neoplastic drug effects, Gene Expression Regulation, Neoplastic genetics, Histones metabolism, Humans, Indoles, Mice, Nuclear Proteins antagonists & inhibitors, Nuclear Proteins genetics, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Real-Time Polymerase Chain Reaction, Receptor, Notch1 antagonists & inhibitors, Receptor, Notch1 genetics, Signal Transduction genetics, Transcription Factors antagonists & inhibitors, Transcription Factors genetics, Triazoles pharmacology, Amyloid Precursor Protein Secretases antagonists & inhibitors, Chromatin genetics, Drug Resistance, Neoplasm genetics, Enzyme Inhibitors therapeutic use, Epigenesis, Genetic genetics, Nuclear Proteins metabolism, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma genetics, Transcription Factors metabolism

Abstract

The identification of activating NOTCH1 mutations in T cell acute lymphoblastic leukemia (T-ALL) led to clinical testing of γ-secretase inhibitors (GSIs) that prevent NOTCH1 activation. However, responses to these inhibitors have been transient, suggesting that resistance limits their clinical efficacy. Here we modeled T-ALL resistance, identifying GSI-tolerant 'persister' cells that expand in the absence of NOTCH1 signaling. Rare persisters are already present in naive T-ALL populations, and the reversibility of their phenotype suggests an epigenetic mechanism. Relative to GSI-sensitive cells, persister cells activate distinct signaling and transcriptional programs and exhibit chromatin compaction. A knockdown screen identified chromatin regulators essential for persister viability, including BRD4. BRD4 binds enhancers near critical T-ALL genes, including MYC and BCL2. The BRD4 inhibitor JQ1 downregulates expression of these targets and induces growth arrest and apoptosis in persister cells, at doses well tolerated by GSI-sensitive cells. Consistently, the GSI-JQ1 combination was found to be effective against primary human leukemias in vivo. Our findings establish a role for epigenetic heterogeneity in leukemia resistance that may be addressed by incorporating epigenetic modulators in combination therapy.

Published

2014

4. Discovery and characterization of super-enhancer-associated dependencies in diffuse large B cell lymphoma.

Author

Chapuy B, McKeown MR, Lin CY, Monti S, Roemer MG, Qi J, Rahl PB, Sun HH, Yeda KT, Doench JG, Reichert E, Kung AL, Rodig SJ, Young RA, Shipp MA, and Bradner JE

Subjects

Azepines pharmacology, Cell Cycle Proteins, DNA-Binding Proteins genetics, Genes, myc, Humans, Promoter Regions, Genetic, Proto-Oncogene Proteins c-bcl-6, Trans-Activators physiology, Transcription, Genetic, Triazoles pharmacology, Enhancer Elements, Genetic, Lymphoma, Large B-Cell, Diffuse genetics, Nuclear Proteins genetics, Transcription Factors genetics

Abstract

Diffuse large B cell lymphoma (DLBCL) is a biologically heterogeneous and clinically aggressive disease. Here, we explore the role of bromodomain and extra-terminal domain (BET) proteins in DLBCL, using integrative chemical genetics and functional epigenomics. We observe highly asymmetric loading of bromodomain 4 (BRD4) at enhancers, with approximately 33% of all BRD4 localizing to enhancers at 1.6% of occupied genes. These super-enhancers prove particularly sensitive to bromodomain inhibition, explaining the selective effect of BET inhibitors on oncogenic and lineage-specific transcriptional circuits. Functional study of genes marked by super-enhancers identifies DLBCLs dependent on OCA-B and suggests a strategy for discovering unrecognized cancer dependencies. Translational studies performed on a comprehensive panel of DLBCLs establish a therapeutic rationale for evaluating BET inhibitors in this disease., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

5. Efficacy of BET bromodomain inhibition in Kras-mutant non-small cell lung cancer.

Author

Shimamura T, Chen Z, Soucheray M, Carretero J, Kikuchi E, Tchaicha JH, Gao Y, Cheng KA, Cohoon TJ, Qi J, Akbay E, Kimmelman AC, Kung AL, Bradner JE, and Wong KK

Subjects

AMP-Activated Protein Kinases, Animals, Apoptosis drug effects, Carcinoma, Non-Small-Cell Lung genetics, Cell Line, Tumor, Cell Proliferation drug effects, Lung Neoplasms genetics, Mice, Mice, Knockout, Nuclear Proteins genetics, Protein Serine-Threonine Kinases genetics, Proto-Oncogene Proteins c-myc antagonists & inhibitors, Proto-Oncogene Proteins c-myc biosynthesis, Proto-Oncogene Proteins c-myc genetics, RNA Interference, RNA, Small Interfering, Signal Transduction drug effects, Transcription Factors genetics, Azepines pharmacology, Carcinoma, Non-Small-Cell Lung drug therapy, Lung Neoplasms drug therapy, Nuclear Proteins antagonists & inhibitors, Proto-Oncogene Proteins p21(ras) genetics, Transcription Factors antagonists & inhibitors, Triazoles pharmacology

Abstract

Purpose: Amplification of MYC is one of the most common genetic alterations in lung cancer, contributing to a myriad of phenotypes associated with growth, invasion, and drug resistance. Murine genetics has established both the centrality of somatic alterations of Kras in lung cancer, as well as the dependency of mutant Kras tumors on MYC function. Unfortunately, drug-like small-molecule inhibitors of KRAS and MYC have yet to be realized. The recent discovery, in hematologic malignancies, that bromodomain and extra-terminal (BET) bromodomain inhibition impairs MYC expression and MYC transcriptional function established the rationale of targeting KRAS-driven non-small cell lung cancer (NSCLC) with BET inhibition., Experimental Design: We performed functional assays to evaluate the effects of JQ1 in genetically defined NSCLC cell lines harboring KRAS and/or LKB1 mutations. Furthermore, we evaluated JQ1 in transgenic mouse lung cancer models expressing mutant kras or concurrent mutant kras and lkb1. Effects of bromodomain inhibition on transcriptional pathways were explored and validated by expression analysis., Results: Although JQ1 is broadly active in NSCLC cells, activity of JQ1 in mutant KRAS NSCLC is abrogated by concurrent alteration or genetic knockdown of LKB1. In sensitive NSCLC models, JQ1 treatment results in the coordinate downregulation of the MYC-dependent transcriptional program. We found that JQ1 treatment produces significant tumor regression in mutant kras mice. As predicted, tumors from mutant kras and lkb1 mice did not respond to JQ1., Conclusion: Bromodomain inhibition comprises a promising therapeutic strategy for KRAS-mutant NSCLC with wild-type LKB1, via inhibition of MYC function. Clinical studies of BET bromodomain inhibitors in aggressive NSCLC will be actively pursued. Clin Cancer Res; 19(22); 6183-92. ©2013 AACR.

Published

2013

6. Oncogenic BRAF regulates oxidative metabolism via PGC1α and MITF.

Author

Haq R, Shoag J, Andreu-Perez P, Yokoyama S, Edelman H, Rowe GC, Frederick DT, Hurley AD, Nellore A, Kung AL, Wargo JA, Song JS, Fisher DE, Arany Z, and Widlund HR

Subjects

Apoptosis, Cell Line, Tumor, Gene Expression Regulation, Neoplastic, Heat-Shock Proteins genetics, Humans, Indoles pharmacology, Melanocytes metabolism, Melanoma genetics, Mitochondria metabolism, Mitogen-Activated Protein Kinases metabolism, Mutation, Oxidative Phosphorylation, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Proto-Oncogene Proteins B-raf antagonists & inhibitors, Proto-Oncogene Proteins B-raf genetics, RNA, Messenger biosynthesis, Signal Transduction, Sulfonamides pharmacology, Transcription Factors genetics, Vemurafenib, Heat-Shock Proteins metabolism, Melanoma metabolism, Microphthalmia-Associated Transcription Factor metabolism, Proto-Oncogene Proteins B-raf metabolism, Transcription Factors metabolism

Abstract

Activating mutations in BRAF are the most common genetic alterations in melanoma. Inhibition of BRAF by small molecules leads to cell-cycle arrest and apoptosis. We show here that BRAF inhibition also induces an oxidative phosphorylation gene program, mitochondrial biogenesis, and the increased expression of the mitochondrial master regulator, PGC1α. We further show that a target of BRAF, the melanocyte lineage factor MITF, directly regulates the expression of PGC1α. Melanomas with activation of the BRAF/MAPK pathway have suppressed levels of MITF and PGC1α and decreased oxidative metabolism. Conversely, treatment of BRAF-mutated melanomas with BRAF inhibitors renders them addicted to oxidative phosphorylation. Our data thus identify an adaptive metabolic program that limits the efficacy of BRAF inhibitors., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

7. Targeting MYCN in neuroblastoma by BET bromodomain inhibition.

Author

Puissant A, Frumm SM, Alexe G, Bassil CF, Qi J, Chanthery YH, Nekritz EA, Zeid R, Gustafson WC, Greninger P, Garnett MJ, McDermott U, Benes CH, Kung AL, Weiss WA, Bradner JE, and Stegmaier K

Subjects

Animals, Apoptosis drug effects, Apoptosis genetics, Azepines pharmacology, Cell Cycle Checkpoints drug effects, Cell Cycle Checkpoints genetics, Cell Cycle Proteins, Cell Growth Processes genetics, Cell Line, Tumor, Child, Down-Regulation drug effects, Female, Gene Amplification, Humans, Mice, Molecular Targeted Therapy, N-Myc Proto-Oncogene Protein, Neuroblastoma genetics, Neuroblastoma metabolism, Neuroblastoma pathology, Nuclear Proteins deficiency, Oncogene Proteins metabolism, Promoter Regions, Genetic, Protein Structure, Tertiary, Proto-Oncogene Proteins c-myc genetics, RNA, Small Interfering administration & dosage, RNA, Small Interfering genetics, Transcription Factors deficiency, Transcription Factors genetics, Transfection, Triazoles pharmacology, Xenograft Model Antitumor Assays, Neuroblastoma drug therapy, Nuclear Proteins antagonists & inhibitors, Nuclear Proteins genetics, Nuclear Proteins metabolism, Oncogene Proteins genetics, Transcription Factors antagonists & inhibitors, Transcription Factors metabolism

Abstract

Bromodomain inhibition comprises a promising therapeutic strategy in cancer, particularly for hematologic malignancies. To date, however, genomic biomarkers to direct clinical translation have been lacking. We conducted a cell-based screen of genetically defined cancer cell lines using a prototypical inhibitor of BET bromodomains. Integration of genetic features with chemosensitivity data revealed a robust correlation between MYCN amplification and sensitivity to bromodomain inhibition. We characterized the mechanistic and translational significance of this finding in neuroblastoma, a childhood cancer with frequent amplification of MYCN. Genome-wide expression analysis showed downregulation of the MYCN transcriptional program accompanied by suppression of MYCN transcription. Functionally, bromodomain-mediated inhibition of MYCN impaired growth and induced apoptosis in neuroblastoma. BRD4 knockdown phenocopied these effects, establishing BET bromodomains as transcriptional regulators of MYCN. BET inhibition conferred a significant survival advantage in 3 in vivo neuroblastoma models, providing a compelling rationale for developing BET bromodomain inhibitors in patients with neuroblastoma.

Published

2013

8. BET bromodomain inhibition targets both c-Myc and IL7R in high-risk acute lymphoblastic leukemia.

Author

Ott CJ, Kopp N, Bird L, Paranal RM, Qi J, Bowman T, Rodig SJ, Kung AL, Bradner JE, and Weinstock DM

Subjects

Animals, Apoptosis, B-Lymphocytes pathology, Biomarkers, Tumor genetics, Biomarkers, Tumor metabolism, Blotting, Western, Cell Cycle Proteins, Cell Line, Tumor, Cell Proliferation, Chromatin Immunoprecipitation, Flow Cytometry, Gene Expression Profiling, Gene Rearrangement, Humans, Janus Kinase 2 genetics, Janus Kinase 2 metabolism, Mice, Mice, Inbred NOD, Oligonucleotide Array Sequence Analysis, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics, Proto-Oncogene Proteins c-myc genetics, RNA, Messenger genetics, Real-Time Polymerase Chain Reaction, Receptors, Interleukin-7 genetics, Reverse Transcriptase Polymerase Chain Reaction, Risk Factors, STAT5 Transcription Factor genetics, STAT5 Transcription Factor metabolism, Xenograft Model Antitumor Assays, Azepines therapeutic use, Nuclear Proteins antagonists & inhibitors, Precursor Cell Lymphoblastic Leukemia-Lymphoma drug therapy, Precursor Cell Lymphoblastic Leukemia-Lymphoma pathology, Proto-Oncogene Proteins c-myc metabolism, Receptors, Cytokine genetics, Receptors, Interleukin-7 metabolism, Transcription Factors antagonists & inhibitors, Triazoles therapeutic use

Abstract

We investigated the therapeutic potential of JQ1, an inhibitor of the BET class of human bromodomain proteins, in B-cell acute lymphoblastic leukemia (B-ALL). We show that JQ1 potently reduces the viability of B-ALL cell lines with high-risk cytogenetics. Among the most sensitive were lines with rearrangements of CRLF2, which is overexpressed in ~ 10% of B-ALL. CRLF2 heterodimerizes with the IL7 receptor (IL7R) and signals through JAK2, JAK1, and STAT5 to drive proliferation and suppress apoptosis. As previously observed, JQ1 induced the down-regulation of MYC transcription, the loss of BRD4 at the MYC promoter, and the reduced expression of c-Myc target genes. Strikingly, JQ1 also down-regulated IL7R transcription, depleted BRD4 from the IL7R promoter, and reduced JAK2 and STAT5 phosphorylation. Genome-wide expression profiling demonstrated a restricted effect of JQ1 on transcription, with MYC and IL7R being among the most down-regulated genes. Indeed, IL7R was the only cytokine receptor in CRLF2-rearranged B-ALL cells significantly down-regulated by JQ1 treatment. In mice xenografted with primary human CRLF2-rearranged B-ALL, JQ1 suppressed c-Myc expression and STAT5 phosphorylation and significantly prolonged survival. Thus, bromodomain inhibition is a promising therapeutic strategy for B-ALL as well as other conditions dependent on IL7R signaling.

Published

2012

9. Selective inhibition of BET bromodomains.

Author

Filippakopoulos P, Qi J, Picaud S, Shen Y, Smith WB, Fedorov O, Morse EM, Keates T, Hickman TT, Felletar I, Philpott M, Munro S, McKeown MR, Wang Y, Christie AL, West N, Cameron MJ, Schwartz B, Heightman TD, La Thangue N, French CA, Wiest O, Kung AL, Knapp S, and Bradner JE

Subjects

Amino Acid Sequence, Animals, Azirines chemical synthesis, Azirines chemistry, Binding Sites, Carcinoma, Squamous Cell physiopathology, Cell Cycle Proteins, Cell Differentiation drug effects, Cell Line, Tumor, Cell Proliferation drug effects, Chromatin metabolism, Dihydropyridines chemical synthesis, Dihydropyridines chemistry, Female, Humans, Mice, Mice, Nude, Molecular Sequence Data, Protein Binding drug effects, Protein Structure, Tertiary, Recombinant Proteins metabolism, Sequence Alignment, Skin Neoplasms physiopathology, Stereoisomerism, Azirines pharmacology, Dihydropyridines pharmacology, Models, Molecular, Nuclear Proteins antagonists & inhibitors, Nuclear Proteins metabolism, Transcription Factors antagonists & inhibitors, Transcription Factors metabolism

Abstract

Epigenetic proteins are intently pursued targets in ligand discovery. So far, successful efforts have been limited to chromatin modifying enzymes, or so-called epigenetic 'writers' and 'erasers'. Potent inhibitors of histone binding modules have not yet been described. Here we report a cell-permeable small molecule (JQ1) that binds competitively to acetyl-lysine recognition motifs, or bromodomains. High potency and specificity towards a subset of human bromodomains is explained by co-crystal structures with bromodomain and extra-terminal (BET) family member BRD4, revealing excellent shape complementarity with the acetyl-lysine binding cavity. Recurrent translocation of BRD4 is observed in a genetically-defined, incurable subtype of human squamous carcinoma. Competitive binding by JQ1 displaces the BRD4 fusion oncoprotein from chromatin, prompting squamous differentiation and specific antiproliferative effects in BRD4-dependent cell lines and patient-derived xenograft models. These data establish proof-of-concept for targeting protein-protein interactions of epigenetic 'readers', and provide a versatile chemical scaffold for the development of chemical probes more broadly throughout the bromodomain family.

Published

2010

10. Signature-based small molecule screening identifies cytosine arabinoside as an EWS/FLI modulator in Ewing sarcoma.

Author

Stegmaier K, Wong JS, Ross KN, Chow KT, Peck D, Wright RD, Lessnick SL, Kung AL, and Golub TR

Subjects

Animals, Antimetabolites, Antineoplastic therapeutic use, Bone Neoplasms genetics, Bone Neoplasms pathology, Cell Line, Tumor, Cytarabine therapeutic use, Drug Delivery Systems, Fluorescent Dyes analysis, Fluorometry, Gene Amplification, Gene Expression Regulation, Neoplastic drug effects, Humans, Mice, Microspheres, Molecular Structure, Molecular Weight, Oncogene Proteins, Fusion biosynthesis, Oncogene Proteins, Fusion genetics, Proto-Oncogene Protein c-fli-1, RNA Interference, RNA-Binding Protein EWS, Sarcoma, Ewing genetics, Sarcoma, Ewing pathology, Transcription Factors biosynthesis, Transcription Factors genetics, Xenograft Model Antitumor Assays, Antimetabolites, Antineoplastic pharmacology, Bone Neoplasms drug therapy, Cytarabine pharmacology, Drug Screening Assays, Antitumor methods, Gene Expression Profiling, Oncogene Proteins, Fusion drug effects, Sarcoma, Ewing drug therapy, Transcription Factors drug effects

Abstract

Background: The presence of tumor-specific mutations in the cancer genome represents a potential opportunity for pharmacologic intervention to therapeutic benefit. Unfortunately, many classes of oncoproteins (e.g., transcription factors) are not amenable to conventional small-molecule screening. Despite the identification of tumor-specific somatic mutations, most cancer therapy still utilizes nonspecific, cytotoxic drugs. One illustrative example is the treatment of Ewing sarcoma. Although the EWS/FLI oncoprotein, present in the vast majority of Ewing tumors, was characterized over ten years ago, it has never been exploited as a target of therapy. Previously, this target has been intractable to modulation with traditional small-molecule library screening approaches. Here we describe a gene expression-based approach to identify compounds that induce a signature of EWS/FLI attenuation. We hypothesize that screening small-molecule libraries highly enriched for FDA-approved drugs will provide a more rapid path to clinical application., Methods and Findings: A gene expression signature for the EWS/FLI off state was determined with microarray expression profiling of Ewing sarcoma cell lines with EWS/FLI-directed RNA interference. A small-molecule library enriched for FDA-approved drugs was screened with a high-throughput, ligation-mediated amplification assay with a fluorescent, bead-based detection. Screening identified cytosine arabinoside (ARA-C) as a modulator of EWS/FLI. ARA-C reduced EWS/FLI protein abundance and accordingly diminished cell viability and transformation and abrogated tumor growth in a xenograft model. Given the poor outcomes of many patients with Ewing sarcoma and the well-established ARA-C safety profile, clinical trials testing ARA-C are warranted., Conclusions: We demonstrate that a gene expression-based approach to small-molecule library screening can identify, for rapid clinical testing, candidate drugs that modulate previously intractable targets. Furthermore, this is a generic approach that can, in principle, be applied to the identification of modulators of any tumor-associated oncoprotein in the rare pediatric malignancies, but also in the more common adult cancers.

Published

2007

11. Small molecule blockade of transcriptional coactivation of the hypoxia-inducible factor pathway.

Author

Kung AL, Zabludoff SD, France DS, Freedman SJ, Tanner EA, Vieira A, Cornell-Kennon S, Lee J, Wang B, Wang J, Memmert K, Naegeli HU, Petersen F, Eck MJ, Bair KW, Wood AW, and Livingston DM

Subjects

Animals, Aryl Hydrocarbon Receptor Nuclear Translocator, Carcinoma, Hepatocellular pathology, Cell Hypoxia genetics, Colonic Neoplasms metabolism, Colonic Neoplasms pathology, Colonic Neoplasms therapy, Disulfides, E1A-Associated p300 Protein, Erythropoietin metabolism, Humans, Hypoxia-Inducible Factor 1, alpha Subunit, Indole Alkaloids, Liver Neoplasms pathology, Luciferases metabolism, Male, Mice, Mice, Nude, Nuclear Proteins genetics, Prostatic Neoplasms metabolism, Prostatic Neoplasms pathology, Prostatic Neoplasms therapy, Protein Binding drug effects, Receptors, Aryl Hydrocarbon genetics, Reverse Transcriptase Polymerase Chain Reaction, Signal Transduction, Trans-Activators genetics, Transcription Factors genetics, Transplantation, Heterologous, Vascular Endothelial Growth Factor A metabolism, Anti-Bacterial Agents pharmacology, DNA-Binding Proteins, Nuclear Proteins metabolism, Receptors, Aryl Hydrocarbon metabolism, Trans-Activators metabolism, Transcription Factors metabolism, Transcription, Genetic drug effects

Abstract

Homeostasis under hypoxic conditions is maintained through a coordinated transcriptional response mediated by the hypoxia-inducible factor (HIF) pathway and requires coactivation by the CBP and p300 transcriptional coactivators. Through a target-based high-throughput screen, we identified chetomin as a disrupter of HIF binding to p300. At a molecular level, chetomin disrupts the structure of the CH1 domain of p300 and precludes its interaction with HIF, thereby attenuating hypoxia-inducible transcription. Systemic administration of chetomin inhibited hypoxia-inducible transcription within tumors and inhibited tumor growth. These results demonstrate a therapeutic window for pharmacological attenuation of HIF activity and further establish the feasibility of disrupting a signal transduction pathway by targeting the function of a transcriptional coactivator with a small molecule.

Published

2004

12. Structural basis for negative regulation of hypoxia-inducible factor-1alpha by CITED2.

Author

Freedman SJ, Sun ZY, Kung AL, France DS, Wagner G, and Eck MJ

Subjects

Amino Acid Motifs, Amino Acid Sequence, Animals, Circular Dichroism, Humans, Hypoxia-Inducible Factor 1, alpha Subunit, Models, Molecular, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Protein Binding, Protein Conformation, Sequence Homology, Amino Acid, Trans-Activators metabolism, Transcription Factors metabolism, DNA-Binding Proteins, Repressor Proteins, Trans-Activators physiology, Transcription Factors chemistry, Transcription Factors physiology

Abstract

Expression of hypoxia-responsive genes is mediated by the heterodimeric transcription factor hypoxia-inducible factor-1 (HIF-1) in complex with the p300/CREB-binding protein (p300/CBP) transcriptional coactivator. The protein CITED2, which binds p300/CBP, is thought to be a negative regulator of HIF-1 transactivation. We show that the CITED2 transactivation domain (TAD) disrupts a complex of the HIF-1alpha C-terminal TAD (C-TAD) and the cysteine-histidine-rich 1 (CH1) domain of p300/CBP by binding CH1 with high affinity. The high-resolution solution structure of the CITED2 TAD-p300 CH1 complex shows that the CITED2 TAD, like the HIF-1alpha C-TAD, folds on a helical, Zn2+-containing CH1 scaffold. The CITED2 TAD binds a different, more extensive surface of CH1 than does the HIF-1alpha C-TAD. However, a conserved 'LPXL' sequence motif in CITED2 and HIF-1alpha interacts with an overlapping binding site on CH1. Mutation of the LPEL sequence in full-length CITED2 abolishes p300 binding in vivo. These findings reveal that CITED2 regulates HIF-1 by competing for a hot spot on the p300 CH1 domain.

Published

2003

13. Inhibition of FLT3 in MLL. Validation of a therapeutic target identified by gene expression based classification.

Author

Armstrong SA, Kung AL, Mabon ME, Silverman LB, Stam RW, Den Boer ML, Pieters R, Kersey JH, Sallan SE, Fletcher JA, Golub TR, Griffin JD, and Korsmeyer SJ

Subjects

Animals, Annexin A5 metabolism, Child, Preschool, Female, Gene Expression, Histone-Lysine N-Methyltransferase, Humans, In Situ Hybridization, Fluorescence, Interleukin-3 metabolism, Mice, Myeloid-Lymphoid Leukemia Protein, Precursor Cell Lymphoblastic Leukemia-Lymphoma enzymology, Protein Kinase C antagonists & inhibitors, Proto-Oncogene Proteins genetics, Receptor Protein-Tyrosine Kinases genetics, Reverse Transcriptase Polymerase Chain Reaction, Transfection, Tumor Cells, Cultured, fms-Like Tyrosine Kinase 3, Antineoplastic Agents pharmacology, DNA-Binding Proteins genetics, Precursor Cell Lymphoblastic Leukemia-Lymphoma genetics, Proto-Oncogene Proteins antagonists & inhibitors, Proto-Oncogenes, Receptor Protein-Tyrosine Kinases antagonists & inhibitors, Staurosporine analogs & derivatives, Staurosporine pharmacology, Transcription Factors

Abstract

We recently found that MLL-rearranged acute lymphoblastic leukemias (MLL) have a unique gene expression profile including high level expression of the receptor tyrosine kinase FLT3. We hypothesized that FLT3 might be a therapeutic target in MLL and found that 5 of 30 MLLs contain mutations in the activation loop of FLT3 that result in constitutive activation. Three are a newly described deletion of I836 and the others are D835 mutations. The recently described FLT3 inhibitor PKC412 proved cytotoxic to Ba/F3 cells dependent upon activated FLT3 containing either mutation. PKC412 is also differentially cytotoxic to leukemia cells with MLL translocations and FLT3 that is activated by either overexpression of the wild-type receptor or mutation. Finally, we developed a mouse model of MLL and used bioluminescent imaging to determine that PKC412 is active against MLL in vivo.

Published

2003

14. Structural basis for recruitment of CBP/p300 by hypoxia-inducible factor-1 alpha.

Author

Freedman SJ, Sun ZY, Poy F, Kung AL, Livingston DM, Wagner G, and Eck MJ

Subjects

Amino Acid Sequence, Animals, Asparagine chemistry, Escherichia coli metabolism, Humans, Hypoxia-Inducible Factor 1, alpha Subunit, Magnetic Resonance Spectroscopy, Models, Molecular, Molecular Sequence Data, Protein Binding, Protein Conformation, Protein Folding, Protein Structure, Secondary, Protein Structure, Tertiary, Sequence Homology, Amino Acid, Transcription Factors metabolism, Transcriptional Activation, Zinc chemistry, Nuclear Proteins chemistry, Trans-Activators chemistry, Transcription Factors chemistry

Abstract

Adaptation to hypoxia is mediated by transactivation of hypoxia-responsive genes by hypoxia-inducible factor-1 (HIF-1) in complex with the CBP and p300 transcriptional coactivators. We report the solution structure of the cysteine/histidine-rich 1 (CH1) domain of p300 bound to the C-terminal transactivation domain of HIF-1 alpha. CH1 has a triangular geometry composed of four alpha-helices with three intervening Zn(2+)-coordinating centers. CH1 serves as a scaffold for folding of the HIF-1 alpha C-terminal transactivation domain, which forms a vise-like clamp on the CH1 domain that is stabilized by extensive hydrophobic and polar interactions. The structure reveals the mechanism of specific recognition of p300 by HIF-1 alpha, and shows how HIF-1 alpha transactivation is regulated by asparagine hydroxylation.

Published

2002

15. Discovery and Characterization of Super-Enhancer-Associated Dependencies in Diffuse Large B Cell Lymphoma

Author

Chapuy, Bjoern, McKeown, Michael R., Lin, Charles Y., Monti, Stefano, Roemer, Margaretha G.M., Qi, Jun, Rahl, Peter B., Sun, Heather H., Yeda, Kelly T., Doench, John G., Reichert, Elaine, Kung, Andrew L., Rodig, Scott J., Young, Richard A., Shipp, Margaret A., Bradner, James E., Massachusetts Institute of Technology. Department of Biology, Whitehead Institute for Biomedical Research, and Young, Richard A.

Subjects

Cancer Research, BRD4, Transcription, Genetic, Genes, myc, Cell Cycle Proteins, Biology, Article, Super-enhancer, immune system diseases, hemic and lymphatic diseases, medicine, Humans, Promoter Regions, Genetic, Enhancer, Transcription factor, Epigenomics, Nuclear Proteins, Azepines, Cell Biology, Triazoles, medicine.disease, Bromodomain, DNA-Binding Proteins, Enhancer Elements, Genetic, Oncology, Proto-Oncogene Proteins c-bcl-6, Trans-Activators, Cancer research, Lymphoma, Large B-Cell, Diffuse, Diffuse large B-cell lymphoma, Chemical genetics, Transcription Factors

Abstract

Diffuse large B cell lymphoma (DLBCL) is a biologically heterogeneous and clinically aggressive disease. Here, we explore the role of bromodomain and extra-terminal domain (BET) proteins in DLBCL, using integrative chemical genetics and functional epigenomics. We observe highly asymmetric loading of bromodomain 4 (BRD4) at enhancers, with approximately 33% of all BRD4 localizing to enhancers at 1.6% of occupied genes. These super-enhancers prove particularly sensitive to bromodomain inhibition, explaining the selective effect of BET inhibitors on oncogenic and lineage-specific transcriptional circuits. Functional study of genes marked by super-enhancers identifies DLBCLs dependent on OCA-B and suggests a strategy for discovering unrecognized cancer dependencies. Translational studies performed on a comprehensive panel of DLBCLs establish a therapeutic rationale for evaluating BET inhibitors in this disease., Broad Institute of MIT and Harvard (Broad New Idea Award), American Society of Hematology, William Lawrence and Blanche Hughes Foundation, Damon Runyon Cancer Research Foundation, Leukemia & Lymphoma Society of America, National Institutes of Health (U.S.), United States. Department of Defense (CDMRP CA120184), American Cancer Society (PF-11-042-01-DMC), Deutsche Forschungsgemeinschaft (DFG Ch 735/1-1)

Published

2013

16. Direct inhibition of the NOTCH transcription factor complex.

Author

Moellering, Raymond E., Cornejo, Melanie, Davis, Tina N., Bianco, Cristina Del, Aster, Jon C., Blacklow, Stephen C., Kung, Andrew L., Gilliland, D. Gary, Verdine, Gregory L., and Bradner, James E.

Subjects

TRANSCRIPTION factors, PROTEINS, CARRIER proteins, COORDINATION compounds, LIGANDS (Biochemistry), HYDROCARBONS, ORGANIC compounds, LYMPHOCYTIC leukemia, LYMPHOPROLIFERATIVE disorders

Abstract

Direct inhibition of transcription factor complexes remains a central challenge in the discipline of ligand discovery. In general, these proteins lack surface involutions suitable for high-affinity binding by small molecules. Here we report the design of synthetic, cell-permeable, stabilized α-helical peptides that target a critical protein–protein interface in the NOTCH transactivation complex. We demonstrate that direct, high-affinity binding of the hydrocarbon-stapled peptide SAHM1 prevents assembly of the active transcriptional complex. Inappropriate NOTCH activation is directly implicated in the pathogenesis of several disease states, including T-cell acute lymphoblastic leukaemia (T-ALL). The treatment of leukaemic cells with SAHM1 results in genome-wide suppression of NOTCH-activated genes. Direct antagonism of the NOTCH transcriptional program causes potent, NOTCH-specific anti-proliferative effects in cultured cells and in a mouse model of NOTCH1-driven T-ALL. [ABSTRACT FROM AUTHOR]

Published

2009

17. Lipocalin 2 promotes breast cancer progression.

Author

Jiang Yang, Bielenberg, Diane R., Rodig, Scott J., Doiron, Robert, Clifton, Matthew C., Kung, Andrew L., Strong, Roland K., Zurakowski, David, and Moses, Marsha A.

Subjects

BREAST cancer, CANCER invasiveness, CANCER cells, CELL motility, CELL migration, TISSUES, TRANSCRIPTION factors, BIOMARKERS

Abstract

Here, we report that lipocalin 2 (Lcn2) promotes breast cancer progression, and we identify the mechanisms underlying this function. We first found that Lcn2 levels were consistently associated with invasive breast cancer in human tissue and urine samples. To investigate the function of Lcn2 in breast cancer progression, Lcn2 was overexpressed in human breast cancer cells and was found to up-regulate mesenchymal markers, including vimentin and fibronectin, down-regulate the epithelial marker E-cadherin, and significantly increase cell motility and invasiveness. These changes in marker expression and cell motility are hallmarks of an epithelial to mesenchymal transition (EMT). In contrast, Lcn2 silencing in aggressive breast cancer cells inhibited cell migration and the mesenchymal phenotype. Furthermore. reduced expression of estrogen receptor (ER) a and increased expression of the key EMT transcription factor Slug were observed with Lcn2 expression. Overexpression of ERα in Lcn2-expressing cells reversed the EMT and reduced Slug expression, suggesting that ERα negatively regulates Lcn2-induced EMT. Finally, orthotopic studies demonstrated that Lcn2-expressing breast tumors displayed a poorly differentiated phenotype and showed increased local tumor invasion and lymph node metastasis. Taken together, these in vitro, in vivo, and human studies demonstrate that Lcn2 promotes breast cancer progression by inducing EMT through the ERα/Slug axis and may be a useful biomarker of breast cancer. [ABSTRACT FROM AUTHOR]

Published

2009

18. Pharmacologic suppression of MITF expression via HDAC inhibitors in the melanocyte lineage.

Author

Yokoyama, Satoru, Feige, Erez, Poling, Laura L., Levy, Carmit, Widlund, Hans R., Khaled, Mehdi, Kung, Andrew L., and Fisher, David E.

Subjects

HISTONE deacetylase, MELANOMA, RENAL cell carcinoma, MELANOCYTES, TRANSCRIPTION factors

Abstract

Melanoma incidence continues to rise at an alarming rate while effective systemic therapies remain very limited. Microphthalmia-associated transcription factor (MITF) is required for development of melanocytes and is an amplified oncogene in a fraction of human melanomas. Microphthalmia-associated transcription factor also plays an oncogenic role in human clear cell sarcomas, which typically exhibit melanoma-like features. Although pharmacologic suppression of MITF is of potential interest in a variety of clinical settings, it is not known to contain intrinsic catalytic activity capable of direct small molecule inhibition. An alternative drug-targeting strategy is to identify and interfere with lineage-restricted mechanisms required for its expression. Here, we report that multiple histone deacetylase (HDAC)-inhibitor drugs potently suppress MITF expression in melanocytes, melanoma and clear cell sarcoma cells. Although HDAC inhibitors may affect numerous cellular targets, we observed suppression of skin pigmentation by topical drug application as well as evidence of anti-melanoma efficacy in vitro and in mouse xenografts. Consequently, HDAC inhibitor drugs are candidates to play therapeutic roles in targeting conditions affecting the melanocyte lineage. [ABSTRACT FROM AUTHOR]

Published

2008

19. Hypoxia-induced transcriptional repression of the melanoma-associated oncogene MITF.

Author

Feige, Erez, Yokoyamaa, Satoru, Levy, Carmit, Khaled, Mehdi, Igras, Vivien, Lin, Richard J., Lee, Stephen, Widlund, Hans R., Granter, Scott R., Kung, Andrew L., and Fishera, David E.

Subjects

TRANSCRIPTION factors, MELANOMA, GENETIC repressors, HYPOXEMIA, HYPOXIA-inducible factors, GENETICS

Abstract

The article presents study to examine the MITF, a transcription factor associated with microphthalmia expression in metastatic melanoma biospecimens. It demonstrates that the decrease in the levels of MITF is due to reduced transcription rate cause by the repression of the promoter of MITF. The study demonstrated that the MITF promoter is presented by the hypoxia-inducible factor 1 (HIF1)-transcriptional repressor (DEC1) axis, which could serve as therapeutic target to suppress MITF.

Published

2011

20. Direct inhibition of the NOTCH transcription factor complex.

Author

Moellering, Raymond E., Cornejo, Melanie, Davis, Tina N., Bianco, Cristina Del, Aster, Jon C., Blacklow, Stephen C., Kung, Andrew L., Gilliland, D. Gary, Verdine, Gregory L., and Bradner, James E.

Subjects

TRANSCRIPTION factors

Abstract

A correction to the article "Direct inhibition of the NOTCH transcription factor complex" that was published in "Nature" in the 2009 issue.

Published

2010

21. NF-κB Directs Dynamic Super Enhancer Formation in Inflammation and Atherogenesis.

Author

Brown, Jonathan D., Lin, Charles Y., Duan, Qiong, Griffin, Gabriel, Federation, Alexander J., Paranal, Ronald M., Bair, Steven, Newton, Gail, Lichtman, Andrew H., Kung, Andrew L., Yang, Tianlun, Wang, Hong, Luscinskas, Francis W., Croce, Kevin J., Bradner, James E., and Plutzky, Jorge

Subjects

*NF-kappa B, *GENE enhancers, *TRANSCRIPTION factors, *CELLULAR signal transduction, *INFLAMMATION, *RNA polymerases, *NECROSIS

Abstract

Summary Proinflammatory stimuli elicit rapid transcriptional responses via transduced signals to master regulatory transcription factors. To explore the role of chromatin-dependent signal transduction in the atherogenic inflammatory response, we characterized the dynamics, structure, and function of regulatory elements in the activated endothelial cell epigenome. Stimulation with tumor necrosis factor alpha prompted a dramatic and rapid global redistribution of chromatin activators to massive de novo clustered enhancer domains. Inflammatory super enhancers formed by nuclear factor-kappa B accumulate at the expense of immediately decommissioned, basal endothelial super enhancers, despite persistent histone hyperacetylation. Mass action of enhancer factor redistribution causes momentous swings in transcriptional initiation and elongation. A chemical genetic approach reveals a requirement for BET bromodomains in communicating enhancer remodeling to RNA Polymerase II and orchestrating the transition to the inflammatory cell state, demonstrated in activated endothelium and macrophages. BET bromodomain inhibition abrogates super enhancer-mediated inflammatory transcription, atherogenic endothelial responses, and atherosclerosis in vivo. [ABSTRACT FROM AUTHOR]

Published

2014

22. Chemical Genomics Identifies Small-Molecule MCL1 Repressors and BCL-xL as a Predictor of MCL1 Dependency

Author

Wei, Guo, Margolin, Adam A., Haery, Leila, Brown, Emily, Cucolo, Lisa, Julian, Bina, Shehata, Shyemaa, Kung, Andrew L., Beroukhim, Rameen, and Golub, Todd R.

Subjects

*LEUKEMIA treatment, *MYELOID leukemia, *GENETIC repressors, *APOPTOSIS, *GENE amplification, *GENE expression, *TRANSCRIPTION factors, *CANCER cells, *PATIENT selection

Abstract

Summary: MCL1, which encodes the antiapoptotic protein MCL1, is among the most frequently amplified genes in human cancer. A chemical genomic screen identified compounds, including anthracyclines, that decreased MCL1 expression. Genomic profiling indicated that these compounds were global transcriptional repressors that preferentially affect MCL1 due to its short mRNA half-life. Transcriptional repressors and MCL1 shRNAs induced apoptosis in the same cancer cell lines and could be rescued by physiological levels of ectopic MCL1 expression. Repression of MCL1 released the proapoptotic protein BAK from MCL1, and Bak deficiency conferred resistance to transcriptional repressors. A computational model, validated in vivo, indicated that high BCL-xL expression confers resistance to MCL1 repression, thereby identifying a patient-selection strategy for the clinical development of MCL1 inhibitors. [Copyright &y& Elsevier]

Published

2012

23. HIF2alpha cooperates with RAS to promote lung tumorigenesis in mice.

Author

Kim, William Y., Perera, Samanthi, Bing Zhou, Carretero, Julian, Jen Jen Yeh, Heathcote, Samuel A., Jackson, Autumn L., Nikolinakos, Petros, Ospina, Beatriz, Naumov, George, Brandstetter, Kathleyn A., Weigman, Victor J., Zaghlul, Sara, Hayes, D. Neil, Padera, Robert F., Heymach, John V., Kung, Andrew L., Sharpless, Norman E., Kaelin Jr., William G., and Kwok-Kin Wong

Subjects

*CARCINOGENESIS, *TRANSCRIPTION factors, *LUNG cancer, *TUMOR growth, *NEOVASCULARIZATION, *HYPOXEMIA, *ANIMAL experimentation, *CANCER invasiveness, *CELL differentiation, *COMPARATIVE studies, *ENDOTHELIUM, *LUNG tumors, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *PROTEINS, *RESEARCH, *RESEARCH funding, *EMBRYOS, *EVALUATION research, *GENE expression profiling

Abstract

Members of the hypoxia-inducible factor (HIF) family of transcription factors regulate the cellular response to hypoxia. In non-small cell lung cancer (NSCLC), high HIF2alpha levels correlate with decreased overall survival, and inhibition of either the protein encoded by the canonical HIF target gene VEGF or VEGFR2 improves clinical outcomes. However, whether HIF2alpha is causal in imparting this poor prognosis is unknown. Here, we generated mice that conditionally express both a nondegradable variant of HIF2alpha and a mutant form of Kras (KrasG12D) that induces lung tumors. Mice expressing both Hif2a and KrasG12D in the lungs developed larger tumors and had an increased tumor burden and decreased survival compared with mice expressing only KrasG12D. Additionally, tumors expressing both KrasG12D and Hif2a were more invasive, demonstrated features of epithelial- mesenchymal transition (EMT), and exhibited increased angiogenesis associated with mobilization of circulating endothelial progenitor cells. These results implicate HIF2alpha causally in the pathogenesis of lung cancer in mice, demonstrate in vivo that HIF2alpha can promote expression of markers of EMT, and define HIF2alpha as a promoter of tumor growth and progression in a solid tumor other than renal cell carcinoma. They further suggest a possible causal relationship between HIF2alpha and prognosis in patients with NSCLC. [ABSTRACT FROM AUTHOR]

Published

2009

24. Cyclin D1 Represses p300 Transactivation through a Cyclin-dependent Kinase-independent Mechanism.

Author

Maofu Fu, Chenguang Wang, Rao, Mahadev, Xiaofang Wu, Bouras, Toula, Xueping Zhang, Zhiping Li, Xuanmao Jiao, Jianguo Yang, Anping Li, Perkins, Neil D., Thimmapaya, Bayar, Kung, Andrew L., Munoz, Alberto, Giordano, Antonio, Lisanti, Michael P., and Pestell, Richard G.

Subjects

*CYCLIN-dependent kinases, *PROTEIN kinases, *PHOSPHOTRANSFERASES, *TRANSCRIPTION factors, *PROTEINS, *BIOCHEMISTRY

Abstract

Cyclin D1 encodes a regulatory subunit, which with its cyclin-dependent kinase (Cdk)-binding partner forms a holoenzyme that phosphorylates and inactivates the retinoblastoma protein. In addition to its Cdk binding-dependent functions, cyclin D1 regulates cellular differentiation in part by modifying several transcription factors and nuclear receptors, The molecular mechanism through which cyclin D1 regulates the function of transcription factors involved in cellular differentiation remains to be clarified. The histone acetyltransferase protein p300 is a co-integrator required for regulation of multiple transcription factors. Here we show that cyclin D1 physically interacts with p300 and represses p300 transactivation. We demonstrated further that the interaction of the two proteins occurs at the peroxisome proliferator-activated receptor γ-responsive element of the lipoprotein lipase promoter in the context of the local chromatin structure. We have mapped the domains in p300 and cyclin D1 involved in this interaction. The bromo domain and cysteine- and histidine-rich domains of p300 were required for repression by cyclin D1. Cyclin D1 repression of p300 was independent of the Cdk. and retinoblastoma protein-binding domains of cyclin D1. Cyclin D1 inhibits histene acetyltransferase activity of p300 in vitro. Microarray analysis identified a signature of genes repressed by cyclin D1 and induced by p300 that promotes cellular differentiation and induces cell cycle arrest. Together, our results suggest that cyclin D1 plays an important role in cellular proliferation and differentiation through regulation of p300. [ABSTRACT FROM AUTHOR]

Published

2005