Your search keyword '"TIP60"' showing total 495 results

201. The Molecular Effects of Sulforaphane and Capsaicin on Metabolism upon Androgen and Tip60 Activation of Androgen Receptor

Author

Kah Ni Tan, Tayner Rodriguez, Vicky M. Avery, and Catalina Carrasco-Pozo

Subjects

Male, sulforaphane, urologic and male genital diseases, capsaicin, lcsh:Chemistry, Prostate cancer, chemistry.chemical_compound, Isothiocyanates, androgen receptor, lcsh:QH301-705.5, Spectroscopy, General Medicine, glycolysis, Computer Science Applications, Gene Expression Regulation, Neoplastic, Tip60, Receptors, Androgen, Sulfoxides, Androgens, Signal Transduction, medicine.drug_class, bcl-X Protein, Catalysis, Article, Lysine Acetyltransferase 5, pyruvate kinase, Inorganic Chemistry, Cell Line, Tumor, LNCaP, medicine, Humans, Physical and Theoretical Chemistry, Molecular Biology, Cell Proliferation, Cell Nucleus, Hexokinase, hexokinase, Cell growth, Organic Chemistry, Prostatic Neoplasms, Prostate-Specific Antigen, medicine.disease, Androgen, Hypoxia-Inducible Factor 1, alpha Subunit, Androgen receptor, lcsh:Biology (General), lcsh:QD1-999, chemistry, Capsaicin, Cancer research, Sulforaphane

Abstract

Androgen receptor (AR) stimulators, such as androgen and Tip60, play a pivotal role in prostatic carcinogenesis as androgen receptor signaling is critical for the growth and transformation of the prostate gland. Moreover, androgen and Tip60 promotes HIF-1&alpha, activation, involved in metabolic reprogramming by increasing glycolysis, a hallmark in cancer initiation and development. In this study we evaluated the effect of androgen and Tip60 stimulus in AR pathway activation and HIF-1&alpha, stabilization, in terms of proliferation and cell metabolism in androgen-sensitive LNCaP cells. The protective role of the bioactive compounds sulforaphane and capsaicin against the effect of these stimuli leading to pro-carcinogenic features was also addressed. Sulforaphane and capsaicin decreased nuclear AR, prostate specific antigen and Bcl-XL levels, and cell proliferation induced by androgen and Tip60 in LNCaP cells. These bioactive compounds prevented the increase in glycolysis, hexokinase and pyruvate kinase activity, and reduced HIF-1&alpha, stabilization induced by androgen and Tip60 in LNCaP cells. The protective role of sulforaphane and capsaicin on prostate cancer may rely on mechanisms involving the inhibition of Tip60, AR and HIF-1&alpha, effects.

Published

2019

202. Enhancer of Polycomb and the Tip60 complex repress hematological tumor initiation by negatively regulating JAK/STAT pathway activity

Author

Bailetti, Alessandro A., Negrón-Piñeiro, Lenny J., Dhruva, Vishal, Harsh, Sneh, Lu, Sean, Bosula, Aisha, and Bach, Erika A.

Subjects

Heterozygote, Carcinogenesis, Chromosomal Proteins, Non-Histone, lcsh:Medicine, Lysine acetyltransferases, Models, Biological, Myeloproliferative neoplasms, lcsh:Pathology, Animals, Drosophila Proteins, Melanoma, Histone Acetyltransferases, Janus Kinases, lcsh:R, E(Pc), Dros, Tumor suppressor, Cell Differentiation, Melanotic tumors, JAK/STAT, Hematopoiesis, STAT Transcription Factors, Drosophila melanogaster, Phenotype, Tip60, Hematologic Neoplasms, Drosophila, lcsh:RB1-214, Research Article, Signal Transduction, Transcription Factors

Abstract

Myeloproliferative neoplasms (MPNs) are clonal hematopoietic disorders that cause excessive production of myeloid cells. Most MPN patients have a point mutation in JAK2 (JAK2V617F), which encodes a dominant-active kinase that constitutively triggers JAK/STAT signaling. In Drosophila, this pathway is simplified, with a single JAK, Hopscotch (Hop), and a single STAT transcription factor, Stat92E. The hopTumorous-lethal [hopTum] allele encodes a dominant-active kinase that induces sustained Stat92E activation. Like MPN patients, hopTum mutants have significantly more myeloid cells, which form invasive tumors. Through an unbiased genetic screen, we found that heterozygosity for Enhancer of Polycomb [E(Pc)], a component of the Tip60 lysine acetyltransferase complex (also known as KAT5 in humans), significantly increased tumor burden in hopTum animals. Hematopoietic depletion of E(Pc) or other Tip60 components in an otherwise wild-type background also induced blood cell tumors. The E(Pc) tumor phenotype was dependent on JAK/STAT activity, as concomitant depletion of hop or Stat92E inhibited tumor formation. Stat92E target genes were significantly upregulated in E(Pc)-mutant myeloid cells, indicating that loss of E(Pc) activates JAK/STAT signaling. Neither the hop nor Stat92E gene was upregulated upon hematopoietic E(Pc) depletion, suggesting that the regulation of the JAK/STAT pathway by E(Pc) is dependent on substrates other than histones. Indeed, E(Pc) depletion significantly increased expression of Hop protein in myeloid cells. This study indicates that E(Pc) works as a tumor suppressor by attenuating Hop protein expression and ultimately JAK/STAT signaling. Since loss-of-function mutations in the human homologs of E(Pc) and Tip60 are frequently observed in cancer, our work could lead to new treatments for MPN patients. This article has an associated First Person interview with the first author of the paper., Editor's choice: Using Drosophila as a low-complexity model for human myeloproliferative neoplasms, the authors identified a conserved mechanism by which the Tip60 lysine acetyltransferase acts as a tumor suppressor by repressing JAK protein expression in a histone-independent manner.

Published

2019

203. Chelidonium majus Induces Apoptosis of Human Ovarian Cancer Cells via ATF3-Mediated Regulation of Foxo3a by Tip60.

Author

Shen L, Lee S, Joo JC, Hong E, Cui ZY, Jo E, Park SJ, and Jang HJ

Subjects

Activating Transcription Factor 3 genetics, Activating Transcription Factor 3 metabolism, Apoptosis genetics, Cell Line, Tumor, Female, Forkhead Transcription Factors genetics, Forkhead Transcription Factors metabolism, Gene Products, tat, Humans, RNA, Small Interfering genetics, bcl-2-Associated X Protein, Chelidonium genetics, Chelidonium metabolism, Forkhead Box Protein O3 metabolism, Ovarian Neoplasms

Abstract

Forkhead transcription factor 3a (Foxo3a) is believed to be a tumor suppressor as its inactivation leads to cell transformation and tumor development. However, further investigation is required regarding the involvement of the activating transcription factor 3 (ATF3)-mediated Tat-interactive protein 60 (Tip60)/Foxo3a pathway in cancer cell apoptosis. This study demonstrated that Chelidonium majus upregulated the expression of ATF3 and Tip60 and promoted Foxo3a nuclear translocation, ultimately increasing the level of Bcl-2-associated X protein (Bax) protein. ATF3 overexpression stimulated Tip60 expression, while ATF3 inhibition by siRNA repressed Tip60 expression. Furthermore, siRNA-mediated Tip60 inhibition significantly promoted Foxo3a phosphorylation, leading to blockade of Foxo3a translocation into the nucleus. Thus, we were able to deduce that ATF3 mediates the regulation of Foxo3a by Tip60. Moreover, siRNA-mediated Foxo3a inhibition suppressed the expression of Bax and subsequent apoptosis. Taken together, our data demonstrate that Chelidonium majus induces SKOV-3 cell death by increasing ATF3 levels and its downstream proteins Tip60 and Foxo3a. This suggests a potential therapeutic role of Chelidonium majus against ovarian cancer.

Published

2022

204. Rap1 regulates TIP60 function during fate transition between two-cell-like and pluripotent states.

Author

Barry RM, Sacco O, Mameri A, Stojaspal M, Kartsonis W, Shah P, De Ioannes P, Hofr C, Côté J, and Sfeir A

Subjects

Animals, Gene Expression Regulation, Genome, Mammals genetics, Mice, Mouse Embryonic Stem Cells metabolism, Telomere metabolism, Telomere-Binding Proteins genetics, Telomere-Binding Proteins metabolism

Abstract

In mammals, the conserved telomere binding protein Rap1 serves a diverse set of nontelomeric functions, including activation of the NF-kB signaling pathway, maintenance of metabolic function in vivo, and transcriptional regulation. Here, we uncover the mechanism by which Rap1 modulates gene expression. Using a separation-of-function allele, we show that Rap1 transcriptional regulation is largely independent of TRF2-mediated binding to telomeres and does not involve direct binding to genomic loci. Instead, Rap1 interacts with the TIP60/p400 complex and modulates its histone acetyltransferase activity. Notably, we show that deletion of Rap1 in mouse embryonic stem cells increases the fraction of two-cell-like cells. Specifically, Rap1 enhances the repressive activity of Tip60/p400 across a subset of two-cell-stage genes, including Zscan4 and the endogenous retrovirus MERVL. Preferential up-regulation of genes proximal to MERVL elements in Rap1-deficient settings implicates these endogenous retroviral elements in the derepression of proximal genes. Altogether, our study reveals an unprecedented link between Rap1 and the TIP60/p400 complex in the regulation of pluripotency., (© 2022 Barry et al.; Published by Cold Spring Harbor Laboratory Press.)

Published

2022

205. Role of histone acetyltransferases MOF and Tip60 in genome stability.

Author

Mir, Ulfat Syed, Bhat, Audesh, Mushtaq, Arjamand, Pandita, Shruti, Altaf, Mohammad, and Pandita, Tej K.

Subjects

*DNA repair, *POST-translational modification, *ACETYLTRANSFERASES, *GENOMES, *DNA damage, *IONIZING radiation, *EUKARYOTIC cells

Abstract

The accurate repair of DNA damage specifically the chromosomal double-strand breaks (DSBs) arising from exposure to physical or chemical agents, such as ionizing radiation (IR) and radiomimetic drugs is critical in maintaining genomic integrity. The DNA DSB response and repair is facilitated by hierarchical signaling networks that orchestrate chromatin structural changes specifically histone modifications which impact cell-cycle checkpoints through enzymatic activities to repair the broken DNA ends. Various histone posttranslational modifications such as phosphorylation, acetylation, methylation and ubiquitylation have been shown to play a role in DNA damage repair. Recent studies have provided important insights into the role of histone-specific modifications in sensing DNA damage and facilitating the DNA repair. Histone modifications have been shown to determine the pathway choice for repair of DNA DSBs. This review will summarize the role of important histone acetyltransferases MOF and Tip60 mediated acetylation in repair of DNA DSBs in eukaryotic cells. [ABSTRACT FROM AUTHOR]

Published

2021

206. Acetylated DNMT1 Downregulation and Related Regulatory Factors Influence Metastatic Melanoma Patients Survival.

Author

Zhang, Xiaoqing, Bustos, Matias A., Shoji, Yoshiaki, Ramos, Romela Irene, Iida, Yuuki, Gentry, Rebecca, Takeshima, Teh-Ling, and Hoon, Dave S. B.

Subjects

*MELANOMA prognosis, *PROTEIN analysis, *PROTEIN metabolism, *DISEASE progression, *DNA, *CONFIDENCE intervals, *MELANOMA, *METASTASIS, *GENE expression, *SURVIVAL analysis (Biometry), *DESCRIPTIVE statistics, *PROPORTIONAL hazards models

Abstract

Simple Summary: DNA methyltransferase-1 (DNMT1) is a key epigenetic regulatory protein of gene expression in cutaneous melanoma. DNMT1 is acetylated by TIP60 promoting its degradation. This study demonstrated that DNMT1 and ac-DNMT1 protein levels were inversely correlated in stage III (n = 17) and stage IV (n = 164) metastatic melanoma tumors, and both influenced melanoma progression. Reduced TIP60 and USP7 protein expression levels were correlated with decreased ac-DNMT1 levels. Of clinical translational relevance, patients with high ac-DNMT1 protein levels, or high-acDNMT1 with concurrent low DNMT1, high TIP60, or high USP7 protein levels showed significantly better prognosis for 4-year melanoma-specific survival. These results suggested that ac-DNMT1 is a significant post-translational modification influencing advanced melanoma patient disease outcomes. The role of post-translational modifications (PTM) of the key epigenetic factor DNMT1 protein has not been well explored in cutaneous metastatic melanoma progression. The acetylated DNMT1 (ac-DNMT1) protein level was assessed using an anti-acetylated lysine antibody in a clinically annotated melanoma patient tumor specimen cohort. In this study, we showed that surgically resected tumors have significantly higher DNMT1 protein expression in metastatic melanoma (stage III metastasis n = 17, p = 0.0009; stage IV metastasis n = 164, p = 0.003) compared to normal organ tissues (n = 19). Additionally, reduced ac-DNMT1 protein levels were associated with melanoma progression. There was a significant inverse correlation between ac-DNMT1 and DNMT1 protein levels in stage IV metastatic melanoma (r = −0.18, p = 0.02, n = 164). Additionally, ac-DNMT1 protein levels were also significantly positively correlated with TIP60 (r = 0.6, p < 0.0001) and USP7 (r = 0.74, p < 0.0001) protein levels in stage IV metastatic melanoma (n = 164). Protein analysis in metastatic melanoma tumor tissues showed that with high ac-DNMT1 (p = 0.006, n = 59), or concurrent high ac-DNMT1 with low DNMT1 (p = 0.05, n = 27), or high TIP60 (p = 0.007, n = 41), or high USP7 (p = 0.01, n = 48) consistently showed better 4-year melanoma-specific survival (MSS). Multivariate Cox proportional hazard analysis showed that ac-DNMT1 level is a significant independent factor associated with MSS (HR, 0.994; 95% confidential interval (CI), 0.990–0.998; p = 0.002). These results demonstrated that low ac-DNMT1 levels may represent an important regulatory factor in controlling metastatic melanoma progression and a promising factor for stratifying aggressive stage IV metastasis. [ABSTRACT FROM AUTHOR]

Published

2021

207. E3 ligase UHRF2 stabilizes the acetyltransferase TIP60 and regulates H3K9ac and H3K14ac via RING finger domain

Author

Changzhu Duan, Ting Zhang, Yangyang Wang, Shengyuan Zeng, Lu Bai, and Yalan Wang

Subjects

0301 basic medicine, Ubiquitin-Protein Ligases, lcsh:Animal biochemistry, Biochemistry, Lysine Acetyltransferase 5, Cell Line, Histones, 03 medical and health sciences, Neoplasms, Drug Discovery, Humans, lcsh:QH573-671, lcsh:QP501-801, UHRF2, acetylation, Histone Acetyltransferases, chemistry.chemical_classification, DNA ligase, biology, lcsh:Cytology, Chemistry, Ubiquitination, Cell Biology, hepatocellular carcinoma, Cell cycle, Molecular biology, Ubiquitin ligase, Neoplasm Proteins, RING finger domain, 030104 developmental biology, Histone, Acetyltransferase, Cancer cell, biology.protein, Signal transduction, TIP60, RING Finger Domains, Biotechnology, Research Article

Abstract

UHRF2 is a ubiquitin-protein ligase E3 that regulates cell cycle, genomic stability and epigenetics. We conducted a co-immunoprecipitation assay and found that TIP60 and HDAC1 interact with UHRF2. We previously demonstrated that UHRF2 regulated H3K9ac and H3K14ac differentially in normal and cancer cells. However, the accurate signal transduction mechanisms were not clear. In this study, we found that TIP60 acted downstream of UHRF2 to regulate H3K9ac and H3K14ac expression. TIP60 is stabilized in normal cells by UHRF2 ubiquitination. However, TIP60 is destabilized in cancer cells. Depletion or inhibition of TIP60 disrupts the regulatory relationship between UHRF2, H3K9ac and H3K14ac. In summary, the findings suggest that UHRF2 mediated the post-translational modification of histones and the initiation and progression of cancer. Electronic supplementary material The online version of this article (doi:10.1007/s13238-016-0324-z) contains supplementary material, which is available to authorized users.

Published

2016

208. Targeting cancer using KAT inhibitors to mimic lethal knockouts

Author

James A. Brown, Emer Bourke, Michael J. Kerin, and Leif A. Eriksson

Subjects

0301 basic medicine, histone-modifying enzymes, chromatin transcription, Bioinformatics, Biochemistry, Neoplasms, curcumin, Molecular Targeted Therapy, Enzyme Inhibitors, Histone Acetyltransferases, Regulation of gene expression, double-strand breaks, lysine acetyltransferases, Molecular Structure, bisubstrate, inhibitor, KAT, NU9056, acetyltransferase, Treatment Outcome, Histone, Tip60, Drug development, Kat5, acetyltransferase activity, Acetyltransferase, MG-149, TH1834, Cell Survival, histone, Computational biology, Biology, ionizing-radiation, Lysine Acetyltransferase 5, Small Molecule Libraries, 03 medical and health sciences, anacardic acid, breast cancer, down-regulation, pentamidine, potential marker, Irish Area Section (Protein Interactions in Biology), medicine, Humans, KAT5, HTATIP, Gene knockout, lysine, garcinol, DNA-damage response, colorectal-cancer, Cancer, medicine.disease, 030104 developmental biology, Lys-CoA, HAT, Mutation, Cancer cell, biology.protein, Biochemical Society Focused Meetings

Abstract

Two opposing enzyme classes regulate fundamental elements of genome maintenance, gene regulation and metabolism, either through addition of an acetyl moiety by histone acetyltransferases (HATs) or its removal by histone de-acetyltransferases (HDAC), and are exciting targets for drug development. Importantly, dysfunctional acetylation has been implicated in numerous diseases, including cancer. Within the HAT superfamily the MYST family holds particular interest, as its members are directly involved in the DNA damage response and repair pathways and crucially, several members have been shown to be down-regulated in common cancers (such as breast and prostate). In the present study we focus on the development of lysine (K) acetyltransferase inhibitors (KATi) targeting the MYST family member Tip60 (Kat5), an essential protein, designed or discovered through screening libraries. Importantly, Tip60 has been demonstrated to be significantly down-regulated in many cancers which urgently require new treatment options. We highlight current and future efforts employing these KATi as cancer treatments and their ability to synergize and enhance current cancer treatments. We investigate the different methods of KATi production or discovery, their mechanisms and their validation models. Importantly, the utility of KATi is based on a key concept: using KATi to abrogate the activity of an already down-regulated essential protein (effectively creating a lethal knockout) provides another innovative mechanism for targeting cancer cells, while significantly minimizing any off-target effects to normal cells. This approach, combined with the rapidly developing interest in KATi, suggests that KATi have a bright future for providing truly personalized therapies.

Published

2016

209. Microbiota-derived acetate activates intestinal innate immunity via the Tip60 histone acetyltransferase complex.

Author

Jugder, Bat-Erdene, Kamareddine, Layla, and Watnick, Paula I.

Subjects

*HISTONE acetyltransferase, *NATURAL immunity, *INTESTINES, *PATTERN perception receptors, *ENTEROENDOCRINE cells, *PEPTIDE antibiotics

Abstract

Microbe-derived acetate activates the Drosophila immunodeficiency (IMD) pathway in a subset of enteroendocrine cells (EECs) of the anterior midgut. In these cells, the IMD pathway co-regulates expression of antimicrobial and enteroendocrine peptides including tachykinin, a repressor of intestinal lipid synthesis. To determine whether acetate acts on a cell surface pattern recognition receptor or an intracellular target, we asked whether acetate import was essential for IMD signaling. Mutagenesis and RNA interference revealed that the putative monocarboxylic acid transporter Tarag was essential for enhancement of IMD signaling by dietary acetate. Interference with histone deacetylation in EECs augmented transcription of genes regulated by the steroid hormone ecdysone including IMD targets. Reduced expression of the histone acetyltransferase Tip60 decreased IMD signaling and blocked rescue by dietary acetate and other sources of intracellular acetyl-CoA. Thus, microbe-derived acetate induces chromatin remodeling within enteroendocrine cells, co-regulating host metabolism and intestinal innate immunity via a Tip60-steroid hormone axis that is conserved in mammals. [Display omitted] • The transporter Tarag is required for the enteroendocrine cell response to acetate • Acetate increases acetyl-CoA pools in tachykinin-expressing enteroendocrine cells • Acetyl-CoA pools modulate the activity of Tip60 histone acetylase complex • The Tip60 complex augments ecdysone-dependent transcription of PGRP-LC Microbe-derived acetate activates the Drosophila immunodeficiency pathway in a subset of intestinal enteroendocrine cells (EECs), which regulates expression of antimicrobial and enteroendocrine peptides. Jugder et al. reveal that acetate induces chromatin remodeling within EECs by specifically modulating the function of the Tip60 histone acetyltransferase complex via a Tip60-steroid hormone axis that is conserved in mammals. [ABSTRACT FROM AUTHOR]

Published

2021

210. Fe65: A Scaffolding Protein of Actin Regulators.

Author

Augustin, Vanessa and Kins, Stefan

Subjects

*SCAFFOLD proteins, *CYTOSKELETON, *AMYLOID beta-protein precursor, *HOMEOSTASIS, *CELL migration, *NEUROPLASTICITY, *ACTIN

Abstract

The scaffolding protein family Fe65, composed of Fe65, Fe65L1, and Fe65L2, was identified as an interaction partner of the amyloid precursor protein (APP), which plays a key function in Alzheimer's disease. All three Fe65 family members possess three highly conserved interaction domains, forming complexes with diverse binding partners that can be assigned to different cellular functions, such as transactivation of genes in the nucleus, modulation of calcium homeostasis and lipid metabolism, and regulation of the actin cytoskeleton. In this article, we rule out putative new intracellular signaling mechanisms of the APP-interacting protein Fe65 in the regulation of actin cytoskeleton dynamics in the context of various neuronal functions, such as cell migration, neurite outgrowth, and synaptic plasticity. [ABSTRACT FROM AUTHOR]

Published

2021

211. Metabolic Roles of Androgen Receptor and Tip60 in Androgen-Dependent Prostate Cancer

Author

Catalina Carrasco-Pozo, Vicky M. Avery, and Kah Ni Tan

Subjects

Male, p53, HIF-1α, Review, Lysine Acetyltransferase 5, Catalysis, lcsh:Chemistry, Inorganic Chemistry, Androgen deprivation therapy, Prostate cancer, Prostate, androgen receptor, medicine, Humans, Physical and Theoretical Chemistry, lcsh:QH301-705.5, Molecular Biology, Spectroscopy, Kinase, Chemistry, Organic Chemistry, Prostatic Neoplasms, Cancer, General Medicine, prostate cancer, medicine.disease, Computer Science Applications, Androgen receptor, Metabolic pathway, c-Myc, medicine.anatomical_structure, Tip60, lcsh:Biology (General), lcsh:QD1-999, Receptors, Androgen, Cancer cell, Cancer research, Energy Metabolism, metabolism

Abstract

Androgen receptor (AR)-mediated signaling is essential for the growth and differentiation of the normal prostate and is the primary target for androgen deprivation therapy in prostate cancer. Tat interactive protein 60 kDa (Tip60) is a histone acetyltransferase that is critical for AR activation. It is well known that cancer cells rewire their metabolic pathways in order to sustain aberrant proliferation. Growing evidence demonstrates that the AR and Tip60 modulate key metabolic processes to promote the survival of prostate cancer cells, in addition to their classical roles. AR activation enhances glucose metabolism, including glycolysis, tricarboxylic acid cycle and oxidative phosphorylation, as well as lipid metabolism in prostate cancer. The AR also interacts with other metabolic regulators, including calcium/calmodulin-dependent kinase kinase 2 and mammalian target of rapamycin. Several studies have revealed the roles of Tip60 in determining cell fate indirectly by modulating metabolic regulators, such as c-Myc, hypoxia inducible factor 1α (HIF-1α) and p53 in various cancer types. Furthermore, Tip60 has been shown to regulate the activity of key enzymes in gluconeogenesis and glycolysis directly through acetylation. Overall, both the AR and Tip60 are master metabolic regulators that mediate cellular energy metabolism in prostate cancer, providing a framework for the development of novel therapeutic targets in androgen-dependent prostate cancer.

Published

2020

212. Study of Epigenetic Modifications depending on Sporadic Breast Cancer Virulence : Involvement of Histone Deacetylase SIRT1 in Tumor Progression

Author

Rifai, Khaldoun, laboratoire OncoGènAuvergne [Centre Jean Perrin, Clermont-Ferrand], Centre Jean Perrin [Clermont-Ferrand] (UNICANCER/CJP), UNICANCER-UNICANCER, Université Clermont Auvergne [2017-2020], and Dominique Bernard-Gallon

Subjects

[SDV.SA]Life Sciences [q-bio]/Agricultural sciences, SIRT1, Breast cancer, Epi-drugs, Épigénétique, Epigenetics, H3K4ac, Épi-drogues, TIP60, Cancer du Sein

Abstract

With 59,000 new cases in 2017, breast cancer is the most frequently diagnosed cancer among French women, and poses a real public health problem in France, but also worldwide. It is well established that the complexity of carcinogenesis involves profound epigenetic deregulations that contribute to the tumorigenesis process. Deregulated H3 and H4 acetylated histone marks are amongst those alterations. Acetylation and deacetylation are major post-translational protein modifications that regulate gene expression and the activity of a myriad of oncoproteins. Aberrant deacetylase activity can promote or suppress tumorigenesis in different types of human cancers, including breast cancer. The deacetylase SIRT1 and the acetyltransferase TIP60 are 2 antagonistic epigenetic enzymes that are well implicated in apoptosis, gene regulation, genomic stability, DNA repair, and cancer development. In this manuscript, we identified the dysregulation of the histones H3 and H4 acetylation profiles in different molecular subtypes of sporadic breast cancer, and investigated the involvement of SIRT1 and TIP60 in breast tumorigenesis. First, we highlighted the roles of SIRT1 and TIP60 as potential prognostic biomarkers by revealing their differential expression patterns depending on breast cancer aggressiveness. Then, we demonstrated their differential epigenetic regulation of histone targets according to molecular subtype, and revealed their modulation of the H3K4ac epigenetic marker. Moreover, Epi-drugs mediated inhibition of these 2 enzymes has proven to be an effective strategy in the treatment of cancer. Thus, this work highlights the potential use of SIRT1 and TIP60 as epigenetic therapeutic targets for sporadic breast cancer.; Avec 59 000 nouveaux cas en 2017, le cancer du sein est le cancer le plus fréquemment diagnostiqué chez les femmes françaises, et pose un réel problème de santé publique en France, mais aussi au niveau mondial. Il est bien établi que la complexité de la carcinogenèse implique des modifications épigénétiques profondes qui contribuent au processus du développement tumoral. La dérégulation des marques d'histones acétylées H3 et H4 font partie de ces modifications. L'acétylation et la désacétylation des protéines sont des modifications posttraductionnelles majeures qui régulent l'expression des gènes liés au cancer et à l'activité d'une myriade d'oncoprotéines. Ainsi, une activité désacétylase aberrante peut alors favoriser ou supprimer la tumorigenèse dans différents types de cancers humains, y compris le cancer du sein. La désacétylase SIRT1 et l’acétyltransférase TIP60 sont 2 enzymes épigénétiques antagonistes qui sont impliquées dans l'apoptose, la régulation des gènes, la stabilité génomique, la réparation de l'ADN, et le développement du cancer. Dans le cadre de cette thèse, nous avons étudié la dérégulation des profils d’acétylation des histones H3 et H4 dans les différents sous-types moléculaires du cancer du sein, et investigué l’implication de SIRT1 et de TIP60 dans la progression tumorale de cancer du sein. Tout d’abord, nous avons signalé les rôles de SIRT1 et de TIP60 comme des biomarqueurs pronostiques potentiels en révélant leurs expressions différentielles en fonction de l’agressivité du cancer. Ensuite, nous avons montré leur régulation épigénétique différentielle des cibles histones en fonction du sous-type moléculaire, ainsi que leur modulation de la marque activatrice H3K4ac. En outre, l’inhibition de ces 2 enzymes par des Épidrogues s’est avérée comme une stratégie efficace dans le traitement du cancer. Ces travaux mettent en relief alors, SIRT1 et TIP60 comme des cibles thérapeutiques potentielles du cancer sporadique du sein.

Published

2018

213. Etude des modifications épigénétiques en fonction de l'agressivité du cancer sporadique du sein : l'implication de l'histone désacétylase SIRT1 dans la progression tumorale

Author

Rifai, Khaldoun, laboratoire OncoGènAuvergne [Centre Jean Perrin, Clermont-Ferrand], Centre Jean Perrin [Clermont-Ferrand] (UNICANCER/CJP), UNICANCER-UNICANCER, Université Clermont Auvergne [2017-2020], and Dominique Bernard-Gallon

Subjects

[SDV.SA]Life Sciences [q-bio]/Agricultural sciences, SIRT1, Breast cancer, Epi-drugs, Épigénétique, Epigenetics, H3K4ac, Épi-drogues, TIP60, Cancer du Sein

Abstract

With 59,000 new cases in 2017, breast cancer is the most frequently diagnosed cancer among French women, and poses a real public health problem in France, but also worldwide. It is well established that the complexity of carcinogenesis involves profound epigenetic deregulations that contribute to the tumorigenesis process. Deregulated H3 and H4 acetylated histone marks are amongst those alterations. Acetylation and deacetylation are major post-translational protein modifications that regulate gene expression and the activity of a myriad of oncoproteins. Aberrant deacetylase activity can promote or suppress tumorigenesis in different types of human cancers, including breast cancer. The deacetylase SIRT1 and the acetyltransferase TIP60 are 2 antagonistic epigenetic enzymes that are well implicated in apoptosis, gene regulation, genomic stability, DNA repair, and cancer development. In this manuscript, we identified the dysregulation of the histones H3 and H4 acetylation profiles in different molecular subtypes of sporadic breast cancer, and investigated the involvement of SIRT1 and TIP60 in breast tumorigenesis. First, we highlighted the roles of SIRT1 and TIP60 as potential prognostic biomarkers by revealing their differential expression patterns depending on breast cancer aggressiveness. Then, we demonstrated their differential epigenetic regulation of histone targets according to molecular subtype, and revealed their modulation of the H3K4ac epigenetic marker. Moreover, Epi-drugs mediated inhibition of these 2 enzymes has proven to be an effective strategy in the treatment of cancer. Thus, this work highlights the potential use of SIRT1 and TIP60 as epigenetic therapeutic targets for sporadic breast cancer.; Avec 59 000 nouveaux cas en 2017, le cancer du sein est le cancer le plus fréquemment diagnostiqué chez les femmes françaises, et pose un réel problème de santé publique en France, mais aussi au niveau mondial. Il est bien établi que la complexité de la carcinogenèse implique des modifications épigénétiques profondes qui contribuent au processus du développement tumoral. La dérégulation des marques d'histones acétylées H3 et H4 font partie de ces modifications. L'acétylation et la désacétylation des protéines sont des modifications posttraductionnelles majeures qui régulent l'expression des gènes liés au cancer et à l'activité d'une myriade d'oncoprotéines. Ainsi, une activité désacétylase aberrante peut alors favoriser ou supprimer la tumorigenèse dans différents types de cancers humains, y compris le cancer du sein. La désacétylase SIRT1 et l’acétyltransférase TIP60 sont 2 enzymes épigénétiques antagonistes qui sont impliquées dans l'apoptose, la régulation des gènes, la stabilité génomique, la réparation de l'ADN, et le développement du cancer. Dans le cadre de cette thèse, nous avons étudié la dérégulation des profils d’acétylation des histones H3 et H4 dans les différents sous-types moléculaires du cancer du sein, et investigué l’implication de SIRT1 et de TIP60 dans la progression tumorale de cancer du sein. Tout d’abord, nous avons signalé les rôles de SIRT1 et de TIP60 comme des biomarqueurs pronostiques potentiels en révélant leurs expressions différentielles en fonction de l’agressivité du cancer. Ensuite, nous avons montré leur régulation épigénétique différentielle des cibles histones en fonction du sous-type moléculaire, ainsi que leur modulation de la marque activatrice H3K4ac. En outre, l’inhibition de ces 2 enzymes par des Épidrogues s’est avérée comme une stratégie efficace dans le traitement du cancer. Ces travaux mettent en relief alors, SIRT1 et TIP60 comme des cibles thérapeutiques potentielles du cancer sporadique du sein.

Published

2018

214. Identification of a panel of MYC and Tip60 co-regulated genes functioning primarily in cell cycle and DNA replication

Author

Ling-Jun Zhao, Maurice Green, and Paul M. Loewenstein

Subjects

0301 basic medicine, Cancer Research, NuA4 complex, p300, MYC, Biology, 03 medical and health sciences, Genetics, medicine, cancer, Gene, chemistry.chemical_classification, Regulation of gene expression, Gene knockdown, DNA replication, Cancer, Histone acetyltransferase, Cell cycle, medicine.disease, 3. Good health, Cell biology, 030104 developmental biology, Enzyme, chemistry, Tip60, biology.protein, Research Paper

Abstract

We recently reported that adenovirus E1A enhances MYC association with the NuA4/Tip60 histone acetyltransferase (HAT) complex to activate a panel of genes enriched for DNA replication and cell cycle. Genes from this panel are highly expressed in examined cancer cell lines when compared to normal fibroblasts. To further understand gene regulation in cancer by MYC and the NuA4 complex, we performed RNA-seq analysis of MD-MB231 breast cancer cells following knockdown of MYC or Tip60 - the HAT enzyme of the NuA4 complex. We identify here a panel of 424 genes, referred to as MYC-Tip60 co-regulated panel (MTcoR), that are dependent on both MYC and Tip60 for expression and likely co-regulated by MYC and the NuA4 complex. The MTcoR panel is most significantly enriched in genes involved in cell cycle and/or DNA replication. In contrast, genes repressed by shMYC but not by shTip60 (224 genes) have a low significance of enrichment in identifiable biological processes other than cell cycle and DNA replication. Genes repressed by shTip60 but not by shMYC (102 genes) have no significant identifiable gene enrichment. We propose that MYC cooperates with the NuA4 complex to activate the MTcoR panel of genes to promote DNA replication and cell cycle.

Published

2018

215. Inhibition of Tip60 Reduces Lytic and Latent Gene Expression of Kaposi’s Sarcoma-Associated Herpes Virus (KSHV) and Proliferation of KSHV-Infected Tumor Cells

Author

Prashant Desai, Sydney Simpson, Netty Santoso, Jian Zhu, Meir Shamay, Maxime Jean, Michael Dieringer, James McGuinness, Guillaume Fiches, and Sinu P. John

Subjects

0301 basic medicine, Microbiology (medical), viruses, lcsh:QR1-502, KSHV, Biology, Microbiology, lcsh:Microbiology, 03 medical and health sciences, Kaposi’s sarcoma, 0302 clinical medicine, Plasmid, Viral life cycle, medicine, Lytic Phase, Kaposi's sarcoma, HHV-8, Original Research, primary effusion lymphoma, HEK 293 cells, virus diseases, biochemical phenomena, metabolism, and nutrition, medicine.disease, Virology, 3. Good health, NU9056, 030104 developmental biology, Lytic cycle, Tip60, 030220 oncology & carcinogenesis, Primary effusion lymphoma, Oncovirus, MG149

Abstract

Kaposi's sarcoma-associated herpesvirus (KSHV) is an oncogenic virus responsible for the development of Kaposi's sarcoma, primary effusion lymphoma (PEL), and Multicentric Castleman's disease in immunocompromised individuals. Despite the burden of these diseases there are few treatment options for afflicted individuals, due in part to our limited understanding of virus-host interactions. Tip60, a histone aceytltransferase (HAT) has been previously shown to interact with both the KSHV latency associated nuclear antigen protein (LANA), which is the main factor in maintaining the viral latent state, and ORF36, a viral kinase expressed in the lytic phase. We further investigated Tip60-virus interaction to ascertain Tip60's role in the viral life cycle and its potential as a target for future therapeutics. Through modulation of Tip60 expression in HEK293T cells harboring a plasmid containing the KSHV viral episome, Bac36, we found that Tip60 is vital for both lytic replication as well as efficient expression of latent genes. Interestingly, Tip60 small molecule inhibitors, MG149 and NU9056, similarly inhibited latent and lytic genes, and reduced virion production in wild-type KSHV+/EBV- PEL, BCBL-1 cells. Long-term treatment with these Tip60 inhibitors selectively decreased the viability of KSHV-infected B lymphoma cells compared to uninfected cells. From this study, we conclude that Tip60 is important for KSHV infection and its associated cancer development, and Tip60 is therefore a potential target for future antiviral and anticancer therapeutics.

Published

2018

216. Interaction mechanisms of epigenetic integrator UHRF1 with TIP60 acetyltransferase

Author

Ashraf, Waseem, STAR, ABES, Laboratoire de Bioimagerie et Pathologies (UMR 7021), Université de Strasbourg (UNISTRA), Université de Strasbourg, Marc Mousli, and Christian Bronner

Subjects

Protein-Protein interaction, FLIM, DNA methylation, Histone acétyltransférase (HAT), [SDV.SP.PHARMA] Life Sciences [q-bio]/Pharmaceutical sciences/Pharmacology, DNMT1, [SDV.SP.PHARMA]Life Sciences [q-bio]/Pharmaceutical sciences/Pharmacology, FRET, Méthylation de l’ADN, Histone acetyltransferase (HAT), UHRF1, TIP60, Interactions protéine-protéine

Abstract

UHRF1 is a nuclear protein maintaining and regulating the epigenome of cells. Its promotes proliferation and is found upregulated in most of cancers. TIP60 is one of the important interacting partner of UHRF1 and is involved in chromatin remodeling and transcriptional regulation through its acetyltransferase activity. Together they regulate the stability and activity of other proteins such as DNMT1 and p53. The aim of this thesis was to explore the mechanism of interaction between UHRF1 and TIP60 by visualizing this interaction in cells. Fluorescent lifetime imaging microscopy and other molecular biology techniques were employed for this purpose. Results of this study showed that UHRF1 interacts directly to the MYST domain of TIP60 and this interaction prevails in the S-phase of cell cycle. Both proteins also showed a similar response to DNA damage predicting a coherence in their function in DNA repair mechanism. Overexpression of TIP60 also downregulated UHRF1 and DNMT1 and induced apoptosis in cells suggesting a role of TIP60 in regulation of oncogenic functions of UHRF1., UHRF1 est une protéine nucléaire responsable du maintien et de la régulation de l'épigénome des cellules. Elle favorise la prolifération cellulaire et est surexprimée dans la plupart des cancers. TIP60, l'un des partenaires le plus important d’UHRF1, est impliqué dans le remodelage de la chromatine et la régulation transcriptionnelle grâce à son activité acétyltransférase. Ensemble, les deux protéines régulent la stabilité et l'activité d'autres protéines telles que la DNMT1 et la p53. Le but de cette étude était d'explorer le mécanisme d'interaction entre UHRF1 et TIP60 en visualisant cette interaction dans les cellules. La microscopie par imagerie à temps de vie de fluorescence et d'autres techniques de biologie moléculaire ont été utilisées. Les résultats ont montré que UHRF1 interagit directement avec le domaine MYST de TIP60 et cette interaction se produit dans la phase S du cycle cellulaire. Les deux protéines ont également montré une réponse similaire aux dommages à l'ADN, ce qui prédit une cohérence dans leur fonction dans le mécanisme de réparation de l'ADN. La surexpression de TIP60 a également induit la baisse du niveau d’UHRF1 et de DNMT1 ainsi qu’une induction d'apoptose dans les cellules ce qui suggère un rôle de TIP60 dans la régulation des fonctions oncogéniques d’UHRF1.

Published

2018

217. TIP60 governs the auto‑ubiquitination of UHRF1 through USP7 dissociation from the UHRF1/USP7 complex.

Author

Ahmad T, Ashraf W, Ibrahim A, Zaayter L, Muller CD, Hamiche A, Mély Y, Bronner C, and Mousli M

Subjects

Apoptosis, CCAAT-Enhancer-Binding Proteins chemistry, Computational Biology, HeLa Cells, Humans, Tumor Protein p73 physiology, Ubiquitin-Protein Ligases chemistry, Ubiquitination, CCAAT-Enhancer-Binding Proteins metabolism, Lysine Acetyltransferase 5 physiology, Ubiquitin-Protein Ligases metabolism, Ubiquitin-Specific Peptidase 7 chemistry

Abstract

Tat interactive protein, 60 kDa (TIP60) is an important partner of ubiquitin‑like, containing PHD and RING finger domains 1 (UHRF1), ensuring various cellular processes through its acetyltransferase activity. TIP60 is believed to play a tumor suppressive role, partly explained by its downregulated expression in a number of cancers. The aim of the present study was to investigate the role and mechanisms of action of TIP60 in the regulation of UHRF1 expression. The results revealed that TIP60 overexpression downregulated the UHRF1 and DNA methyltransferase 1 (DNMT1) expression levels. TIP60 interfered with USP7‑UHRF1 association and induced the degradation of UHRF1 in an auto‑ubiquitination‑dependent manner. Moreover, TIP60 activated the p73‑mediated apoptotic pathway. Taken together, the data of the present study suggest that the tumor suppressor role of TIP60 is mediated by its regulation to UHRF1.

Published

2021

218. A Novel Mechanism of Ataxia Telangiectasia Mutated Mediated Regulation of Chromatin Remodeling in Hypoxic Conditions.

Author

Likhatcheva M, Gieling RG, Brown JAL, Demonacos C, and Williams KJ

Abstract

The effects of genotoxic stress can be mediated by activation of the Ataxia Telangiectasia Mutated (ATM) kinase, under both DNA damage-dependent (including ionizing radiation), and independent (including hypoxic stress) conditions. ATM activation is complex, and primarily mediated by the lysine acetyltransferase Tip60. Epigenetic changes can regulate this Tip60-dependent activation of ATM, requiring the interaction of Tip60 with tri-methylated histone 3 lysine 9 (H3K9me3). Under hypoxic stress, the role of Tip60 in DNA damage-independent ATM activation is unknown. However, epigenetic changes dependent on the methyltransferase Suv39H1, which generates H3K9me3, have been implicated. Our results demonstrate severe hypoxic stress (0.1% oxygen) caused ATM auto-phosphorylation and activation (pS1981), H3K9me3, and elevated both Suv39H1 and Tip60 protein levels in FTC133 and HCT116 cell lines. Exploring the mechanism of ATM activation under these hypoxic conditions, siRNA-mediated Suv39H1 depletion prevented H3K9me3 induction, and Tip60 inhibition (by TH1834) blocked ATM auto-phosphorylation. While MDM2 (Mouse double minute 2) can target Suv39H1 for degradation, it can be blocked by sirtuin-1 (Sirt1). Under severe hypoxia MDM2 protein levels were unchanged, and Sirt1 levels depleted. SiRNA-mediated depletion of MDM2 revealed MDM2 dependent regulation of Suv39H1 protein stability under these conditions. We describe a novel molecular circuit regulating the heterochromatic state (H3K9me3 positive) under severe hypoxic conditions, showing that severe hypoxia-induced ATM activation maintains H3K9me3 levels by downregulating MDM2 and preventing MDM2-mediated degradation of Suv39H1. This novel mechanism is a potential anti-cancer therapeutic opportunity, which if exploited could target the hypoxic tumor cells known to drive both tumor progression and treatment resistance., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Likhatcheva, Gieling, Brown, Demonacos and Williams.)

Published

2021

219. TIP60-miR-22 axis as a prognostic marker of breast cancer progression

Author

Henry Yang, Sudhakar Jha, Siting Zhang, Greg Tucker-Kellogg, Ying Li, Amit Kumar Pandey, and Yanzhou Zhang

Subjects

Pathology, medicine.medical_specialty, Epithelial-Mesenchymal Transition, miR-22, Breast Neoplasms, Kaplan-Meier Estimate, Lysine Acetyltransferase 5, Cell Line, Metastasis, Breast cancer, Cell Movement, Cell Line, Tumor, microRNA, Biomarkers, Tumor, medicine, Humans, cancer, Epithelial–mesenchymal transition, KAT5, 3' Untranslated Regions, Histone Acetyltransferases, Microscopy, Confocal, Reverse Transcriptase Polymerase Chain Reaction, business.industry, EMT, Cancer, Prognosis, medicine.disease, Metastatic breast cancer, Gene Expression Regulation, Neoplastic, MicroRNAs, HEK293 Cells, Oncology, Cancer cell, Disease Progression, MCF-7 Cells, Cancer research, Female, TIP60, business, Research Paper

Abstract

MicroRNAs (miRNAs) are 22- to 24-nucleotide, small, non-coding RNAs that bind to the 3′UTR of target genes to control gene expression. Consequently, their dysregulation contributes to many diseases, including diabetes and cancer. miR-22 is up-regulated in numerous metastatic cancers and recent studies have suggested a role for miR-22 in promoting stemness and metastasis. TIP60 is a lysine acetyl-transferase reported to be down-regulated in cancer but the molecular mechanism of this reduction is still unclear. In this study, we identify TIP60 as a target of miR-22. We show a negative correlation in the expression of TIP60 and miR-22 in breast cancer patients, and show that low levels of TIP60 and high levels of miR-22 are associated with poor overall survival. Furthermore, pathway analysis using high miR-22/low TIP60 and low miR-22/high TIP60 breast cancer patient datasets suggests association of TIP60/miR-22 with epithelial-mesenchymal transition (EMT), a key alteration in progression of cancer cells. We show that blocking endogenous miR-22 can restore TIP60 levels, which in turn decreases the migration and invasion capacity of metastatic breast cancer cell line. These results provide mechanistic insight into TIP60 regulation and evidence for the utility of the combination of TIP60 and miR-22 as prognostic indicator of breast cancer progression.

Published

2015

220. Baculoviruses and nucleosome management

Author

Loy E. Volkman

Subjects

Insecta, Negatively-supercoiled ds DNA, Genome, Viral, macromolecular substances, Virus Replication, Medical and Health Sciences, INO80, chemistry.chemical_compound, Transcription (biology), SWI/SNF, INO80, TIP60, Virology, Genetics, Nucleosome, Animals, Topoisomerase 2, Viral, Baculovirus, Actin, Cytochalasin D, Genome, biology, Agricultural and Veterinary Sciences, AcMNPV, Biological Sciences, Molecular biology, SWI/SNF, Actin-containing chromatin modification complexes, Chromatin, Cell biology, Nucleosomes, Histone, chemistry, Nucleosome mobilization, Autographa californica M nucleopolyhedrovirus, biology.protein, Insect Proteins, Viral chromatin, TIP60, Baculoviridae, DNA

Abstract

© 2014 The Authors. Negatively-supercoiled-ds DNA molecules, including the genomes of baculoviruses, spontaneously wrap around cores of histones to form nucleosomes when present within eukaryotic nuclei. Hence, nucleosome management should be essential for baculovirus genome replication and temporal regulation of transcription, but this has not been documented. Nucleosome mobilization is the dominion of ATP-dependent chromatin-remodeling complexes. SWI/SNF and INO80, two of the best-studied complexes, as well as chromatin modifier TIP60, all contain actin as a subunit. Retrospective analysis of results of AcMNPV time course experiments wherein actin polymerization was blocked by cytochalasin D drug treatment implicate actin-containing chromatin modifying complexes in decatenating baculovirus genomes, shutting down host transcription, and regulating late and very late phases of viral transcription. Moreover, virus-mediated nuclear localization of actin early during infection may contribute to nucleosome management.

Published

2015

221. Evidence that the acetyltransferase Tip60 induces the DNA damage response and cell-cycle arrest in neonatal cardiomyocytes.

Author

Wang X, Lupton C, Lauth A, Wan TC, Foster P, Patterson M, Auchampach JA, and Lough JW

Subjects

Animals, Animals, Newborn, Apoptosis genetics, Biomarkers, Disease Models, Animal, Echocardiography, Gene Expression, Immunohistochemistry, Lysine Acetyltransferase 5 genetics, Mice, Mice, Transgenic, Myocardial Infarction diagnostic imaging, Myocardial Infarction etiology, Myocardial Infarction metabolism, Myocardial Infarction pathology, Myocardium metabolism, Myocardium pathology, Ploidies, Trans-Activators genetics, Wound Healing, Cell Cycle Checkpoints, DNA Damage, Lysine Acetyltransferase 5 metabolism, Myocytes, Cardiac metabolism, Trans-Activators metabolism

Abstract

Tip60, a pan-acetyltransferase encoded by the Kat5 gene, is enriched in the myocardium; however, its function in the heart is unknown. In cancer cells, Tip60 acetylates Atm (Ataxia-telangiectasia mutated), enabling its auto-phosphorylation (pAtm), which activates the DNA damage response (DDR). It was recently reported that activation of pAtm at the time of birth induces the DDR in cardiomyocytes (CMs), resulting in proliferative senescence. We therefore hypothesized that Tip60 initiates this process, and that depletion of Tip60 accordingly diminishes the DDR while extending the duration of CM cell-cycle activation. To test this hypothesis, an experimental model was used wherein a Myh6-driven Cre-recombinase transgene was activated on postnatal day 0 (P0) to recombine floxed Kat5 alleles and induce Tip60 depletion in neonatal CMs, without causing pathogenesis. Depletion of Tip60 resulted in reduced numbers of pAtm-positive CMs during the neonatal period, which correlated with reduced numbers of pH2A.X-positive CMs and decreased expression of genes encoding markers of the DDR as well as inflammation. This was accompanied by decreased expression of the cell-cycle inhibitors Meis1 and p27, activation of the cell-cycle in CMs, reduced CM size, and increased numbers of mononuclear/diploid CMs. Increased expression of fetal markers suggested that Tip60 depletion promotes a fetal-like proliferative state. Finally, infarction of Tip60-depleted hearts at P7 revealed improved cardiac function at P39 accompanied by reduced fibrosis, increased CM cell-cycle activation, and reduced apoptosis in the remote zone. These findings indicate that, among its pleiotropic functions, Tip60 induces the DDR in CMs, contributing to proliferative senescence., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

222. EPC1/TIP60-mediated histone acetylation facilitates spermiogenesis in mice

Author

Dong, Yixin, Isono, Kyo Ichi, Ohbo, Kazuyuki, Endo, Takaho A., Ohara, Osamu, Maekawa, Mamiko, Toyama, Yoshiro, Ito, Chizuru, Toshimori, Kiyotaka, Helin, Kristian, Ogonuki, Narumi, Inoue, Kimiko, Ogura, Atsuo, Yamagata, Kazutsune, Kitabayashi, Issay, Koseki, Haruhiko, Dong, Yixin, Isono, Kyo Ichi, Ohbo, Kazuyuki, Endo, Takaho A., Ohara, Osamu, Maekawa, Mamiko, Toyama, Yoshiro, Ito, Chizuru, Toshimori, Kiyotaka, Helin, Kristian, Ogonuki, Narumi, Inoue, Kimiko, Ogura, Atsuo, Yamagata, Kazutsune, Kitabayashi, Issay, and Koseki, Haruhiko

Abstract

Global histone hyperacetylation is suggested to play a critical role for replacement of histones by transition proteins and protamines to compact the genome during spermiogenesis. However, the underlying mechanisms for hyperacetylation-mediated histone replacement remains poorly understood. Here, we report that EPC1 and TIP60, two critical components of the mammalian nucleosome acetyltransferase of H4 (NuA4) complexes, are coexpressed in male germ cells. Strikingly, genetic ablation of either Epc1 or Tip60 disrupts hyperacetylation and impairs histone replacement, in turn causing aberrant spermatid development. Taking these observations together, we reveal an essential role of the NuA4 complexes for histone hyperacetylation and subsequent compaction of the spermatid genome., Global histone hyperacetylation is suggested to play a critical role for replacement of histones by transition proteins and protamines to compact the genome during spermiogenesis. However, the underlying mechanisms for hyperacetylation- mediated histone replacement remains poorly understood. Here, we report that EPC1 and TIP60, two critical components of the mammalian nucleosome acetyltransferase of H4 (NuA4) complexes, are coexpressed in male germ cells. Strikingly, genetic ablation of either Epc1 or Tip60 disrupts hyperacetylation and impairs histone replacement, in turn causing aberrant spermatid development. Taking these observations together, we reveal an essential role of the NuA4 complexes for histone hyperacetylation and subsequent compaction of the spermatid genome.

Published

2017

223. Tat-interactive Protein-60KDA (TIP60) Regulates the Tumorigenesis of Lung Cancer In Vitro

Author

Daru Lu, Xiao Zhou, Jian Sun, Yang Yang, Ting Chen, Zengyue Tao, Xianwei Zhang, and Feng Tian

Subjects

0301 basic medicine, Gene knockdown, Akt/PKB signaling pathway, cDNA library, AKT, Myc, Biology, medicine.disease_cause, medicine.disease, In vitro, 03 medical and health sciences, lung cancer, 030104 developmental biology, Oncology, medicine, Cancer research, Viability assay, Carcinogenesis, Lung cancer, TIP60, Protein kinase B, cell viability, Research Paper

Abstract

Histone acetyltransferases (HATs) play vital functions in the tumorigenesis of many solid organ malignancies. We previously screened a human HATs cDNA library and identified Tat-interactive protein-60KDa (TIP60) as a candidate critical HATs in the origination of lung cancer. In this study, our data suggested that overexpression of TIP60 inhibited the cell viability of A549 and H1299 cells since day 2. Compared to the control group, the viability of these two lung cancer cells was inhibited by 25% and 19% at day 6 with the overexpression of TIP60. It increased by 36% and 26% when TIP60 was knockdown for 6 days. The invasion ability of these two cells was also restrained when TIP60 was overexpressed. While knockdown of TIP60 had the opposite effect. Inhibition of TIP60 significantly promoted the expression of molecules in AKT signaling pathway especially c-Myc. Furthermore, compared to paired tumor-adjacent tissue, lung cancer tumors had low expression of TIP60. Therefore, we concluded that TIP60 might inhibit the viability and invasion ability of lung cancer cells through down-regulation of AKT signaling pathway.

Published

2017

224. Bypassing the Requirement for an Essential MYST Acetyltransferase

Author

Lorraine Pillus and Ana Lilia Torres-Machorro

Subjects

Saccharomyces cerevisiae Proteins, Lysine Acetyltransferases, DNA Repair, 1.1 Normal biological development and functioning, Saccharomyces cerevisiae, Investigations, Models, Biological, ESA1/KAT5, Histone Deacetylases, Histones, Essential, Models, Underpinning research, Genetics, DNA damage repair, 2.1 Biological and endogenous factors, Aetiology, Histone Acetyltransferases, Genes, Essential, biology, Cell Cycle, Temperature, HDACs, Acetylation, Biological, biology.organism_classification, Chromatin, Rpd3L, Histone, Genes, Tip60, Biochemistry, Acetyltransferase, Mutation, Sirtuin, biology.protein, Genetic Fitness, Gene Deletion, DNA Damage, Protein Binding, Developmental Biology

Abstract

Histone acetylation is a key regulatory feature for chromatin that is established by opposing enzymatic activities of lysine acetyltransferases (KATs/HATs) and deacetylases (KDACs/HDACs). Esa1, like its human homolog Tip60, is an essential MYST family enzyme that acetylates histones H4 and H2A and other nonhistone substrates. Here we report that the essential requirement for ESA1 in Saccharomyces cerevisiae can be bypassed upon loss of Sds3, a noncatalytic subunit of the Rpd3L deacetylase complex. By studying the esa1∆ sds3∆ strain, we conclude that the essential function of Esa1 is in promoting the cellular balance of acetylation. We demonstrate this by fine-tuning acetylation through modulation of HDACs and the histone tails themselves. Functional interactions between Esa1 and HDACs of class I, class II, and the Sirtuin family define specific roles of these opposing activities in cellular viability, fitness, and response to stress. The fact that both increased and decreased expression of the ESA1 homolog TIP60 has cancer associations in humans underscores just how important the balance of its activity is likely to be for human well-being.

Published

2014

225. Metabolic Roles of Androgen Receptor and Tip60 in Androgen-Dependent Prostate Cancer.

Author

Tan, Kah Ni, Avery, Vicky M., and Carrasco-Pozo, Catalina

Subjects

*ANDROGEN receptors, *PROSTATE cancer, *GLYCOLYSIS, *KREBS cycle, *CALMODULIN, *TAT protein, *HISTONE acetyltransferase

Abstract

Androgen receptor (AR)-mediated signaling is essential for the growth and differentiation of the normal prostate and is the primary target for androgen deprivation therapy in prostate cancer. Tat interactive protein 60 kDa (Tip60) is a histone acetyltransferase that is critical for AR activation. It is well known that cancer cells rewire their metabolic pathways in order to sustain aberrant proliferation. Growing evidence demonstrates that the AR and Tip60 modulate key metabolic processes to promote the survival of prostate cancer cells, in addition to their classical roles. AR activation enhances glucose metabolism, including glycolysis, tricarboxylic acid cycle and oxidative phosphorylation, as well as lipid metabolism in prostate cancer. The AR also interacts with other metabolic regulators, including calcium/calmodulin-dependent kinase kinase 2 and mammalian target of rapamycin. Several studies have revealed the roles of Tip60 in determining cell fate indirectly by modulating metabolic regulators, such as c-Myc, hypoxia inducible factor 1α (HIF-1α) and p53 in various cancer types. Furthermore, Tip60 has been shown to regulate the activity of key enzymes in gluconeogenesis and glycolysis directly through acetylation. Overall, both the AR and Tip60 are master metabolic regulators that mediate cellular energy metabolism in prostate cancer, providing a framework for the development of novel therapeutic targets in androgen-dependent prostate cancer. [ABSTRACT FROM AUTHOR]

Published

2020

226. Regulation of ΔNp63α by TIP60 promotes cellular proliferation

Author

Stacy, Andrew Jared

Subjects

Biochemistry, Biomedical Research, Cellular Biology, Molecular Biology, Oncology, p63, TIP60, acetylation, p21, cell proliferation, cell cycle, cancer, non-melanoma skin cancer, squamous cell carcinoma

Abstract

ΔNp63α is a p53 transcription factor family member that promotes cellular proliferation and survival. In squamous cell carcinoma (SCC), ΔNp63α overexpression is associated with poor prognosis and survival, implicating it as a proto-oncogene. Despite its importance in SCC, the mechanisms regulating ΔNp63α expression are poorly understood. We have identified the acetyltransferase TIP60 as a novel upstream regulator of ΔNp63α levels. We discovered that TIP60 regulates ΔNp63α via two mechanisms. First, TIP60 upregulates ΔNp63α mRNA levels. Moreover, pharmacological inhibition of TIP60 activity reduces ΔNp63α transcript levels, indicating that TIP60-cataltyic activity is vital to amplified transcription of ΔNp63α. Second, we have demonstrated that TIP60 promotes ΔNp63α protein stability by preventing its ubiquitination and proteasomal degradation. This study further shows that TIP60 co-localizes with, interacts with, and directly acetylates ΔNp63α. Utilizing mass spectrometry and site directed mutagenesis, we found that TIP60 acetylates ΔNp63α residues K138, K139, and K494, respectively. We additionally revealed that preventing acetylation of these sites inhibit TIP60-mediated stabilization of ΔNp63α, providing evidence that acetylation by TIP60 enhances ΔNp63α protein stability. We further investigated the functions of the TIP60-ΔNp63α axis in the regulation of SCC proliferation. We discovered that regulation of ΔNp63α by TIP60 increases cellular proliferation. In accordance with the functional role of ΔNp63α, pharmacological inhibition of TIP60 reduced SCC cell proliferation suggesting TIP60 may have therapeutic potential in cancers exhibiting ΔNp63α overexpression. Furthermore, we investigated the mechanisms by which TIP60 regulation of ΔNp63α enhances cancer cell proliferation. We discovered that TIP60 upregulation of ΔNp63α represses p21Cip1/Waf1 levels, resulting in increased G2/M progression. In conclusion, this study uncovers a novel mechanism promoting ΔNp63α-mediated cellular proliferation in SCC. These findings may be critical for designing new therapeutic strategies for the treatment of SCC by targeting ΔNp63α expression and activity.

Published

2020

227. Regulation of the Human Papillomavirus Life Cycle by DNA Damage Repair Pathways and Epigenetic Factors.

Author

Albert, Ekaterina and Laimins, Laimonis

Subjects

*HUMAN life cycle, *DNA damage, *DNA repair, *EPIGENETICS, *PAPILLOMAVIRUS diseases, *VIRAL proteins, *OROPHARYNGEAL cancer

Abstract

Human papillomaviruses are the causative agents of cervical and other anogenital cancers along with approximately 60% of oropharyngeal cancers. These small double-stranded DNA viruses infect stratified epithelia and link their productive life cycles to differentiation. HPV proteins target cellular factors, such as those involved in DNA damage repair, as well as epigenetic control of host and viral transcription to regulate the productive life cycle. HPVs constitutively activate the ATM and ATR DNA repair pathways and preferentially recruit these proteins to viral genomes to facilitate productive viral replication. In addition, the sirtuin deacetylases along with histone acetyltransferases, including Tip60, are targeted in HPV infections to regulate viral transcription and replication. These pathways provide potential targets for drug therapy to treat HPV-induced disease. [ABSTRACT FROM AUTHOR]

Published

2020

228. Histone acetyltransferase promotes fluoride toxicity in LS8 cells.

Author

Deng, Huidan, Fujiwara, Natsumi, Cui, Hengmin, Whitford, Gary M., Bartlett, John D., and Suzuki, Maiko

Subjects

*HISTONE acetyltransferase, *CYTOCHROME c, *FLUORIDES, *POST-translational modification, *P53 protein, *DNA damage, *GENETIC markers

Abstract

Previously we demonstrated that fluoride increased acetylated-p53 (Ac-p53) in LS8 cells that are derived from mouse enamel organ epithelia and in rodent ameloblasts. However, how p53 is acetylated by fluoride and how the p53 upstream molecular pathway responds to fluoride is not well characterized. Here we demonstrate that fluoride activates histone acetyltransferases (HATs) including CBP, p300, PCAF and Tip60 to acetylate p53. HAT activity is regulated by post-translational modifications such as acetylation and phosphorylation. HAT proteins and their post-translational modifications (p300, Acetyl-p300, CBP, Acetyl-CBP, Tip60 and phospho-Tip60) were analyzed by Western blots. p53-HAT binding was detected by co-immunoprecipitation (co-IP). Cell growth inhibition was analyzed by MTT assays. LS8 cells were treated with NaF with/without HAT inhibitors MG149 (Tip60 inhibitor) and Anacardic Acid (AA; inhibits p300/CBP and PCAF). MG149 or AA was added 1 h prior to NaF treatment. Co-IP results showed that NaF increased p53-CBP binding and p53-PCAF binding. NaF increased active Acetyl-p300, Acetyl-CBP and phospho-Tip60 levels, suggesting that fluoride activates these HATs. Fluoride-induced phospho-Tip60 was decreased by MG149. MG149 or AA treatment reversed fluoride-induced cell growth inhibition at 24 h. MG149 or AA treatment decreased fluoride-induced p53 acetylation to inhibit caspase-3 cleavage, DNA damage marker γH2AX expression and cytochrome-c release into the cytosol. These results suggest that acetylation of p53 by HATs contributes, at least in part, to fluoride-induced toxicity in LS8 cells via cell growth inhibition, apoptosis, DNA damage and mitochondrial damage. Modulation of HAT activity may, therefore, be a potential therapeutic target to mitigate fluoride toxicity in ameloblasts. • Fluoride activates histone acetyltransferase (HAT) in enamel organ-derived LS8 cells. • HAT inhibitors suppressed fluoride-mediated acetylation of p53 and cell toxicity. • Modulation of HAT activity may be a potential target to mitigate fluoride toxicity. [ABSTRACT FROM AUTHOR]

Published

2020

229. Structural Basis for EPC1-Mediated Recruitment of MBTD1 into the NuA4/TIP60 Acetyltransferase Complex.

Author

Zhang, Heng, Devoucoux, Maëva, Song, Xiaosheng, Li, Li, Ayaz, Gamze, Cheng, Harry, Tempel, Wolfram, Dong, Cheng, Loppnau, Peter, Côté, Jacques, and Min, Jinrong

Abstract

MBTD1, a H4K20me reader, has recently been identified as a component of the NuA4/TIP60 acetyltransferase complex, regulating gene expression and DNA repair. NuA4/TIP60 inhibits 53BP1 binding to chromatin through recognition of the H4K20me mark by MBTD1 and acetylation of H2AK15, blocking the ubiquitination mark required for 53BP1 localization at DNA breaks. The NuA4/TIP60 non-catalytic subunit EPC1 enlists MBTD1 into the complex, but the detailed molecular mechanism remains incompletely explored. Here, we present the crystal structure of the MBTD1-EPC1 complex, revealing a hydrophobic C-terminal fragment of EPC1 engaging the MBT repeats of MBTD1 in a site distinct from the H4K20me binding site. Different cellular assays validate the physiological significance of the key residues involved in the MBTD1-EPC1 interaction. Our study provides a structural framework for understanding the mechanism by which MBTD1 recruits the NuA4/TIP60 acetyltransferase complex to influence transcription and DNA repair pathway choice. • The crystal structure of EPC1 bound to MBTD1 is determined • MBTD1 employs two distinct regions to recognize H4K20me and EPC1 • Mutations at the MBTD1-EPC1 interface affect gene expression and DNA repair EPC1 is a critical component of the NuA4/TIP60 acetyltransferase complex involved in gene expression and genome maintenance. Zhang et al. illuminate the structural and molecular basis for EPC1 bound to the H4K20me reader MBTD1, highlighting the important role of their association in gene transcription and DNA repair. [ABSTRACT FROM AUTHOR]

Published

2020

230. Hippocampal stimulation promotes intracellular Tip60 dynamics with concomitant genome reorganization and synaptic gene activation.

Author

Karnay, Ashley, Karisetty, Bhanu Chandra, Beaver, Mariah, and Elefant, Felice

Subjects

*GENETIC regulation, *RNA polymerase II, *LONG-term potentiation, *FLUORESCENCE in situ hybridization, *HISTONE acetyltransferase, *THETA rhythm

Abstract

Genomic reorganizations mediating the engagement of target genes to transcription factories (TFs), characterized as specialized nuclear subcompartments enriched in hyperphosphorylated RNA polymerase II (RNAPII) and transcriptional regulators, act as an important layer of control in coordinating efficient gene transcription. However, their presence in hippocampal neurons and potential role in activity-dependent coregulation of genes within the brain remains unclear. Here, we investigate whether the well-characterized role for the histone acetyltransferase (HAT) Tip60 in mediating epigenetic control of inducible neuroplasticity genes involves TF associated chromatin reorganization in the hippocampus. We show that Tip60 shuttles into the nucleus following extracellular stimulation of rat hippocampal neurons with concomitant enhancement of Tip60 binding and activation of specific synaptic plasticity genes. Multicolor three-dimensional (3D) DNA fluorescent in situ hybridization (DNA-FISH) reveals that hippocampal stimulation mobilizes these same synaptic plasticity genes and Tip60 to RNAPII-rich TFs. Our data support a model by which external hippocampal stimulation promotes intracellular Tip60 HAT dynamics with concomitant TF associated genome reorganization to initiate Tip60mediated synaptic gene activation. • Transcription factory (TF) function in activity-dependent neuroplasticity gene control in the brain is unclear. • Extracellular stimulation leads to subcellular redistribution of Tip60 within hippocampal neurons. • Tip60 is recruited to inducible neuroplasticity genes that are activated following extracellular stimulation. • Tip60 neuroplasticity gene targets associate with TFs in response to extracellular stimulation. • Neuroplasticity genes and Tip60 co-associate with the same TF following extracellular stimulation. [ABSTRACT FROM AUTHOR]

Published

2019

231. MRGBP, a member of the NuA4 complex, inhibits DNA double-strand break repair.

Author

Rivero S, Rodríguez-Real G, Marín I, and Huertas P

Subjects

Cell Line, Tumor, DNA Breaks, Double-Stranded, DNA End-Joining Repair, Humans, Recombinational DNA Repair, DNA Repair, Down-Regulation, Histone Acetyltransferases metabolism, Nuclear Proteins metabolism

Abstract

The repair of DNA breaks takes place in the context of chromatin and thus involves the activity of chromatin remodelers. The nucleosome acetyltransferase of H4 (NuA4) remodeler complex enables DNA break repair by relaxing flanking chromatin. Here, we show that MRG domain binding protein (MRGBP), a member of this complex, acts as a general inhibitor of DNA double-strand break repair. Upon its downregulation, repair is generally increased. This is particularly evident for the stimulation of early events of homologous recombination. Thus, MRGBP has an opposing role to the main catalytic subunits of the NuA4 complex. Our data suggest that MRGBP acts by limiting the activity of this complex in DNA repair, specifically by narrowing the extent of DNA-end resection., (© 2020 The Authors. FEBS Open Bio published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.)

Published

2021

232. RGS6 suppresses Ras-induced cellular transformation by facilitating Tip60-mediated Dnmt1 degradation and promoting apoptosis

Author

Huang, J, Stewart, A, Maity, B, Hagen, J, Fagan, R L, Yang, J, Quelle, D E, Brenner, C, and Fisher, R A

Published

2014

233. DMAP1 is an essential regulator of ATM activity and function

Author

Penicud, K and Behrens, A

Published

2014

234. FOXP3 and Tip60 Structural Interactions Relevant to IPEX Development Lead to Potential Therapeutics to Increase FOXP3 Dependent Suppressor T Cell Functions.

Author

Grover P, Goel PN, Piccirillo CA, and Greene MI

Abstract

Regulatory T (Treg) cells play a role in the maintenance of immune homeostasis and are critical mediators of immune tolerance. The Forkhead box P3 (FOXP3) protein acts as a regulator for Treg development and function. Mutations in the FOXP3 gene can lead to autoimmune diseases such as Immunodysregulation, polyendocrinopathy, enteropathy, and X-linked (IPEX) syndrome in humans, often resulting in death within the first 2 years of life and a scurfy like phenotype in Foxp3 mutant mice. We discuss biochemical features of the FOXP3 ensemble including its regulation at various levels (epigenetic, transcriptional, and post-translational modifications) and molecular functions. The studies also highlight the interactions of FOXP3 and Tat-interacting protein 60 (Tip60), a principal histone acetylase enzyme that acetylates FOXP3 and functions as an essential subunit of the FOXP3 repression ensemble complex. Lastly, we have emphasized the role of allosteric modifiers that help stabilize FOXP3:Tip60 interactions and discuss targeting this interaction for the therapeutic manipulation of Treg activity., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Grover, Goel, Piccirillo and Greene.)

Published

2021

235. JAZF1, A Novel p400/TIP60/NuA4 Complex Member, Regulates H2A.Z Acetylation at Regulatory Regions.

Author

Procida T, Friedrich T, Jack APM, Peritore M, Bönisch C, Eberl HC, Daus N, Kletenkov K, Nist A, Stiewe T, Borggrefe T, Mann M, Bartkuhn M, and Hake SB

Subjects

Acetylation, Cell Line, Chromatin Assembly and Disassembly, Computational Biology methods, DNA Helicases metabolism, Enhancer Elements, Genetic, Gene Expression Regulation, Genomics methods, Humans, Introns, Lysine Acetyltransferase 5 metabolism, Molecular Chaperones metabolism, Multiprotein Complexes, Protein Binding, Ribosomes, Transcription Factors metabolism, Co-Repressor Proteins metabolism, DNA-Binding Proteins metabolism, Histones metabolism, Regulatory Sequences, Nucleic Acid

Abstract

Histone variants differ in amino acid sequence, expression timing and genomic localization sites from canonical histones and convey unique functions to eukaryotic cells. Their tightly controlled spatial and temporal deposition into specific chromatin regions is accomplished by dedicated chaperone and/or remodeling complexes. While quantitatively identifying the chaperone complexes of many human H2A variants by using mass spectrometry, we also found additional members of the known H2A.Z chaperone complexes p400/TIP60/NuA4 and SRCAP. We discovered JAZF1, a nuclear/nucleolar protein, as a member of a p400 sub-complex containing MBTD1 but excluding ANP32E. Depletion of JAZF1 results in transcriptome changes that affect, among other pathways, ribosome biogenesis. To identify the underlying molecular mechanism contributing to JAZF1's function in gene regulation, we performed genome-wide ChIP-seq analyses. Interestingly, depletion of JAZF1 leads to reduced H2A.Z acetylation levels at > 1000 regulatory sites without affecting H2A.Z nucleosome positioning. Since JAZF1 associates with the histone acetyltransferase TIP60, whose depletion causes a correlated H2A.Z deacetylation of several JAZF1-targeted enhancer regions, we speculate that JAZF1 acts as chromatin modulator by recruiting TIP60's enzymatic activity. Altogether, this study uncovers JAZF1 as a member of a TIP60-containing p400 chaperone complex orchestrating H2A.Z acetylation at regulatory regions controlling the expression of genes, many of which are involved in ribosome biogenesis.

Published

2021

236. Role of histone acetyltransferase inhibitors in cancer therapy.

Author

Shanmugam MK, Dharmarajan A, Warrier S, Bishayee A, Kumar AP, Sethi G, and Ahn KS

Subjects

Humans, Antineoplastic Agents therapeutic use, Enzyme Inhibitors therapeutic use, Histone Acetyltransferases antagonists & inhibitors, Histone Acetyltransferases metabolism, Neoplasm Proteins antagonists & inhibitors, Neoplasm Proteins metabolism, Neoplasms drug therapy, Neoplasms enzymology

Abstract

The development of cancer is a complex phenomenon driven by various extrinsic as well as intrinsic risk factors including epigenetic modifications. These post-translational modifications are encountered in diverse cancer cells and appear for a relatively short span of time. These changes can significantly affect various oncogenic genes and proteins involved in cancer initiation and progression. Histone lysine acetylation and deacetylation processes are controlled by two opposing classes of enzymes that modulate gene regulation either by adding an acetyl moiety on a histone lysine residue by histone lysine acetyltransferases (KATs) or via removing it by histone deacetylases (KDACs). Deregulated KAT activity has been implicated in the development of several diseases including cancer and can be targeted for the development of anti-neoplastic drugs. Here, we describe the predominant epigenetic changes that can affect key KAT superfamily members during carcinogenesis and briefly highlight the pharmacological potential of employing lysine acetyltransferase inhibitors (KATi) for cancer therapy., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2021

237. Transcription Factor RBPJ as a Molecular Switch in Regulating the Notch Response.

Author

Giaimo BD, Gagliani EK, Kovall RA, and Borggrefe T

Subjects

Chromatin genetics, Chromatin metabolism, Humans, Signal Transduction, Gene Expression Regulation, Immunoglobulin J Recombination Signal Sequence-Binding Protein metabolism, Receptors, Notch metabolism

Abstract

The Notch signal transduction cascade requires cell-to-cell contact and results in the proteolytic processing of the Notch receptor and subsequent assembly of a transcriptional coactivator complex containing the Notch intracellular domain (NICD) and transcription factor RBPJ. In the absence of a Notch signal, RBPJ remains at Notch target genes and dampens transcriptional output. Like in other signaling pathways, RBPJ is able to switch from activation to repression by associating with corepressor complexes containing several chromatin-modifying enzymes. Here, we focus on the recent advances concerning RBPJ-corepressor functions, especially in regard to chromatin regulation. We put this into the context of one of the best-studied model systems for Notch, blood cell development. Alterations in the RBPJ-corepressor functions can contribute to the development of leukemia, especially in the case of acute myeloid leukemia (AML). The versatile role of transcription factor RBPJ in regulating pivotal target genes like c-MYC and HES1 may contribute to the better understanding of the development of leukemia.

Published

2021

238. Inhibition of PfMYST Histone Acetyltransferase Activity Blocks Plasmodium falciparum Growth and Survival.

Author

Sen U, Nayak A, Khurana J, Sharma D, and Gupta A

Subjects

Acetylation, Animals, Erythrocytes metabolism, Histone Acetyltransferases genetics, Histone Acetyltransferases metabolism, Plasmodium falciparum genetics, Plasmodium falciparum metabolism, Protozoan Proteins genetics, Protozoan Proteins metabolism, Schizonts metabolism, Antimalarials pharmacology, Malaria, Falciparum

Abstract

One of the major barriers in the prevention and control of malaria programs worldwide is the growing emergence of multidrug resistance in Plasmodium parasites, and this necessitates continued efforts to discover and develop effective drug molecules targeting novel proteins essential for parasite survival. In recent years, epigenetic regulators have evolved as an attractive drug target option owing to their crucial role in survival and development of Plasmodium at different stages of its life cycle. PfMYST, a histone acetyltransferase protein, is known to regulate key cellular processes, such as cell cycle progression, DNA damage repair, and antigenic variation, that facilitate parasite growth, adaptation, and survival inside its host. With the aim of assessing the therapeutic potential of PfMYST as a novel drug target, we examined the effect of NU9056 (an HsTIP60 inhibitor) on the rate of parasite growth and survival. In the present study, by using a yeast complementation assay, we established that PfMYST is a true homolog of TIP60 and showed that NU9056 can inhibit PfMYST catalytic activity and kill P. falciparum parasites in culture. Inhibiting the catalytic activity of PfMYST arrests the parasite in the trophozoite stage and inhibits its further transition to the schizont stage, eventually leading to its death. Overall, our study provides proof of concept that PfMYST catalytic activity is essential for parasite growth and survival and that PfMYST can be a potential target for antimalarial therapy., (Copyright © 2020 American Society for Microbiology.)

Published

2020

239. Tip60 protects against amyloid-β-induced transcriptomic alterations via different modes of action in early versus late stages of neurodegeneration.

Author

Zhang H, Karisetty BC, Bhatnagar A, Armour EM, Beaver M, Roach TV, Mortazavi S, Mandloi S, and Elefant F

Subjects

Acetylation, Alzheimer Disease genetics, Alzheimer Disease metabolism, Animals, Apoptosis, Association Learning physiology, Disease Models, Animal, Drosophila melanogaster growth & development, Drosophila melanogaster metabolism, Epigenesis, Genetic, Gene Expression Regulation, Histone Code, Histone Deacetylase 2 physiology, Larva, Locomotion, Longevity, Maze Learning, Odorants, Protein Processing, Post-Translational, Smell physiology, Amyloid beta-Peptides toxicity, Drosophila Proteins physiology, Drosophila melanogaster genetics, Histone Acetyltransferases physiology, Nerve Degeneration genetics, Peptide Fragments toxicity, Transcriptome

Abstract

Alzheimer's disease (AD) is an age-related neurodegenerative disorder hallmarked by amyloid-β (Aβ) plaque accumulation, neuronal cell death, and cognitive deficits that worsen during disease progression. Histone acetylation dysregulation, caused by an imbalance between reduced histone acetyltransferases (HAT) Tip60 and increased histone deacetylase 2 (HDAC2) levels, can directly contribute to AD pathology. However, whether such AD-associated neuroepigenetic alterations occur in response to Aβ peptide production and can be protected against by increasing Tip60 levels over the course of neurodegenerative progression remains unknown. Here we profile Tip60 HAT/HDAC2 dynamics and transcriptome-wide changes across early and late stage AD pathology in the Drosophila brain produced solely by human amyloid-β 42 . We show that early Aβ 42 induction leads to disruption of Tip60 HAT/HDAC2 balance during early neurodegenerative stages preceding Aβ plaque accumulation that persists into late AD stages. Correlative transcriptome-wide studies reveal alterations in biological processes we classified as transient (early-stage only), late-onset (late-stage only), and constant (both). Increasing Tip60 HAT levels in the Aβ 42 fly brain protects against AD functional pathologies that include Aβ plaque accumulation, neural cell death, cognitive deficits, and shorter life-span. Strikingly, Tip60 protects against Aβ 42 -induced transcriptomic alterations via distinct mechanisms during early and late stages of neurodegeneration. Our findings reveal distinct modes of neuroepigenetic gene changes and Tip60 neuroprotection in early versus late stages in AD that can serve as early biomarkers for AD, and support the therapeutic potential of Tip60 over the course of AD progression., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

240. PRMT5-Dependent Methylation of the TIP60 Coactivator RUVBL1 Is a Key Regulator of Homologous Recombination

Author

Thomas L, Clarke, Maria Pilar, Sanchez-Bailon, Kelly, Chiang, John J, Reynolds, Joaquin, Herrero-Ruiz, Tiago M, Bandeiras, Pedro M, Matias, Sarah L, Maslen, J Mark, Skehel, Grant S, Stewart, and Clare C, Davies

Subjects

Protein-Arginine N-Methyltransferases, Time Factors, RUVBL1, DNA repair, Mice, Transgenic, homologous recombination, Ataxia Telangiectasia Mutated Proteins, Arginine, Transfection, Methylation, 52BP1, Genomic Instability, Lysine Acetyltransferase 5, Article, Histones, Mice, Animals, Humans, DNA Breaks, Double-Stranded, Histone Acetyltransferases, DNA Helicases, Recombinational DNA Repair, Acetylation, arginine methylation, HEK293 Cells, ATPases Associated with Diverse Cellular Activities, PRMT5, RNA Interference, Carrier Proteins, Tumor Suppressor p53-Binding Protein 1, TIP60, Protein Processing, Post-Translational, HeLa Cells

Abstract

Summary Protein post-translation modification plays an important role in regulating DNA repair; however, the role of arginine methylation in this process is poorly understood. Here we identify the arginine methyltransferase PRMT5 as a key regulator of homologous recombination (HR)-mediated double-strand break (DSB) repair, which is mediated through its ability to methylate RUVBL1, a cofactor of the TIP60 complex. We show that PRMT5 targets RUVBL1 for methylation at position R205, which facilitates TIP60-dependent mobilization of 53BP1 from DNA breaks, promoting HR. Mechanistically, we demonstrate that PRMT5-directed methylation of RUVBL1 is critically required for the acetyltransferase activity of TIP60, promoting histone H4K16 acetylation, which facilities 53BP1 displacement from DSBs. Interestingly, RUVBL1 methylation did not affect the ability of TIP60 to facilitate ATM activation. Taken together, our findings reveal the importance of PRMT5-mediated arginine methylation during DSB repair pathway choice through its ability to regulate acetylation-dependent control of 53BP1 localization., Graphical Abstract, Highlights • PRMT5 is a regulator of homologous recombination-mediated double-strand break repair • PRMT5 methylates RUVBL1 at R205, regulating TIP60-mediated histone acetylation • Loss of RUVBL1 methylation leads to 53BP1 retention at break ends • Arginine methylation crosstalks with histone acetylation to regulate repair pathway choice, Clarke et al. show that methylation of RUVBL1 by the arginine methyltransferase PRMT5 is required for homologous recombination-mediated double-strand break repair by promoting TIP60-mediated histone H4K16 acetylation. Loss of PRMT5 activity and defective RUVBL1 methylation leads to 53BP1 retention, increased sensitivity to DNA damaging agents, and genome instability.

Published

2016

241. Tip60 degradation by adenovirus relieves transcriptional repression of viral transcriptional activator EIA

Author

Ashish Gupta, David A. Ornelles, Anindya Dutta, Daniel A. Engel, and Sudhakar Jha

Subjects

Gene Expression Regulation, Viral, Cancer Research, Leupeptins, DNA damage, viruses, Repressor, Biology, Article, Lysine Acetyltransferase 5, Cell Line, EIA, Gene expression, Genetics, Adenovirus, Humans, Promoter Regions, Genetic, Molecular Biology, Gene, Histone Acetyltransferases, Regulation of gene expression, DNA replication, Epithelial Cells, Cell cycle, HCT116 Cells, Virology, Tip60, Gene Knockdown Techniques, HAT, DNA, Viral, Adenovirus E1A Proteins, Proteasome Inhibitors, Adenovirus E4 Proteins

Abstract

Adenoviruses are linear double stranded DNA viruses that infect human and rodent cell lines, occasionally transform them and cause tumors in animal models. The host cell challenges the virus in multifaceted ways to restrain viral gene expression and DNA replication, and sometimes even eliminates the infected cells by programmed cell death. To combat these challenges, adenoviruses abrogate the cellular DNA damage response pathway. Tip60 is a lysine acetyltransferase that acetylates histones and other proteins to regulate gene expression, DNA damage response, apoptosis and cell cycle regulation. Tip60 is a bona fide tumor suppressor since mice that are haploid for Tip60 are predisposed to tumors. We have discovered that Tip60 is degraded by adenovirus oncoproteins EIB55K and E4orf6 by a proteasome-mediated pathway. Tip60 binds to the immediate early adenovirus promoter and suppresses adenovirus EIA gene expression, which is a master regulator of adenovirus transcription, at least partly through retention of the virally encoded repressor pVII on this promoter. Thus degradation of Tip60 by the adenoviral early proteins is important for efficient viral early gene transcription and for changes in expression of cellular genes.

Published

2012

242. Endoplasmic Reticulum (ER) Stress Enhances Tip60 (A Histone Acetyltransferase) Binding to the Concanavalin A

Author

Sang Sun Kang, Jaesun Chun, Eun Jeoung Lee, Sung Hwa Shin, and Sunghee Hyun

Subjects

biology, Chemistry, Endoplasmic reticulum, Mutant, N-glycosylation, Cell cycle, Histone acetyltransferase, Article, General Biochemistry, Genetics and Molecular Biology, Cell biology, Histone acetyltransferase binding, Tip60, N-linked glycosylation, Biochemistry, Concanavalin A, HAT, Unfolded protein response, biology.protein, ER stress, Nuclear localization sequence

Abstract

Herein, we report that the concanavalin A binding of Tip60 (a target of the human immunodeficiency virus type 1-encoded transactivator Tat interacting protein 60 KD; a histone acetyltransferase; HAT) is enhanced as the result of endoplasmic reticulum (ER) stress. The cell expression of Tip60 combined with site-directed mutagenesis analysis was used to identify the glutamine 324 residue as the lecithin binding (Concanavalin A; Con A) site. The Tip60 N324A mutant strain, which seems to be the Con A binding-deficient, was attenuated the protein-protein interactions with FE65 and its protein stability, but its ability of G0-G1 cell cycle arrest was not interrupted. Interestingly, both HAT activity and the nuclear localization of Tip60 N324A mutant were enhanced than those of Tip60 WT. Thus, our results indicate that the Con A binding deficient of Tip60 seems to be one of the most pivotal posttranslational modifications (such as N-glycosylation) for its functional regulation signal, which is generated in response to ER stress.

Published

2012

243. TRIM29 negatively regulates p53 via inhibition of Tip60

Author

Takeshi Kondo, Tomonobu Sato, Jun Cheng, Tadasuke Tsukiyama, Takuya Sho, Takashi Saku, Shigetsugu Hatakeyama, and Masahiro Asaka

Subjects

p53, Immunoblotting, Apoptosis, medicine.disease_cause, Lysine Acetyltransferase 5, Ataxia-telangiectasia, Mice, Ubiquitin, Cell Line, Tumor, Two-Hybrid System Techniques, medicine, Animals, Humans, Immunoprecipitation, Molecular Biology, Cell Proliferation, Histone Acetyltransferases, Oncogene, biology, Cell growth, Lysine, HEK 293 cells, TRIM29, Acetylation, Cell Biology, HCT116 Cells, Molecular biology, DNA-Binding Proteins, HEK293 Cells, Tip60, Acetyltransferase, biology.protein, NIH 3T3 Cells, RNA Interference, Tumor Suppressor Protein p53, Carcinogenesis, HeLa Cells, Protein Binding, Transcription Factors

Abstract

Ataxia-telangiectasia (AT) is an autosomal recessive genetic disease characterized by immunological deficiencies, neurological degeneration, developmental abnormalities and an increased risk of cancer. Ataxia-telangiectasia group D (ATDC) was initially described as a gene related to AT. Ataxia-telangiectasia group D, also known as TRIM29, is structurally a member of the tripartite motif (TRIM) family of proteins, some of which have been reported to be highly expressed in some human carcinomas, but the involvement of TRIM29 in carcinogenesis has not been fully elucidated. In this study, we found by using yeast two-hybrid screening that TRIM29 binds to Tip60, which has been reported as a cellular acetyltransferase protein. Overexpression of TRIM29 promoted degradation and changed localization of Tip60 and reduced acetylation of p53 at lysine 120 by Tip60, resulting in enhancement of cell growth and transforming activity. In addition, we found that TRIM29 suppresses apoptosis induced by UV irradiation in HCT116 cell lines. These findings suggest that TRIM29 functions as an oncogene that promotes tumor growth.

Published

2011

244. Tip60 degradation by adenovirus relieves transcriptional repression of viral transcriptional activator EIA

Author

Gupta, A, Jha, S, Engel, D A, Ornelles, D A, and Dutta, A

Published

2013

245. Blocking H2A.Z Incorporation via Tip60 Inhibition Promotes Systems Consolidation of Fear Memory in Mice

Author

Firyal Ramzan, Amber B. Azam, Brandon J. Walters, Klotilda Narkaj, Iva B. Zovkic, Malak Wahdan, Carl Frank David Steininger, and Gilda Stefanelli

Subjects

Male, Hippocampus, Hippocampal formation, Histone Deacetylases, Lysine Acetyltransferase 5, Histones, 03 medical and health sciences, Cognition, 0302 clinical medicine, Memory, Animals, histone variants, 030304 developmental biology, 0303 health sciences, Confirmation, epigenetics, Recall, biology, Chemistry, General Neuroscience, H2A.Z, histone acetylation, Fear, General Medicine, Nucleosomes, Chromatin, Cell biology, Mice, Inbred C57BL, Thiazoles, Histone, Cognition and Behavior, Tip60, 1.6, Acetylation, Trans-Activators, biology.protein, chromatin, Memory consolidation, Histone deacetylase, 030217 neurology & neurosurgery

Abstract

Memory formation is a protracted process that initially involves the hippocampus and becomes increasingly dependent on the cortex over time, but the mechanisms of this transfer are unclear. We recently showed that hippocampal depletion of the histone variant H2A.Z enhances both recent and remote memories, but the use of virally mediated depletion reduced H2A.Z levels throughout testing, making its temporally specific function unclear. Given the lack of drugs that target histone variants, we tested existing drugs for efficacy against H2A.Z based on their targeting of known H2A.Z regulators. The Tip60 (part of H2A.Z deposition complex) inhibitor Nu9056 reduced H2A.Z binding, whereas the histone deacetylase (HDAC) inhibitor Trichostatin-A increased H2A.Z acetylation without influencing total H2A.Z in cultured hippocampal neurons. Tip60 (but not HDAC) inhibition 23 h after learning enhanced remote (tested at 7 d) and not recent (tested at 24 h) contextual fear memory in mice. In contrast, Tip60 inhibition 30 d after learning impaired recall of remote memory after 1 h, but protected the memory from further decline 24 h later. These data provide the first evidence of a delayed postlearning role for histone variants in supporting memory transfer during systems consolidation.

Published

2018

246. Amyloid-β Peptide Impact on Synaptic Function and Neuroepigenetic Gene Control Reveal New Therapeutic Strategies for Alzheimer's Disease.

Author

Karisetty BC, Bhatnagar A, Armour EM, Beaver M, Zhang H, and Elefant F

Abstract

Amyloid-β (Aβ) peptides can form protease-resistant aggregates within and outside of neurons. Accumulation of these aggregates is a hallmark of Alzheimer's disease (AD) neuropathology and contributes to devastating cognitive deficits associated with this disorder. The primary etiological factor for Aβ aggregation is either an increase in Aβ production or a decrease in its clearance. Aβ is produced by the sequential activity of β- and γ-secretase on the amyloid precursor protein (APP) and the clearance is mediated by chaperone-mediated mechanisms. The Aβ aggregates vary from soluble monomers and oligomers to insoluble senile plaques. While excess intraneuronal oligomers can transduce neurotoxic signals into neurons causing cellular defects like oxidative stress and neuroepigenetic mediated transcriptional dysregulation, extracellular senile plaques cause neurodegeneration by impairing neural membrane permeabilization and cell signaling pathways. Paradoxically, senile plaque formation is hypothesized to be an adaptive mechanism to sequester excess toxic soluble oligomers while leaving native functional Aβ levels intact. This hypothesis is strengthened by the absence of positive outcomes and side effects from immunotherapy clinical trials aimed at complete Aβ clearance, and support beneficial physiological roles for native Aβ in cellular function. Aβ has been shown to modulate synaptic transmission, consolidate memory, and protect against excitotoxicity. We discuss the current understanding of beneficial and detrimental roles for Aβ in synaptic function and epigenetic gene control and the future promising prospects of early therapeutic interventions aimed at mediating Aβ induced neuroepigenetic and synaptic dysfunctions to delay AD onset., (Copyright © 2020 Karisetty, Bhatnagar, Armour, Beaver, Zhang and Elefant.)

Published

2020

247. Nuclear Localization Is Not Required for Tip60 Tumor Suppressor Activity in Breast and Lung Cancer Cells.

Author

Ravichandran P, Davis SA, Vashishtha H, Gucwa AL, and Ginsburg DS

Subjects

Acetylation, Breast Neoplasms pathology, Cell Line, Tumor, Cytoplasm genetics, DNA Damage genetics, DNA Repair genetics, Female, Gene Expression Regulation, Neoplastic genetics, Histones genetics, Humans, Lung Neoplasms pathology, Breast Neoplasms genetics, Cell Nucleus genetics, Lung Neoplasms genetics, Lysine Acetyltransferase 5 genetics

Abstract

The Tip60 lysine acetyltransferase is a tumor suppressor in most cancers but an oncogene in prostate and gastric cancer. Tip60 is commonly found in the nucleus, where it acetylates proteins involved in transcription, DNA repair, and chromatin; however, it has also been shown to acetylate cytoplasmic targets. In this study, we investigated the relationship between Tip60 localization and breast and lung cancer. In cell fractionation experiments, cancer-derived cell lines showed a shift from nuclear to cytoplasmic endogenous Tip60 compared with cell lines derived from normal cells. With immunofluorescence, we observed four different localization patterns of overexpressed Tip60 and found that cancer cells had increased cytoplasmic localization of Tip60 compared with HEK-293 cells. The addition of a nuclear localization signal (NLS) increased the number of cells containing nuclear Tip60, whereas mutation of a putative endogenous NLS increased the number of cells with cytoplasmic Tip60. Overexpression of Tip60 increased cancer cell line sensitivity to paclitaxel regardless of changes in localization. These results suggest that dysregulation of Tip60 in breast and lung cancer is not limited to reduced expression but may also involve subcellular localization.

Published

2020

248. TIP60/P400/H4K12ac Plays a Role as a Heterochromatin Back-up Skeleton in Breast Cancer.

Author

Idrissou M, Boisnier T, Sanchez A, Khoufaf FZH, Penault-Llorca F, Bignon YJ, and Bernard-Gallon D

Subjects

Acetylation, Biomarkers, Tumor genetics, Breast Neoplasms genetics, Breast Neoplasms metabolism, Chromatin, DNA Helicases genetics, DNA-Binding Proteins genetics, Female, Heterochromatin, Histones genetics, Humans, Lysine Acetyltransferase 5 genetics, Middle Aged, Prognosis, Biomarkers, Tumor metabolism, Breast Neoplasms pathology, DNA Helicases metabolism, DNA-Binding Proteins metabolism, Gene Expression Regulation, Neoplastic, Histones metabolism, Lysine Acetyltransferase 5 metabolism

Abstract

Background/aim: In breast cancer, initiation of carcinogenesis leads to epigenetic dysregulation, which can lead for example to the loss of the heterochromatin skeleton SUV39H1/H3K9me3/HP1 or the supposed secondary skeleton TIP60/P400/H4K12ac/BRD (2/4), which allows the maintenance of chromatin integrity and plasticity. This study investigated the relationship between TIP60, P400 and H4K12ac and their implications in breast tumors., Materials and Methods: Seventy-seven patients diagnosed with breast cancer were included in this study. Chromatin immunoprecipitation (ChIP) assay was used to identify chromatin modifications. Western blot and reverse transcription and quantitative real-time PCR were used to determine protein and gene expression, respectively., Results: We verified the variation in H4K12ac enrichment and the co-localization of H4K12ac and TIP60 on the euchromatin and heterochromatin genes, respectively, by ChIP-qPCR and ChIP-reChIP, which showed an enrichment of H4K12ac on specific genes in tumors compared to the adjacent healthy tissue and a co-localization of H4K12ac with TIP60 in different breast tumor types. Furthermore, RNA and protein expression of TIP60 and P400 was investigated and overexpression of TIP60 and P400 mRNA was associated with tumor aggressiveness., Conclusion: There is a potential interaction between H4K12ac and TIP60 in heterochromatin or euchromatin in breast tumors., (Copyright© 2020, International Institute of Anticancer Research (Dr. George J. Delinasios), All rights reserved.)

Published

2020

249. Digging Deeper into Breast Cancer Epigenetics: Insights from Chemical Inhibition of Histone Acetyltransferase TIP60 In Vitro .

Author

Idrissou M, Lebert A, Boisnier T, Sanchez A, Houfaf Khoufaf FZ, Penault-Llorca F, Bignon YJ, and Bernard-Gallon D

Subjects

Binding Sites, Breast Neoplasms drug therapy, Breast Neoplasms pathology, Cell Line, Tumor, Chromatin Immunoprecipitation Sequencing, Female, Gene Expression Regulation, Neoplastic drug effects, Histone Deacetylase Inhibitors pharmacology, Histones metabolism, Humans, Lysine Acetyltransferase 5 antagonists & inhibitors, Protein Binding, Breast Neoplasms genetics, Breast Neoplasms metabolism, Epigenesis, Genetic, Epigenomics methods, Lysine Acetyltransferase 5 metabolism

Abstract

Breast cancer is often sporadic due to several factors. Among them, the deregulation of epigenetic proteins may be involved. TIP60 or KAT5 is an acetyltransferase that regulates gene transcription through the chromatin structure. This pleiotropic protein acts in several cellular pathways by acetylating proteins. RNA and protein expressions of TIP60 were shown to decrease in some breast cancer subtypes, particularly in triple-negative breast cancer (TNBC), where a low expression of TIP60 was exhibited compared with luminal subtypes. In this study, the inhibition of the residual activity of TIP60 in breast cancer cell lines was investigated by using two chemical inhibitors, TH1834 and NU9056, first on the acetylation of the specific target, lysine 4 of histone 3 (H3K4) by immunoblotting, and second, by chromatin immunoprecipitation (ChIP)-qPCR (-quantitative Polymerase Chain Reaction). Subsequently, significant decreases or a trend toward decrease of H3K4ac in the different chromatin compartments were observed. In addition, the expression of 48 human nuclear receptors was studied with TaqMan Low-Density Array in these breast cancer cell lines treated with TIP60 inhibitors. The statistical analysis allowed us to comprehensively characterize the androgen receptor and NR3C2 receptors in TNBC cell lines after TH1834 or NU9056 treatment. The understanding of the residual activity of TIP60 in the evolution of breast cancer might be a major asset in the fight against this disease, and could allow TIP60 to be used as a biomarker or therapeutic target for breast cancer progression in the future.

Published

2020

250. De Novo KAT5 Variants Cause a Syndrome with Recognizable Facial Dysmorphisms, Cerebellar Atrophy, Sleep Disturbance, and Epilepsy.

Author

Humbert J, Salian S, Makrythanasis P, Lemire G, Rousseau J, Ehresmann S, Garcia T, Alasiri R, Bottani A, Hanquinet S, Beaver E, Heeley J, Smith ACM, Berger SI, Antonarakis SE, Yang XJ, Côté J, and Campeau PM

Subjects

Abnormalities, Multiple diagnostic imaging, Abnormalities, Multiple genetics, Abnormalities, Multiple physiopathology, Adolescent, Adult, Atrophy diagnostic imaging, Atrophy physiopathology, Cerebellar Diseases diagnostic imaging, Cerebellar Diseases physiopathology, Child, Preschool, Chromatin genetics, Chromatin Assembly and Disassembly genetics, DNA Repair genetics, Epilepsy diagnostic imaging, Epilepsy genetics, Epilepsy physiopathology, Female, Heterozygote, Histones genetics, Humans, Intellectual Disability diagnostic imaging, Intellectual Disability physiopathology, Male, Mutation, Missense genetics, Protein Processing, Post-Translational genetics, Atrophy genetics, Cerebellar Diseases genetics, Intellectual Disability genetics, Lysine Acetyltransferase 5 genetics

Abstract

KAT5 encodes an essential lysine acetyltransferase, previously called TIP60, which is involved in regulating gene expression, DNA repair, chromatin remodeling, apoptosis, and cell proliferation; but it remains unclear whether variants in this gene cause a genetic disease. Here, we study three individuals with heterozygous de novo missense variants in KAT5 that affect normally invariant residues, with one at the chromodomain (p.Arg53His) and two at or near the acetyl-CoA binding site (p.Cys369Ser and p.Ser413Ala). All three individuals have cerebral malformations, seizures, global developmental delay or intellectual disability, and severe sleep disturbance. Progressive cerebellar atrophy was also noted. Histone acetylation assays with purified variant KAT5 demonstrated that the variants decrease or abolish the ability of the resulting NuA4/TIP60 multi-subunit complexes to acetylate the histone H4 tail in chromatin. Transcriptomic analysis in affected individual fibroblasts showed deregulation of multiple genes that control development. Moreover, there was also upregulated expression of PER1 (a key gene involved in circadian control) in agreement with sleep anomalies in all of the individuals. In conclusion, dominant missense KAT5 variants cause histone acetylation deficiency with transcriptional dysregulation of multiples genes, thereby leading to a neurodevelopmental syndrome with sleep disturbance, cerebellar atrophy, and facial dysmorphisms, and suggesting a recognizable syndrome., (Copyright © 2020 American Society of Human Genetics. Published by Elsevier Inc. All rights reserved.)

Published

2020