Elucidation Of Chromatin Remodeling Machinery Involved In Regulation Of Estrogen Receptor Alpha Expression In Human Breast Cancer Cells

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Elucidation of Chromatin Remodeling Machinery Involved in Regulation of Estrogen Receptor Alpha Expression in Human Breast Cancer Cells

Author :
Publisher :
ISBN 13 :
Total Pages : 30 pages
Book Rating : 4.:/5 (742 download)

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Book Synopsis Elucidation of Chromatin Remodeling Machinery Involved in Regulation of Estrogen Receptor Alpha Expression in Human Breast Cancer Cells by :

Download or read book Elucidation of Chromatin Remodeling Machinery Involved in Regulation of Estrogen Receptor Alpha Expression in Human Breast Cancer Cells written by and published by . This book was released on 2005 with total page 30 pages. Available in PDF, EPUB and Kindle. Book excerpt: Estrogen receptor alpha (ER) is an epigenetically regulated gene. Inhibitors of DNA methyltransferases (DNMT) and histone deacetylases (HDAC) synergistically activate the methylated ER gene promoter in ER negative MDA-MB-23 1 human breast cancer cells. Using chromatin immunoprecipitation (ChIP), we examined the chromatin status and repressor complex associated with silenced ER and changes in the key regulatory factors during reactivation by inhibitors of DNMT (5-aza-2'deoxycytidine or 5-aza-dC) and HDAC (trichostatin A or TSA). The silencing of ER due to CpG hyperrnethylation correlates with binding of specific methyl-binding proteins, DNA methyltransferases and HDAC proteins. Inhibition of HDAC activity by TSA results in the increased accumulation of hyperacetylated core histones. The activation of ER gene expression by 5aza-dC also involves the release of the repressor complex involving various methyl binding proteins, DNMTs, and HDACl. HDAC and DNMT inhibitors also modulated histone methylation at H3-K9 and H3-K4 to fonn a more open chromatin structure. Together our results impart a befter understanding of molecular mechanisms of chromatin remodeling during ER reactivation by DNMT and HDAC inhibitors.

Integrative Approach to Targeting Chromatin Remodeling in Breast Cancer Therapy

Author : Shamim Mollah
Publisher :
ISBN 13 :
Total Pages : 143 pages
Book Rating : 4.:/5 (111 download)

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Book Synopsis Integrative Approach to Targeting Chromatin Remodeling in Breast Cancer Therapy by : Shamim Mollah

Download or read book Integrative Approach to Targeting Chromatin Remodeling in Breast Cancer Therapy written by Shamim Mollah and published by . This book was released on 2019 with total page 143 pages. Available in PDF, EPUB and Kindle. Book excerpt: With the advent of high-throughput technologies, large-scale multi-omics data integration approaches have revolutionized our understanding of cancer and its progression. In this dissertation, we focus on deciphering the molecular mechanisms of various targeted cancer treatments and growth factors on chromatin remodeling through integrative analyses of multi-omics data. Chromatin remodeling is involved in the stability of genome structure, gene expression, and DNA repair, as well as, cell growth and progression; therefore, it plays an essential role in tumor suppression. The regulation of chromatin remodeling is carried out by the precise coordination of covalent histone modifications and remodeler proteins through catalytic activities. Disruption of these regulated activities confers a unique ability for healthy cells to reprogram their genome for the maintenance of oncogenic phenotypes. Hence, these histone modifications and remodeler proteins are potential targets for cancer treatments. While many drugs have the potential to target histone modifications and remodeler proteins, their precise mechanisms of action, i.e., alterations in cellular reprogramming, are not well studied. To address this gap, we utilized latent space models to integrate multi-omics data such as proteomic/phosphoproteomic, transcriptomic, and epigenomic data to understand the effects of various drugs and growth factors on specific genes, proteins, and phosphoproteins that are involved in the regulation of a wide range of cellular processes (growth, proliferation, and cell division) and gene activity states in cancer and healthy cell lines. In addition to providing mechanistically-driven targets that can impact chromatin remodeling, the chromatin fingerprints generated from our study can serve as a signature for assessing the efficacy of a given drug in treating cancer. Further, increasing evidence, supported by our study of breast cancer, indicates that this paradigm applies to various cancers, and further analysis can provide insights into more detailed chromatin-based mechanisms. Our study implies that the cancer state is one where chromatin gets remodeled, and effective drugs attempt to restore the chromatin state to that of a healthy cell. Overall, the integrative frameworks we developed reveal the mechanisms of action of specific drugs on chromatin remodeling machinery in breast cancer cells and of growth factors on cellular phenotypes in normal breast cells, which lay the foundation for improved development of chromatin-based cancer therapy.

Epigenetic Basis for the Regulation of Estrogen Receptor Alpha Activity in Breast Cancer Cells

Author :
Publisher :
ISBN 13 :
Total Pages : 47 pages
Book Rating : 4.:/5 (69 download)

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Book Synopsis Epigenetic Basis for the Regulation of Estrogen Receptor Alpha Activity in Breast Cancer Cells by :

Download or read book Epigenetic Basis for the Regulation of Estrogen Receptor Alpha Activity in Breast Cancer Cells written by and published by . This book was released on 2009 with total page 47 pages. Available in PDF, EPUB and Kindle. Book excerpt: A key factor involved in breast cancer development and progression is the estrogen receptor alpha (ER). Genome-wide computational studies on ER have identified over 70,000 putative Estrogen Response Elements (EREs) in the human genome. However, a genome-wide functional study using ChIP-Chip, has indicated that less than 1/10 of all putative ER binding sites are recognized by the receptor following estrogen stimulation in breast cancer cells. Through genome-wide positional analyses, we demonstrate that ER recruitment is dependent on a specific epigenetic signature characterized by mono and dimethylation of lysine 4 on histone 3 (H3K4me1/me2). Furthermore the pioneer factor FoxA1 translates this epigenetic signature into changes in chromatin structure in a cell type-specific manner for transcription factors, such as ER. Hence, this allows for the establishment of lineage-specific transcriptional enhancers and programs.

Chromatin Remodelling

Author : Danuta Radzioch
Publisher : BoD – Books on Demand
ISBN 13 : 953511087X
Total Pages : 237 pages
Book Rating : 4.5/5 (351 download)

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Book Synopsis Chromatin Remodelling by : Danuta Radzioch

Download or read book Chromatin Remodelling written by Danuta Radzioch and published by BoD – Books on Demand. This book was released on 2013-04-17 with total page 237 pages. Available in PDF, EPUB and Kindle. Book excerpt: The term "chromatin remodelling" is widely used to describe changes in chromatin structure which is controlled by histone-modifying enzymes, chromatin remodelling complexes, non-histone DNA-binding proteins and noncoding RNAs. Many human diseases such as cancer, various genetic syndromes, autism and infectious disease have been linked to the disruption of these control processes by genetic, environmental or microbial factors. Therefore, to unravel the mechanisms by which they operate is one of the most exciting and rapid developing fields of modern biology and will contribute to new ways in treatment of these diseases. The chapters in this book will focus on recent advances in our understanding of the mechanisms that govern the dynamic structural of chromatin, thereby providing important insights into gene regulation, DNA repair, and human diseases.

Chromatin Remodeling Complexes and Transcriptional Coregulators

Author :
Publisher : Elsevier
ISBN 13 : 0443160074
Total Pages : 208 pages
Book Rating : 4.4/5 (431 download)

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Book Synopsis Chromatin Remodeling Complexes and Transcriptional Coregulators by :

Download or read book Chromatin Remodeling Complexes and Transcriptional Coregulators written by and published by Elsevier. This book was released on 2023-10 with total page 208 pages. Available in PDF, EPUB and Kindle. Book excerpt: Chromatin Remodeling Complexes and Transcriptional Coregulators, Volume 53, the latest release in The Enzymes series highlights new advances in the field, with interesting new chapters that cover Perspectives on Chromatin Remodeling, The functions of ISWI-type remodelers in yeast, Conserved mechanisms of NuRD function in hematopoietic gene expression, The SIN3 complex as a metabolic epigenetic regulator, Soft repression and chromatin modification by conserved transcriptional corepressors, The NPAC-LSD2 complex in nucleosome demethylation, Role of intrinsically disordered domains in transcriptional regulation, and Regulation of the Recovery of Cancer from Therapy Exposure by Noncoding RNAs.

Cross-modulatory Actions of Cell Cycle Machinery on Estrogen Receptor-alpha Level and Transcriptional Activity in Breast Cancer Cells

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Author : Shweta Bhatt
Publisher :
ISBN 13 :
Total Pages : pages
Book Rating : 4.:/5 (776 download)

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Book Synopsis Cross-modulatory Actions of Cell Cycle Machinery on Estrogen Receptor-alpha Level and Transcriptional Activity in Breast Cancer Cells by : Shweta Bhatt

Download or read book Cross-modulatory Actions of Cell Cycle Machinery on Estrogen Receptor-alpha Level and Transcriptional Activity in Breast Cancer Cells written by Shweta Bhatt and published by . This book was released on 2010 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt:

The Role of Histone Variant H2A.Z in the Regulation of Gene Expression in Breast Cancer Cells

Author : Luca Bellucci
Publisher :
ISBN 13 :
Total Pages : 123 pages
Book Rating : 4.:/5 (868 download)

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Book Synopsis The Role of Histone Variant H2A.Z in the Regulation of Gene Expression in Breast Cancer Cells by : Luca Bellucci

Download or read book The Role of Histone Variant H2A.Z in the Regulation of Gene Expression in Breast Cancer Cells written by Luca Bellucci and published by . This book was released on 2013 with total page 123 pages. Available in PDF, EPUB and Kindle. Book excerpt: During my PhD, I studied the mechanisms of regulation of gene expression in breast cancer. In particular, I was interested in the epigenetic regulation of p21 gene expression in an estrogen receptor negative breast cancer cells (MDA-MB231 cells). We found that in these cells a TSA treatment stimulated p21 expression and increased acetylation of H2A.Z present at the p21 promoter. H2A.Z was strongly associated with the transcription start site of p21. Moreover, depleting the cellular pool of H2A.Z compromised p21 activation and response to HDACi. Acetylation of H2A.Z rather than its association of regulatory element per se was important for p21 expression. My studies led to a publication (Bellucci et al., 2013 [1]) which shows that p21 gene activation in MDA-MB231 cells is p53-independent and controlled by the H2A.Z histone variant and its acetylation. Normally, activation of p21 expression can be p53-independent or dependent, according to the cell system used. But the mechanism behind p21 activation, via HDACi, remains poorly understood. Moreover, p21 regulation depends on the binding of the histone variant H2A.Z. Using the Cyclin D1 gene as a model, I also participated in a project, which shows how, in this case too, H2A.Z acetylation is critical for gene regulation in estrogen receptor positive and negative breast cancer cells. We identified the enzymes involved in H2A.Z acetylation (Tip60) and in chromatin remodeling (Tip48), to propose a model for transcription activation of this gene.

Regulation of E2F-1 Gene Expression in Human Breast Cancer Cells

Author : Sharon Khethiwe Ngwenya
Publisher :
ISBN 13 :
Total Pages : pages
Book Rating : 4.:/5 (621 download)

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Book Synopsis Regulation of E2F-1 Gene Expression in Human Breast Cancer Cells by : Sharon Khethiwe Ngwenya

Download or read book Regulation of E2F-1 Gene Expression in Human Breast Cancer Cells written by Sharon Khethiwe Ngwenya and published by . This book was released on 2005 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: 17[beta]-Estradiol induces E2F-1 gene expression in ZR-75 and MCF-7 human breast cancer cells. Analysis of the E2F-1 gene promoter in MCF-7 cells previously showed that hormone-induced transactivation required interactions between estrogen receptor [alpha] (ER[alpha])/Sp1 bound to upstream GC-rich sites and NFYA bound to downstream CCAAT sites within the -169 to -54 promoter region. This promoter region was also E2-responsive in ER[alpha]-positive ZR-75 cells; however, further analysis of the promoter showed that cooperative ER[alpha]/Sp1/NFY interactions were not necessary for hormone-inducedtransactivation in ZR-75 cells. The upstream GC-rich motifs are activated independently by ER[alpha]/Sp1 in ZR-75 but not MCF-7 cells, and the downstream CCAAT sites were also E2-responsive. E2 also induced reporter gene activity in ZR-75 cells transfected with an expression plasmid containing the yeast GAL4 DNA binding domain fused to pM-NFYA and a construct containing five tandem GAL4 response elements. Subsequent studies showed that hormonal activation of pE2F-1j[subscript]m1 and pM-NFYA are dependent on non-genomic pathways in which E2 activates cAMP/protein kinase A. Hormone-dependent regulation of E2F-1gene expression in ZR-75 and MCF-7 involves different mechanisms, demonstrating the importance of cell context on transactivation pathways, even among ER-positive breast cancer cell lines. TCDD inhibited ER[alpha]-mediated responses in MCF-7 and ZR-75 cells. E2-induced E2F-1protein and mRNA levels in MCF-7 and ZR-75 cells and this response was inhibited by TCDD. Constructs containing GC-rich sites alone orin combination with the downstream NFY sites were used in transactivation studies to investigate the mechanism of inhibitory AhR-ER[alpha] crosstalk. AlthoughTCDD inhibited E2-induced mRNA, protein and reporter gene actitivity, it was not possible to determine if the inhibitory response was due to limiting ER[alpha]protein levels due to proteasome degradation since proteaome inhibitors aloneblocke hormone-dependent responses. TCDD also inhibited the cAMP/PKApathway by inhibiting adenyl cyclase activity. In Drosophila SL-2 cells cotransfected with the GC-rich -169 to -54 region, ER[alpha] and Sp1 plasmids E2 induced transactivation in cells cotransfected with AhR/Arnt expression plasmids suggesting that the AhR complex suppressed ER[alpha]/Sp1 action. These results demonstrate that TCDD inhibits E2-dependent activation of both non-genomic and genomic pathways of ER-mediated E2F-1 gene expression.

Epigenetic Regulation by Estrogen Receptor in Breast Cancer Cells

Author : Athéna Sklias
Publisher :
ISBN 13 :
Total Pages : 0 pages
Book Rating : 4.:/5 (112 download)

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Book Synopsis Epigenetic Regulation by Estrogen Receptor in Breast Cancer Cells by : Athéna Sklias

Download or read book Epigenetic Regulation by Estrogen Receptor in Breast Cancer Cells written by Athéna Sklias and published by . This book was released on 2019 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt: Previous epidemiological and experimental studies have strongly implicated estrogens in breast cancer risk and Estrogen Receptor (ER), the transcription factor to which estrogen binds, is considered as the major molecular driver of around 70% breast cancers. The importance of the deregulated estrogen signalling is further highlighted by increasing evidence that current chemopreventive and therapeutic strategies that target hormonally responsive breast cancers frequently result in the development of resistance to anti-estrogens and metastatic progression, highlighting the need for understanding the molecular underlying mechanisms. While until recently, ER was believed to act as a stand-alone transcription factor, which can directly bind its motifs in DNA, it is now accepted that ER activity is a complex and dynamic process that requires highly concerted actions of a dozen transcriptional cofactors and various chromatin regulators at DNA. Recent studies focused on characterising ER-associated cofactors and their role in opening the chromatin provided a remarkable insight into transcriptional regulation mediated by ER. However DNA methylation and histone acetylation are poorly understood in the context of ER's dynamic binding. In this thesis, I combined a cell culture protocol adapted for studying estradiol (E2) deprivation and re-stimulation in stricto sensu in ER-positive breast cancer cells with the latest methylation array, that allowed a genome-wide interrogation of DNA methylation (including a comprehensive panel of enhancers). I further investigated histone acetylation (ChIP-seq) and transcriptome (RNA-seq) after E2 deprivation and re-stimulation to better characterise the ability of ER to coordinate gene regulation. I found that E2 deprivation and re-stimulation result in time-dependent DNA methylation changes and in histone acetylation across diverse genomic regions, many of which overlap with enhancers. Further enrichment analysis of transcription factor (TF) binding and motif occurrence highlights the importance of ER tethering mainly through two partner TF families, AP-1 and FOX, in the proximity of enhancers that are differentially methylated and acetylated. This is the first study that comprehensively characterized DNA methylation at enhancers in response to inhibition and activation of ER signalling. The transcriptome and genome occupancy data further reinforced the notion that ER activity may orchestrate a broad transcriptional programme through regulating a limited panel of critical enhancers. Finally, the E2 re-stimulation experiments revealed that although the majority of the observed epigenetic changes induced by E2 deprivation could be largely reversed when the cells were re-stimulated we show that DNA hypermethylation and H3K27 acetylation at enhancers as well as several gene expression changes are selectively retained. The partial reversibility can be interpreted as a sign of treatment efficiency but also as a mechanism by which ER activity may contribute to endocrine resistance. This study provides entirely new information that constitutes a major advance in our understanding of the events by which ER and its cofactors mediate changes in DNA methylation and chromatin states at enhancers. These findings should open new avenues for studying role of the deregulated estrogen signalling in the mechanism underlying the “roots” of endocrine resistance that commonly develops in response to anti-estrogen therapy.

Mechanisms Underlying the Pharmacologic Reversal of Genetic and Epigenetic Components of Tumor Suppressor Gene Silencing in Human Breast Cancer

Download Mechanisms Underlying the Pharmacologic Reversal of Genetic and Epigenetic Components of Tumor Suppressor Gene Silencing in Human Breast Cancer PDF Online Free

Author :
Publisher :
ISBN 13 :
Total Pages : 352 pages
Book Rating : 4.:/5 (137 download)

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Book Synopsis Mechanisms Underlying the Pharmacologic Reversal of Genetic and Epigenetic Components of Tumor Suppressor Gene Silencing in Human Breast Cancer by :

Download or read book Mechanisms Underlying the Pharmacologic Reversal of Genetic and Epigenetic Components of Tumor Suppressor Gene Silencing in Human Breast Cancer written by and published by . This book was released on 2006 with total page 352 pages. Available in PDF, EPUB and Kindle. Book excerpt: In women, tumors of the breast remain the most frequently diagnosed malignancy and the second leading cause of cancer-related deaths. One of the hallmarks of carcinogenesis is the abnormal silencing of tumor supprsssor genes by both genetic and epigenetic alterations, leading to defects in cell-cycle control, DNA repair, apoptosis and cell adhesion. This dissertation focuses on the elucidation of the genetic and epigenetic mechanisms associated with tumor suppressor gene silencing in human epithelial breast tumor cells, and the development of pharmacologic strategies aimed at reversing these types of repression through gene therapy and chromatin remodeling. Desmocollin 3 (DSC3) and MASPIN are anti-metastatic tumor suppressor genes that are silenced in a large percentage of breast tumors via aberrant DNA hypermethylation and histone hypoacetylation of their promoters. DSC3 and MASPIN are also p53-target genes, requiring its transcriptional activation to promote normal expression levels, yet a significant fraction of breast tumor cell lines express mutant forms of p53. Adenoviral-mediated re-introduction of wild type (wt) p53 into mutant p53-expressing breast tumor cells resulted in significant up-regulation of DSC3 and MASPIN expression, although not to the levels seen in normal breast epithelial cells. Mechanistically, the addition of wt p53 to these tumor cells resulted in increased histone acetylation and enhanced chromatin accessibility of the DSC3 and MASPIN promoters, despite continued cytosine hypermethylation. Pre-treatment with the DNA methyltransferase inhibitor 5-aza-2'-deoxycytidine (5-aza-CdR) prior to wt p53 addition produced synergistic reactivation of both DSC3 and MASPIN in breast cancer cells, approaching their levelsin normal mammary cells. However, 5-aza-CdR did not significantly reduce DNA methylation in many cases as originally theorized. Therefore, follow-up studies focused on the identification of alternative, novel mechanisms of 5-aza-CdR-mediated induction of epigenetically silenced genes, finding that it consistently reduced transcriptionally repressive histone H3 lysine 9 (K9) methylation levels in the promoter regions of both DSC3 and MASPIN in breast tumor cells, by mediating global decreases in the histone H3 K9 methyltransferase, G9A. In summary, these results clearly show that cancer treatments targeting both genetic and epigenetic facets of gene regulation may be a useful strategy towards the therapeutic transcriptional reprogramming of cancer cells.

Grainyhead-like Protein 2 Regulates the Transcriptional Activity of Estrogen Receptor Alpha Phosphorylated at Serine 118 in Breast Cancer

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Author : Rebecca M. Reese
Publisher :
ISBN 13 :
Total Pages : 0 pages
Book Rating : 4.:/5 (137 download)

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Book Synopsis Grainyhead-like Protein 2 Regulates the Transcriptional Activity of Estrogen Receptor Alpha Phosphorylated at Serine 118 in Breast Cancer by : Rebecca M. Reese

Download or read book Grainyhead-like Protein 2 Regulates the Transcriptional Activity of Estrogen Receptor Alpha Phosphorylated at Serine 118 in Breast Cancer written by Rebecca M. Reese and published by . This book was released on 2022 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt: The Grainyhead-like protein family, composed of GRHL1, GRHL2, and GRHL3, are nuclear transcription factors that regulate epithelial differentiation. GRHL2 is characterized as having oncogenic and tumor suppressive roles across many cancers. GRHL2 is also associated with several nuclear hormone receptors, including progesterone receptor (PR), androgen receptor (AR), and more recently, estrogen receptor (ER). ER is expressed in over 70% of breast cancers and is a major therapeutic target. GRHL2 is more highly expressed in ER-positive over ER-negative breast cancers, and studies suggest that GRHL2 modulates ER recruitment to chromatin. GRHL2 is hypothesized to enhance ER-transcriptional activity by recruiting histone modifiers like MLL3 to enhancers, but it can also repress ER-transcriptional activity by suppressing the catalytic activity of the histone acetyltransferase p300. Our group found a specific association of the GRHL2 motif with ER phosphorylated at serine 118 (pS118-ER), a post-translational modification activated by estrogen (E2) that is required for maximal ER-transcriptional activity. As a whole, the mechanisms by which GRHL2 regulates ER-transcriptional activity and, more specifically, pS118-ER transcriptional activity are not well understood. In the work presented here, I take cistromic and transcriptomic approaches to explore the role of GRHL2 in facilitating pS118-ER recruitment to chromatin and downstream transcriptional activity. I find that GRHL2 is critical for maximal pS118-ER chromatin-recruitment, GRHL2 can both enhance and antagonize E2-mediated pS118-ER transcriptional activity, and ER/GRHL2 co-regulated genes are involved in cellular migration. The dual roles of GRHL2 in pS118-ER transcriptional regulation may be due to the pioneering activities of GRHL2 which allow the factor to promote an open chromatin structure and subsequently recruit or modulate coregulators present at a given locus. I also explore the function of a portion of the poorly defined GRHL2 transactivation domain and find a 52 amino acid portion of the domain is important for GRHL2 transactivation activity. These studies further our understanding of the function of GRHL2 in regulating pS118-ER transcriptional activity in breast cancer and provide a basis for future studies to expand our knowledge of the interaction between these two transcription factors.

Genome Wide Analyses of Transcriptional Regulation Mediated by Estrogen Receptor Alpha in Human Breast Cancer Cell Line MCF-7

Author : Wei Sun
Publisher :
ISBN 13 :
Total Pages : 97 pages
Book Rating : 4.:/5 (86 download)

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Book Synopsis Genome Wide Analyses of Transcriptional Regulation Mediated by Estrogen Receptor Alpha in Human Breast Cancer Cell Line MCF-7 by : Wei Sun

Download or read book Genome Wide Analyses of Transcriptional Regulation Mediated by Estrogen Receptor Alpha in Human Breast Cancer Cell Line MCF-7 written by Wei Sun and published by . This book was released on 2012 with total page 97 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Estrogen and Retinoid Regulation of DNA Repair in Breast Cancer

Author :
Publisher :
ISBN 13 :
Total Pages : 10 pages
Book Rating : 4.:/5 (742 download)

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Book Synopsis Estrogen and Retinoid Regulation of DNA Repair in Breast Cancer by :

Download or read book Estrogen and Retinoid Regulation of DNA Repair in Breast Cancer written by and published by . This book was released on 2003 with total page 10 pages. Available in PDF, EPUB and Kindle. Book excerpt: Chemotherapeutic agents used in the treatment breast cancer produce their cytotoxic effects by creating DNA damage. Estrogen (ER) and retinoic acid receptors (RAR) are members of a family of ligand dependent transcription factors. ER, RAR, and BRCAl require CREB binding protein (CBP) to activate target gene transcription. The application proposed a new mechanism by which ER and RAR regulate BRCAl mediated DNA repair via CBP. In the second year of the project, we determined that RARalpha overexpression in ER negative breast cancer cell lines enhances the deleterious effects of RA on DNA damage induced apoptosis. Treatment with the DNA methyltransferase inhibitor ADC failed to induce additional BRCAl expression in BR negative breast cancer cell lines. A novel BRCAl mutant protein repressed expression of a number of double strand break repair proteins in the Rad and XRCC groups. However, both T47D and MDA-MBA68 clones expressing the novel BRCAl mutant protein were more resistant to the effects of etoposide treatment These results may be due to the pronounced cell cycle inhibitory effect of the BRCAl mutant protein, thereby rendering the slower dividing cells less sensitive to the topoisomerase inhibitor.

Genome Stability

Author : Igor Kovalchuk
Publisher : Academic Press
ISBN 13 : 0323856802
Total Pages : 762 pages
Book Rating : 4.3/5 (238 download)

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Book Synopsis Genome Stability by : Igor Kovalchuk

Download or read book Genome Stability written by Igor Kovalchuk and published by Academic Press. This book was released on 2021-07-17 with total page 762 pages. Available in PDF, EPUB and Kindle. Book excerpt: Genome Stability: From Virus to Human Application, Second Edition, a volume in the Translational Epigenetics series, explores how various species maintain genome stability and genome diversification in response to environmental factors. Here, across thirty-eight chapters, leading researchers provide a deep analysis of genome stability in DNA/RNA viruses, prokaryotes, single cell eukaryotes, lower multicellular eukaryotes, and mammals, examining how epigenetic factors contribute to genome stability and how these species pass memories of encounters to progeny. Topics also include major DNA repair mechanisms, the role of chromatin in genome stability, human diseases associated with genome instability, and genome stability in response to aging. This second edition has been fully revised to address evolving research trends, including CRISPRs/Cas9 genome editing; conventional versus transgenic genome instability; breeding and genetic diseases associated with abnormal DNA repair; RNA and extrachromosomal DNA; cloning, stem cells, and embryo development; programmed genome instability; and conserved and divergent features of repair. This volume is an essential resource for geneticists, epigeneticists, and molecular biologists who are looking to gain a deeper understanding of this rapidly expanding field, and can also be of great use to advanced students who are looking to gain additional expertise in genome stability. - A deep analysis of genome stability research from various kingdoms, including epigenetics and transgenerational effects - Provides comprehensive coverage of mechanisms utilized by different organisms to maintain genomic stability - Contains applications of genome instability research and outcomes for human disease - Features all-new chapters on evolving areas of genome stability research, including CRISPRs/Cas9 genome editing, RNA and extrachromosomal DNA, programmed genome instability, and conserved and divergent features of repair

Breast Cancer

Author : Phuc Van Pham
Publisher : BoD – Books on Demand
ISBN 13 : 9535129996
Total Pages : 570 pages
Book Rating : 4.5/5 (351 download)

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Book Synopsis Breast Cancer by : Phuc Van Pham

Download or read book Breast Cancer written by Phuc Van Pham and published by BoD – Books on Demand. This book was released on 2017-04-05 with total page 570 pages. Available in PDF, EPUB and Kindle. Book excerpt: Breast Cancer - From Biology to Medicine thoroughly examines breast cancer from basic definitions, to cellular and molecular biology, to diagnosis and treatment. This book also has some additional focus on preclinical and clinical results in diagnosis and treatment of breast cancer. The book begins with introduction on epidemiology and pathophysiology of breast cancer in Section 1. In Section 2, the subsequent chapters introduce molecular and cellular biology of breast cancer with some particular signaling pathways, the gene expression, as well as the gene methylation and genomic imprinting, especially the existence of breast cancer stem cells. In Section 3, some new diagnostic methods and updated therapies from surgery, chemotherapy, hormone therapy, immunotherapy, radiotherapy, and some complementary therapies are discussed. This book provides a succinct yet comprehensive overview of breast cancer for advanced students, graduate students, and researchers as well as those working with breast cancer in a clinical setting.

Handbook of Nutrition, Diet, and Epigenetics

Author : Vinood B. Patel
Publisher : Springer
ISBN 13 : 9783319555294
Total Pages : 0 pages
Book Rating : 4.5/5 (552 download)

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Book Synopsis Handbook of Nutrition, Diet, and Epigenetics by : Vinood B. Patel

Download or read book Handbook of Nutrition, Diet, and Epigenetics written by Vinood B. Patel and published by Springer. This book was released on 2019-02-27 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt: This multivolume reference work addresses the fact that the well being of humankind is predicated not only on individuals receiving adequate nutrition but also on their genetic makeup. The work includes more than 100 chapters organized in the following major sections: Introduction and Overview; Epigenetics of Organs and Diseases in Relation to Diet and Nutrition; Detailed Processes in Epigenetics of Diet and Nutrition; Modulating Epigenetics with Diet and Nutrition; and Practical Techniques. While it is well known that genes may encode proteins responsible for structural and dynamic components, there is an increasing body of evidence to suggest that nutrition itself may alter the way in which genes are expressed via the process of epigenetics. This is where chemically imposed alteration in the DNA sequence occurs or where the functional expression of DNA is modulated. This may include changes in DNA methylation, non-coding RNA, chromatin, histone acetylation or methylation, and genomic imprinting. Knowledge regarding the number of dietary components that impact on epigenetic processes is increasing almost daily. Marshalling all the information on the complex relationships between diet, nutrition, and epigenetic processes is somewhat difficult due to the wide myriad of material. It is for this reason that the present work has been compiled.

Diagnosis and Management of Ovarian Disorders

Author : Albert Altchek
Publisher : Elsevier
ISBN 13 : 008049451X
Total Pages : 595 pages
Book Rating : 4.0/5 (84 download)

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Book Synopsis Diagnosis and Management of Ovarian Disorders by : Albert Altchek

Download or read book Diagnosis and Management of Ovarian Disorders written by Albert Altchek and published by Elsevier. This book was released on 2003-09-04 with total page 595 pages. Available in PDF, EPUB and Kindle. Book excerpt: This updated second edition of Diagnosis and Management of Ovarian Disorders provides thorough, yet succinct insight into the ever-changing realm of ovarian disorders. It presents a novel multidisciplinary approach to the subject as described by clinicians, surgeons, pathologists, basic scientists and related medical researchers. Topics covered include reproductive technology, early diagnosis of ovarian cancer, and management of menopause among others. The breadth of information provided by this book will appeal to clinicians and researchers involved in the study and treatment of ovarian disorders.KEY FEATURES* Includes updated information on early diagnosis of ovarian cancer* Reviews new diagnostic techniques for ovarian disorders* Discusses latest information on reproductive technology* Presents translational treatment linking laboratory research with clinical medicine