Functional Alterations of Human DNA Polymerase Delta (POL Delta) in Response to DNA Damage

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ISBN 13 :
Total Pages : 273 pages
Book Rating : 4.:/5 (664 download)

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Book Synopsis Functional Alterations of Human DNA Polymerase Delta (POL Delta) in Response to DNA Damage by : Xiao Meng

Download or read book Functional Alterations of Human DNA Polymerase Delta (POL Delta) in Response to DNA Damage written by Xiao Meng and published by . This book was released on 2010 with total page 273 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Human Dna Polymerases: Biology, Medicine And Biotechnology

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Publisher : World Scientific
ISBN 13 : 9813226420
Total Pages : 398 pages
Book Rating : 4.8/5 (132 download)

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Book Synopsis Human Dna Polymerases: Biology, Medicine And Biotechnology by : Giovanni Maga

Download or read book Human Dna Polymerases: Biology, Medicine And Biotechnology written by Giovanni Maga and published by World Scientific. This book was released on 2017-11-10 with total page 398 pages. Available in PDF, EPUB and Kindle. Book excerpt: Maintenance of the information embedded in the genomic DNA sequence is essential for life. DNA polymerases play pivotal roles in the complex processes that maintain genetic integrity. Besides their tasks in vivo, DNA polymerases are the workhorses in numerous biotechnology applications such as the polymerase chain reaction (PCR), cDNA cloning, next generation sequencing, nucleic acids based diagnostics and in techniques to analyze ancient and otherwise damaged DNA (e.g. for forensic applications). Moreover, some diseases are related to DNA polymerase defects and chemotherapy through inhibition of DNA polymerases is used to fight HIV, Herpes and Hepatitis B and C infections. This book focuses on (i) biology of DNA polymerases, (ii) medical aspects of DNA polymerases and (iii) biotechnological applications of DNA polymerases. It is intended for a wide audience from basic scientists, to diagnostic laboratories, to companies and to clinicians, who seek a better understanding and the practical use of these fascinating enzymes.

Functional Regulation of Human DNA Polymerase Delta by Phosphorylation

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ISBN 13 :
Total Pages : 158 pages
Book Rating : 4.:/5 (89 download)

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Book Synopsis Functional Regulation of Human DNA Polymerase Delta by Phosphorylation by : Amal Ali Rahmeh

Download or read book Functional Regulation of Human DNA Polymerase Delta by Phosphorylation written by Amal Ali Rahmeh and published by . This book was released on 2006 with total page 158 pages. Available in PDF, EPUB and Kindle. Book excerpt:

The Roles and Regulation of Specialized DNA Polymerases in Mitigating Replication Stress and Replicating Common Fragile Sites

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ISBN 13 :
Total Pages : pages
Book Rating : 4.:/5 (12 download)

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Book Synopsis The Roles and Regulation of Specialized DNA Polymerases in Mitigating Replication Stress and Replicating Common Fragile Sites by : Ryan Barnes

Download or read book The Roles and Regulation of Specialized DNA Polymerases in Mitigating Replication Stress and Replicating Common Fragile Sites written by Ryan Barnes and published by . This book was released on 2017 with total page pages. Available in PDF, EPUB and Kindle. Book excerpt: Replicative DNA polymerases serve as the essential enzymes that duplicate our genome with high fidelity and efficiency. This function is compromised however, when repetitive DNA sequences adopt a structure differing from the Watson-Crick B-form or during conditions of replicative stress. However, cells also possess specialized DNA polymerases that can compensate for the replicative polymerases when they are inhibited. The goals of this thesis were to investigate how the specialized DNA polymerases (Pols) eta () and kappa () 1) cooperate with the replicative polymerase delta () in the synthesis of repetitive DNA derived from chromosomal fragile sites, and 2) understand how these enzymes function during cellular replication stress. Common fragile sites (CFSs) are genomic loci that display recurrent instability in cells experiencing replication stress. Replication stress, defined as the slowing or stalling of replication forks, occurs when cells are treated with agents that inhibit DNA synthesis or are deficient in DNA repair/replication enzymes. CFSs are sensitive to replication stress, and one rationale for this is their enrichment in repetitive DNA sequences that can adopt a non-B DNA structure. Previous work in the Eckert lab has shown that all three replicative, human DNA polymerases are inhibited by repetitive CFS sequences in vitro whereas polymerases and can replicate the same sequences with high efficiency. In chapter 3, I test the hypothesis that Pols and can cooperate with Pol in CFS sequence replication in vitro. To investigate this, I developed a model of lagging strand synthesis using primed ssDNA templates containing RFC-loaded PCNA, the processivity factor of Pol . This system was designed to allow RFC and Pols , , and to function optimally in the same reaction conditions. Using this system, I found that Pols and can indeed rescue the Pol holoenzyme (Pol / RFC-loaded PCNA; Pol HE) stalled at CFS sequences containing different repetitive DNA motifs. I found this polymerase cooperativity was not mediated by PCNA however, as reactions where RFC was omitted displayed no defect in replication rescue. Moreover, using this system I did not observe any enhancement of cooperativity between Pol and Pols and using mono-ubiquitinated PCNA (Ub-PCNA), a post-translational modification thought to regulate polymerase exchange at DNA lesions. Finally, by modeling replication stress in vitro using Aph, a drug that directly inhibits replicative polymerases, I found that Pols and become indispensable for repetitive CFS sequence replication. In total, the data in this chapter advances our understanding of human DNA polymerase exchange, and how repetitive DNA replication is accomplished by multiple polymerases. While the relationship between CFS stability and Pol has been characterized by work in the Eckert lab and others, we did not know how Pol might impact the cell cycle and checkpoint signaling in replication stressed cells. To study this, I employed several models of cellular Pol deficiency and uncovered a role for Pol in G2/M phase progression during replication stress. Pol -deficient cells also display increased replication checkpoint signaling during replication stress. Interestingly, this checkpoint signaling can be suppressed in cells expressing a wild-type POLH gene, as well as a POLH gene mutated at the PCNA interaction motif, but not in cells expressing a POLH gene mutated at the ubiquitin binding domain. Moreover, analysis of Pol -deficient cells recovering from replication stress revealed a persistence of replication defects and apoptosis up to 24 hours after treatment, concomitant with reduced colony formation. This chapter reveals a global role for Pol in proper cell cycle progression during and following replication stress. After uncovering these cellular phenotypes, I began a study of Y-family polymerase expression during replication stress. In Chapter 5, I present my results showing that POLH transcript and Pol protein levels significantly increase in numerous normal and transformed cell lines using two models of replication stress. Interestingly, this induction of Pol was independent of p53 status, which has been shown to regulate Pol levels. In addition, I also observed stabilization of exogenous Pol protein and increased ubiquitination of Pol during replication stress. Among the related Y family polymerases, Pol displayed no significant induction following replication stress, and while POLK mRNA did not increase, Pol protein did increase with Aph treatment. Finally, I discovered that Pol relocalizes to chromatin and forms nuclear foci during replication stress, independent of Rad18, the primary E3 ligase of PCNA. To understand what protein/pathway may be regulating Pol during replication stress, I focused on the checkpoint kinase ATR. In this chapter I detail my results showing cell-type specific regulation of Pol by ATR during replication stress, at the level of protein expression and ubiquitination. Moreover, I show that ATR protects Pol -deficient cells from apoptotic signaling during replication stress, thereby increasing their viability. Consistent with this, Pol -deficient cells depleted of ATR had a dramatic reduction in survival in comparison to ATR-proficient cells. In total, the data presented in this chapter greatly advance our understanding of Y-family polymerase regulation outside the context of DNA damage. This data in combination with Chapter 4 demonstrably shows Y-family polymerases are an integral component of the replication stress response. In the Appendix I present my studies on A/T repeat mutagenesis. CFSs are enriched in A/T repeats, and non-B DNA structures formed by these sequences are proposed to induce CFS instability. I developed several new ex vivo reporter assays to examine mutagenesis during replication of A/T repeat rich, CFS derived sequences in human cells. Here I also detail my studies of the most recently identified DNA polymerase/primase, PrimPol. Using the Eckert labs established in vitro HSV-tk mutagenesis assay, I demonstrated for the first time that PrimPol is a highly error-prone DNA polymerase, and has a unique error signature on random, B-DNA. However, PrimPols error signature on the A/T repeats is similar to Pol s, suggesting a conserved mode of repeat replication.The work presented in this thesis advances our understanding of the roles specialized DNA polymerases have in human cells, and how these enzymes are orchestrated in the face of replication stress. Taking these results together, the findings of this thesis are biologically significant because I have elucidated the mechanism underlying the fragile chromosome phenotype of Pol -deficient cells. By generating the optimal DNA template, Pol has an essential role in completing genome duplication at difficult-to-replicate sequences and traversing the mitotic checkpoint, ensuring that cells properly enter the next cell cycle after replication stress release. The human genome is characterized by its DNA sequence complexity and high repetitive DNA content, and the presence of repetitive sequences directly impacts genome stability. I provide here a new conceptual framework, wherein specialized DNA polymerases of varied biochemical properties are essential for complete duplication of highly complex genomes, functioning in each cell division.

Physical and Functional Interaction Between the Bloom's Syndrome Helicase and Human DNA Polymerase Delta

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Publisher :
ISBN 13 :
Total Pages : 129 pages
Book Rating : 4.:/5 (637 download)

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Book Synopsis Physical and Functional Interaction Between the Bloom's Syndrome Helicase and Human DNA Polymerase Delta by : Nives Selak

Download or read book Physical and Functional Interaction Between the Bloom's Syndrome Helicase and Human DNA Polymerase Delta written by Nives Selak and published by . This book was released on 2005 with total page 129 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Post-Genomic Cardiology

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Publisher : Academic Press
ISBN 13 : 0124046428
Total Pages : 935 pages
Book Rating : 4.1/5 (24 download)

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Book Synopsis Post-Genomic Cardiology by : José Marín-García

Download or read book Post-Genomic Cardiology written by José Marín-García and published by Academic Press. This book was released on 2014-05-09 with total page 935 pages. Available in PDF, EPUB and Kindle. Book excerpt: In this second edition of Post-Genomic Cardiology, developing and new technologies such as translational genomics, next generation sequencing (NGS), bioinformatics, and systems biology in molecular cardiology are assessed in light of their therapeutic potential. As new methods of mutation screening emerge, both for the genome and for the “epigenome, comprehensive understanding of the many mutations that underlie cardiovascular diseases and adverse drug reactions is within our reach. This book, written by respected cardiologist José Marín-García, features discussion on the Hap-Map: the largest international effort to date aiming to define the differences between our individual genomes. This unique reference further reviews and investigates genome sequences from our evolutionary relatives that could help us decipher the signals of genes, and offers a comprehensive and critical evaluation of regulatory elements from the complicated network of the background DNA. Offers updated discussion of cutting-edge molecular techniques including new genomic sequencing / NGS / Hap-Map / bioinformatics / systems biology approaches Analyzes mitochondria dynamics and their role in cardiac dysfunction, up-to-date analysis of cardio-protection, and cardio-metabolic syndrome Presents recent translational studies, gene therapy, transplantation of stem cells, and pharmacological treatments in CVDs

DNA Repair and Replication

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Publisher : Academic Press
ISBN 13 : 9780120342693
Total Pages : 368 pages
Book Rating : 4.3/5 (426 download)

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Book Synopsis DNA Repair and Replication by :

Download or read book DNA Repair and Replication written by and published by Academic Press. This book was released on 2004-12-23 with total page 368 pages. Available in PDF, EPUB and Kindle. Book excerpt: DNA Repair and Replication contains an up-to-date review of general principles of DNA replication and an overview of the multiple pathways involved in DNA repair. Specific DNA repair pathways, including base-excision repair, light-dependent direct reversal of UV-damage, nucleotide-excision repair, transcription-coupled repair, double-strand break repair, and mismatch repair, are each discussed in separate chapters. Selected Contents: Base Excision Repair Eukaryotic DNA Mismatch Repair Double Strand Break Repair Functions of DNA Polymerases Somatic Hypermutation: A Mutational Panacea

Reconstitution and Characterization of Human DNA Polymerase Delta Four Subunit Holoenzyme and Proteomic Analysis of DNA Polymerase Delta Complex

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ISBN 13 :
Total Pages : 162 pages
Book Rating : 4.:/5 (192 download)

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Book Synopsis Reconstitution and Characterization of Human DNA Polymerase Delta Four Subunit Holoenzyme and Proteomic Analysis of DNA Polymerase Delta Complex by : Nayef Ali Mazloum

Download or read book Reconstitution and Characterization of Human DNA Polymerase Delta Four Subunit Holoenzyme and Proteomic Analysis of DNA Polymerase Delta Complex written by Nayef Ali Mazloum and published by . This book was released on 2002 with total page 162 pages. Available in PDF, EPUB and Kindle. Book excerpt:

Tracking of Progressing Human DNA Polymerase Holoenzymes Reveals Distributions of DNA Lesion Bypass Activities

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ISBN 13 :
Total Pages : 0 pages
Book Rating : 4.:/5 (138 download)

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Book Synopsis Tracking of Progressing Human DNA Polymerase Holoenzymes Reveals Distributions of DNA Lesion Bypass Activities by : Joseph Cardina

Download or read book Tracking of Progressing Human DNA Polymerase Holoenzymes Reveals Distributions of DNA Lesion Bypass Activities written by Joseph Cardina and published by . This book was released on 2023 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt: In lagging strand DNA synthesis, DNA polymerase [delta] (pol [delta]) holoenzymes composed of pol [delta] and the proliferating cell nuclear antigen (PCNA) sliding clamp perform high fidelity DNA synthesis with little error. The pol [delta] holoenzyme occasionally encounters structural deformities in the native DNA sequence called DNA lesions. Upon encountering these lesions, it was previously believed that pol [delta] would stall on the DNA template at some point before the lesion launching a DNA damage tolerance (DDT) pathway to replicate the lesion and remaining DNA before allowing pol [delta] to resume its typical high fidelity DNA synthesis. Recent literature within the past 20 years or so has challenged this perspective by showing human pol [delta] can replicate various DNA lesions. These studies have questioned the role that DDT plays in lagging strand DNA synthesis upon encounter of a DNA lesion, thus providing a need for further analysis. As a result, we aimed to quantitatively characterize the encounters of pol [delta] with several biologically relevant DNA lesions at physiological conditions. Our results show that pol [delta] supports dNTP incorporation while inserting across from, extending from, and elongating past several different DNA lesions, and the exact extent of these values is dependent on the exonuclease activity of pol [delta] and the identity of the lesion itself. We also found that of the pol [delta] that dissociates upon encountering the lesion, the dissociation events are unevenly distributed around the lesion with different distributions depending on the lesion. Our findings show that lagging strand DNA synthesis is more complex than previously thought while advancing our understanding of the role of DDT in lagging strand DNA synthesis.

Molecular Biology of The Cell

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Publisher :
ISBN 13 : 9780815332183
Total Pages : 0 pages
Book Rating : 4.3/5 (321 download)

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Book Synopsis Molecular Biology of The Cell by : Bruce Alberts

Download or read book Molecular Biology of The Cell written by Bruce Alberts and published by . This book was released on 2002 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt:

G-Quadruplexes and Inflammation

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ISBN 13 :
Total Pages : 0 pages
Book Rating : 4.:/5 (142 download)

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Book Synopsis G-Quadruplexes and Inflammation by : MaryElizabeth Stein

Download or read book G-Quadruplexes and Inflammation written by MaryElizabeth Stein and published by . This book was released on 2023 with total page 0 pages. Available in PDF, EPUB and Kindle. Book excerpt: Accurate and efficient genome duplication is necessary to preserve genome stability. Two factors that challenge the genome are repetitive sequences that form secondary DNA structures (non-B DNA) and chronic inflammatory features like oxidative stress. Defects in replication mechanisms and/or repair pathways to resolve these blocks can lead to stalled replication forks, increased mutagenesis, DNA breaks, and, ultimately, genome instability. Therefore, DNA polymerase recruitment, in coordination with DNA repair, is critical in the cellular response to non-B DNA and oxidative stress. Importantly, specialized polymerase recruitment is implicated in overcoming stalling at and synthesizing through non-B DNA and oxidative DNA lesions. My dissertation looks at contributions by these determinants to genome instability independently: (1) the impact to DNA polymerase fidelity by one type of non-B DNA, G-quadruplexes (G4s) and (2) gene expression changes of two specialized DNA polymerases and histological disease activity in chronically inflamed tissues. G4s are evolutionarily conserved and function in a wide variety of cellular processes. G4s can also compromise genome integrity and are sources of small- and large-scale mutagenesis. However, the precise impact of G4s on human DNA polymerase fidelity that contributes to this mutagenesis is not known. I used an in vitro forward mutation assay to investigate the fidelity of human replicative DNA polymerase delta (pol [delta]) and specialized polymerases kappa ([kappa]) and eta ([eta]) during synthesis of G4 motifs that differ in sequence, topology, and stability. I observed both small (e.g., frameshifts) and large (e.g., deletion of the G4 and part of the flanking sequence) polymerase errors within and surrounding the G4s. These errors were dependent on the polymerase, G4 topology and stability. Notably, the frequency of large-scale errors increased in substrates containing G4 motifs with parallel strands. Pol [eta] errors occurred in the 3' sequences flanking the stable, parallel G4 motifs, whereas pol [kappa] errors were frameshifts within the G-tracts of these stable G4 motifs. In silico analysis showed that most polymerase errors are predicted to maintain the G4 structure, and pol [kappa] may better maintain a stable, parallel G4 compared to pol [eta]. Both pol [eta] and [kappa] can also facilitate the bypass of oxidative DNA lesions. However, the roles of these polymerases in inflammatory diseases remain undefined. Wide-spread tissue damage due to oxidative stress, including alterations in DNA, proteins, and lipids, has been demonstrated in mouse models and patient colonic biopsies of inflammatory bowel disease (IBD). Using ulcerative colitis (UC), a form of IBD, as a chronic inflammatory disease model, I retrospectively assessed three groups of non-cancerous colon tissues: (1) UC + high grade dysplasia (HGD)/cancer (Progressors), (2) UC with no HGD/cancer (Nonprogressors), and (3) healthy Controls. In this discovery phase study, I measured pol [eta] gene (POLH) and pol [kappa] gene (POLK) expression in RNA isolated from frozen tissues of two to three colon regions per patient. Microscopic inflammation was evaluated by pathologists in formalin-fixed, paraffin embedded tissues from each patient using a histological index, the Geboes score. Importantly, I found context-dependent differential expression of POLH and POLK genes. POLH expression was upregulated in UC tissues compared to Controls, independent of inflammation severity, whereas POLK expression was downregulated in tissues with active inflammation. I determined distinct disease activity differences between Progressor and Nonprogressor colon tissues, where more Progressor tissues had chronically inactive disease. Differences in histological inflammation suggest that underlying molecular differences may distinguish between UC patient groups. Taken together, my work expands on our understanding of how G4s and chronic inflammation can challenge genome integrity. G4 motif heterogeneity differentially impacts DNA polymerase fidelity, creating mutational hotspots. Histological assessment of disease activity in UC colon tissues underscores important changes induced by microscopic inflammation. Importantly, further studies are needed to determine the mechanisms of pol [eta] and pol [kappa], which may function differently at sites of G4s and oxidative damage.

Biomedical Index to PHS-supported Research

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ISBN 13 :
Total Pages : 1108 pages
Book Rating : 4.:/5 (319 download)

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Book Synopsis Biomedical Index to PHS-supported Research by :

Download or read book Biomedical Index to PHS-supported Research written by and published by . This book was released on 1988 with total page 1108 pages. Available in PDF, EPUB and Kindle. Book excerpt:

DNA Replication

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Publisher : Springer
ISBN 13 : 9811069557
Total Pages : 581 pages
Book Rating : 4.8/5 (11 download)

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Book Synopsis DNA Replication by : Hisao Masai

Download or read book DNA Replication written by Hisao Masai and published by Springer. This book was released on 2018-01-22 with total page 581 pages. Available in PDF, EPUB and Kindle. Book excerpt: This book reviews the latest trends and future directions of DNA replication research. The contents reflect upon the principles that have been established through the genetic and enzymatic studies of bacterial, viral, and cellular replication during the past decades. The book begins with a historical overview of the studies on eukaryotic DNA replication by Professor Thomas Kelly, a pioneer of the field. The following chapters include genome-wide studies of replication origins and initiation factor binding, as well as the timing of DNA replications, mechanisms of initiation, DNA chain elongation and termination of DNA replication, the structural basis of functions of protein complexes responsible for execution of DNA replication, cell cycle-dependent regulation of DNA replication, the nature of replication stress and cells’ strategy to deal with the stress, and finally how all these phenomena are interconnected to genome instability and development of various diseases. By reviewing the existing concepts ranging from the old principles to the newest ideas, the book gives readers an opportunity to learn how the classical replication principles are now being modified and new concepts are being generated to explain how genome DNA replication is achieved with such high adaptability and plasticity. With the development of new methods including cryoelectron microscopy analyses of huge protein complexes, single molecular analyses of initiation and elongation of DNA replication, and total reconstitution of eukaryotic DNA replication with purified factors, the field is enjoying one of its most exciting moments, and this highly timely book conveys that excitement to all interested readers.

New Research Directions in DNA Repair

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Publisher : BoD – Books on Demand
ISBN 13 : 9535111140
Total Pages : 676 pages
Book Rating : 4.5/5 (351 download)

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Book Synopsis New Research Directions in DNA Repair by : Clark Chen

Download or read book New Research Directions in DNA Repair written by Clark Chen and published by BoD – Books on Demand. This book was released on 2013-05-22 with total page 676 pages. Available in PDF, EPUB and Kindle. Book excerpt: This book is intended for students and scientists working in the field of DNA repair. Select topics are presented here to illustrate novel concepts in DNA repair, the cross-talks between DNA repair and other fundamental cellular processes, and clinical translational efforts based on paradigms established in DNA repair. The book should serve as a supplementary text in courses and seminars as well as a general reference for biologists with an interest in DNA repair.

Health Risks from Exposure to Low Levels of Ionizing Radiation

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Publisher : National Academies Press
ISBN 13 : 0309133343
Total Pages : 422 pages
Book Rating : 4.3/5 (91 download)

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Book Synopsis Health Risks from Exposure to Low Levels of Ionizing Radiation by : Committee to Assess Health Risks from Exposure to Low Levels of Ionizing Radiation

Download or read book Health Risks from Exposure to Low Levels of Ionizing Radiation written by Committee to Assess Health Risks from Exposure to Low Levels of Ionizing Radiation and published by National Academies Press. This book was released on 2006-03-23 with total page 422 pages. Available in PDF, EPUB and Kindle. Book excerpt: This book is the seventh in a series of titles from the National Research Council that addresses the effects of exposure to low dose LET (Linear Energy Transfer) ionizing radiation and human health. Updating information previously presented in the 1990 publication, Health Effects of Exposure to Low Levels of Ionizing Radiation: BEIR V, this book draws upon new data in both epidemiologic and experimental research. Ionizing radiation arises from both natural and man-made sources and at very high doses can produce damaging effects in human tissue that can be evident within days after exposure. However, it is the low-dose exposures that are the focus of this book. So-called “late” effects, such as cancer, are produced many years after the initial exposure. This book is among the first of its kind to include detailed risk estimates for cancer incidence in addition to cancer mortality. BEIR VII offers a full review of the available biological, biophysical, and epidemiological literature since the last BEIR report on the subject and develops the most up-to-date and comprehensive risk estimates for cancer and other health effects from exposure to low-level ionizing radiation.

Chemically-Induced DNA Damage, Mutagenesis, and Cancer

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Publisher : MDPI
ISBN 13 : 3038971294
Total Pages : 275 pages
Book Rating : 4.0/5 (389 download)

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Book Synopsis Chemically-Induced DNA Damage, Mutagenesis, and Cancer by : Ashis K. Basu

Download or read book Chemically-Induced DNA Damage, Mutagenesis, and Cancer written by Ashis K. Basu and published by MDPI. This book was released on 2018-08-27 with total page 275 pages. Available in PDF, EPUB and Kindle. Book excerpt: This book is a printed edition of the Special Issue " Chemically-Induced DNA Damage, Mutagenesis, and Cancer" that was published in IJMS

DNA Repair and Mutagenesis

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Publisher : American Society for Microbiology Press
ISBN 13 : 1555813194
Total Pages : 2587 pages
Book Rating : 4.5/5 (558 download)

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Book Synopsis DNA Repair and Mutagenesis by : Errol C. Friedberg

Download or read book DNA Repair and Mutagenesis written by Errol C. Friedberg and published by American Society for Microbiology Press. This book was released on 2005-11-22 with total page 2587 pages. Available in PDF, EPUB and Kindle. Book excerpt: An essential resource for all scientists researching cellular responses to DNA damage. • Introduces important new material reflective of the major changes and developments that have occurred in the field over the last decade. • Discussed the field within a strong historical framework, and all aspects of biological responses to DNA damage are detailed. • Provides information on covering sources and consequences of DNA damage; correcting altered bases in DNA: DNA repair; DNA damage tolerance and mutagenesis; regulatory responses to DNA damage in eukaryotes; and disease states associated with defective biological responses to DNA damage.