Methionine Dependence of Cancer and Aging

Methionine Dependence of Cancer and Aging
Author: Robert M. Hoffman
Publisher: Humana
Total Pages: 0
Release: 2019-02-07
Genre: Medical
ISBN: 9781493987955

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This book explores the methionine dependence of cancer and its effects on aging, a great story of science that is not widely known. The chapters in this book describe the discovery of methionine dependence of cancer; the molecular basis for the increased methionine demand of cancer cells and tumors; the clinical application of methionine dependence of cancer in PET imaging with [11C]methionine; the development of methioninases as cancer drugs; the anti-aging and anti-diabetes effects of methionine restriction; and the future of targeting methionine in the body for the elimination of cancer and for the extension of a healthy life-span. Written in the highly successful Methods in Molecular Biology series format, chapters include introductions to their respective topics, lists of the necessary materials and reagents, step-by-step, readily reproducible laboratory protocols, and tips on troubleshooting and avoiding known pitfalls. Cutting-edge and thorough, Methionine Dependence of Cancer and Aging: Methods and Protocols is an important resource for researchers and scientists wishing to pursue this exciting and vital area of study."

Methionine Metabolism and Cell Cycle Control

Methionine Metabolism and Cell Cycle Control
Author: Stacey Borrego
Publisher:
Total Pages: 134
Release: 2016
Genre:
ISBN: 9781369227796

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The majority of cancer cells have a unique metabolic addiction to methionine in contrast to normal cells. This "methionine-dependent" phenotype describes the inability of cancer cells to proliferate in methionine stress conditions, where methionine has been replaced with its metabolic precursor, homocysteine, in the growth media. Methionine-dependence is implicated as a signature of cancer and upon spontaneous reversion to a methionine-independent phenotype, cells lose anchorage independent growth, a hallmark of tumorigenicity. Comparing methionine-dependent and -independent cell lines is critical for a clear interpretation of our results as we investigate the molecular mechanisms behind methionine-dependence and malignancy. For this purpose, we use the methionine-dependent, triple negative, breast cancer cell line MDA-MB-468 and derived a methionine-independent variant, MDA-MB-468res-R8. With this breast cancer cell pair we are able to compare cancer and normal-like cells due to their similar genetic backgrounds, proliferation rates, and media requirements.Previous studies on methionine-dependence identified a reduction in the synthesis of S-adenosylmethionine (SAM) during methionine stress. SAM is the principal methyl donor in the cell and, interestingly, cancer cells have been shown to have higher methylation activity as compared to normal cells. Therefore, the studies presented in this thesis focus on the early response to methionine stress and how the resultant decrease in SAM is communicated throughout the cell. We used mass spectroscopy methods to understand the metabolic response to methionine stress in both cell lines over a 24 hour period. We observed methionine stress induced oxidative stress in both cell types resulting in a redirection of homocysteine metabolism toward synthesis of the antioxidant glutathione. Additionally, lipidomic analyses indicated a complete reprogramming of lipid synthesis in the methionine-dependent cell line that may be caused by irreversible oxidative damage and limited SAM availability for the synthesis of SAM-dependent lipids such as phospho- and sphingolipids.To further understand how SAM levels are communicated to initiate a cellular response for protection of cell integrity, we focused on SAM as a co-factor for substrate methylation. SAM is a universal methyl donor and can serve as a co-factor for protein, lipid, chromatin, and RNA methylation events. Particularly, we focus on mRNA 5' cap methylation and it's influence on protein translation as a possible mechanism to communicate SAM levels. We employed both human cell lines and yeast strains to develop a methyl cap purification method for use in high-throughput RNA sequencing and have thus far identified unique, gene-specific responses to SAM depletion in regards to methyl cap stability. Continuing our efforts to fully understand this unique, metabolic requirement of cancer will allow us to shed light on an undefined molecular area essential for the development and use for cancer therapeutics in methionine-dependent cancers.

How Tobacco Smoke Causes Disease

How Tobacco Smoke Causes Disease
Author: United States. Public Health Service. Office of the Surgeon General
Publisher:
Total Pages: 728
Release: 2010
Genre: Government publications
ISBN:

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This report considers the biological and behavioral mechanisms that may underlie the pathogenicity of tobacco smoke. Many Surgeon General's reports have considered research findings on mechanisms in assessing the biological plausibility of associations observed in epidemiologic studies. Mechanisms of disease are important because they may provide plausibility, which is one of the guideline criteria for assessing evidence on causation. This report specifically reviews the evidence on the potential mechanisms by which smoking causes diseases and considers whether a mechanism is likely to be operative in the production of human disease by tobacco smoke. This evidence is relevant to understanding how smoking causes disease, to identifying those who may be particularly susceptible, and to assessing the potential risks of tobacco products.

Epigenetics of Aging

Epigenetics of Aging
Author: Trygve O. Tollefsbol
Publisher: Springer Science & Business Media
Total Pages: 462
Release: 2009-11-11
Genre: Medical
ISBN: 1441906398

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Recent studies have indicated that epigenetic processes may play a major role in both cellular and organismal aging. These epigenetic processes include not only DNA methylation and histone modifications, but also extend to many other epigenetic mediators such as the polycomb group proteins, chromosomal position effects, and noncoding RNA. The topics of this book range from fundamental changes in DNA methylation in aging to the most recent research on intervention into epigenetic modifications to modulate the aging process. The major topics of epigenetics and aging covered in this book are: 1) DNA methylation and histone modifications in aging; 2) Other epigenetic processes and aging; 3) Impact of epigenetics on aging; 4) Epigenetics of age-related diseases; 5) Epigenetic interventions and aging: and 6) Future directions in epigenetic aging research. The most studied of epigenetic processes, DNA methylation, has been associated with cellular aging and aging of organisms for many years. It is now apparent that both global and gene-specific alterations occur not only in DNA methylation during aging, but also in several histone alterations. Many epigenetic alterations can have an impact on aging processes such as stem cell aging, control of telomerase, modifications of telomeres, and epigenetic drift can impact the aging process as evident in the recent studies of aging monozygotic twins. Numerous age-related diseases are affected by epigenetic mechanisms. For example, recent studies have shown that DNA methylation is altered in Alzheimer’s disease and autoimmunity. Other prevalent diseases that have been associated with age-related epigenetic changes include cancer and diabetes. Paternal age and epigenetic changes appear to have an effect on schizophrenia and epigenetic silencing has been associated with several of the progeroid syndromes of premature aging. Moreover, the impact of dietary or drug intervention into epigenetic processes as they affect normal aging or age-related diseases is becoming increasingly feasible.

The Heterogeneity of Cancer Metabolism

The Heterogeneity of Cancer Metabolism
Author: Anne Le
Publisher: Springer
Total Pages: 186
Release: 2018-06-26
Genre: Medical
ISBN: 331977736X

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Genetic alterations in cancer, in addition to being the fundamental drivers of tumorigenesis, can give rise to a variety of metabolic adaptations that allow cancer cells to survive and proliferate in diverse tumor microenvironments. This metabolic flexibility is different from normal cellular metabolic processes and leads to heterogeneity in cancer metabolism within the same cancer type or even within the same tumor. In this book, we delve into the complexity and diversity of cancer metabolism, and highlight how understanding the heterogeneity of cancer metabolism is fundamental to the development of effective metabolism-based therapeutic strategies. Deciphering how cancer cells utilize various nutrient resources will enable clinicians and researchers to pair specific chemotherapeutic agents with patients who are most likely to respond with positive outcomes, allowing for more cost-effective and personalized cancer therapeutic strategies.

Long-lived Proteins in Human Aging and Disease

Long-lived Proteins in Human Aging and Disease
Author: Roger J. W. Truscott
Publisher: John Wiley & Sons
Total Pages: 224
Release: 2021-04-19
Genre: Science
ISBN: 3527347283

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This authoritative overview on an emerging topic in the molecular life sciences covers all aspects of the aging of (long-lived) proteins. It describes the molecular mechanisms of aging on the protein level, in particular the most common side chain modifications and includes analytical methods to study protein half-life and the accumulation of modifications. Finally, the impact of protein aging on several age-related disases in humans is dissected, and their role in limiting human lifespan is discussed.

Geriatric Oncology

Geriatric Oncology
Author: Martine Extermann
Publisher: Springer
Total Pages: 1150
Release: 2020-01-30
Genre: Medical
ISBN: 9783319574141

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This book is intended as a comprehensive resource for clinicians and researchers seeking in-depth information on geriatric oncology. The coverage encompasses epidemiology, the biology and (patho)physiology of aging and cancer, geriatric assessment and management, hematologic malignancies, solid tumors, issues in patient care, and research methods. Since cancer is a disease of aging and people are living longer, most cancer patients are now aged 70 and older. Yet the more we age, the more diverse we become in terms of our health, biologic fitness, and cancer behavior. Typically, however, general oncology clinical trials address only a selected healthier and younger population of patients. Geriatric oncology is the area of oncology that addresses these issues but while a wealth of knowledge has been accumulated, information is often difficult to retrieve or insufficiently detailed. The SpringerReference program, in which this book is published, offers an ideal format for overcoming these limitations since it combines thorough coverage with access to living editions constantly updated chapter by chapter via a dynamic peer-review process, ensuring that information remains current and pertinent.

Cancer as a Metabolic Disease

Cancer as a Metabolic Disease
Author: Thomas Seyfried
Publisher: John Wiley & Sons
Total Pages: 482
Release: 2012-05-18
Genre: Science
ISBN: 1118310306

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The book addresses controversies related to the origins of cancer and provides solutions to cancer management and prevention. It expands upon Otto Warburg's well-known theory that all cancer is a disease of energy metabolism. However, Warburg did not link his theory to the "hallmarks of cancer" and thus his theory was discredited. This book aims to provide evidence, through case studies, that cancer is primarily a metabolic disease requring metabolic solutions for its management and prevention. Support for this position is derived from critical assessment of current cancer theories. Brain cancer case studies are presented as a proof of principle for metabolic solutions to disease management, but similarities are drawn to other types of cancer, including breast and colon, due to the same cellular mutations that they demonstrate.

Protein Oxidation and Aging

Protein Oxidation and Aging
Author: Tilman Grune
Publisher: John Wiley & Sons
Total Pages: 0
Release: 2013-01-04
Genre: Science
ISBN: 9780470878286

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Reviews our current understanding of the role of protein oxidation in aging and age-related diseases Protein oxidation is at the core of the aging process. Setting forth a variety of new methods and approaches, this book helps researchers conveniently by exploring the aging process and developing more effective therapies to prevent or treat age-related diseases. There have been many studies dedicated to the relationship between protein oxidation and age-related pathology; now it is possible for researchers and readers to learn new techniques as utilizing protein oxidation products as biomarkers for aging. Protein Oxidation and Aging begins with a description of the tremendous variety of protein oxidation products. Furthermore, it covers: Major aspects of the protein oxidation process Cellular mechanisms for managing oxidized proteins Role of protein oxidation in aging Influence of genetic and environmental factors on protein oxidation Measuring protein oxidation in the aging process Protein oxidation in age-related diseases References at the end of each chapter serve as a gateway to the growing body of original research studies and reviews in the field.

Nutrient Metabolism

Nutrient Metabolism
Author: Martin Kohlmeier
Publisher: Elsevier
Total Pages: 841
Release: 2003-10-01
Genre: Medical
ISBN: 0080537898

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Nutrient Metabolism defines the molecular fate of nutrients and other dietary compounds in humans, as well as outlining the molecular basis of processes supporting nutrition, such as chemical sensing and appetite control. It focuses on the presentation of nutritional biochemistry; and the reader is given a clear and specific perspective on the events that control utilization of dietary compounds. Slightly over 100 self-contained chapters cover all essential and important nutrients as well as many other dietary compounds with relevance for human health. An essential read for healthcare professionals and researchers in all areas of health and nutrition who want to access the wealth of nutrition knowledge available today in one single source. Key Features * Highly illustrated with relevant chemical structures and metabolic pathways * Foreword by Steven Zeisel, Editor-in-chief of the Journal of Nutritional Biochemistry * First comprehensive work on the subject