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By amplifying cell death signals, scientists make precancerous cells self-destruct
August 18, 2008When a cell begins to multiply in a dangerously abnormal way, a series of death signals trigger it to self-destruct before it turns cancerous. Now, in research to appear in the August 15 issue of Genes & Development, Rockefeller University scientists have figured out a way in mice to amplify the signals that tell these precancerous cells to die. The trick: Inactivating a protein that normally helps cells to avoid self-destruction.
The work, led by Hermann Steller, Strang Professor and head of the Laboratory of Apoptosis and Cancer Biology, is the first to reveal the mechanism by which a class of proteins called IAPs regulates cell death. By exposing the mechanism in a living animal, the finding also marks a breakthrough in the field and opens the door for developing a new class of drugs that could aid in cancer therapy and prevention.
"In a way, these mice are guiding clinical trials," says Steller, who is also a Howard Hughes Medical Institute investigator. "We now can study how IAPs contribute to the development of cancer in a living animal and develop drugs to prevent or thwart the disease."
IAP stands for "inhibitor of apoptosis protein," and these proteins do exactly what their name implies. By inhibiting apoptosis, or programmed cell death, they keep cells alive by directly binding to executioner enzymes called caspases. But until now, precisely how IAPs save cells from death has remained unclear.
With graduate student Andrew Schile and postdoc Maria Garcia-Fernandez, Steller studied the X-linked inhibitor of apoptosis protein, or XIAP, and the role of its largely ignored RING domain, which has been implicated in promoting cell death as well as survival. Steller, Schile and Garcia-Fernandez found that genetically targeting and removing RING affected only some cell types in healthy mice. And even though the mice without the RING had more cell death than the mice with the RING, both lived normal lives under normal laboratory conditions.
But when the scientists compared mice that were genetically predisposed to developing cancer, they found that those without the RING lived twice as long as those with it.
"Cancer cells thrive by disabling the molecular machinery that tells sick cells to die," says Steller. "By removing the RING, we wanted to see whether we would trick the machinery to turn back on. And that's what happened. Cells die more readily, making it much more difficult for cancer to be established."
Steller and his team specifically showed that the RING transfers molecular tags on caspases that label these enzymes for destruction. The more tags, the stronger the signal to save the cell from death. However, when the RING is removed, fewer molecular tags are transferred to caspases and often, the signal to save the cell from death is not strong enough. So, more cells die.
The game is not over. Several distinct IAP genes are known to exist, but which ones are important in the development of cancer has also stymied researchers. "We need to use genetics to sort out which individual IAPs contribute to tumors and which IAPS we need to target in order to cure cancer," says Steller. "This was a very big step in understanding what role IAPs play in cancer, but it isn't the last."
The Rockefeller University
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Means to and End: Apoptosis and Other Cell Death Mechanisms by Douglas R Green (Editor) Apoptosis (programmed cell death) plays a critical role in development, normal physiology, and many diseases, including cancer. Apoptosis researchers form a distinct research community but investigators in many areas of cell, developmental, and molecular biology, as well as immunology and neurobiology, also study the process. This short book describes our detailed understanding of the mechanisms involved in apoptotic signaling and execution, covering signal transducers, caspases, BCL-2family proteins, mitochondrial molecules, and IAPs. It also critically discusses key questions that remain in the field, for example, whether caspases are always necessary, the distinction between the intrinsic and extrinsic pathways of apoptosis, and the role of mitochondria, that are often glossed over or... |
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Cell Death (Encyclopedia of Life Sciences) by Gerry Melino (Editor), David Vaux (Editor) This book on cell death contains 29 self-contained, peer-reviewed articles written by leading scientists in each field. It features overview articles aimed at undergraduates and non-specialists, which present basic information and provide entry into the following advanced articles. These advanced articles are written for postgraduate students and research workers, containing detailed information and key references allowing the reader to investigate a specific area in more depth. The book is an essential resource for educational purposes as well as a reference work for experienced researchers in the field. The articles will also be available electronically as part of the acclaimed Encyclopedia of Life Sciences (ELS).Key features:Provides a comprehensive overview on the research of... |
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Cell 2455, Death Row: A Condemned Man's Own Story by Caryl Chessman (Author), Joseph Longstreth (Introduction) In June 1948, 27-year-old petty criminal Caryl Chessman was sentenced in California on two counts of sexual assault, receiving two death sentences as punishment in a case that remains one of the most baffling episodes in American legal history. Maintaining his innocence of these crimes, Chessman lived in Cell 2455, a four-by-ten foot space on Death Row in San Quentin for the twelve years between his sentencing and eventual execution. He spent this time, punctuated by eight separate stays of execution, writing this memoir — a moving and pitiless account of his life in crime and the early life that produced it. Chessman's clarity of mind and ability to bring his thoughts directly to the page, even within the stifling walls of San Quentin, help make this work the most literate and... |
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CELLULAR AGING: CELL DEATH: An entry from Macmillan Reference USA's Encyclopedia of Aging by RICHARD A. LOCKSHIN (Author), ZAHRA ZAKERI (Author) As the Baby Boomers head toward retirement, the four-volume “Encyclopedia of Aging” offers a timely resource encompassing all aspects of aging. Covering a variety of disciplines—biology, medicine, economics, law, psychology, sociology and history—the Encyclopedia also explores related issues such as religion, spirituality, and ethics. | |
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Road Map for LC-MS, Antioxidant Activity, Total Phenolic Content, Toxicity and Anticancer Activity (Cell Cycle, Cell Death) Analysis for Natural Products Roadmap For Researchers Full Test Procedures for Antioxidant Activity, Total Phenolic Content, Toxicity and Anticancer Activity (Cell Cycle, Cell Death) Analysis for olive leaf. Full Data Analysis for Each Test. Method Development for LC-MS Quantification of Phenolic, Flavonoidic and Triterpenic Compounds, Chromatographic Condetions are Provided. |
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Dead Man's Cell Phone by Sarah Ruhl (Author) “Satire is her oxygen. . . . In her new oddball comedy, Dead Man’s Cell Phone, Sarah Ruhl is forever vital in her lyrical and biting takes on how we behave.”—The Washington Post“Ruhl’s zany probe of the razor-thin line between life and death delivers a fresh and humorous look at the times we live in.”—Variety“Sarah Ruhl is deliriously imaginative and fearless in her choice of subject matter. She is an original.”—Molly Smith, artistic director, Arena StageAn incessantly ringing cell phone in a quiet café. A stranger at the next table who has had enough. And a dead man—with a lot of loose ends. So begins Dead Man’s Cell Phone, a wildly imaginative new comedy by playwright Sarah Ruhl, recipient of a MacArthur “Genius” Grant and Pulitzer Prize finalist for her... |
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The Biology of Death: Origins of Mortality (Comstock Books) by Andre Klarsfeld (Author), Frederic Revah (Author), Lydia Brady (Translator) Why do we die? Do all living creatures share this fate? Is the body's slow degradation with the passage of time unavoidable, or can the secrets of longevity be unlocked? Over the past two decades, scientists studying the workings of genes and cells have uncovered some of the clues necessary to solve these mysteries. In this fascinating and accessible book, two neurobiologists share the often-surprising findings from that research, including the possibility that aging and natural death may not be forever a certainty for most living beings. André Klarsfeld and Frédéric Revah discuss in detail the latest scientific findings and views on death and longevity. They challenge many popular assumptions, such as the idea that the death of individual organisms serves to rejuvenate species or... |
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When Cells Die: A Comprehensive Evaluation of Apoptosis and Programmed Cell Death by Richard A. Lockshin (Editor), Zahra Zakeri (Editor), Jonathan L. Tilly (Editor) When Cells Die A Comprehensive Evaluation of Apoptosis and Programmed Cell Death Edited by Richard A. Lockshin, Zahra Zakeri, and Jonathan L. Tilly Cell death is fast becoming one of the most dynamic areas of biological research -involving as it does the study of apoptosis and programmed cell death and the role these phenomena play in development and homeostasis on the one hand, and aging and disease on the other. The profound implications for medicine and agriculture from the manipulation of these processes have spawned a deluge of research papers, articles, approaches, and methods -making it difficult for scientists to get an overview of the field. When Cells Die establishes a coherent framework for the study of cell death -cutting across viewpoints and... |
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Cell Death in Mammalian Ovary by Gerardo H. Vázquez-Nin (Author), María Luisa Escobar (Author), M. De Felici (Author), Olga Margarita Echeverría (Author), Francesca Gioia Klinger (Author) The ovary is a suitable organ for studying the processes of cell death. Cell death was first described in the rabbit ovary (Graaffian follicles), the phenomenon being called ‘chromatolysis’. To date, it is recognized that various forms of cell death (programmed cell death, apoptosis and autophagy) are essential components of ovarian development and function. Programmed cell death is responsable for the ovarian endowment of primordial follicles around birth; in the prepuberal and adult period, apoptosis is a basic mechanism by which oocytes are eliminated by cancer therapies and environmental toxicants; in the ovarian cycle, follicular atresia and luteal regression involve follicular cell apoptosis. Finally, abnormalities in cell death processes may lead to ovarian disease such as... |
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When Cells Die II: A Comprehensive Evaluation of Apoptosis and Programmed Cell Death by Richard A. Lockshin (Editor), Zahra Zakeri (Editor) Cell death is fast becoming one of the most dynamic areas of biological research-involving as it does the study of apoptosis and programmed cell death and the role these phenomena play in development and homeostasis on the one hand, and aging and disease on the other. The profound implications for medicine and agriculture from the manipulation of these processes have spawned a deluge of research papers, articles, approaches, and methods-making it difficult for scientists to get an overview of the field. When Cells Die II: A Comprehensive Evaluation of Apoptosis and Programmed Cell Death offers the most thorough, cutting-edge coverage of this field since publication of the acclaimed first edition. Leading international researchers present an up-to-date yet accessible survey ranging from... |
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