Your search keyword '"Edward Fielder"' showing total 16 results

1. Short senolytic or senostatic interventions rescue progression of radiation-induced frailty and premature ageing in mice

Author

Edward Fielder, Tengfei Wan, Ghazaleh Alimohammadiha, Abbas Ishaq, Evon Low, B Melanie Weigand, George Kelly, Craig Parker, Brigid Griffin, Diana Jurk, Viktor I Korolchuk, Thomas von Zglinicki, and Satomi Miwa

Subjects

ageing, senescence, senolytic, metformin, frailty, Medicine, Science, Biology (General), QH301-705.5

Abstract

Cancer survivors suffer from progressive frailty, multimorbidity, and premature morbidity. We hypothesise that therapy-induced senescence and senescence progression via bystander effects are significant causes of this premature ageing phenotype. Accordingly, the study addresses the question whether a short anti-senescence intervention is able to block progression of radiation-induced frailty and disability in a pre-clinical setting. Male mice were sublethally irradiated at 5 months of age and treated (or not) with either a senolytic drug (Navitoclax or dasatinib + quercetin) for 10 days or with the senostatic metformin for 10 weeks. Follow-up was for 1 year. Treatments commencing within a month after irradiation effectively reduced frailty progression (p

Published

2022

2. Temporal inhibition of autophagy reveals segmental reversal of ageing with increased cancer risk

Author

Liam D. Cassidy, Andrew R. J. Young, Christopher N. J. Young, Elizabeth J. Soilleux, Edward Fielder, Bettina M. Weigand, Anthony Lagnado, Rebecca Brais, Nicholas T. Ktistakis, Kimberley A. Wiggins, Katerina Pyrillou, Murray C. H. Clarke, Diana Jurk, Joao F. Passos, and Masashi Narita

Subjects

Science

Abstract

Autophagy declines with age, yet it is unclear if restoration of autophagy extends lifespan. Here, the authors demonstrate in murine models that the inhibition of Atg5 induces ageing phenotypes and reduces lifespan, whilst autophagy restoration partially reverses these phenotypes with accelerated tumorigenesis.

Published

2020

3. Senolytics and senostatics as adjuvant tumour therapy

Author

Susan Short, Edward Fielder, Satomi Miwa, and Thomas von Zglinicki

Subjects

Medicine, Medicine (General), R5-920

Abstract

Cell senescence is a driver of ageing, frailty, age-associated disease and functional decline. In oncology, tumour cell senescence may contribute to the effect of adjuvant therapies, as it blocks tumour growth. However, this is frequently incomplete, and tumour cells that recover from senescence may gain a more stem-like state with increased proliferative potential. This might be exaggerated by the induction of senescence in the surrounding niche cells. Finally, senescence will spread through bystander effects, possibly overwhelming the capacity of the immune system to ablate senescent cells. This induces a persistent system-wide senescent cell accumulation, which we hypothesize is the cause for the premature frailty, multi-morbidity and increased mortality in cancer survivors.Senolytics, drugs that selectively kill senescent cells, have been developed recently and have been proposed as second-line adjuvant tumour therapy. Similarly, by blocking accelerated senescence following therapy, senolytics might prevent and potentially even revert premature frailty in cancer survivors.Adjuvant senostatic interventions, which suppress senescence-associated bystander signalling, might also have therapeutic potential. This becomes pertinent because treatments that are senostatic in vitro (e.g. dietary restriction mimetics) persistently reduce numbers of senescent cells in vivo, i.e. act as net senolytics in immunocompetent hosts. Keywords: Cancer, Glioma, Senolytics, Senostatics, Therapy, Survivor

Published

2019

4. Author response: Short senolytic or senostatic interventions rescue progression of radiation-induced frailty and premature ageing in mice

Author

Tengfei Wan, Edward Fielder, Ghazaleh Alimohammadiha, Abbas Ishaq, Evon Low, B Melanie Weigand, George Kelly, Craig Parker, Brigid Griffin, Diana Jurk, Viktor I Korolchuk, Thomas von Zglinicki, and Satomi Miwa

Published

2022

5. Temporal inhibition of autophagy reveals segmental reversal of ageing with increased cancer risk

Author

João F. Passos, Anthony B. Lagnado, Elizabeth J. Soilleux, Katerina Pyrillou, Rebecca Brais, Nicholas T. Ktistakis, Liam D. Cassidy, Diana Jurk, Bettina M. Weigand, Masashi Narita, Murray C.H. Clarke, Kimberley A. Wiggins, Edward Fielder, Andrew R. J. Young, Christopher N. J. Young, Cassidy, Liam D [0000-0002-9312-6256], Young, Christopher N J [0000-0001-7512-8971], Pyrillou, Katerina [0000-0003-0375-7810], Jurk, Diana [0000-0003-4486-0857], Narita, Masashi [0000-0001-7764-577X], Apollo - University of Cambridge Repository, Cassidy, Liam D. [0000-0002-9312-6256], Young, Christopher N. J. [0000-0001-7512-8971], and Young, Christopher NJ [0000-0001-7512-8971]

Subjects

0301 basic medicine, Male, Aging, General Physics and Astronomy, Autophagy-Related Protein 5, Mice, 0302 clinical medicine, Neoplasms, Sequestosome-1 Protein, 692/308/1426, lcsh:Science, 13/89, Bone Marrow Transplantation, Skin, Cancer, Mice, Knockout, Multidisciplinary, Muscles, article, Phenotype, 3. Good health, Experimental models of disease, 631/80/39/2346, 030220 oncology & carcinogenesis, Muscle, Female, 64/60, ATG5, medicine.symptom, 631/67, Science, Longevity, Inflammation, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 13/21, Macroautophagy, medicine, Autophagy, Animals, General Chemistry, medicine.disease, Mice, Inbred C57BL, Ageing, Disease Models, Animal, 030104 developmental biology, 13/51, Cancer research, lcsh:Q, Cancer risk

Abstract

Autophagy is an important cellular degradation pathway with a central role in metabolism as well as basic quality control, two processes inextricably linked to ageing. A decrease in autophagy is associated with increasing age, yet it is unknown if this is causal in the ageing process, and whether autophagy restoration can counteract these ageing effects. Here we demonstrate that systemic autophagy inhibition induces the premature acquisition of age-associated phenotypes and pathologies in mammals. Remarkably, autophagy restoration provides a near complete recovery of morbidity and a significant extension of lifespan; however, at the molecular level this rescue appears incomplete. Importantly autophagy-restored mice still succumb earlier due to an increase in spontaneous tumour formation. Thus, our data suggest that chronic autophagy inhibition confers an irreversible increase in cancer risk and uncovers a biphasic role of autophagy in cancer development being both tumour suppressive and oncogenic, sequentially., Autophagy declines with age, yet it is unclear if restoration of autophagy extends lifespan. Here, the authors demonstrate in murine models that the inhibition of Atg5 induces ageing phenotypes and reduces lifespan, whilst autophagy restoration partially reverses these phenotypes with accelerated tumorigenesis.

Published

2020

6. Short senolytic or senostatic interventions rescue progression of radiation-induced frailty and premature ageing in mice

Author

Tengfei Wan, Edward Fielder, Ghazaleh Alimohammadiha, Abbas Ishaq, Evon Low, B Melanie Weigand, George Kelly, Craig Parker, Brigid Griffin, Diana Jurk, Viktor I Korolchuk, Thomas von Zglinicki, and Satomi Miwa

Subjects

Male, Mice, General Immunology and Microbiology, Frailty, Senotherapeutics, General Neuroscience, Animals, Aging, Premature, General Medicine, General Biochemistry, Genetics and Molecular Biology, Cellular Senescence, Metformin

Abstract

Cancer survivors suffer from progressive frailty, multimorbidity, and premature morbidity. We hypothesise that therapy-induced senescence and senescence progression via bystander effects are significant causes of this premature ageing phenotype. Accordingly, the study addresses the question whether a short anti-senescence intervention is able to block progression of radiation-induced frailty and disability in a pre-clinical setting. Male mice were sublethally irradiated at 5 months of age and treated (or not) with either a senolytic drug (Navitoclax or dasatinib + quercetin) for 10 days or with the senostatic metformin for 10 weeks. Follow-up was for 1 year. Treatments commencing within a month after irradiation effectively reduced frailty progression (p0.05) and improved muscle (p0.01) and liver (p0.05) function as well as short-term memory (p0.05) until advanced age with no need for repeated interventions. Senolytic interventions that started late, after radiation-induced premature frailty was manifest, still had beneficial effects on frailty (p0.05) and short-term memory (p0.05). Metformin was similarly effective as senolytics. At therapeutically achievable concentrations, metformin acted as a senostatic neither via inhibition of mitochondrial complex I, nor via improvement of mitophagy or mitochondrial function, but by reducing non-mitochondrial reactive oxygen species production via NADPH oxidase 4 inhibition in senescent cells. Our study suggests that the progression of adverse long-term health and quality-of-life effects of radiation exposure, as experienced by cancer survivors, might be rescued by short-term adjuvant anti-senescence interventions.Cancer treatments save lives, but they can also be associated with long-term side effects which greatly reduce quality of life; former patients often face fatigue, memory loss, frailty, higher likelihood of developing other cancers, and overall accelerated aging. Senescence is a change in a cell’s state that follows damage and is associated with aging. When a cell becomes senescent it stops dividing, can promote inflammation and may damage other cells. Research has shown that cancer treatment increases the numbers of cells entering senescence, potentially explaining the associated long-term side effects. A new class of drugs known as senolytics can kill senescent cells, but whether they could help to counteract the damaging effects of cancer treatments remain unclear. To explore this question, Fielder et al. focused on mice having received radiation therapy, which also exhibit the long-term health defects observed in human patients. In these animals, a single, short senolytic treatment after irradiation nearly erased premature aging; frailty did not increase faster than normal, new cancers were less prevalent, and the rodents retained good memory and muscle function for at least one year after irradiation. Even mice treated later in life, after frailty was already established, showed some improvement. In addition, multiple tissues, including the brain and the liver, hosted fewer senescent cells in the animals treated with senolytics, even up to old age. Research should now explore whether these remarkable effects could also be true for humans.

Published

2021

7. Mitochondrial dysfunction and cell senescence: deciphering a complex relationship

Author

João F. Passos, Edward Fielder, and James Chapman

Subjects

Senescence, Aging, Cell, Biophysics, Context (language use), Biology, Mitochondrion, Biochemistry, 03 medical and health sciences, Structural Biology, Genetics, medicine, Animals, Humans, Molecular Biology, Cellular Senescence, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Reactive oxygen species, 030302 biochemistry & molecular biology, Cell Biology, Phenotype, Mitochondria, Cell biology, medicine.anatomical_structure, chemistry, Ageing, Homeostasis

Abstract

Cellular senescence and mitochondrial dysfunction have both been defined as classical hallmarks of the ageing process. Here, we review the intricate relationship between the two. In the context of ageing, it is now well regarded that cellular senescence is a key driver in both ageing and the onset of a number of age-related pathologies. Emerging evidence has pinpointed mitochondria as one of the key modulators in the development of the senescence phenotype, particularly the pro-inflammatory senescence associated secretory phenotype (SASP). This review focuses on the contribution of homeostatic mechanisms, as well as of reactive oxygen species and mitochondrial metabolites in the senescence programme. Furthermore, we discuss emerging pathways and mitochondrial-mediated mechanisms that may be influencing the SASP and, subsequently, explore how these may be exploited to open up new therapeutic avenues.

Published

2019

8. Whole‐body senescent cell clearance alleviates age‐related brain inflammation and cognitive impairment in mice

Author

Yi Zhu, João F. Passos, Kurt O. Johnson, Marissa J. Schafer, Diana Jurk, Edward Fielder, Christine Inman, Bettina M. Weigand, James L. Kirkland, Mikolaj Ogrodnik, Tamar Pirtskhalava, Shane A. Evans, Nicola Neretti, Ayush D. Patel, Thomas von Zglinicki, David B. Allison, Hanna Salmonowicz, Stella Victorelli, Nathan K. LeBrasseur, Tamar Tchkonia, Patrick Krüger, Azucena Rocha, and Stephanie L. Dickinson

Subjects

cognition, 0301 basic medicine, Senescence, Aging, medicine.medical_specialty, senescence, Cell cycle checkpoint, brain, Population, Hippocampus, Mice, Transgenic, Inflammation, Biology, SASP, senolytic, memory, Mice, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Animals, Cognitive Dysfunction, Senolytic, education, Cellular Senescence, Cyclin-Dependent Kinase Inhibitor p16, Original Paper, education.field_of_study, Microglia, Neurodegeneration, Age Factors, neurodegeneration, Cell Biology, telomeres, medicine.disease, Original Papers, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, Encephalitis, medicine.symptom, 030217 neurology & neurosurgery

Abstract

Cellular senescence is characterized by an irreversible cell cycle arrest and a pro‐inflammatory senescence‐associated secretory phenotype (SASP), which is a major contributor to aging and age‐related diseases. Clearance of senescent cells has been shown to improve brain function in mouse models of neurodegenerative diseases. However, it is still unknown whether senescent cell clearance alleviates cognitive dysfunction during the aging process. To investigate this, we first conducted single‐nuclei and single‐cell RNA‐seq in the hippocampus from young and aged mice. We observed an age‐dependent increase in p16Ink4a senescent cells, which was more pronounced in microglia and oligodendrocyte progenitor cells and characterized by a SASP. We then aged INK‐ATTAC mice, in which p16Ink4a‐positive senescent cells can be genetically eliminated upon treatment with the drug AP20187 and treated them either with AP20187 or with the senolytic cocktail Dasatinib and Quercetin. We observed that both strategies resulted in a decrease in p16Ink4a exclusively in the microglial population, resulting in reduced microglial activation and reduced expression of SASP factors. Importantly, both approaches significantly improved cognitive function in aged mice. Our data provide proof‐of‐concept for senolytic interventions' being a potential therapeutic avenue for alleviating age‐associated cognitive impairment., Senescence is a major contributor to aging and age‐related diseases. However, it is still unknown whether senolytics impact on cognitive function during the aging process. We found that both pharmacogenetic clearance of p16Ink4a senescent cells or treatment with senolytic cocktail Dasatinib and Quercetin, reduced senescent microglia in the hippocampus and improved cognitive function in aged mice.

Published

2021

9. Anti-inflammatory treatment rescues memory deficits during aging in nfkb1

Author

Caroline L. Wilson, Diana Jurk, Fiona E. N. LeBeau, João F. Passos, Clare Tweedy, Derek A. Mann, Thomas von Zglinicki, Fiona Oakley, and Edward Fielder

Subjects

0301 basic medicine, Senescence, Premature aging, Male, medicine.medical_specialty, Aging, senescence, hippocampus, Hippocampus, Inflammation, Disease, Biology, neuroinflammation, memory, 03 medical and health sciences, Mice, 0302 clinical medicine, Internal medicine, medicine, Animals, Cognitive decline, Neuroinflammation, Memory Disorders, Original Paper, Anti-Inflammatory Agents, Non-Steroidal, NF-kappa B, Cell Biology, NFKB1, cognitive decline, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Endocrinology, medicine.symptom, 030217 neurology & neurosurgery

Abstract

Chronic inflammation is a common feature of many age‐related conditions including neurodegenerative diseases such as Alzheimer's disease. Cellular senescence is a state of irreversible cell‐cycle arrest, thought to contribute to neurodegenerative diseases partially via induction of a chronic pro‐inflammatory phenotype. In this study, we used a mouse model of genetically enhanced NF‐κB activity (nfκb1 −/−), characterized by low‐grade chronic inflammation and premature aging, to investigate the impact of inflammaging on cognitive decline. We found that during aging, nfkb1 −/− mice show an early onset of memory loss, combined with enhanced neuroinflammation and increased frequency of senescent cells in the hippocampus and cerebellum. Electrophysiological measurements in the hippocampus of nfkb1 −/− mice in vitro revealed deficits in gamma frequency oscillations, which could explain the decline in memory capacity. Importantly, treatment with the nonsteroidal anti‐inflammatory drug (NASID) ibuprofen reduced neuroinflammation and senescent cell burden resulting in significant improvements in cognitive function and gamma frequency oscillations. These data support the hypothesis that chronic inflammation is a causal factor in the cognitive decline observed during aging., Chronic inflammation induces cellular senescence and leads to premature aging and cognitive decline. Anti‐inflammatory treatment reduces neuroinflammation and senescent cell burden, and ameliorates cognitive impairment.

Published

2020

10. Sublethal whole-body irradiation causes progressive premature frailty in mice

Author

Edward, Fielder, Melanie, Weigand, Julien, Agneessens, Brigid, Griffin, Craig, Parker, Satomi, Miwa, and Thomas, von Zglinicki

Subjects

Male, Disease Models, Animal, Mice, Aging, FI, frailty Index, Tumor survivor, Frailty, Animals, Aging, Premature, Irradiation, Whole-Body Irradiation, Article, IR, irradiation

Abstract

Highlights • Mice that survive irradiation develop progressive frailty. • Irradiation-induced premature frailty is phenotypically equal to frailty in old animals. • Premature frailty is associated with mortality and low cognition. • Sub-lethal whole body irradiation may constitute a good mouse model to test efficiency of anti-ageing interventions., There is an unmet need to develop and validate therapies that can treat or at least prevent premature therapy-induced frailty, multi-morbidity and mortality in long-term tumour survivors. In an approach to develop a first mouse model for therapy-induced long-term frailty, we irradiated male C57Bl/6 mice at 5–6 months of age sub-lethally with 3 × 3 Gy (whole body) and assessed subsequent frailty for up to 6 months using a Rockwood-type frailty index (FI). Frailty scorers were trained to obtain excellent inter- and intra-observer reproducibility. Irradiated mice developed progressive frailty approximately twice as fast as controls. This was premature frailty; it was phenotypically identical to that in non-irradiated mice at higher age. As expected, frailty was associated with decreased cognition and predicted mortality. In irradiated mice, frailty and neuromuscular performance, measured by Rotarod and Hanging Wire tests, were not associated with each other, probably because of long-term decreased body weights after irradiation. We conclude that progressive frailty following sub-lethal irradiation comprises a sensitive and easy to use test bed for interventions to stop premature ageing in long-term tumour survivors.

Published

2019

11. Temporal inhibition of autophagy reveals segmental reversal of aging with increased cancer risk

Author

João F. Passos, Liam D. Cassidy, Kimberley A. Wiggins, Rebecca Brais, Diana Jurk, Christopher N. J. Young, Masashi Narita, Edward Fielder, Andrew R. J. Young, Bettina M Weigand, Murray C.H. Clarke, and Elizabeth J. Soilleux

Subjects

Cellular degradation, Molecular level, Spontaneous tumor, Autophagy, Cancer research, Cancer development, Biology, Cancer risk, Phenotype

Abstract

Autophagy is an important cellular degradation pathway with a central role in metabolism as well as basic quality control, two processes inextricably linked to aging. A decrease in autophagy is associated with increasing age, yet it is unknown if this is causal in the aging process, and whether autophagy restoration can counteract these aging effects. Here we demonstrate that systemic autophagy inhibition induces the premature acquisition of age-associated phenotypes and pathologies in mammals. Remarkably, autophagy restoration provides a near complete recovery of morbidity and a significant extension of lifespan, however, at the molecular level this rescue appears incomplete. Importantly autophagy-restored mice still succumb earlier due to an increase in spontaneous tumor formation. Thus our data suggest that chronic autophagy inhibition confers an irreversible increase in cancer risk and uncovers a biphasic role of autophagy in cancer development being both tumor suppressive and oncogenic, sequentially.

Published

2019

12. Length‐independent telomere damage drives post‐mitotic cardiomyocyte senescence

Author

Rhys Anderson, Anthony Lagnado, Damien Maggiorani, Anna Walaszczyk, Emily Dookun, James Chapman, Jodie Birch, Hanna Salmonowicz, Mikolaj Ogrodnik, Diana Jurk, Carole Proctor, Clara Correia‐Melo, Stella Victorelli, Edward Fielder, Rolando Berlinguer‐Palmini, Andrew Owens, Laura C Greaves, Kathy L Kolsky, Angelo Parini, Victorine Douin‐Echinard, Nathan K LeBrasseur, Helen M Arthur, Simon Tual

Published

2019

13. Rapamycin improves healthspan but not inflammaging in nfκb1 −/− mice

Author

Anthony B. Lagnado, Dina Rahmatika, Diana Jurk, João F. Passos, Jodie Birch, Edward Fielder, Clara Correia-Melo, Bernadette Carroll, Satomi Miwa, Jelena Mann, James Chapman, Gavin D. Richardson, Derek A. Mann, Fiona Oakley, Viktor I. Korolchuk, and Jennifer Taylor

Subjects

0301 basic medicine, Senescence, Aging, Tissue architecture, senescence, Longevity, Inflammation, Context (language use), Biology, Chronic liver disease, SASP, law.invention, 03 medical and health sciences, 0302 clinical medicine, law, medicine, Animals, PI3K/AKT/mTOR pathway, Mice, Knockout, Sirolimus, Original Paper, rapamycin, aging, NF-kappa B, Cell Biology, medicine.disease, Original Papers, Phenotype, Mitochondria, 3. Good health, Mice, Inbred C57BL, 030104 developmental biology, Cancer research, mTOR, Suppressor, inflammaging, medicine.symptom, Biomarkers, 030217 neurology & neurosurgery

Abstract

Increased activation of the major pro-inflammatory NF-κB pathway leads to numerous age-related diseases, including chronic liver disease (CLD). Rapamycin, an inhibitor of mTOR, extends lifespan and healthspan, potentially via suppression of inflammaging, a process which is partially dependent on NF-κB signalling. However, it is unknown if rapamycin has beneficial effects in the context of compromised NF-κB signalling, such as that which occurs in several age-related chronic diseases. In this study, we investigated whether rapamycin could ameliorate age-associated phenotypes in a mouse model of genetically enhanced NF-κB activity (nfκb1−/−) characterized by low-grade chronic inflammation, accelerated aging and CLD. We found that, despite showing no beneficial effects in lifespan and inflammaging, rapamycin reduced frailty and improved long-term memory, neuromuscular coordination and tissue architecture. Importantly, markers of cellular senescence, a known driver of age-related pathology, were alleviated in rapamycin-fed animals. Our results indicate that, in conditions of genetically enhanced NF-κB, rapamycin delays aging phenotypes and improves healthspan uncoupled from its role as a suppressor of inflammation.

Published

2019

14. Length-independent telomere damage drives cardiomyocyte senescence

Author

Douin-Echinard, Marissa J. Schafer, João F. Passos, Diana Jurk, Stella Victorelli, Rolando Berlinguer-Palmini, Helen M. Arthur, Neil Robertson, Damien Maggiorani, Emily Dookun, Laura C. Greaves, Simon Tual-Chalot, Carolyn M Roos, Clara Correia-Melo, Jordan D. Miller, Mikolaj Ogrodnik, Rhys Anderson, Anna Walaszczyk, Anthony B. Lagnado, Carole J. Proctor, James L. Kirkland, Edward Fielder, Jelena Mann, James Chapman, Gavin D. Richardson, Tamara Tchkonia, Nathan K. LeBrasseur, A Owens, Hanna Salmonowicz, Angelo Parini, Peter D. Adams, Kathy L Kolsky, Jodie Birch, and Jeanne Mialet-Perez

Subjects

Senescence, Fibrosis, DNA damage, Ageing, Regeneration (biology), medicine, Biology, medicine.disease, Phenotype, Mitosis, Telomere, Cell biology

Abstract

Ageing is the biggest risk factor for cardiovascular health and is associated with increased incidence of cardiovascular disease. Cellular senescence, a process driven in part by telomere shortening, has been implicated in age-related tissue dysfunction. Here, we address the question of how senescence is induced in rarely dividing/post-mitotic cardiomyocytes and investigate if clearance of senescent cells attenuates age related cardiac dysfunction. During ageing, human and murine cardiomyocytes acquire a senescent-like phenotype characterised by persistent DNA damage at telomere regions that can be driven by mitochondrial dysfunction, and crucially can occur independently of cell-division and telomere length. Length-independent telomere damage in cardiomyocytes activates the classical senescence-inducing pathways, p21CIPand p16INK4aand results in a non-canonical senescence-associated secretory phenotype. Pharmacological or genetic clearance of senescent cells in mice alleviates myocardial hypertrophy and fibrosis, detrimental features of cardiac ageing, and promotes cardiomyocyte regeneration. Our data describes a mechanism by which senescence can occur and contribute to ageing in post-mitotic tissues.

Published

2018

15. The DNA Damage Response in Neurons: Die by Apoptosis or Survive in a Senescence-Like State?

Author

Thomas von Zglinicki, Diana Jurk, and Edward Fielder

Subjects

0301 basic medicine, Senescence, Gerontology, DNA damage, Cell, Apoptosis, Biology, Models, Biological, Histones, 03 medical and health sciences, Ataxia Telangiectasia, medicine, Animals, Cellular Senescence, Neurons, Kinase, General Neuroscience, Neurodegeneration, Cell Cycle, General Medicine, medicine.disease, Phenotype, Cell biology, Psychiatry and Mental health, Clinical Psychology, 030104 developmental biology, medicine.anatomical_structure, Neuron, Geriatrics and Gerontology, DNA Damage

Abstract

Neurons are exposed to high levels of DNA damage from both physiological and pathological sources. Neurons are post-mitotic and their loss cannot be easily recovered from; to cope with DNA damage a complex pathway called the DNA damage response (DDR) has evolved. This recognizes the damage, and through kinases such as ataxia-telangiectasia mutated (ATM) recruits and activates downstream factors that mediate either apoptosis or survival. This choice between these opposing outcomes integrates many inputs primarily through a number of key cross-road proteins, including ATM, p53, and p21. Evidence of re-entry into the cell-cycle by neurons can be seen in aging and diseases such as Alzheimer's disease. This aberrant cell-cycle re-entry is lethal and can lead to the apoptotic death of the neuron. Many downstream factors of the DDR promote cell-cycle arrest in response to damage and appear to protect neurons from apoptotic death. However, neurons surviving with a persistently activated DDR show all the features known from cell senescence; including metabolic dysregulation, mitochondrial dysfunction, and the hyper-production of pro-oxidant, pro-inflammatory and matrix-remodeling factors. These cells, termed senescence-like neurons, can negatively influence the extracellular environment and may promote induction of the same phenotype in surrounding cells, as well as driving aging and age-related diseases. Recently developed interventions targeting the DDR and/or the senescent phenotype in a range of non-neuronal tissues are being reviewed as they might become of therapeutic interest in neurodegenerative diseases.

Published

2017

16. Obesity-Induced Cellular Senescence Drives Anxiety and Impairs Neurogenesis

Author

Yuji Ikeno, Allyson K. Palmer, Patrick Krüger, Kurt O. Johnson, Grigori Enikolopov, Mikolaj Ogrodnik, João F. Passos, Nino Giorgadze, Christine Inman, Marissa J. Schafer, Tamar Pirtskhalava, James L. Kirkland, Thomas von Zglinicki, Terry C. Burns, Larissa G.P. Langhi, Diana Jurk, Tamar Tchkonia, Edward Fielder, Rifqha A. Ruswhandi, Stella Victorelli, Ming Xu, Yi Zhu, Oleg Podgorni, and Moritz Weigl

Subjects

Male, Physiology, Neurogenesis, Dasatinib, Cellular senescence, Mice, Transgenic, Anxiety, Diet, High-Fat, Tacrolimus, Article, Mice, 03 medical and health sciences, 0302 clinical medicine, Animals, Medicine, Obesity, Molecular Biology, Cells, Cultured, Cellular Senescence, Cyclin-Dependent Kinase Inhibitor p16, 030304 developmental biology, 0303 health sciences, Behavior, Animal, business.industry, Brain, Lipid Droplets, Cell Biology, Fibroblasts, medicine.disease, Cell biology, Mice, Inbred C57BL, Disease Models, Animal, Cell metabolism, Astrocytes, Female, Quercetin, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Cellular senescence entails a stable cell-cycle arrest and a pro-inflammatory secretory phenotype, which contributes to aging and age-related diseases. Obesity is associated with increased senescent cell burden and neuropsychiatric disorders, including anxiety and depression. To investigate the role of senescence in obesity-related neuropsychiatric dysfunction, we used the INK-ATTAC mouse model, from which p16(Ink4a)-expressing senescent cells can be eliminated, and senolytic drugs dasatinib and quercetin. We found that obesity results in the accumulation of senescent glial cells in proximity to the lateral ventricle, a region in which adult neurogenesis occurs. Furthermore, senescent glial cells exhibit excessive fat deposits, a phenotype we termed “accumulation of lipids in senescence.” Clearing senescent cells from high fat-fed or leptin receptor-deficient obese mice restored neurogenesis and alleviated anxiety-related behavior. Our study provides proof-of-concept evidence that senescent cells are major contributors to obesity-induced anxiety and that senolytics are a potential new therapeutic avenue for treating neuropsychiatric disorders.

Published

2019