Your search keyword '"Croteau DL"' showing total 15 results

1. DNA damage and mitochondria in cancer and aging.

Author

Patel J, Baptiste BA, Kim E, Hussain M, Croteau DL, and Bohr VA

Subjects

Aging genetics, Animals, Humans, Neoplasms genetics, Signal Transduction, Telomere, Aging pathology, DNA Damage, DNA Repair, Mitochondria genetics, Neoplasms pathology

Abstract

Age and DNA repair deficiencies are strong risk factors for developing cancer. This is reflected in the comorbidity of cancer with premature aging diseases associated with DNA damage repair deficiencies. Recent research has suggested that DNA damage accumulation, telomere dysfunction and the accompanying mitochondrial dysfunction exacerbate the aging process and may increase the risk of cancer development. Thus, an area of interest in both cancer and aging research is the elucidation of the dynamic crosstalk between the nucleus and the mitochondria. In this review, we discuss current research on aging and cancer with specific focus on the role of mitochondrial dysfunction in cancer and aging as well as how nuclear to mitochondrial DNA damage signaling may be a driving factor in the increased cancer incidence with aging. We suggest that therapeutic interventions aimed at the induction of autophagy and mediation of nuclear to mitochondrial signaling may provide a mechanism for healthier aging and reduced tumorigenesis., (Published by Oxford University Press 2020.)

Published

2020

2. Heterochromatin: an epigenetic point of view in aging.

Author

Lee JH, Kim EW, Croteau DL, and Bohr VA

Subjects

Age Factors, Animals, Chromatin genetics, Chromatin metabolism, Gene Expression Regulation, Heterochromatin metabolism, Histones metabolism, Humans, Longevity, Aging genetics, Epigenesis, Genetic, Epigenomics methods, Heterochromatin genetics

Abstract

Aging is an inevitable process of life. Defined by progressive physiological and functional loss of tissues and organs, aging increases the risk of mortality for the organism. The aging process is affected by various factors, including genetic and epigenetic ones. Here, we review the chromatin-specific epigenetic changes that occur during normal (chronological) aging and in premature aging diseases. Taking advantage of the reversible nature of epigenetic modifications, we will also discuss possible lifespan expansion strategies through epigenetic modulation, which was considered irreversible until recently.

Published

2020

3. Mitophagy and DNA damage signaling in human aging.

Author

Babbar M, Basu S, Yang B, Croteau DL, and Bohr VA

Subjects

Aging genetics, DNA Repair, Humans, Signal Transduction, Aging physiology, DNA Damage, Mitophagy physiology

Abstract

Aging is associated with multiple human pathologies. In the past few years mitochondrial homeostasis has been well correlated with age-related disorders and longevity. Mitochondrial homeostasis involves generation, biogenesis and removal of dysfunctional mitochondria via mitophagy. Mitophagy is regulated by various mitochondrial and extra-mitochondrial factors including morphology, oxidative stress and DNA damage. For decades, DNA damage and inefficient DNA repair have been considered as major determinants for age-related disorders. Although defects in DNA damage recognition and repair and mitophagy are well documented to be major factors in age-associated diseases, interactivity between these is poorly understood. Mitophagy efficiency decreases with age leading to accumulation of dysfunctional mitochondria enhancing the severity of age-related disorders including neurodegenerative diseases, inflammatory diseases, cancer, diabetes and many more. Therefore, mitophagy is being targeted for intervention in age-associated disorders. NAD + supplementation has emerged as one intervention to target both defective DNA repair and mitophagy. In this review, we discuss the molecular signaling pathways involved in regulation of DNA damage and repair and of mitophagy, and we highlight the opportunities for clinical interventions targeting these processes to improve the quality of life during aging., (Published by Elsevier B.V.)

Published

2020

4. Ageing as a risk factor for neurodegenerative disease.

Author

Hou Y, Dan X, Babbar M, Wei Y, Hasselbalch SG, Croteau DL, and Bohr VA

Subjects

Aging pathology, Brain pathology, DNA Damage physiology, Epigenesis, Genetic physiology, Humans, Mitophagy physiology, Neurodegenerative Diseases pathology, Risk Factors, Aging genetics, Aging metabolism, Brain metabolism, Neurodegenerative Diseases genetics, Neurodegenerative Diseases metabolism

Abstract

Ageing is the primary risk factor for most neurodegenerative diseases, including Alzheimer disease (AD) and Parkinson disease (PD). One in ten individuals aged ≥65 years has AD and its prevalence continues to increase with increasing age. Few or no effective treatments are available for ageing-related neurodegenerative diseases, which tend to progress in an irreversible manner and are associated with large socioeconomic and personal costs. This Review discusses the pathogenesis of AD, PD and other neurodegenerative diseases, and describes their associations with the nine biological hallmarks of ageing: genomic instability, telomere attrition, epigenetic alterations, loss of proteostasis, mitochondrial dysfunction, cellular senescence, deregulated nutrient sensing, stem cell exhaustion and altered intercellular communication. The central biological mechanisms of ageing and their potential as targets of novel therapies for neurodegenerative diseases are also discussed, with potential therapies including NAD + precursors, mitophagy inducers and inhibitors of cellular senescence.

Published

2019

5. Toward understanding genomic instability, mitochondrial dysfunction and aging.

Author

Fakouri NB, Hou Y, Demarest TG, Christiansen LS, Okur MN, Mohanty JG, Croteau DL, and Bohr VA

Subjects

Aging metabolism, Animals, Energy Metabolism, Humans, Mitochondria metabolism, Mitophagy, Poly(ADP-ribose) Polymerases metabolism, Aging pathology, Genomic Instability, Homeostasis, Mitochondria pathology, Oxidative Stress

Abstract

The biology of aging is an area of intense research, and many questions remain about how and why cell and organismal functions decline over time. In mammalian cells, genomic instability and mitochondrial dysfunction are thought to be among the primary drivers of cellular aging. This review focuses on the interrelationship between genomic instability and mitochondrial dysfunction in mammalian cells and its relevance to age-related functional decline at the molecular and cellular level. The importance of oxidative stress and key DNA damage response pathways in cellular aging is discussed, with a special focus on poly (ADP-ribose) polymerase 1, whose persistent activation depletes cellular energy reserves, leading to mitochondrial dysfunction, loss of energy homeostasis, and altered cellular metabolism. Elucidation of the relationship between genomic instability, mitochondrial dysfunction, and the signaling pathways that connect these pathways/processes are keys to the future of research on human aging. An important component of mitochondrial health preservation is mitophagy, and this and other areas that are particularly ripe for future investigation will be discussed., (Published 2018. This article is a U.S. Government work and is in the public domain in the USA.)

Published

2019

6. NAD + in Aging: Molecular Mechanisms and Translational Implications.

Author

Fang EF, Lautrup S, Hou Y, Demarest TG, Croteau DL, Mattson MP, and Bohr VA

Subjects

Alzheimer Disease pathology, Alzheimer Disease therapy, Animals, Cardiovascular Diseases pathology, Cardiovascular Diseases therapy, Humans, Muscular Atrophy pathology, Muscular Atrophy therapy, NAD, Parkinson Disease pathology, Parkinson Disease therapy, Aging metabolism, Alzheimer Disease metabolism, Cardiovascular Diseases metabolism, Energy Metabolism, Muscular Atrophy metabolism, Parkinson Disease metabolism

Abstract

The coenzyme NAD + is critical in cellular bioenergetics and adaptive stress responses. Its depletion has emerged as a fundamental feature of aging that may predispose to a wide range of chronic diseases. Maintenance of NAD + levels is important for cells with high energy demands and for proficient neuronal function. NAD + depletion is detected in major neurodegenerative diseases, such as Alzheimer's and Parkinson's diseases, cardiovascular disease and muscle atrophy. Emerging evidence suggests that NAD + decrements occur in various tissues during aging, and that physiological and pharmacological interventions bolstering cellular NAD + levels might retard aspects of aging and forestall some age-related diseases. Here, we discuss aspects of NAD + biosynthesis, together with putative mechanisms of NAD + action against aging, including recent preclinical and clinical trials., (Published by Elsevier Ltd.)

Published

2017

7. Cockayne syndrome: Clinical features, model systems and pathways.

Author

Karikkineth AC, Scheibye-Knudsen M, Fivenson E, Croteau DL, and Bohr VA

Subjects

Animals, Cognition, Humans, Models, Biological, Symptom Assessment methods, Transcriptional Activation, Aging physiology, Aging, Premature genetics, Aging, Premature physiopathology, Cockayne Syndrome diagnosis, Cockayne Syndrome genetics, Cockayne Syndrome physiopathology, Cockayne Syndrome psychology, DNA Repair physiology, Mitochondria physiology

Abstract

Cockayne syndrome (CS) is a disorder characterized by a variety of clinical features including cachectic dwarfism, severe neurological manifestations including microcephaly and cognitive deficits, pigmentary retinopathy, cataracts, sensorineural deafness, and ambulatory and feeding difficulties, leading to death by 12 years of age on average. It is an autosomal recessive disorder, with a prevalence of approximately 2.5 per million. There are several phenotypes (1-3) and two complementation groups (CSA and CSB), and CS overlaps with xeroderma pigmentosum (XP). It has been considered a progeria, and many of the clinical features resemble accelerated aging. As such, the study of CS affords an opportunity to better understand the underlying mechanisms of aging. The molecular basis of CS has traditionally been ascribed to defects in transcription and transcription-coupled nucleotide excision repair (TC-NER). However, recent work suggests that defects in base excision DNA repair and mitochondrial functions may also play key roles. This opens up the possibility for molecular interventions in CS, and by extrapolation, possibly in aging., (Published by Elsevier B.V.)

Published

2017

8. Nuclear DNA damage signalling to mitochondria in ageing.

Author

Fang EF, Scheibye-Knudsen M, Chua KF, Mattson MP, Croteau DL, and Bohr VA

Subjects

Animals, Apoptosis, Cell Nucleus genetics, DNA Repair, Genomic Instability, Humans, Mitophagy, Reactive Oxygen Species metabolism, Signal Transduction, Aging, DNA Damage, Mitochondria physiology

Abstract

Mitochondrial dysfunction is a hallmark of ageing, and mitochondrial maintenance may lead to increased healthspan. Emerging evidence suggests a crucial role for signalling from the nucleus to mitochondria (NM signalling) in regulating mitochondrial function and ageing. An important initiator of NM signalling is nuclear DNA damage, which accumulates with age and may contribute to the development of age-associated diseases. DNA damage-dependent NM signalling constitutes a network that includes nuclear sirtuins and controls genomic stability and mitochondrial integrity. Pharmacological modulation of NM signalling is a promising novel approach for the prevention and treatment of age-associated diseases., Competing Interests: statement The authors declare competing interests: see Web version for details.

Published

2016

9. DNA Damage, DNA Repair, Aging, and Neurodegeneration.

Author

Maynard S, Fang EF, Scheibye-Knudsen M, Croteau DL, and Bohr VA

Subjects

Adult Stem Cells physiology, Aging, Premature genetics, Animals, Biological Evolution, Cellular Senescence genetics, DNA, Mitochondrial genetics, Disease Models, Animal, Forecasting, Homeostasis genetics, Humans, Mitochondrial Diseases genetics, Mitochondrial Diseases metabolism, Neurodegenerative Diseases metabolism, Telomere genetics, Aging genetics, DNA Damage genetics, DNA Repair genetics, Neurodegenerative Diseases genetics

Abstract

Aging in mammals is accompanied by a progressive atrophy of tissues and organs, and stochastic damage accumulation to the macromolecules DNA, RNA, proteins, and lipids. The sequence of the human genome represents our genetic blueprint, and accumulating evidence suggests that loss of genomic maintenance may causally contribute to aging. Distinct evidence for a role of imperfect DNA repair in aging is that several premature aging syndromes have underlying genetic DNA repair defects. Accumulation of DNA damage may be particularly prevalent in the central nervous system owing to the low DNA repair capacity in postmitotic brain tissue. It is generally believed that the cumulative effects of the deleterious changes that occur in aging, mostly after the reproductive phase, contribute to species-specific rates of aging. In addition to nuclear DNA damage contributions to aging, there is also abundant evidence for a causative link between mitochondrial DNA damage and the major phenotypes associated with aging. Understanding the mechanistic basis for the association of DNA damage and DNA repair with aging and age-related diseases, such as neurodegeneration, would give insight into contravening age-related diseases and promoting a healthy life span., (Copyright © 2015 Cold Spring Harbor Laboratory Press; all rights reserved.)

Published

2015

10. The role of DNA repair in brain related disease pathology.

Author

Canugovi C, Misiak M, Ferrarelli LK, Croteau DL, and Bohr VA

Subjects

Animals, Brain metabolism, DNA Damage, Disease Models, Animal, Humans, Neurons cytology, Neurons pathology, Oxidative Stress, Aging genetics, Brain pathology, DNA Repair, Neurodegenerative Diseases genetics, Neurodegenerative Diseases pathology

Abstract

Oxidative DNA damage is implicated in brain aging, neurodegeneration and neurological diseases. Damage can be created by normal cellular metabolism, which accumulates with age, or by acute cellular stress conditions which create bursts of oxidative damage. Brain cells have a particularly high basal level of metabolic activity and use distinct oxidative damage repair mechanisms to remove oxidative damage from DNA and dNTP pools. Accumulation of this damage in the background of a functional DNA repair response is associated with normal aging, but defective repair in brain cells can contribute to neurological dysfunction. Emerging research strongly associates three common neurodegenerative conditions, Alzheimer's, Parkinson's and stroke, with defects in the ability to repair chronic or acute oxidative damage in neurons. This review explores the current knowledge of the role of oxidative damage repair in preserving brain function and highlights the emerging models and methods being used to advance our knowledge of the pathology of neurodegenerative disease., (Published by Elsevier B.V.)

Published

2013

11. A novel diagnostic tool reveals mitochondrial pathology in human diseases and aging.

Author

Scheibye-Knudsen M, Scheibye-Alsing K, Canugovi C, Croteau DL, and Bohr VA

Subjects

Aging genetics, Humans, Mitochondria genetics, Mitochondrial Diseases genetics, Mitochondrial Diseases pathology, Mutation, Phenotype, Aging pathology, Mitochondria pathology, Mitochondrial Diseases diagnosis

Abstract

The inherent complex and pleiotropic phenotype of mitochondrial diseases poses a significant diagnostic challenge for clinicians as well as an analytical barrier for scientists. To overcome these obstacles we compiled a novel database, www.mitodb.com, containing the clinical features of primary mitochondrial diseases. Based on this we developed a number of qualitative and quantitative measures, enabling us to determine whether a disorder can be characterized as mitochondrial. These included a clustering algorithm, a disease network, a mitochondrial barcode and two scoring algorithms. Using these tools we detected mitochondrial involvement in a number of diseases not previously recorded as mitochondrial. As a proof of principle Cockayne syndrome, ataxia with oculomotor apraxia 1 (AOA1), spinocerebellar ataxia with axonal neuropathy 1 (SCAN1) and ataxia-telangiectasia have recently been shown to have mitochondrial dysfunction and those diseases showed strong association with mitochondrial disorders. We next evaluated mitochondrial involvement in aging and detected two distinct categories of accelerated aging disorders, one of them being associated with mitochondrial dysfunction. Normal aging seemed to associate stronger with the mitochondrial diseases than the non-mitochondrial partially supporting a mitochondrial theory of aging.

Published

2013

12. RECQL4 in genomic instability and aging.

Author

Croteau DL, Singh DK, Hoh Ferrarelli L, Lu H, and Bohr VA

Subjects

Animals, Humans, Mice, Mitochondria genetics, Mitochondria metabolism, RecQ Helicases chemistry, Rothmund-Thomson Syndrome genetics, Telomere genetics, Telomere metabolism, Aging genetics, Genomic Instability, RecQ Helicases genetics, RecQ Helicases metabolism

Abstract

Helicases are ubiquitous proteins that unwind DNA and participate in DNA metabolism including replication, repair, transcription, and chromatin organization. The highly conserved RecQ helicase family proteins are important in these transactions and have been termed the guardians of the genome. Humans have five members of this family: WRN, BLM, RECQL4, RECQL1, and RECQL5. The first three of are associated with premature aging and cancer prone syndromes, but the latter two proteins have not yet been implicated in any human disease. Although WRN and BLM have been fairly well characterized, RECQL4 has only recently been intensively investigated. The sum of this work to date has shown that RECQL4 has helicase activity and localizes to telomeres and mitochondria. In addition, new protein partners are emerging, implicating RECQL4 in novel processes. Here, we describe these recent findings which place RECQL4 at the crossroads of genomic instability and aging processes., (Published by Elsevier Ltd.)

Published

2012

13. Age-related disease association of endogenous γ-H2AX foci in mononuclear cells derived from leukapheresis.

Author

Schurman SH, Dunn CA, Greaves R, Yu B, Ferrucci L, Croteau DL, Seidman MM, and Bohr VA

Subjects

Female, Humans, Male, Middle Aged, Phosphorylation, Aging metabolism, Histones metabolism, Leukapheresis, Monocytes metabolism

Abstract

The phosphorylated form of histone H2AX (γ-H2AX) forms immunohistochemically detectable foci at DNA double strand breaks. In peripheral blood mononuclear cells (PBMCs) derived from leukapheresis from patients enrolled in the Baltimore Longitudinal Study of Aging, γ-H2AX foci increased in a linear fashion with regards to age, peaking at ~57 years. The relationship between the frequency of γ-H2AX foci and age-related pathologies was assessed. We found a statistically significant (p = 0.023) 50% increase in foci in PBMCs derived from patients with a known history of vitamin D deficiency. In addition, there were trends toward increased γ-H2AX foci in patients with cataracts (34% increase, p<0.10) and in sleep apnea patients (44%, p<0.10). Among patients ≥57 y/o, we found a significant (p = 0.037) 36% increase in the number of γ-H2AX foci/cell for patients with hypertension compared to non-hypertensive patients. Our results support a role for increased DNA damage in the morbidity of age-related diseases. γ -H2AX may be a biomarker for human morbidity in age-related diseases.

Published

2012

14. Werner syndrome resembles normal aging.

Author

Kyng K, Croteau DL, and Bohr VA

Subjects

DNA Damage genetics, DNA Damage physiology, Exodeoxyribonucleases genetics, Humans, RecQ Helicases genetics, Werner Syndrome metabolism, Werner Syndrome Helicase, Adipogenesis physiology, Aging genetics, Exodeoxyribonucleases physiology, RecQ Helicases physiology, Werner Syndrome genetics

Published

2009

15. Age-associated increase in 8-oxo-deoxyguanosine glycosylase/AP lyase activity in rat mitochondria.

Author

Souza-Pinto NC, Croteau DL, Hudson EK, Hansford RG, and Bohr VA

Subjects

8-Hydroxy-2'-Deoxyguanosine, Aging genetics, Animals, DNA-(Apurinic or Apyrimidinic Site) Lyase, DNA-Formamidopyrimidine Glycosylase, Deoxyguanosine metabolism, Deoxyribonuclease IV (Phage T4-Induced), Male, Mitochondria, Heart genetics, Mitochondria, Liver genetics, Rats, Rats, Wistar, Uracil-DNA Glycosidase, Aging metabolism, Carbon-Oxygen Lyases metabolism, DNA Glycosylases, DNA Repair, DNA, Mitochondrial, Deoxyguanosine analogs & derivatives, Mitochondria, Heart enzymology, Mitochondria, Liver enzymology, N-Glycosyl Hydrolases metabolism

Abstract

The mitochondrial theory of aging postulates that organisms age due to the accumulation of DNA damage and mutations in the multiple mitochondrial genomes, leading to mitochondrial dysfunction. Among the wide variety of DNA damage, 8-oxo-deoxyguanosine (8-oxo-dG) has received the most attention due to its mutagenicity and because of the possible correlation between its accumulation and pathological processes like cancer, degenerative diseases and aging. Although still controversial, many studies show that 8-oxo-dG accumulates with age in the mitochondrial (mt) DNA. However, little is known about the processing of this lesion and no study has yet examined whether mtDNA repair changes with age. Here, we report the first study on age-related changes in mtDNA repair, accomplished by assessing the cleavage activity of mitochondrial extracts towards an 8-oxo-dG-containing substrate. In this study, mitochondria obtained from rat heart and liver were used. We find that this enzymatic activity is higher in 12 and 23 month-old rats than in 6 month-old rats, in both liver and heart extracts. These mitochondrial extracts also cleave oligonucleotides containing a U:A mismatch, at the uracil position, reflecting the combined action of mitochondrial uracil DNA glycosylase (mtUDG) and mitochondrial apurinic/apyrimidinic (AP) endonucleases. The mtUDG activity did not change with age in liver mitochondria, but there was a small increase in activity from 6 to 23 months in rat heart extracts, after normalization to citrate synthase activity. Endonuclease G activity, measured by a plasmid relaxation assay, did not show any age-associated change in liver, but there was a significant decrease from 6 to 23 months in heart mitochondria. Our results suggest that the mitochondrial capacity to repair 8-oxo-dG, the main oxidative base damage suggested to accumulate with age in mtDNA, does not decrease, but rather increases with age. The specific increase in 8-oxo-dG endonuclease activity, rather than a general up-regulation of DNA repair in mitochondria, suggests an induction of the 8-oxo-dG-specific repair pathway with age.

Published

1999