Your search keyword '"Finkel, Toren"' showing total 39 results

1. Mitohormesis.

Author

Cheng, Yu-Wei, Liu, Jie, and Finkel, Toren

Abstract

Perturbation of mitochondrial function can trigger a host of cellular responses that seek to restore cellular metabolism, cytosolic proteostasis, and redox homeostasis. In some cases, these responses persist even after the stress is relieved, leaving the cell or tissue in a less vulnerable state. This process—termed mitohormesis—is increasingly viewed as an important aspect of normal physiology and a critical modulator of various disease processes. Here, we review aspects of mitochondrial stress signaling that, among other things, can rewire the cell's metabolism, activate the integrated stress response, and alter cytosolic quality-control pathways. We also discuss how these pathways are implicated in various disease states from pathogen challenge to chemotherapeutic resistance and how their therapeutic manipulation can lead to new strategies for a host of chronic conditions including aging itself. Cheng et al. review the recent progress on the phenomenon known as mitohormesis. This stress-induced program encompasses the complex interactions between impaired mitochondria and the cells and tissues where they function. Molecular mechanisms, disease implications, and therapeutic opportunities are discussed. [ABSTRACT FROM AUTHOR]

Published

2023

2. Mitochondria, oxidants, and aging

Author

Balaban, Robert S., Nemoto, Shino, and Finkel, Toren

Subjects

Oxidizing agents -- Research, Aging -- Research, Mitochondria -- Research, Biological sciences

Abstract

The various theories that agree and disagree with the free radical theory are reviewed and the relationship between mitochondrial metabolism, oxidant formation and the process of aging is investigated. The findings suggest that the free radical theory provides an explanation for the process of aging in a wide variety of species and the presence of many short-lived and long-lived organisms, which bring about changes in the mitochondrial metabolism, oxidant formation, reactive oxygen species (ROS) and aging, thus revealing the possibility of a link between them.

Published

2005

3. Redox-dependent signal transduction

Author

Finkel, Toren

Published

2000

4. Homocysteine accelerates endothelial cell senescence

Author

Xu, Dong, Neville, Richard, and Finkel, Toren

Published

2000

5. TGF-β receptor 1 regulates progenitors that promote browning of white fat.

Author

Wankhade, Umesh D., Lee, Ji-Hyeon, Dagur, Pradeep K., Yadav, Hariom, Shen, Michael, Chen, Weiping, Kulkarni, Ashok B., McCoy, J. Philip, Finkel, Toren, Cypess, Aaron M., and Rane, Sushil G.

Abstract

Abstract Objective Beige/brite adipose tissue displays morphological characteristics and beneficial metabolic traits of brown adipose tissue. Previously, we showed that TGF-β signaling regulates the browning of white adipose tissue. Here, we inquired whether TGF-β signals regulated presumptive beige progenitors in white fat and investigated the TGF-β regulated mechanisms involved in beige adipogenesis. Methods We deleted TGF-β receptor 1 (TβRI) in adipose tissue (TβRIAdKO mice) and, using flow-cytometry based assays, identified and isolated presumptive beige progenitors located in the stromal vascular cells of white fat. These cells were molecularly characterized to examine beige/brown marker expression and to investigate TGF-β dependent mechanisms. Further, the cells were transplanted into athymic nude mice to examine their adipogenesis potential. Results Deletion of TβRI promotes beige adipogenesis while reducing the detrimental effects of high fat diet feeding. Interaction of TGF-β signaling with the prostaglandin pathway regulated the appearance of beige adipocytes in white fat. Using flow cytometry techniques and stromal vascular fraction from white fat, we isolated presumptive beige stem/progenitor cells (iBSCs). Upon genetic or pharmacologic inhibition of TGF-β signaling, these cells express high levels of predominantly beige markers. Transplantation of TβRI-deficient stromal vascular cells or iBSCs into athymic nude mice followed by high fat diet feeding and stimulation of β-adrenergic signaling via CL316,243 injection or cold exposure promoted robust beige adipogenesis in vivo. Conclusions TβRI signals target the prostaglandin network to regulate presumptive beige progenitors in white fat capable of developing into beige adipocytes with functional attributes. Controlled inhibition of TβRI signaling and concomitant PGE2 stimulation has the potential to promote beige adipogenesis and improve metabolism. Graphical abstract Wankhade et al. show that loss of TβRI in adipose tissue promotes beige adipogenesis. Interaction between the TGF-β and prostaglandin pathways regulates presumptive progenitors in white fat that develop into beige adipocytes with functional attributes. These findings provide mechanistic insight into signals regulating beige adipogenesis. Image 1 Highlights • Loss of TβRI in adipose tissue promotes beige adipogenesis. • TβRI regulates presumptive beige adipocyte progenitors in white fat. • TβRI signals interact with the PGE2/Cox2 pathway during beige adipogenesis. • TβRI regulates thermogenesis, mitochondrial bioenergetics and beige adipogenesis. [ABSTRACT FROM AUTHOR]

Published

2018

6. Premature aging and reduced cancer incidence associated with near-complete body-wide Myc inactivation.

Author

Wang, Huabo, Lu, Jie, Stevens, Taylor, Roberts, Alexander, Mandel, Jordan, Avula, Raghunandan, Ma, Bingwei, Wu, Yijen, Wang, Jinglin, Land, Clinton Van't, Finkel, Toren, Vockley, Jerry E., Airik, Merlin, Airik, Rannar, Muzumdar, Radhika, Gong, Zhenwei, Torbenson, Michel S., and Prochownik, Edward V.

Abstract

MYC proto-oncogene dysregulation alters metabolism, translation, and other functions in ways that support tumor induction and maintenance. Although Myc +/− mice are healthier and longer-lived than control mice, the long-term ramifications of more complete Myc loss remain unknown. We now describe the chronic consequences of body-wide Myc inactivation initiated postnatally. " Myc KO" mice acquire numerous features of premature aging, including altered body composition and habitus, metabolic dysfunction, hepatic steatosis, and dysregulation of gene sets involved in functions that normally deteriorate with aging. Yet, Myc KO mice have extended lifespans that correlate with a 3- to 4-fold lower lifetime cancer incidence. Aging tissues from normal mice and humans also downregulate Myc and gradually alter many of the same Myc target gene sets seen in Myc KO mice. Normal aging and its associated cancer predisposition are thus highly linked via Myc. [Display omitted] • Postnatal body-wide deletion of the Myc gene in mice causes premature aging • " Myc KO" mice dysregulate numerous genes involved in aging, senescence, and cancer • Myc KO mice live longer and have a low lifetime cancer incidence • Normal aging in mice and humans is associated with Myc downregulation Wang et al. show that the postnatal elimination of Myc causes premature aging and the deterioration of age-sensitive functions. Yet, these mice have extended lifespans and a reduced cancer incidence. Gradual Myc downregulation accompanies normal aging in many tissues. Thus, the strong relationship between aging and cancer can be severed by eliminating a single gene. [ABSTRACT FROM AUTHOR]

Published

2023

7. Autophagy as a regulator of cardiovascular redox homeostasis.

Author

Yan, Ye and Finkel, Toren

Subjects

*AUTOPHAGY, *OXIDATION-reduction reaction, *HOMEOSTASIS, *CARDIOVASCULAR diseases, *PROTEINS

Abstract

Autophagy is a highly regulated process involving the removal of damaged proteins and organelles from cells and tissues through a lysosomal-mediated pathway. Accumulating evidence suggests that autophagy is necessary to maintain redox homeostasis. Here, we explore the connection between autophagy and reactive oxygen species (ROS). In particular, we discuss how oxidant-dependent signaling can modulate autophagic flux and how autophagy can, in turn, modulate ROS levels. Finally, we discuss how a decline or disruption of autophagy might contribute to redox-dependent cardiovascular pathology and help fuel the age-dependent decline in cardiovascular function. [ABSTRACT FROM AUTHOR]

Published

2017

8. Key proteins and pathways that regulate lifespan.

Author

Haihui Pan and Finkel, Toren

Subjects

*PROTEINS, *GROWTH factors, *CELL communication, *LABORATORY mice, *RAPAMYCIN

Abstract

Here, we review three sets of key proteins and their corresponding downstream pathways that have been linked to extending lifespan and promoting health span in a wide range of organisms. In particular, we review the biology of the sirtuin family of proteins, the insulin/insulin-like growth factor (IGF) signaling (IIS) pathway, and the mechanistic target of rapamycin (mTOR). Using insights derived from simple model organisms, mice, and humans we discuss how these proteins and pathways may potentially alter the rate of aging. We further describe how knowledge of these pathways may lead to the rational design of small molecules that modulate aging and hence alter the propensity for a host of age-related diseases. [ABSTRACT FROM AUTHOR]

Published

2017

9. MICU1 Serves as a Molecular Gatekeeper to Prevent In Vivo Mitochondrial Calcium Overload.

Author

Liu, Julia C., Liu, Jie, Holmström, Kira M., Menazza, Sara, Parks, Randi J., Fergusson, Maria M., Yu, Zu-Xi, Springer, Danielle A., Halsey, Charles, Liu, Chengyu, Murphy, Elizabeth, and Finkel, Toren

Abstract

Summary MICU1 is a component of the mitochondrial calcium uniporter, a multiprotein complex that also includes MICU2, MCU, and EMRE. Here, we describe a mouse model of MICU1 deficiency. MICU1 −/− mitochondria demonstrate altered calcium uptake, and deletion of MICU1 results in significant, but not complete, perinatal mortality. Similar to afflicted patients, viable MICU1 −/− mice manifest marked ataxia and muscle weakness. Early in life, these animals display a range of biochemical abnormalities, including increased resting mitochondrial calcium levels, altered mitochondrial morphology, and reduced ATP. Older MICU1 −/− mice show marked, spontaneous improvement coincident with improved mitochondrial calcium handling and an age-dependent reduction in EMRE expression. Remarkably, deleting one allele of EMRE helps normalize calcium uptake while simultaneously rescuing the high perinatal mortality observed in young MICU1 −/− mice. Together, these results demonstrate that MICU1 serves as a molecular gatekeeper preventing calcium overload and suggests that modulating the calcium uniporter could have widespread therapeutic benefits. [ABSTRACT FROM AUTHOR]

Published

2016

10. Celastrol Protects against Obesity and Metabolic Dysfunction through Activation of a HSF1-PGC1α Transcriptional Axis.

Author

Ma, Xinran, Xu, Lingyan, Alberobello, Anna Teresa, Gavrilova, Oksana, Bagattin, Alessia, Skarulis, Monica, Liu, Jie, Finkel, Toren, and Mueller, Elisabetta

Abstract

Summary Altering the balance between energy intake and expenditure is a potential strategy for treating obesity and metabolic syndrome. Nonetheless, despite years of progress in identifying diverse molecular targets, biological-based therapies are limited. Here we demonstrate that heat shock factor 1 (HSF1) regulates energy expenditure through activation of a PGC1α-dependent metabolic program in adipose tissues and muscle. Genetic modulation of HSF1 levels altered white fat remodeling and thermogenesis, and pharmacological activation of HSF1 via celastrol was associated with enhanced energy expenditure, increased mitochondrial function in fat and muscle and protection against obesity, insulin resistance, and hepatic steatosis during high-fat diet regimens. The beneficial metabolic changes elicited by celastrol were abrogated in HSF1 knockout mice. Overall, our findings identify the temperature sensor HSF1 as a regulator of energy metabolism and demonstrate that augmenting HSF1 via celastrol represents a possible therapeutic strategy to treat obesity and its myriad metabolic consequences. [ABSTRACT FROM AUTHOR]

Published

2015

11. Mitohormesis.

Author

Yun, Jeanho and Finkel, Toren

Abstract

For many years, mitochondria were viewed as semiautonomous organelles, required only for cellular energetics. This view has been largely supplanted by the concept that mitochondria are fully integrated into the cell and that mitochondrial stresses rapidly activate cytosolic signaling pathways that ultimately alter nuclear gene expression. Remarkably, this coordinated response to mild mitochondrial stress appears to leave the cell less susceptible to subsequent perturbations. This response, termed mitohormesis, is being rapidly dissected in many model organisms. A fuller understanding of mitohormesis promises to provide insight into our susceptibility for disease and potentially provide a unifying hypothesis for why we age. [Copyright &y& Elsevier]

Published

2014

12. Metabolic regulation of the cell cycle.

Author

Lee, In Hye and Finkel, Toren

Subjects

*METABOLIC regulation, *CELL cycle, *DISEASE progression, *MOLECULAR biology, *BIOSYNTHESIS, *STEM cells, *METABOLIC disorders

Abstract

There is a growing appreciation that metabolic signals are integrated and coupled to cell cycle progression. However, the molecular wiring that connects nutrient availability, biosynthetic intermediates and energetic balance to the core cell cycle machinery remains incompletely understood. In this review, we explore the recent progress in this area with particular emphasis on how nutrient and energetic status is sensed within the cell to ultimately regulate cell growth and division. The role these pathways play in normal cell function including stem cell biology is also discussed. Furthermore, we describe the growing appreciation that dysregulation of these pathways might contribute to a variety of pathological conditions including metabolic diseases and tumor formation. [Copyright &y& Elsevier]

Published

2013

13. Increased Mammalian Lifespan and a Segmental and Tissue-Specific Slowing of Aging after Genetic Reduction of mTOR Expression.

Author

Wu, J. Julie, Liu, Jie, Chen, Edmund B., Wang, Jennifer J., Cao, Liu, Narayan, Nisha, Fergusson, Marie M., Rovira, Ilsa I., Allen, Michele, Springer, Danielle A., Lago, Cory U., Zhang, Shuling, DuBois, Wendy, Ward, Theresa, deCabo, Rafael, Gavrilova, Oksana, Mock, Beverly, and Finkel, Toren

Abstract

Summary: We analyzed aging parameters using a mechanistic target of rapamycin (mTOR) hypomorphic mouse model. Mice with two hypomorphic (mTORΔ/Δ) alleles are viable but express mTOR at approximately 25% of wild-type levels. These animals demonstrate reduced mTORC1 and mTORC2 activity and exhibit an approximately 20% increase in median survival. While mTORΔ/Δ mice are smaller than wild-type mice, these animals do not demonstrate any alterations in normalized food intake, glucose homeostasis, or metabolic rate. Consistent with their increased lifespan, mTORΔ/Δ mice exhibited a reduction in a number of aging tissue biomarkers. Functional assessment suggested that, as mTORΔ/Δ mice age, they exhibit a marked functional preservation in many, but not all, organ systems. Thus, in a mammalian model, while reducing mTOR expression markedly increases overall lifespan, it affects the age-dependent decline in tissue and organ function in a segmental fashion. [Copyright &y& Elsevier]

Published

2013

14. Signal Transduction by Mitochondrial Oxidants.

Author

Finkel, Toren

Subjects

*OXIDIZING agents, *MICROBIAL genetics, *REACTIVE oxygen species, *NATURAL immunity, *STEM cells, *BIOCHEMISTRY

Abstract

The production of mitochondrial reactive oxygen species occurs as a consequence of aerobic metabolism. Mitochondrial oxidants are increasingly viewed less as byproducts of metabolism and more as important signaling molecules. Here, I review several notable examples, including the cellular response to hypoxia, aspects of innate immunity, the regulation of autophagy, and stem cell self-renewal capacity, where evidence suggests an important regulatory role for mitochondrial oxidants. [ABSTRACT FROM AUTHOR]

Published

2012

15. Protection from Obesity and Diabetes by Blockade of TGF-β/Smad3 Signaling.

Author

Yadav, Hariom, Quijano, Celia, Kamaraju, Anil K., Gavrilova, Oksana, Malek, Rana, Chen, Weiping, Zerfas, Patricia, Zhigang, Duan, Wright, Elizabeth C., Stuelten, Christina, Sun, Peter, Lonning, Scott, Skarulis, Monica, Sumner, Anne E., Finkel, Toren, and Rane, Sushil G.

Subjects

OBESITY, DIABETES, TRANSFORMING growth factors, CELLULAR signal transduction, HOMEOSTASIS, GLUCOSE, FAT cells, EPIDEMICS, LABORATORY mice

Abstract

Summary: Imbalances in glucose and energy homeostasis are at the core of the worldwide epidemic of obesity and diabetes. Here, we illustrate an important role of the TGF-β/Smad3 signaling pathway in regulating glucose and energy homeostasis. Smad3-deficient mice are protected from diet-induced obesity and diabetes. Interestingly, the metabolic protection is accompanied by Smad3 − /− white adipose tissue acquiring the bioenergetic and gene expression profile of brown fat/skeletal muscle. Smad3 −/− adipocytes demonstrate a marked increase in mitochondrial biogenesis, with a corresponding increase in basal respiration, and Smad3 acts as a repressor of PGC-1α expression. We observe significant correlation between TGF-β1 levels and adiposity in rodents and humans. Further, systemic blockade of TGF-β signaling protects mice from obesity, diabetes, and hepatic steatosis. Together, these results demonstrate that TGF-β signaling regulates glucose tolerance and energy homeostasis and suggest that modulation of TGF-β activity might be an effective treatment strategy for obesity and diabetes. [ABSTRACT FROM AUTHOR]

Published

2011

16. Regulation of Autophagy by the p300 Acetyltransferase.

Author

Lee, In Hye and Finkel, Toren

Subjects

*REGULATION of cell metabolism, *STARVATION, *ACETYLATION, *ACETYLTRANSFERASES, *BIOCHEMISTRY

Abstract

Autophagy is a regulated process of intracellular catabolism required for normal cellular maintenance, as well as serving as an adaptive response under various stress conditions, including starvation. The molecular regulation of autophagy in mammalian cells remains incompletely understood. Here we demonstrate a role for protein acetylation in the execution and regulation of autophagy. In particular, we demonstrate that the p300 acetyltransferase can regulate the acetylation of various known components of the autophagy machinery. Knockdown of p300 reduces acetylation of Atg5, Atg7, Atg8, and Atgl2, although overexpressed p300 increases the acetylation of these same proteins. Furthermore, p300 and Atg7 colocalize within cells, and the two proteins physically interact. The interaction between p300 and Atg7 is dependent on nutrient availability. Finally, we demonstrate that knockdown of p300 can stimulate autophagy, whereas overexpression of p300 inhibits starvation-induced autophagy. These results demonstrate a role for protein acetylation and particularly p300 in the regulation of autophagy under conditions of limited nutrient availability. [ABSTRACT FROM AUTHOR]

Published

2009

17. Xanthine Oxidoreductase Is a Regulator of Adipogenesis and PPARγ Activity.

Author

Cheung, Kevin J., Tzameli, Iphigenia, Pissios, Pavlos, Rovira, Ilsa, Gavrilova, Oksana, Ohtsubo, Toshio, Chen, Zhu, Finkel, Toren, Flier, Jeffrey S., and Friedman, Jeffrey M.

Subjects

XANTHINE, OXIDOREDUCTASES, ADIPOSE tissues, HYPERURICEMIA

Abstract

Summary: In an effort to identify novel candidate regulators of adipogenesis, gene profiling of differentiating 3T3-L1 preadipocytes was analyzed using a novel algorithm. We report here the characterization of xanthine oxidoreductase (XOR) as a novel regulator of adipogenesis. XOR lies downstream of C/EBPβ and upstream of PPARγ, in the cascade of factors that control adipogenesis, and it regulates PPARγ activity. In vitro, knockdown of XOR inhibits adipogenesis and PPARγ activity while constitutive overexpression increases activity of the PPARγ receptor in both adipocytes and preadipocytes. In vivo, XOR −/− mice demonstrate 50% reduction in adipose mass versus wild-type littermates while obese ob/ob mice exhibit increased concentrations of XOR mRNA and urate in the adipose tissue. We propose that XOR is a novel regulator of adipogenesis and of PPARγ activity and essential for the regulation of fat accretion. Our results identify XOR as a potential therapeutic target for metabolic abnormalities beyond hyperuricemia. [Copyright &y& Elsevier]

Published

2007

18. Oxidant signals and oxidative stress

Author

Finkel, Toren

Subjects

*PHYSIOLOGICAL oxidation, *REACTIVE oxygen species, *CARCINOGENESIS

Abstract

Although oxidants clearly possess the capacity to behave in a random and destructive fashion, growing evidence suggests that in many instances the production of reactive oxygen species is tightly regulated and their downstream targets exquisitely specific. This past year, several notable advances have been made in defining the specific redox-dependent targets of intracellular oxidants, as well as the myriad pathways that appear to employ oxidants as effector molecules. These new studies have significantly altered our understanding of how reactive oxygen species participate in diverse processes from tumourigenesis to ageing. [Copyright &y& Elsevier]

Published

2003

19. TOR and Aging: Less Is More.

Author

Schieke, Stefan M. and Finkel, Toren

Subjects

METABOLISM, BIOCHEMISTRY, LONGEVITY, MITOCHONDRIA

Abstract

Metabolism and mitochondrial activity are thought to be important determinants of life span. A new study in this issue of Cell Metabolism () suggests that the TOR pathway controls mitochondrial respiration in yeast and that the harder mitochondria work, the longer yeast live. [Copyright &y& Elsevier]

Published

2007

20. Tissue-Resident PDGFRα+ Progenitor Cells Contribute to Fibrosis versus Healing in a Context- and Spatiotemporally Dependent Manner.

Author

Santini, Maria Paola, Malide, Daniela, Hoffman, Gabriel, Pandey, Gaurav, D'Escamard, Valentina, Nomura-Kitabayashi, Aya, Rovira, Ilsa, Kataoka, Hiroshi, Ochando, Jordi, Harvey, Richard P., Finkel, Toren, and Kovacic, Jason C.

Abstract

PDGFRα+ mesenchymal progenitor cells are associated with pathological fibro-adipogenic processes. Conversely, a beneficial role for these cells during homeostasis or in response to revascularization and regeneration stimuli is suggested, but remains to be defined. We studied the molecular profile and function of PDGFRα+ cells in order to understand the mechanisms underlying their role in fibrosis versus regeneration. We show that PDGFRα+ cells are essential for tissue revascularization and restructuring through injury-stimulated remodeling of stromal and vascular components, context-dependent clonal expansion, and ultimate removal of pro-fibrotic PDGFRα+-derived cells. Tissue ischemia modulates the PDGFRα+ phenotype toward cells capable of remodeling the extracellular matrix and inducing cell-cell and cell-matrix adhesion, likely favoring tissue repair. Conversely, pathological healing occurs if PDGFRα+-derived cells persist as terminally differentiated mesenchymal cells. These studies support a context-dependent "yin-yang" biology of tissue-resident mesenchymal progenitor cells, which possess an innate ability to limit injury expansion while also promoting fibrosis in an unfavorable environment. • Skeletal muscle PDGFRα+ cells have dual pro-regenerative and pro-fibrotic functions • PDGFRα+ cells are necessary for the restoration of tissue integrity after ischemia • PDGFRα+ cells remodel extracellular matrix and support revascularization after ischemia • PDGFRα+ cells induce pathological outcomes if they persist as differentiated cells Santini et al. show that progenitor PDGFRα+ cells residing in skeletal muscle are mesenchymal stromal cells with a dual function, which on the one hand can stabilize newly formed blood vessels and limit injury expansion after ischemia, but on the other hand are also capable of promoting fibrosis in an unfavorable environment. [ABSTRACT FROM AUTHOR]

Published

2020

21. Neutrophils with a License to Kill: Permeabilized, Not Stirred

Author

Finkel, Toren

Subjects

*NEUTROPHILS, *MICROORGANISMS, *OXIDASES

Abstract

The neutrophil responds to invading microorganisms in part by assembling the NADPH oxidase complex and producing superoxide radicals. Relatively little is known about the intracellular assembly or activation of the oxidase, but Brown et al. in the January issue of Molecular Cell provide a useful strategy involving permeabilized neutrophils to tackle this question. [Copyright &y& Elsevier]

Published

2003

22. Metabolic Regulation of Cell Fate and Function.

Author

Ghosh-Choudhary, Shohini, Liu, Jie, and Finkel, Toren

Subjects

*CELL physiology, *METABOLIC regulation, *CELLULAR control mechanisms, *ESSENTIAL fatty acids, *ACETYLCOENZYME A, *CELL metabolism

Abstract

Increasing evidence implicates metabolic pathways as key regulators of cell fate and function. Although the metabolism of glucose, amino acids, and fatty acids is essential to maintain overall energy homeostasis, the choice of a given metabolic pathway and the levels of particular substrates and intermediates increasingly appear to modulate specific cellular activities. This connection is likely related to the growing appreciation that molecules such as acetyl-CoA act as a shared currency between metabolic flux and chromatin modification. We review recent evidence for a role of metabolism in modulating cellular function in four distinct contexts. These areas include the immune system, the tumor microenvironment, the fibrotic response, and stem cell function. Together, these examples suggest that metabolic pathways do not simply provide the fuel that powers cellular activities but instead help to shape and determine cellular identity. Metabolites such as acetyl-CoA directly connect metabolism to the regulation of protein function and chromatin modification. The metabolic substrates that cells use provide more than bioenergetics and help to shape cellular identity. Understanding the connection between metabolism and cell fate could usher in a wave of new therapies. [ABSTRACT FROM AUTHOR]

Published

2020

23. E3 ubiquitin ligase ZBTB25 suppresses beta coronavirus infection through ubiquitination of the main viral protease MPro.

Author

Lear, Travis B., Boudreau, Áine N., Lockwood, Karina C., Chu, Elise, Camarco, Daniel P., Qing Cao, Nguyen, Matthew, Evankovich, John W., Finkel, Toren, Yuan Liu, and Chen, Bill B.

Subjects

*UBIQUITIN ligases, *SARS-CoV-2, *COVID-19, *VIRAL proteins, *UBIQUITINATION

Abstract

The main protease of severe acute respiratory syndrome coronavirus 2, Mpro, is a key viral protein essential for viral infection and replication. Mpro has been the target of many pharmacological efforts; however, the host-specific regulation of Mpro protein remains unclear. Here, we report the ubiquitin-proteasome-dependent degradation of Mpro protein in human cells, facilitated by the human E3 ubiquitin ligase ZBTB25. We demonstrate that Mpro has a short half-life that is prolonged via proteasomal inhibition, with its Lys-100 residue serving as a potential ubiquitin acceptor. Using in vitro binding assays, we observed ZBTB25 and Mpro bind to each other in vitro, and using progressive deletional mapping, we further uncovered the required domains for this interaction. Finally, we used an orthologous beta-coronavirus infection model and observed that genetic ablation of ZBTB25 resulted in a more highly infective virus, an effect lost upon reconstitution of ZBTB25 to deleted cells. In conclusion, these data suggest a new mechanism of Mpro protein regulation as well as identify ZBTB25 as an anticoronaviral E3 ubiquitin ligase. [ABSTRACT FROM AUTHOR]

Published

2023

24. Stem Cells and Oxidants: Too Little of a Bad Thing.

Author

Liu, Jie and Finkel, Toren

Abstract

Oxidants are thought to damage cells, and stem cells are viewed as particularly vulnerable to oxidative stress. Now, a new study (Morimoto et al., 2013) suggests that the self-renewal of certain stem cells may actually require reactive oxygen species (ROS). [Copyright &y& Elsevier]

Published

2013

25. Welcome to Drug Discovery Today: Disease Mechanisms.

Author

Bartfai, Tamas and Finkel, Toren

Published

2004

26. Mitochondrial and Redox Regulation of Stem Cell Biology

Author

Finkel, Toren

Published

2010

27. Oxidants, metabolism, and stem cell biology

Author

Liu, Jie, Cao, Liu, and Finkel, Toren

Subjects

*OXIDIZING agents, *METABOLISM, *STEM cells, *OXIDATIVE stress, *LABORATORY mice, *HOMEOSTASIS

Abstract

Abstract: Adult stem cells persist throughout the lifetime of the organism and may therefore require specific mechanisms to limit the effects of chronic oxidative stress. Recently, several instructive genetic mouse models have demonstrated the unique susceptibility of stem cells to perturbations in metabolic or redox homeostasis. These results have implications not only for stem cell biology but also suggest a mechanistic link between intracellular oxidants and the decline in regenerative function that occurs as a normal consequence of aging. [Copyright &y& Elsevier]

Published

2011

28. SIRT1 Functionally Interacts with the Metabolic Regulator and Transcriptional Coactivator PGC-1α.

Author

Nemoto, Shino, Fergusson, Maria M., and Finkel, Toren

Subjects

*ENZYMES, *GENETIC transcription regulation, *MITOCHONDRIA formation, *GENETIC transcription, *GENETIC regulation, *AMINO acids

Abstract

In lower organisms, increased expression of the NAD-dependent deacetylase Sir2 augments lifespan. The mechanism through which this life extension is mediated remains incompletely understood. Here we have examined the cellular effects of overexpression of SIRT1, the closest mammalian ortholog of Sir2. In PC12 cells, increased expression of the NAD-dependent deacetylase SIRT1 reduces cellular oxygen consumption by ∼25%. We further demonstrate that SIRT1 expression can alter the transcriptional activity of the mitochondrial biogenesis coactivator PGC-1α. In addition, SIRT1 and PGC-1α directly interact and can be co-immunoprecipitated as a molecular complex. A single amino acid mutation in the putative ADP-ribosyltransferase domain of SIRT1 inhibits the interaction of SIRT1 with PGC-1α but does not effect the interaction of SIRT1 with either p53 or Foxo3a. We further show that PGC-1α is acetylated in vivo. This acetylation is augmented by treatment with the SIRT1 inhibitor nicotinamide or by expression of the transcriptional coactivator p300. Finally we demonstrate that SIRT1 catalyzes PGC-1α deacetylation both in vitro and in vivo. These results provide a direct link between the sirtuins, a family of proteins linked to lifespan determination and PGC-α, a coactivator that regulates cellular metabolism. [ABSTRACT FROM AUTHOR]

Published

2005

29. Kelch-like protein 42 is a profibrotic ubiquitin E3 ligase involved in systemic sclerosis.

Author

Lear, Travis B., Lockwood§, Karina C., Larsen, Mads, Tuncer, Ferhan, Kennerdell, Jason R., Morse, Christina, Valenzi, Eleanor, Tabib, Tracy, Jurczak, Michael J., Kass, Daniel J., Evankovich, John W., Finkel, Toren, Lafyatis, Robert, Yuan Liu, and Chen, Bill B.

Subjects

*SYSTEMIC scleroderma, *TRANSCRIPTION factors, *PROTEINS, *PULMONARY fibrosis, *CONNECTIVE tissues

Abstract

Systemic scleroderma (SSc) is an autoimmune disease that affects over 2.5 million people globally. SSc results in dysfunctional connective tissues with excessive profibrotic signaling, affecting skin, cardiovascular, and particularly lung tissue. Over three-quarters of individuals with SSc develop pulmonary fibrosis within 5 years, the main cause of SSc mortality. No approved medicines to manage lung SSc currently exist. Recent research suggests that profibrotic signaling by transforming growth factor ⓹ (TGF-β) is directly tied to SSc. Previous studies have also shown that ubiquitin E3 ligases potently control TGF-β signaling through targeted degradation of key regulatory proteins; however, the roles of these ligases in SSc-TGF-β signaling remain unclear. Here we utilized primary SSc patient lung cells for high-throughput screening of TGF-β signaling via high-content imaging of nuclear translocation of the profibrotic transcription factor SMAD family member 2/3 (SMAD2/3). We screened an RNAi library targeting ubiquitin E3 ligases and observed that knockdown of the E3 ligase Kelch-like protein 42 (KLHL42) impairs TGF-β-dependent profibrotic signaling. KLHL42 knockdown reduced fibrotic tissue production and decreased TGF-β-mediated SMAD activation. Using unbiased ubiquitin proteomics, we identified phosphatase 2 regulatory subunit B'epsilon (PPP2R5e) as a KLHL42 substrate. Mechanistic experiments validated ubiquitin-mediated control of PPP2R5e stability through KLHL42. PPP2R5e knockdown exacerbated TGF-β-mediated profibrotic signaling, indicating a role of PPP2R5e in SSc. Our findings indicate that theKLHL42-PPP2R5e axis controls profibrotic signaling in SSc lung fibroblasts. We propose that future studies could investigate whether chemical inhibition of KLHL42 may ameliorate profibrotic signaling in SSc. [ABSTRACT FROM AUTHOR]

Published

2020

30. Endothelial to Mesenchymal Transition in Cardiovascular Disease: JACC State-of-the-Art Review.

Author

Kovacic, Jason C, Dimmeler, Stefanie, Harvey, Richard P, Finkel, Toren, Aikawa, Elena, Krenning, Guido, and Baker, Andrew H

Abstract

Endothelial to mesenchymal transition (EndMT) is a process whereby an endothelial cell undergoes a series of molecular events that lead to a change in phenotype toward a mesenchymal cell (e.g., myofibroblast, smooth muscle cell). EndMT plays a fundamental role during development, and mounting evidence indicates that EndMT is involved in adult cardiovascular diseases (CVDs), including atherosclerosis, pulmonary hypertension, valvular disease, and fibroelastosis. Therefore, the targeting of EndMT may hold therapeutic promise for treating CVD. However, the field faces a number of challenges, including the lack of a precise functional and molecular definition, a lack of understanding of the causative pathological role of EndMT in CVDs (versus being a "bystander-phenomenon"), and a lack of robust human data corroborating the extent and causality of EndMT in adult CVDs. Here, we review this emerging but exciting field, and propose a framework for its systematic advancement at the molecular and translational levels. [ABSTRACT FROM AUTHOR]

Published

2019

31. Strategic Positioning and Biased Activity of the Mitochondrial Calcium Uniporter in Cardiac Muscle.

Author

De La Fuente, Sergio, Fernandez-Sanz, Celia, Vail, Caitlin, Agra, Elorm J., Holmstrom, Kira, Junhui Sun, Mishra, Jyotsna, Williams, Dewight, Finkel, Toren, Murphy, Elizabeth, Joseph, Suresh K., Shey-Shing Sheu, and Csordás, György

Subjects

*MYOCARDIUM physiology, *MITOCHONDRIAL physiology, *BIOENERGETICS, *RYANODINE receptors, *SARCOPLASMIC reticulum, *PROTEIN folding

Abstract

Control of myocardial energetics by Ca2+ signal propagation to the mitochondrial matrix includes local Ca2+ delivery from sarcoplasmic reticulum (SR) ryanodine receptors (RyR2) to the inner mitochondrial membrane (IMM) Ca2+ uniporter (mtCU). mtCU activity in cardiac mitochondria is relatively low, whereas the IMM surface is large, due to extensive cristae folding. Hence, stochastically distributed mtCU may not suffice to support local Ca2+ transfer. We hypothesized that mtCU concentrated at mitochondria-SR associations would promote the effective Ca2+ transfer. mtCU distribution was determined by tracking MCU and EMRE, the proteins essential for channel formation. Both proteins were enriched in the IMM-outer mitochondrial membrane (OMM) contact point submitochondrial fraction and, as super-resolution microscopy revealed, located more to the mitochondrial periphery (inner boundary membrane) than inside the cristae, indicating high accessibility to cytosol-derived Ca2+ inputs. Furthermore, MCU immunofluorescence distribution was biased toward the mitochondria-SR interface (RyR2), and this bias was promoted by Ca2+ signaling activity in intact cardiomyocytes. The SR fraction of heart homogenate contains mitochondria with extensive SR associations, and these mitochondria are highly enriched in EMRE. Size exclusion chromatography suggested for EMRE- and MCU-containing complexes a wide size range and also revealed MCU-containing complexes devoid of EMRE (thus disabled) in the mitochondrial but not the SR fraction. Functional measurements suggested more effective mtCU-mediated Ca2+ uptake activity by the mitochondria of the SR than of the mitochondrial fraction. Thus, mtCU "hot spots" can be formed at the cardiac muscle mitochondria-SR associations via localization and assembly bias, serving local Ca2+ signaling and the excitation-energetics coupling. [ABSTRACT FROM AUTHOR]

Published

2016

32. Oxidants Painting the Cysteine Chapel: Redox Regulation of PTPs.

Author

Xu, Dong, Rovira, Ilsa I., and Finkel, Toren

Subjects

*OXIDIZING agents, *REACTIVE oxygen species

Abstract

Growth factors and cytokines appear to stimulate the intracellular production of reactive oxygen species (ROS). Evidence suggests that this alteration in the cellular redox state is essential for downstream signaling, but the precise mechanism has remained elusive. A new study now demonstrates that ligand-stimulated intracellular hydrogen peroxide can specifically and reversibly regulate the activity of protein tyrosine phosphatases. [Copyright &y& Elsevier]

Published

2002

33. The Essential Autophagy Gene ATG7 Modulates Organ Fibrosis via Regulation of Endothelial-to-Mesenchymal Transition.

Author

Singh, Krishna K., Lovren, Fina, Yi Pan, Quan, Adrian, Ramadan, Azza, Matkar, Pratiek N., Ehsan, Mehroz, Sandhu, Paul, Mantella, Laura E., Gupta, Nandini, Hwee Teoh, Parotto, Matteo, Arata Tabuchi, Kuebler, Wolfgang M., Al-Omran, Mohammed, Finkel, Toren, and Verma, Subodh

Subjects

*AUTOPHAGY, *VESICLES (Cytology), *PULMONARY fibrosis, *LUNG diseases, *FIBROBLASTS

Abstract

Pulmonary fibrosis is a progressive disease characterized by fibroblast proliferation and excess deposition of collagen and other extracellular matrix components. Although the origin of fibroblasts is multifactorial, recent data implicate endothelial-to- mesenchymal transition as an important source of fibroblasts. We report herein that loss of the essential autophagy gene ATG7 in endothelial cells (ECs) leads to impaired autophagic flux accompanied by marked changes in EC architecture, loss of endothelial, and gain of mesenchymal markers consistent with endothelial-to-mesenchymal transition. Loss of ATG7 also up-regulates TGFβ signaling and key pro-fibrotic genes in vitro. In vivo, EC-specific ATG7 knock-out mice exhibit a basal reduction in endothelial-specific markers and demonstrate an increased susceptibility to bleomycin-induced pulmonary fibrosis and collagen accumulation. Our findings help define the role of endothelial autophagy as a potential therapeutic target to limit organ fibrosis, a condition for which presently there are no effective available treatments. [ABSTRACT FROM AUTHOR]

Published

2015

34. Cyclin B1/Cdk1 Coordinates Mitochondrial Respiration for Cell-Cycle G2/M Progression.

Author

Wang, Zhaoqing, Fan, Ming, Candas, Demet, Zhang, Tie-Qiao, Qin, Lili, Eldridge, Angela, Wachsmann-Hogiu, Sebastian, Ahmed, Kazi?M., Chromy, Brett?A., Nantajit, Danupon, Duru, Nadire, He, Fuchu, Chen, Min, Finkel, Toren, Weinstein, Lee?S., and Li, Jian?Jian

Subjects

*CYCLIN-dependent kinases, *REGULATION of respiration, *CELL cycle, *MITOCHONDRIAL proteins, *PHOSPHORYLATION, *OXYGEN consumption

Abstract

Summary: A substantial amount of mitochondrial energy is required for cell-cycle progression. The mechanisms underlying the coordination of the mitochondrial respiration with cell-cycle progression, especially the G2/M transition, remain to be elucidated. Here, we show that a fraction of cyclin B1/Cdk1 proteins localizes to the matrix of mitochondria and phosphorylates a cluster of mitochondrial proteins, including the complex I (CI) subunits in the respiratory chain. Cyclin B1/Cdk1-mediated CI phosphorylation enhances CI activity, whereas deficiency of such phosphorylation in each of the relevant CI subunits results in impairment of CI function. Mitochondria-targeted cyclin B1/Cdk1 increases mitochondrial respiration with enhanced oxygen consumption and ATP generation, which provides cells with efficient bioenergy for G2/M transition and shortens overall cell-cycle time. Thus, cyclin B1/Cdk1-mediated phosphorylation of mitochondrial substrates allows cells to sense and respond to increased energy demand for G2/M transition and, subsequently, to upregulate mitochondrial respiration for successful cell-cycle progression. [Copyright &y& Elsevier]

Published

2014

35. Caenorhabditis elegans UCP4 Protein Controls Complex II-mediated Oxidative Phosphorylation through Succinate Transport.

Author

Pfeiffer, Matthew, Kayzer, Ernst-Bernhard, Xianmei Yang, Abramson, Ellen, Kenaston, M. Alexander, Lago, Cory U., Herng-Hsiang Lo, Sedensky, Margaret M., Lunceford, Adam, Clarke, Catherine F., Wu, Sarah J., McLeod, Chris, Finkel, Toren, Morgan, Philip G., and Mills, Edward M.

Subjects

*CAENORHABDITIS elegans, *ELECTRON transport, *MITOCHONDRIAL membranes, *INSULIN, *PHOSPHORYLATION

Abstract

The novel uncoupling proteins (UCP2-5) are implicated in the mitochondrial control of oxidant production, insulin signaling, and aging. Attempts to understand their functions have been complicated by overlapping expression patterns in most organisms. Caenorhabditis elegans nematodes are unique because they express only one UCP ortholog, ceUCP4 (ucp4). Here, we performed detailed metabolic analyzes in genetically modified nematodes to define the function of the ceUCP4. The knock-out mutant ucp4 (ok195) exhibited sharply decreased mitochondrial succinate-driven (complex II) respiration. However, respiratory coupling and electron transport chain function were normal in ucp4 mitochondria. Surprisingly, isolated ucp4 mitochondria showed markedly decreased succinate uptake. Similarly, ceUCP4 inhibition blocked succinate respiration and import in wild type mitochondria. Genetic and pharmacologic inhibition of complex I function was selectively lethal to ucp4 worms, arguing that ceUCP4-regulated succinate transport is required for optimal complex II function in vivo. Additionally, ceUCP4 deficiency prolonged lifespan in the short-lived mev1 mutant that exhibits complex II-generated oxidant production. These results identify a novel function for ceUCP4 in the regulation of complex II-based metabolism through an unexpected mechanism involving succinate transport. [ABSTRACT FROM AUTHOR]

Published

2011

36. Mitochondrial Metabolism Modulates Differentiation and Teratoma Formation Capacity in Mouse Embryonic Stem Cells.

Author

Schieke, Stefan M., Mingchao Ma, Liu Cao, McCoy Jr., J. Philip, Chengyu Liu, Hensel, Nancy F., Barrett, A. John, Boehm, Manfred, and Finkel, Toren

Subjects

*MITOCHONDRIA, *TERATOMA, *EMBRYONIC stem cells, *IMMUNOSUPPRESSIVE agents, *CELL membranes, *RAPAMYCIN

Abstract

Relatively little is known regarding the role of mitochondrial metabolism in stem cell biology. Here we demonstrate that mouse embryonic stem cells sorted for low and high resting mitochondrial membrane potential (ΔΨmL and ΔΨmH) are indistinguishable morphologically and by the expression of pluripotency markers, whereas markedly differing in metabolic rates. Interestingly, ΔΨmL cells are highly efficient at in vitro mesodermal differentiation yet fail to efficiently form teratomas in vivo, whereasΔΨmH cells behave in the opposite fashion. We further demonstrate that ΔΨm reflects the degree of overall mammalian target of rapamycin (mTOR) activation and that the mTOR inhibitor rapamycin reduces metabolic rate, augments differentiation, and inhibits tumor formation of the mouse embryonic stem cells with a high metabolic rate. Taken together, our results suggest a coupling between intrinsic metabolic parameters and stem cell fate that might form a basis for novel enrichment strategies and therapeutic options. [ABSTRACT FROM AUTHOR]

Published

2008

37. Redox-based regulation of signal transduction: Principles, pitfalls, and promises

Author

Janssen-Heininger, Yvonne M.W., Mossman, Brooke T., Heintz, Nicholas H., Forman, Henry J., Kalyanaraman, Balaraman, Finkel, Toren, Stamler, Jonathan S., Rhee, Sue Goo, and van der Vliet, Albert

Subjects

*CELLULAR signal transduction, *AEROBIC metabolism, *PROKARYOTES, *MAMMALS

Abstract

Abstract: Oxidants are produced as a by-product of aerobic metabolism, and organisms ranging from prokaryotes to mammals have evolved with an elaborate and redundant complement of antioxidant defenses to confer protection against oxidative insults. Compelling data now exist demonstrating that oxidants are used in physiological settings as signaling molecules with important regulatory functions controlling cell division, migration, contraction, and mediator production. These physiological functions are carried out in an exquisitely regulated and compartmentalized manner by mild oxidants, through subtle oxidative events that involve targeted amino acids in proteins. The precise understanding of the physiological relevance of redox signal transduction has been hampered by the lack of specificity of reagents and the need for chemical derivatization to visualize reversible oxidations. In addition, it is difficult to measure these subtle oxidation events in vivo. This article reviews some of the recent findings that illuminate the significance of redox signaling and exciting future perspectives. We also attempt to highlight some of the current pitfalls and the approaches needed to advance this important area of biochemical and biomedical research. [Copyright &y& Elsevier]

Published

2008

38. The Mammalian Longevity-associated Gene Product p66shc Regulates Mitochondrial Metabolism.

Author

Nemoto, Shino, Combs, Christian A., French, Stephanie, Bong-Hyun Ahn, Fergusson, Maria M., Balaban, Robert S., and Finkel, Toren

Subjects

*BLOOD testing, *LABORATORY mice, *MITOCHONDRIA, *FIBROBLASTS, *RODENTS, *BIOCHEMISTRY

Abstract

Previous studies have determined that mice with a homozygous deletion in the adapter protein p66shc have an extended life span and that cells derived from these mice exhibit lower levels of reactive oxygen species. Here we demonstrate that a fraction of p66shc localizes to the mitochondria and that p66shc-/- fibroblasts have altered mitochondrial energetics. In particular, despite similar cytochrome content, under basal conditions, the oxygen consumption of spontaneously immortalized p6shc-/- mouse embryonic fibroblasts were lower than similarly maintained wild type cells. Differences in oxygen consumption were particularly evident under chemically uncoupled conditions, demonstrating that p66shc-/- cells have a reduction in both their resting and maximal oxidative capacity. We further demonstrate that reconstitution of p66shc expression in p66shc-/- cells increases oxygen consumption. The observed defect in oxidative capacity seen in p66shc-/- cells is partially offset by augmented levels of aerobic glycolysis. This metabolic switch is manifested by p66shc-/- cells exhibiting an increase in lactate production and a stricter requirement for extracellular glucose in order to maintain intracellular ATP levels. In addition, using an in vivo NADH photobleaching technique, we demonstrate that mitochondrial NADH metabolism is reduced in p6shc-/- cells. These results demonstrate that p66shc regulates mitochondrial oxidative capacity and suggest that p66shc may extend life span by repartitioning metabolic energy conversion away from oxidative and toward glycolytic pathways. [ABSTRACT FROM AUTHOR]

Published

2006

39. Chimeric vascular endothelial growth factor fusion protein selectively inhibits Flk-1 endothelial progenitor cells

Author

Hill, Jonathan M., Backer, Marina V., Backer, Joseph M., and Finkel, Toren

Published

2002