40 results on '"Petrascheck, M"'
Search Results
2. The DrugAge database of aging-related drugs
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Barardo, D, Thornton, D, Thoppil, H, Walsh, M, Sharifi, S, Ferreira, S, Anžič, A, Fernandes, M, Monteiro, P, Grum, T, Cordeiro, R, De-Souza, EA, Budovsky, A, Araujo, N, Gruber, J, Petrascheck, M, Fraifeld, VE, Zhavoronkov, A, Moskalev, A, and de Magalhães, JP
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FOS: Computer and information sciences ,Pharmacology ,Lifespan ,Bioinformatics ,Compound ,Longevity ,Functional genomics - Abstract
Aging is a major worldwide medical challenge. Not surprisingly, identifying drugs and compounds that extend lifespan in model organisms is a growing research area. Here, we present DrugAge (http://genomics.senescence.info/drugs/), a curated database of lifespan-extending drugs and compounds. At the time of writing, DrugAge contains 1316 entries featuring 418 different compounds from studies across 27 model organisms, including worms, flies, yeast and mice. Data were manually curated from 324 publications. Using drug–gene interaction data, we also performed a functional enrichment analysis of targets of lifespan-extending drugs. Enriched terms include various functional categories related to glutathione and antioxidant activity, ion transport and metabolic processes. In addition, we found a modest but significant overlap between targets of lifespan-extending drugs and known aging-related genes, suggesting that some but not most aging-related pathways have been targeted pharmacologically in longevity studies. DrugAge is freely available online for the scientific community and will be an important resource for biogerontologists., Aging Cell, 16 (3), ISSN:1474-9718, ISSN:1474-9728, ISSN:1474-9726
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- 2017
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3. DNA looping induced by a transcriptional enhancer in vivo
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Petrascheck, M., primary
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- 2005
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4. Activity-dependent synthesis of Emerin gates neuronal plasticity by regulating proteostasis.
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Xie Y, Wang R, McClatchy DB, Ma Y, Diedrich J, Sanchez-Alavez M, Petrascheck M, Yates JR, and Cline HT
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Neurons dynamically regulate their proteome in response to sensory input, a key process underlying experience-dependent plasticity. We characterized the visual experience-dependent nascent proteome within a brief, defined time window after stimulation using an optimized metabolic labeling approach. Visual experience induced cell type-specific and age-dependent alterations in the nascent proteome, including proteostasis-related processes. We identified Emerin as the top activity-induced candidate plasticity protein and demonstrated that its rapid activity-induced synthesis is transcription-independent. In contrast to its nuclear localization and function in myocytes, activity-induced neuronal Emerin is abundant in the endoplasmic reticulum and broadly inhibits protein synthesis, including translation regulators and synaptic proteins. Downregulating Emerin shifted the dendritic spine population from predominantly mushroom morphology to filopodia and decreased network connectivity. In mice, decreased Emerin reduced visual response magnitude and impaired visual information processing. Our findings support an experience-dependent feed-forward role for Emerin in temporally gating neuronal plasticity by negatively regulating translation.
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- 2024
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5. Multiple Targets, One Goal: Compounding life-extending effects through Polypharmacology.
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Avchaciov K, Clay KJ, Denisov K, Burmistrova O, Petrascheck M, and Fedichev P
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Analysis of lifespan-extending compounds suggested the most effective geroprotectors target multiple biogenic amine receptors. To test this hypothesis, we used graph neural networks to predict such polypharmacological compounds and evaluated them in C. elegans . Over 70% of the selected compounds extended lifespan, with effect sizes in the top 5% compared to the DrugAge database. This reveals that rationally designing polypharmacological compounds enables the design of geroprotectors with exceptional efficacy., Competing Interests: AK, KD, OB, and PF are employed by Gero and declare no conflict of interest.
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- 2024
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6. Quantifying Food Intake in Caenorhabditis elegans by Measuring Bacterial Clearance.
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Clark C, To A, and Petrascheck M
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- Animals, Aging, Longevity, Bacteria metabolism, Eating, Caenorhabditis elegans metabolism, Caenorhabditis elegans Proteins metabolism
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Feeding is an essential biological process for an organism's growth, reproduction, and survival. This assay aims to measure the food intake of Caenorhabditis elegans (C. elegans), an important parameter when studying the genetics of aging or metabolism. In most species, feeding is determined by measuring the difference between the amount of food provided and the amount left after a given time interval. The method presented here uses the same strategy to determine the feeding of C. elegans. It measures the amount of bacteria, the food source of C. elegans, cleared within 72 h. This method uses 96-well microtiter plates and has allowed the screening of hundreds of drugs for their ability to modulate food intake at a speed and depth not possible in other animal models. The strength of this assay is that it allows to measure feeding and lifespan simultaneously and directly measures the disappearance of food and, thus, is based on the same principles used for other organisms, facilitating species-to-species comparison.
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- 2024
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7. Proteostasis is differentially modulated by inhibition of translation initiation or elongation.
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Clay KJ, Yang Y, Clark C, and Petrascheck M
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- Animals, Transcription Factors genetics, Transcription Factors metabolism, Proteostasis, Protein Aggregates, Proteasome Endopeptidase Complex metabolism, Caenorhabditis elegans physiology, Heat Shock Transcription Factors genetics, Heat Shock Transcription Factors metabolism, Caenorhabditis elegans Proteins genetics, Caenorhabditis elegans Proteins metabolism
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Recent work has revealed an increasingly important role for mRNA translation in maintaining proteostasis. Here, we use chemical inhibitors targeting discrete steps of translation to compare how lowering the concentration of all or only translation initiation-dependent proteins rescues Caenorhabditis elegans from proteotoxic stress. We systematically challenge proteostasis and show that pharmacologically inhibiting translation initiation or elongation elicits a distinct protective profile. Inhibiting elongation protects from heat and proteasome dysfunction independently from HSF-1 but does not protect from age-associated protein aggregation. Conversely, inhibition of initiation protects from heat and age-associated protein aggregation and increases lifespan, dependent on hsf-1 , but does not protect from proteotoxicity caused by proteasome dysfunction. Surprisingly, we find that the ability of the translation initiation machinery to control the concentration of newly synthesized proteins depends on HSF-1. Inhibition of translation initiation in wild-type animals reduces the concentration of newly synthesized proteins but increases it in hsf-1 mutants. Our findings suggest that the HSF-1 pathway is not only a downstream target of translation but also directly cooperates with the translation initiation machinery to control the concentration of newly synthesized proteins to restore proteostasis., Competing Interests: KC, MP is a scientific founder and advisor to Cyclone Therapeutics, Inc, a biotech company developing therapeutics targeting translation, YY, CC No competing interests declared, (© 2023, Clay et al.)
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- 2023
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8. Targeting Clic1 for the treatment of obesity: A novel therapeutic strategy to reduce food intake and body weight.
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Zapata RC, Zhang D, Yoon D, Nasamran CA, Chilin-Fuentes DR, Libster A, Chaudry BS, Lopez-Valencia M, Ponnalagu D, Singh H, Petrascheck M, and Osborn O
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- Animals, Mice, Mice, Obese, Body Weight, Mice, Knockout, Eating, Chloride Channels genetics, Antigens, Neoplasm, Proteins, Obesity, Weight Gain
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Objective: Despite great advances in obesity therapeutics in recent years, there is still a need to identify additional therapeutic targets for the treatment of this disease. We previously discovered a signature of genes, including Chloride intracellular channel 1 (Clic1), whose expression was associated with drug-induced weight gain, and in these studies, we assess the effect of Clic1 inhibition on food intake and body weight in mice., Methods: We studied the impact of Clic1 inhibition in mouse models of binge-eating, diet-induced obese mice and genetic models of obesity (Magel2 KO mice)., Results: Clic1 knockout (KO) mice ate significantly less and had a lower body weight than WT littermates when either fed chow or high fat diet. Furthermore, pharmacological inhibition of Clic1 in diet-induced obese mice resulted in suppression of food intake and promoted highly efficacious weight loss. Clic1 inhibition also reduced food intake in binge-eating models and hyperphagic Magel2 KO mice. We observed that chronic obesity resulted in a significant change in subcellular localization of Clic1 with an increased ratio of Clic1 in the membrane in the obese state. These observations provide a novel therapeutic strategy to block Clic1 translocation as a potential mechanism to reduce food intake and lower body weight., Conclusions: These studies attribute a novel role of Clic1 as a driver of food intake and overconsumption. In summary, we have identified hypothalamic expression of Clic1 plays a key role in food intake, providing a novel therapeutic target to treat overconsumption that is the root cause of modern obesity., (Copyright © 2023 The Authors. Published by Elsevier GmbH.. All rights reserved.)
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- 2023
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9. Adipocytes control food intake and weight regain via Vacuolar-type H + ATPase.
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Zapata RC, Carretero M, Reis FCG, Chaudry BS, Ofrecio J, Zhang D, Sasik R, Ciaraldi T, Petrascheck M, and Osborn O
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- Adipocytes metabolism, Animals, Caenorhabditis elegans genetics, Caenorhabditis elegans metabolism, Eating physiology, Humans, Mice, Mice, Inbred C57BL, Mice, Obese, Vacuolar Proton-Translocating ATPases genetics, Weight Gain, Weight Loss, Diet, High-Fat adverse effects, Obesity genetics, Obesity metabolism, Vacuolar Proton-Translocating ATPases metabolism
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Energy metabolism becomes dysregulated in individuals with obesity and many of these changes persist after weight loss and likely play a role in weight regain. In these studies, we use a mouse model of diet-induced obesity and weight loss to study the transcriptional memory of obesity. We found that the 'metabolic memory' of obesity is predominantly localized in adipocytes. Utilizing a C. elegans-based food intake assay, we identify 'metabolic memory' genes that play a role in food intake regulation. We show that expression of ATP6v0a1, a subunit of V-ATPase, is significantly induced in both obese mouse and human adipocytes that persists after weight loss. C. elegans mutants deficient in Atp6v0A1/unc32 eat less than WT controls. Adipocyte-specific Atp6v0a1 knockout mice have reduced food intake and gain less weight in response to HFD. Pharmacological disruption of V-ATPase assembly leads to decreased food intake and less weight re-gain. In summary, using a series of genetic tools from invertebrates to vertebrates, we identify ATP6v0a1 as a regulator of peripheral metabolic memory, providing a potential target for regulation of food intake, weight loss maintenance and the treatment of obesity., (© 2022. The Author(s).)
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- 2022
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10. A chemical biology approach to identifying molecular pathways associated with aging.
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Currais A, Huang L, Petrascheck M, Maher P, and Schubert D
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- Animals, Brain metabolism, Mice, Mice, Transgenic, Mitochondria, Aging genetics, Alzheimer Disease drug therapy, Alzheimer Disease genetics
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The understanding of how aging contributes to dementia remains obscure. To address this problem, a chemical biology approach was used employing CAD031, an Alzheimer's disease (AD) drug candidate identified using a discovery platform based upon phenotypic screens that mimic toxicities associated with the aging brain. Since CAD031 has therapeutic efficacy when fed to old symptomatic transgenic AD mice, the chemical biology hypothesis is that it can be used to determine the molecular pathways associated with age-related disease by identifying those that are modified by the compound. Here we show that when CAD031 was fed to rapidly aging SAMP8 mice starting in the last quadrant of their lifespan, it reduced many of the changes in gene, protein, and small molecule expression associated with mitochondrial aging, maintaining mitochondria at the younger molecular phenotype. Network analysis integrating the metabolomics and transcription data followed by mechanistic validation showed that CAD031 targets acetyl-CoA and fatty acid metabolism via the AMPK/ACC1 pathway. Importantly, CAD031 extended the median lifespan of SAMP8 mice by about 30%. These data show that specific alterations in mitochondrial composition and metabolism highly correlate with aging, supporting the use AD drug candidates that limit physiological aging in the brain.
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- 2021
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11. Rapamycin-mediated mouse lifespan extension: Late-life dosage regimes with sex-specific effects.
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Strong R, Miller RA, Bogue M, Fernandez E, Javors MA, Libert S, Marinez PA, Murphy MP, Musi N, Nelson JF, Petrascheck M, Reifsnyder P, Richardson A, Salmon AB, Macchiarini F, and Harrison DE
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- Animals, Antibiotics, Antineoplastic pharmacology, Female, Male, Mice, Sex Factors, Sirolimus pharmacology, Antibiotics, Antineoplastic therapeutic use, Longevity drug effects, Sirolimus therapeutic use
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To see if variations in timing of rapamycin (Rapa), administered to middle aged mice starting at 20 months, would lead to different survival outcomes, we compared three dosing regimens. Initiation of Rapa at 42 ppm increased survival significantly in both male and female mice. Exposure to Rapa for a 3-month period led to significant longevity benefit in males only. Protocols in which each month of Rapa treatment was followed by a month without Rapa exposure were also effective in both sexes, though this approach was less effective than continuous exposure in female mice. Interpretation of these results is made more complicated by unanticipated variation in patterns of weight gain, prior to the initiation of the Rapa treatment, presumably due to the use of drug-free food from two different suppliers. The experimental design included tests of four other drugs, minocycline, β-guanidinopropionic acid, MitoQ, and 17-dimethylaminoethylamino-17-demethoxygeldanamycin (17-DMAG), but none of these led to a change in survival in either sex., (© 2020 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.)
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- 2020
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12. The aging transcriptome: read between the lines.
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Perez-Gomez A, Buxbaum JN, and Petrascheck M
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- Brain, Gene Expression Profiling, Gene Expression Regulation, Transcriptome genetics
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The increasing sophistication of gene expression technologies has given rise to the idea that aging could be understood by analyzing transcriptomes. Mapping trajectories of gene expression changes in aging organisms, across different tissues and brain regions has provided insights on how biological functions change with age. However, recent publications suggest that transcriptional regulation itself deteriorates with age. Loss of transcriptional regulation will lead to non-regulated gene expression changes, but current analysis strategies were not designed to disentangle mixtures of regulated and non-regulated changes. Disentangling transcriptional data to distinguish adaptive, regulatory changes, from those that are the consequence of the age-associated deterioration is likely to create an analytical challenge but promises to unlock yet poorly understood aspects of many age-associated transcriptomes., (Copyright © 2020 Elsevier Ltd. All rights reserved.)
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- 2020
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13. Design and Analysis of Pharmacological Studies in Aging.
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Clay KJ and Petrascheck M
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- Aging drug effects, Animals, Caenorhabditis elegans drug effects, Longevity drug effects, Phenotype, Aging genetics, Caenorhabditis elegans genetics, Longevity genetics, Mutation genetics
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Measuring lifespan of the model organism, Caenorhabditis elegans, in a 96-well format enables the screening of large chemical libraries to identify biologically active molecules. Furthermore, the wide availability of these animals with specific genetic mutations allows the identification of genes that influence lifespan, and by extension, age-related biological pathways. Here, we present a method for measuring the lifespan of C. elegans in 96-well microtiter plates to identify and study pharmacologically active molecules that extend lifespan. The format of this assay is readily adapted for automated liquid handling systems and imaging of phenotypes.
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- 2020
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14. Elevating acetyl-CoA levels reduces aspects of brain aging.
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Currais A, Huang L, Goldberg J, Petrascheck M, Ates G, Pinto-Duarte A, Shokhirev MN, Schubert D, and Maher P
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- Acetyl Coenzyme A drug effects, Acetyl Coenzyme A metabolism, Acetyl-CoA Carboxylase genetics, Acetylation drug effects, Aging pathology, Alzheimer Disease physiopathology, Animals, Brain diagnostic imaging, Brain pathology, Curcumin analogs & derivatives, Curcumin pharmacology, Humans, Memory drug effects, Memory physiology, Mice, Mitochondria drug effects, Protein Processing, Post-Translational drug effects, Signal Transduction drug effects, Aging drug effects, Alzheimer Disease drug therapy, Brain drug effects, Mitochondria metabolism
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Because old age is the greatest risk factor for dementia, a successful therapy will require an understanding of the physiological changes that occur in the brain with aging. Here, two structurally distinct Alzheimer's disease (AD) drug candidates, CMS121 and J147, were used to identify a unique molecular pathway that is shared between the aging brain and AD. CMS121 and J147 reduced cognitive decline as well as metabolic and transcriptional markers of aging in the brain when administered to rapidly aging SAMP8 mice. Both compounds preserved mitochondrial homeostasis by regulating acetyl-coenzyme A (acetyl-CoA) metabolism. CMS121 and J147 increased the levels of acetyl-CoA in cell culture and mice via the inhibition of acetyl-CoA carboxylase 1 (ACC1), resulting in neuroprotection and increased acetylation of histone H3K9 in SAMP8 mice, a site linked to memory enhancement. These data show that targeting specific metabolic aspects of the aging brain could result in treatments for dementia., Competing Interests: AC, LH, JG, MP, GA, AP, MS, PM No competing interests declared, DS is an unpaid advisor for Abrexa Pharmaceuticals, a company working on the development of J147 for AD therapy. The Salk Institute holds the patents for CMS121 and J147, (© 2019, Currais et al.)
- Published
- 2019
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15. Pharmacological convergence reveals a lipid pathway that regulates C. elegans lifespan.
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Chen AL, Lum KM, Lara-Gonzalez P, Ogasawara D, Cognetta AB 3rd, To A, Parsons WH, Simon GM, Desai A, Petrascheck M, Bar-Peled L, and Cravatt BF
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- Animals, Benzodioxoles chemistry, Caenorhabditis elegans metabolism, Endocannabinoids metabolism, Enzyme Inhibitors chemistry, Molecular Structure, Monoacylglycerol Lipases metabolism, Piperidines chemistry, Benzodioxoles pharmacology, Caenorhabditis elegans drug effects, Endocannabinoids antagonists & inhibitors, Enzyme Inhibitors pharmacology, Longevity drug effects, Monoacylglycerol Lipases antagonists & inhibitors, Piperidines pharmacology
- Abstract
Phenotypic screening has identified small-molecule modulators of aging, but the mechanism of compound action often remains opaque due to the complexities of mapping protein targets in whole organisms. Here, we combine a library of covalent inhibitors with activity-based protein profiling to coordinately discover bioactive compounds and protein targets that extend lifespan in Caenorhabditis elegans. We identify JZL184-an inhibitor of the mammalian endocannabinoid (eCB) hydrolase monoacylglycerol lipase (MAGL or MGLL)-as a potent inducer of longevity, a result that was initially perplexing as C. elegans does not possess an MAGL ortholog. We instead identify FAAH-4 as a principal target of JZL184 and show that this enzyme, despite lacking homology with MAGL, performs the equivalent metabolic function of degrading eCB-related monoacylglycerides in C. elegans. Small-molecule phenotypic screening thus illuminates pure pharmacological connections marking convergent metabolic functions in distantly related organisms, implicating the FAAH-4/monoacylglyceride pathway as a regulator of lifespan in C. elegans.
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- 2019
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16. Loss of genomic integrity induced by lysosphingolipid imbalance drives ageing in the heart.
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Ahuja G, Bartsch D, Yao W, Geissen S, Frank S, Aguirre A, Russ N, Messling JE, Dodzian J, Lagerborg KA, Vargas NE, Muck JS, Brodesser S, Baldus S, Sachinidis A, Hescheler J, Dieterich C, Trifunovic A, Papantonis A, Petrascheck M, Klinke A, Jain M, Valenzano DR, and Kurian L
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- Animals, Curcumin chemistry, Curcumin pharmacology, DNA Damage drug effects, Energy Metabolism, Epigenesis, Genetic, Evolution, Molecular, Fundulidae, Gene Expression Profiling, Gene Expression Regulation, Genomics methods, Histone Acetyltransferases chemistry, Histone Acetyltransferases metabolism, Histone Deacetylase Inhibitors chemistry, Histone Deacetylase Inhibitors pharmacology, Histones metabolism, Humans, Models, Molecular, Myocytes, Cardiac metabolism, Sphingosine analogs & derivatives, Sphingosine metabolism, Structure-Activity Relationship, Vertebrates genetics, Vertebrates metabolism, Aging genetics, Aging metabolism, Genetic Variation, Genomic Instability, Myocardium metabolism, Sphingolipids metabolism
- Abstract
Cardiac dysfunctions dramatically increase with age. Revealing a currently unknown contributor to cardiac ageing, we report the age-dependent, cardiac-specific accumulation of the lysosphingolipid sphinganine (dihydrosphingosine, DHS) as an evolutionarily conserved hallmark of the aged vertebrate heart. Mechanistically, the DHS-derivative sphinganine-1-phosphate (DHS1P) directly inhibits HDAC1, causing an aberrant elevation in histone acetylation and transcription levels, leading to DNA damage. Accordingly, the pharmacological interventions, preventing (i) the accumulation of DHS1P using SPHK2 inhibitors, (ii) the aberrant increase in histone acetylation using histone acetyltransferase (HAT) inhibitors, (iii) the DHS1P-dependent increase in transcription using an RNA polymerase II inhibitor, block DHS-induced DNA damage in human cardiomyocytes. Importantly, an increase in DHS levels in the hearts of healthy young adult mice leads to an impairment in cardiac functionality indicated by a significant reduction in left ventricular fractional shortening and ejection fraction, mimicking the functional deterioration of aged hearts. These molecular and functional defects can be partially prevented in vivo using HAT inhibitors. Together, we report an evolutionarily conserved mechanism by which increased DHS levels drive the decline in cardiac health., (© 2019 The Authors.)
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- 2019
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17. A phenotypic Caenorhabditis elegans screen identifies a selective suppressor of antipsychotic-induced hyperphagia.
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Perez-Gomez A, Carretero M, Weber N, Peterka V, To A, Titova V, Solis G, Osborn O, and Petrascheck M
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- Animals, Antipsychotic Agents toxicity, CCAAT-Binding Factor genetics, Chemotherapy, Adjuvant, DNA-Binding Proteins genetics, Eating drug effects, Gene Expression drug effects, Gene Expression Profiling, Hyperphagia chemically induced, Hyperphagia drug therapy, Hypothalamus metabolism, Mice, Phenotype, Transcription Factors genetics, Vemurafenib pharmacology, Caenorhabditis elegans genetics, Caenorhabditis elegans Proteins genetics, Eating genetics, Hyperphagia genetics
- Abstract
Antipsychotic (AP) drugs are used to treat psychiatric disorders but are associated with significant weight gain and metabolic disease. Increased food intake (hyperphagia) appears to be a driving force by which APs induce weight gain but the mechanisms are poorly understood. Here we report that administration of APs to C. elegans induces hyperphagia by a mechanism that is genetically distinct from basal food intake. We exploit this finding to screen for adjuvant drugs that suppress AP-induced hyperphagia in C. elegans and mice. In mice AP-induced hyperphagia is associated with a unique hypothalamic gene expression signature that is abrogated by adjuvant drug treatment. Genetic analysis of this signature using C. elegans identifies two transcription factors, nhr-25/Nr5a2 and nfyb-1/NFYB to be required for AP-induced hyperphagia. Our study reveals that AP-induced hyperphagia can be selectively suppressed without affecting basal food intake allowing for novel drug discovery strategies to combat AP-induced metabolic side effects.
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- 2018
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18. Geroneuroprotectors: Effective Geroprotectors for the Brain.
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Schubert D, Currais A, Goldberg J, Finley K, Petrascheck M, and Maher P
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- Aging pathology, Alzheimer Disease prevention & control, Animals, Brain growth & development, Humans, Neuroprotective Agents therapeutic use, Aging drug effects, Alzheimer Disease drug therapy, Brain drug effects, Drug Discovery methods, Neuroprotective Agents pharmacology
- Abstract
Geroprotectors are compounds that slow the rate of biological aging and therefore may reduce the incidence of age-associated diseases such as Alzheimer's disease (AD). However, few have therapeutic efficacy in mammalian AD models. Here we describe the identification of geroneuroprotectors (GNPs), novel AD drug candidates that meet the criteria for geroprotectors., (Copyright © 2018 Elsevier Ltd. All rights reserved.)
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- 2018
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19. Translation attenuation by minocycline enhances longevity and proteostasis in old post-stress-responsive organisms.
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Solis GM, Kardakaris R, Valentine ER, Bar-Peled L, Chen AL, Blewett MM, McCormick MA, Williamson JR, Kennedy B, Cravatt BF, and Petrascheck M
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- Animals, Protein Aggregation, Pathological prevention & control, Ribosomes drug effects, Ribosomes metabolism, Caenorhabditis elegans drug effects, Caenorhabditis elegans physiology, Longevity drug effects, Minocycline metabolism, Protein Biosynthesis drug effects, Protein Synthesis Inhibitors metabolism, Proteostasis drug effects
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Aging impairs the activation of stress signaling pathways (SSPs), preventing the induction of longevity mechanisms late in life. Here, we show that the antibiotic minocycline increases lifespan and reduces protein aggregation even in old, SSP-deficient Caenorhabditis elegans by targeting cytoplasmic ribosomes, preferentially attenuating translation of highly translated mRNAs. In contrast to most other longevity paradigms, minocycline inhibits rather than activates all major SSPs and extends lifespan in mutants deficient in the activation of SSPs, lysosomal or autophagic pathways. We propose that minocycline lowers the concentration of newly synthesized aggregation-prone proteins, resulting in a relative increase in protein-folding capacity without the necessity to induce protein-folding pathways. Our study suggests that in old individuals with incapacitated SSPs or autophagic pathways, pharmacological attenuation of cytoplasmic translation is a promising strategy to reduce protein aggregation. Altogether, it provides a geroprotecive mechanism for the many beneficial effects of tetracyclines in models of neurodegenerative disease., Editorial Note: This article has been through an editorial process in which the authors decide how to respond to the issues raised during peer review. The Reviewing Editor's assessment is that all the issues have been addressed (see decision letter)., Competing Interests: GS, RK, EV, LB, AC, MB, MM, JW, BK, MP No competing interests declared, BC Reviewing editor, eLife, (© 2018, Solis et al.)
- Published
- 2018
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20. The mitochondrial ATP synthase is a shared drug target for aging and dementia.
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Goldberg J, Currais A, Prior M, Fischer W, Chiruta C, Ratliff E, Daugherty D, Dargusch R, Finley K, Esparza-Moltó PB, Cuezva JM, Maher P, Petrascheck M, and Schubert D
- Subjects
- Humans, Mitochondria metabolism, Aging genetics, Dementia genetics, Mitochondria enzymology, Mitochondrial Proton-Translocating ATPases genetics
- Abstract
Aging is a major driving force underlying dementia, such as that caused by Alzheimer's disease (AD). While the idea of targeting aging as a therapeutic strategy is not new, it remains unclear how closely aging and age-associated diseases are coupled at the molecular level. Here, we discover a novel molecular link between aging and dementia through the identification of the molecular target for the AD drug candidate J147. J147 was developed using a series of phenotypic screening assays mimicking disease toxicities associated with the aging brain. We have previously demonstrated the therapeutic efficacy of J147 in several mouse models of AD. Here, we identify the mitochondrial α-F
1 -ATP synthase (ATP5A) as a target for J147. By targeting ATP synthase, J147 causes an increase in intracellular calcium leading to sustained calcium/calmodulin-dependent protein kinase kinase β (CAMKK2)-dependent activation of the AMPK/mTOR pathway, a canonical longevity mechanism. Accordingly, modulation of mitochondrial processes by J147 prevents age-associated drift of the hippocampal transcriptome and plasma metabolome in mice and extends lifespan in drosophila. Our results link aging and age-associated dementia through ATP synthase, a molecular drug target that can potentially be exploited for the suppression of both. These findings demonstrate that novel screens for new AD drug candidates identify compounds that act on established aging pathways, suggesting an unexpectedly close molecular relationship between the two., (© 2018 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.)- Published
- 2018
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21. Computational Analysis of Lifespan Experiment Reproducibility.
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Petrascheck M and Miller DL
- Abstract
Independent reproducibility is essential to the generation of scientific knowledge. Optimizing experimental protocols to ensure reproducibility is an important aspect of scientific work. Genetic or pharmacological lifespan extensions are generally small compared to the inherent variability in mean lifespan even in isogenic populations housed under identical conditions. This variability makes reproducible detection of small but real effects experimentally challenging. In this study, we aimed to determine the reproducibility of C. elegans lifespan measurements under ideal conditions, in the absence of methodological errors or environmental or genetic background influences. To accomplish this, we generated a parametric model of C. elegans lifespan based on data collected from 5,026 wild-type N2 animals. We use this model to predict how different experimental practices, effect sizes, number of animals, and how different "shapes" of survival curves affect the ability to reproduce real longevity effects. We find that the chances of reproducing real but small effects are exceedingly low and would require substantially more animals than are commonly used. Our results indicate that many lifespan studies are underpowered to detect reported changes and that, as a consequence, stochastic variation alone can account for many failures to reproduce longevity results. As a remedy, we provide power of detection tables that can be used as guidelines to plan experiments with statistical power to reliably detect real changes in lifespan and limit spurious false positive results. These considerations will improve best-practices in designing lifespan experiment to increase reproducibility.
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- 2017
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22. The DrugAge database of aging-related drugs.
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Barardo D, Thornton D, Thoppil H, Walsh M, Sharifi S, Ferreira S, Anžič A, Fernandes M, Monteiro P, Grum T, Cordeiro R, De-Souza EA, Budovsky A, Araujo N, Gruber J, Petrascheck M, Fraifeld VE, Zhavoronkov A, Moskalev A, and de Magalhães JP
- Subjects
- Aging genetics, Aging metabolism, Animals, Antioxidants chemistry, Caenorhabditis elegans drug effects, Caenorhabditis elegans genetics, Caenorhabditis elegans growth & development, Caenorhabditis elegans metabolism, Computational Biology methods, Drosophila melanogaster drug effects, Drosophila melanogaster genetics, Drosophila melanogaster growth & development, Drosophila melanogaster metabolism, Geriatrics methods, Humans, Membrane Transport Modulators chemistry, Mice, Saccharomyces cerevisiae drug effects, Saccharomyces cerevisiae genetics, Saccharomyces cerevisiae growth & development, Saccharomyces cerevisiae metabolism, User-Computer Interface, Aging drug effects, Antioxidants pharmacology, Databases, Pharmaceutical, Membrane Transport Modulators pharmacology, Metabolic Networks and Pathways drug effects
- Abstract
Aging is a major worldwide medical challenge. Not surprisingly, identifying drugs and compounds that extend lifespan in model organisms is a growing research area. Here, we present DrugAge (http://genomics.senescence.info/drugs/), a curated database of lifespan-extending drugs and compounds. At the time of writing, DrugAge contains 1316 entries featuring 418 different compounds from studies across 27 model organisms, including worms, flies, yeast and mice. Data were manually curated from 324 publications. Using drug-gene interaction data, we also performed a functional enrichment analysis of targets of lifespan-extending drugs. Enriched terms include various functional categories related to glutathione and antioxidant activity, ion transport and metabolic processes. In addition, we found a modest but significant overlap between targets of lifespan-extending drugs and known aging-related genes, suggesting that some but not most aging-related pathways have been targeted pharmacologically in longevity studies. DrugAge is freely available online for the scientific community and will be an important resource for biogerontologists., (© 2017 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.)
- Published
- 2017
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23. C. elegans as Model for Drug Discovery.
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Carretero M, Solis GM, and Petrascheck M
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- Animals, Small Molecule Libraries pharmacology, Caenorhabditis elegans drug effects, Drug Discovery methods, Models, Animal
- Abstract
Small molecule screens using C. elegans as a model are becoming increasingly popular as the number of high-throughput methodologies has steadily increased over the years. Here we focus on the biology that underlies this increased popularity and outline the reasons that make C. elegans an attractive model for drug discovery. We discuss successful C. elegans based drug discovery projects in the literature and future challenges ahead., (Copyright© Bentham Science Publishers; For any queries, please email at epub@benthamscience.org.)
- Published
- 2017
- Full Text
- View/download PDF
24. Correction: Suppression of transcriptional drift extends C. elegans lifespan by postponing the onset of mortality.
- Author
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Rangaraju S, Solis GM, Thompson RC, Gomez-Amaro RL, Kurian L, Encalada SE, Niculescu AB, Salomon DR, and Petrascheck M
- Published
- 2016
- Full Text
- View/download PDF
25. Proton Pump Inhibitors Accelerate Endothelial Senescence.
- Author
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Yepuri G, Sukhovershin R, Nazari-Shafti TZ, Petrascheck M, Ghebre YT, and Cooke JP
- Subjects
- Cell Line, Endothelial Cells metabolism, Endothelial Cells physiology, Humans, Cellular Senescence drug effects, Endothelial Cells drug effects, Proton Pump Inhibitors pharmacology
- Abstract
Rationale: Proton pump inhibitors (PPIs) are popular drugs for gastroesophageal reflux, which are now available for long-term use without medical supervision. Recent reports suggest that PPI use is associated with cardiovascular, renal, and neurological morbidity., Objective: To study the long-term effect of PPIs on endothelial dysfunction and senescence and investigate the mechanism involved in PPI-induced vascular dysfunction., Methods and Results: Chronic exposure to PPIs impaired endothelial function and accelerated human endothelial senescence by reducing telomere length., Conclusions: Our data may provide a unifying mechanism for the association of PPI use with increased risk of cardiovascular, renal, and neurological morbidity and mortality., (© 2016 American Heart Association, Inc.)
- Published
- 2016
- Full Text
- View/download PDF
26. Metabolic drift in the aging brain.
- Author
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Ivanisevic J, Stauch KL, Petrascheck M, Benton HP, Epstein AA, Fang M, Gorantla S, Tran M, Hoang L, Kurczy ME, Boska MD, Gendelman HE, Fox HS, and Siuzdak G
- Subjects
- Animals, Metabolomics, Mice, Oxidative Phosphorylation, Proteomics, Aging metabolism, Brain metabolism, Energy Metabolism physiology
- Abstract
Brain function is highly dependent upon controlled energy metabolism whose loss heralds cognitive impairments. This is particularly notable in the aged individuals and in age-related neurodegenerative diseases. However, how metabolic homeostasis is disrupted in the aging brain is still poorly understood. Here we performed global, metabolomic and proteomic analyses across different anatomical regions of mouse brain at different stages of its adult lifespan. Interestingly, while severe proteomic imbalance was absent, global-untargeted metabolomics revealed an energymetabolic drift or significant imbalance in core metabolite levels in aged mouse brains. Metabolic imbalance was characterized by compromised cellular energy status (NAD decline, increased AMP/ATP, purine/pyrimidine accumulation) and significantly altered oxidative phosphorylation and nucleotide biosynthesis and degradation. The central energy metabolic drift suggests a failure of the cellular machinery to restore metabostasis (metabolite homeostasis) in the aged brain and therefore an inability to respond properly to external stimuli, likely driving the alterations in signaling activity and thus in neuronal function and communication.
- Published
- 2016
- Full Text
- View/download PDF
27. C. elegans S6K Mutants Require a Creatine-Kinase-like Effector for Lifespan Extension.
- Author
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McQuary PR, Liao CY, Chang JT, Kumsta C, She X, Davis A, Chu CC, Gelino S, Gomez-Amaro RL, Petrascheck M, Brill LM, Ladiges WC, Kennedy BK, and Hansen M
- Subjects
- AMP-Activated Protein Kinases metabolism, Animals, Caenorhabditis elegans Proteins metabolism, Enzyme Activation, Female, Male, Mice, Knockout, Neuroglia enzymology, Protein Serine-Threonine Kinases metabolism, Arginine Kinase physiology, Caenorhabditis elegans physiology, Caenorhabditis elegans Proteins physiology, Creatine Kinase physiology, Longevity, Ribosomal Protein S6 Kinases, 70-kDa physiology
- Abstract
Deficiency of S6 kinase (S6K) extends the lifespan of multiple species, but the underlying mechanisms are unclear. To discover potential effectors of S6K-mediated longevity, we performed a proteomics analysis of long-lived rsks-1/S6K C. elegans mutants compared to wild-type animals. We identified the arginine kinase ARGK-1 as the most significantly enriched protein in rsks-1/S6K mutants. ARGK-1 is an ortholog of mammalian creatine kinase, which maintains cellular ATP levels. We found that argk-1 is possibly a selective effector of rsks-1/S6K-mediated longevity and that overexpression of ARGK-1 extends C. elegans lifespan, in part by activating the energy sensor AAK-2/AMPK. argk-1 is also required for the reduced body size and increased stress resistance observed in rsks-1/S6K mutants. Finally, creatine kinase levels are increased in the brains of S6K1 knockout mice. Our study identifies ARGK-1 as a longevity effector in C. elegans with reduced RSKS-1/S6K levels., (Copyright © 2016 The Authors. Published by Elsevier Inc. All rights reserved.)
- Published
- 2016
- Full Text
- View/download PDF
28. Suppression of transcriptional drift extends C. elegans lifespan by postponing the onset of mortality.
- Author
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Rangaraju S, Solis GM, Thompson RC, Gomez-Amaro RL, Kurian L, Encalada SE, Niculescu AB 3rd, Salomon DR, and Petrascheck M
- Subjects
- Animals, Gene Expression Profiling, Mianserin administration & dosage, Aging, Caenorhabditis elegans drug effects, Caenorhabditis elegans physiology, Gene Expression Regulation drug effects, Longevity drug effects, Serotonin Antagonists administration & dosage, Transcription, Genetic
- Abstract
Longevity mechanisms increase lifespan by counteracting the effects of aging. However, whether longevity mechanisms counteract the effects of aging continually throughout life, or whether they act during specific periods of life, preventing changes that precede mortality is unclear. Here, we uncover transcriptional drift, a phenomenon that describes how aging causes genes within functional groups to change expression in opposing directions. These changes cause a transcriptome-wide loss in mRNA stoichiometry and loss of co-expression patterns in aging animals, as compared to young adults. Using Caenorhabditis elegans as a model, we show that extending lifespan by inhibiting serotonergic signals by the antidepressant mianserin attenuates transcriptional drift, allowing the preservation of a younger transcriptome into an older age. Our data are consistent with a model in which inhibition of serotonergic signals slows age-dependent physiological decline and the associated rise in mortality levels exclusively in young adults, thereby postponing the onset of major mortality., Competing Interests: The author declares that no competing interests exist.
- Published
- 2015
- Full Text
- View/download PDF
29. Atypical antidepressants extend lifespan of Caenorhabditis elegans by activation of a non-cell-autonomous stress response.
- Author
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Rangaraju S, Solis GM, Andersson SI, Gomez-Amaro RL, Kardakaris R, Broaddus CD, Niculescu AB 3rd, and Petrascheck M
- Subjects
- Aging physiology, Animals, Caenorhabditis elegans Proteins metabolism, Catalase metabolism, Fluoxetine pharmacology, Histamine H1 Antagonists pharmacology, Longevity physiology, Mianserin analogs & derivatives, Mianserin pharmacology, Mirtazapine, Peroxiredoxins metabolism, Reactive Oxygen Species metabolism, Serotonin Antagonists pharmacology, Selective Serotonin Reuptake Inhibitors pharmacology, Superoxide Dismutase metabolism, Synaptic Transmission drug effects, Aging drug effects, Antidepressive Agents, Second-Generation pharmacology, Caenorhabditis elegans physiology, Life Expectancy, Longevity drug effects, Oxidative Stress drug effects
- Abstract
Oxidative stress has long been associated with aging and has recently been linked to psychiatric disorders, including psychosis and depression. We identified multiple antipsychotics and antidepressants that extend Caenorhabditis elegans lifespan and protect the animal from oxidative stress. Here, we report that atypical antidepressants activate a neuronal mechanism that regulates the response to oxidative stress throughout the animal. While the activation of the oxidative stress response by atypical antidepressants depends on synaptic transmission, the activation by reactive oxygen species does not. Lifespan extension by atypical antidepressants depends on the neuronal oxidative stress response activation mechanism. Neuronal regulation of the oxidative stress response is likely to have evolved as a survival mechanism to protect the organism from oxidative stress, upon detection of adverse or dangerous conditions by the nervous system., (© 2015 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.)
- Published
- 2015
- Full Text
- View/download PDF
30. Measuring Food Intake and Nutrient Absorption in Caenorhabditis elegans.
- Author
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Gomez-Amaro RL, Valentine ER, Carretero M, LeBoeuf SE, Rangaraju S, Broaddus CD, Solis GM, Williamson JR, and Petrascheck M
- Subjects
- Animals, Body Size, Mass Spectrometry, Mutation, Protein Biosynthesis drug effects, Serotonin metabolism, Serotonin pharmacology, Animal Feed, Caenorhabditis elegans physiology, Feeding Behavior
- Abstract
Caenorhabditis elegans has emerged as a powerful model to study the genetics of feeding, food-related behaviors, and metabolism. Despite the many advantages of C. elegans as a model organism, direct measurement of its bacterial food intake remains challenging. Here, we describe two complementary methods that measure the food intake of C. elegans. The first method is a microtiter plate-based bacterial clearing assay that measures food intake by quantifying the change in the optical density of bacteria over time. The second method, termed pulse feeding, measures the absorption of food by tracking de novo protein synthesis using a novel metabolic pulse-labeling strategy. Using the bacterial clearance assay, we compare the bacterial food intake of various C. elegans strains and show that long-lived eat mutants eat substantially more than previous estimates. To demonstrate the applicability of the pulse-feeding assay, we compare the assimilation of food for two C. elegans strains in response to serotonin. We show that serotonin-increased feeding leads to increased protein synthesis in a SER-7-dependent manner, including proteins known to promote aging. Protein content in the food has recently emerged as critical factor in determining how food composition affects aging and health. The pulse-feeding assay, by measuring de novo protein synthesis, represents an ideal method to unequivocally establish how the composition of food dictates protein synthesis. In combination, these two assays provide new and powerful tools for C. elegans research to investigate feeding and how food intake affects the proteome and thus the physiology and health of an organism., (Copyright © 2015 by the Genetics Society of America.)
- Published
- 2015
- Full Text
- View/download PDF
31. Pharmacological classes that extend lifespan of Caenorhabditis elegans.
- Author
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Carretero M, Gomez-Amaro RL, and Petrascheck M
- Abstract
Recent progress in the field of aging has resulted in ever increasing numbers of compounds that extend lifespan in Caenorhabditis elegans. Lifespan extending compounds include metabolites and synthetic compounds, as well as natural products. For many of these compounds, mammalian pharmacology is known, and for some the actual targets have been experimentally identified. In this review, we explore the data available in C. elegans to provide an overview of which pharmacological classes have potential for identification of further compounds that extend lifespan.
- Published
- 2015
- Full Text
- View/download PDF
32. High-throughput small-molecule screening in Caenorhabditis elegans.
- Author
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Rangaraju S, Solis GM, and Petrascheck M
- Subjects
- Animals, Caenorhabditis elegans drug effects, Drug Evaluation, Preclinical methods, High-Throughput Screening Assays, Small Molecule Libraries
- Abstract
Chemical compounds, which modulate enzymatic activities or those which induce specific phenotypes of interest, are valuable probes to study biological phenomena, as they allow modulation of enzymatic activities and temporal control of protein action. Here, we describe the methodology to conduct large-scale screens for chemical compounds that induce a desired phenotype in the roundworm Caenorhabditis elegans (C. elegans) using 96- or 384-well microtiter plates.
- Published
- 2015
- Full Text
- View/download PDF
33. The metabolite α-ketoglutarate extends lifespan by inhibiting ATP synthase and TOR.
- Author
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Chin RM, Fu X, Pai MY, Vergnes L, Hwang H, Deng G, Diep S, Lomenick B, Meli VS, Monsalve GC, Hu E, Whelan SA, Wang JX, Jung G, Solis GM, Fazlollahi F, Kaweeteerawat C, Quach A, Nili M, Krall AS, Godwin HA, Chang HR, Faull KF, Guo F, Jiang M, Trauger SA, Saghatelian A, Braas D, Christofk HR, Clarke CF, Teitell MA, Petrascheck M, Reue K, Jung ME, Frand AR, and Huang J
- Subjects
- Animals, Cell Line, Enzyme Activation drug effects, Enzyme Inhibitors pharmacology, Gene Knockdown Techniques, HEK293 Cells, Humans, Jurkat Cells, Longevity drug effects, Longevity genetics, Mice, Mitochondrial Proton-Translocating ATPases genetics, Protein Binding, Caenorhabditis elegans drug effects, Ketoglutaric Acids pharmacology, Longevity physiology, Mitochondrial Proton-Translocating ATPases metabolism, TOR Serine-Threonine Kinases metabolism
- Abstract
Metabolism and ageing are intimately linked. Compared with ad libitum feeding, dietary restriction consistently extends lifespan and delays age-related diseases in evolutionarily diverse organisms. Similar conditions of nutrient limitation and genetic or pharmacological perturbations of nutrient or energy metabolism also have longevity benefits. Recently, several metabolites have been identified that modulate ageing; however, the molecular mechanisms underlying this are largely undefined. Here we show that α-ketoglutarate (α-KG), a tricarboxylic acid cycle intermediate, extends the lifespan of adult Caenorhabditis elegans. ATP synthase subunit β is identified as a novel binding protein of α-KG using a small-molecule target identification strategy termed drug affinity responsive target stability (DARTS). The ATP synthase, also known as complex V of the mitochondrial electron transport chain, is the main cellular energy-generating machinery and is highly conserved throughout evolution. Although complete loss of mitochondrial function is detrimental, partial suppression of the electron transport chain has been shown to extend C. elegans lifespan. We show that α-KG inhibits ATP synthase and, similar to ATP synthase knockdown, inhibition by α-KG leads to reduced ATP content, decreased oxygen consumption, and increased autophagy in both C. elegans and mammalian cells. We provide evidence that the lifespan increase by α-KG requires ATP synthase subunit β and is dependent on target of rapamycin (TOR) downstream. Endogenous α-KG levels are increased on starvation and α-KG does not extend the lifespan of dietary-restricted animals, indicating that α-KG is a key metabolite that mediates longevity by dietary restriction. Our analyses uncover new molecular links between a common metabolite, a universal cellular energy generator and dietary restriction in the regulation of organismal lifespan, thus suggesting new strategies for the prevention and treatment of ageing and age-related diseases.
- Published
- 2014
- Full Text
- View/download PDF
34. A pharmacological network for lifespan extension in Caenorhabditis elegans.
- Author
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Ye X, Linton JM, Schork NJ, Buck LB, and Petrascheck M
- Subjects
- Animals, Humans, Oxidative Stress drug effects, Stress, Physiological drug effects, Caenorhabditis elegans drug effects, Caenorhabditis elegans physiology, Longevity drug effects, Longevity physiology, Small Molecule Libraries pharmacology
- Abstract
One goal of aging research is to find drugs that delay the onset of age-associated disease. Studies in invertebrates, particularly Caenorhabditis elegans, have uncovered numerous genes involved in aging, many conserved in mammals. However, which of these encode proteins suitable for drug targeting is unknown. To investigate this question, we screened a library of compounds with known mammalian pharmacology for compounds that increase C. elegans lifespan. We identified 60 compounds that increase longevity in C. elegans, 33 of which also increased resistance to oxidative stress. Many of these compounds are drugs approved for human use. Enhanced resistance to oxidative stress was associated primarily with compounds that target receptors for biogenic amines, such as dopamine or serotonin. A pharmacological network constructed with these data reveal that lifespan extension and increased stress resistance cluster together in a few pharmacological classes, most involved in intercellular signaling. These studies identify compounds that can now be explored for beneficial effects on aging in mammals, as well as tools that can be used to further investigate the mechanisms underlying aging in C. elegans., (© 2013 The Authors. Aging Cell published by the Anatomical Society and John Wiley & Sons Ltd.)
- Published
- 2014
- Full Text
- View/download PDF
35. Measuring Caenorhabditis elegans life span in 96 well microtiter plates.
- Author
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Solis GM and Petrascheck M
- Subjects
- Animals, Antidepressive Agents, Tricyclic pharmacology, Caenorhabditis elegans drug effects, Drug Evaluation, Preclinical methods, Longevity drug effects, Mianserin analogs & derivatives, Mianserin pharmacology, Mirtazapine, Models, Animal, Caenorhabditis elegans physiology, Longevity physiology
- Abstract
Lifespan is a biological process regulated by several genetic pathways. One strategy to investigate the biology of aging is to study animals that harbor mutations in components of age-regulatory pathways. If these mutations perturb the function of the age-regulatory pathway and therefore alter the lifespan of the entire organism, they provide important mechanistic insights. Another strategy to investigate the regulation of lifespan is to use small molecules to perturb age-regulatory pathways. To date, a number of molecules are known to extend lifespan in various model organisms and are used as tools to study the biology of aging. The number of molecules identified thus far is small compared to the genetic "toolset" that is available to study the biology of aging. Caenorhabditis elegans is one of the principle models used to study aging because of its excellent genetics and short lifespan of three weeks. More recently, C.elegans has emerged as a model organism for phenotype based drug screens because of its small size and its ability to grow in microtiter plates. Here we present an assay to measure C.elegans lifespan in 96 well microtiter plates. The assay was developed and successfully used to screen large libraries for molecules that extend C.elegans lifespan. The reliability of the assay was evaluated in multiple tests: first, by measuring the lifespan of wild type animals grown at different temperatures; second, by measuring the lifespan of mutants with altered lifespans; third, by measuring changes in lifespan in response to different concentrations of the antidepressant Mirtazepine. Mirtazepine has previously been shown to extend lifespan in C.elegans. The results of these tests show that the assay is able to replicate previous findings from other assays and is quantitative. The microtiter format also makes this lifespan assay compatible with automated liquid handling systems and allows integration into automated platforms.
- Published
- 2011
- Full Text
- View/download PDF
36. A high-throughput screen for chemicals that increase the lifespan of Caenorhabditis elegans.
- Author
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Petrascheck M, Ye X, and Buck LB
- Subjects
- Animals, Caenorhabditis elegans physiology, Caenorhabditis elegans drug effects, Longevity drug effects, Mianserin pharmacology, Octopamine pharmacology, Serotonin Antagonists pharmacology
- Abstract
One long-term goal of aging research is to find drugs that can delay aging and the onset of age-associated diseases. With this in mind, we screened 88,000 chemicals for the ability to increase the lifespan of Caenorhabditis elegans nematodes. We found that mianserin, a serotonin receptor antagonist used as an antidepressant in humans, can increase C. elegans lifespan when given only during adulthood. This effect is reduced or abolished by mutations that affect serotonin synthesis or serotonin reuptake at synapses. It also requires a serotonin receptor and an octopamine receptor, both of which are inhibited by the drug. Mianserin has no effect on the lifespan of animals with increased longevity due to dietary restriction or with a mutation that reduces food intake, indicating that the drug extends lifespan via mechanisms linked to dietary restriction. These studies indicate that lifespan can be increased by inhibiting certain kinds of neurotransmission previously implicated in food sensing, possibly by mimicking a physiological state associated with dietary restriction.
- Published
- 2009
- Full Text
- View/download PDF
37. An antidepressant that extends lifespan in adult Caenorhabditis elegans.
- Author
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Petrascheck M, Ye X, and Buck LB
- Subjects
- Aging, Animals, Antidepressive Agents chemistry, Caloric Restriction, Humans, Methiothepin pharmacology, Mianserin pharmacology, Receptors, Biogenic Amine antagonists & inhibitors, Receptors, Biogenic Amine metabolism, Receptors, Serotonin, 5-HT4 metabolism, Serotonin biosynthesis, Serotonin 5-HT4 Receptor Antagonists, Serotonin Antagonists pharmacology, Signal Transduction drug effects, Starvation metabolism, Antidepressive Agents pharmacology, Caenorhabditis elegans drug effects, Caenorhabditis elegans physiology, Longevity drug effects, Longevity physiology, Octopamine metabolism, Serotonin metabolism
- Abstract
The mechanisms that determine the lifespan of an organism are still largely a mystery. One goal of ageing research is to find drugs that would increase lifespan and vitality when given to an adult animal. To this end, we tested 88,000 chemicals for the ability to extend the lifespan of adult Caenorhabditis elegans nematodes. Here we report that a drug used as an antidepressant in humans increases C. elegans lifespan. In humans, this drug blocks neural signalling by the neurotransmitter serotonin. In C. elegans, the effect of the drug on lifespan is reduced or eradicated by mutations that affect serotonin synthesis, serotonin re-uptake at synapses, or either of two G-protein-coupled receptors: one that recognizes serotonin and the other that detects another neurotransmitter, octopamine. In vitro studies show that the drug acts as an antagonist at both receptors. Testing of the drug on dietary-restricted animals or animals with mutations that affect lifespan indicates that its effect on lifespan involves mechanisms associated with lifespan extension by dietary restriction. These studies indicate that lifespan can be extended by blocking certain types of neurotransmission implicated in food sensing in the adult animal, possibly leading to a state of perceived, although not real, starvation.
- Published
- 2007
- Full Text
- View/download PDF
38. Quenching accumulation of toxic galactose-1-phosphate as a system to select disruption of protein-protein interactions in vivo.
- Author
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Gunde T, Tanner S, Auf der Maur A, Petrascheck M, and Barberis A
- Subjects
- Two-Hybrid System Techniques, Fungal Proteins genetics, Fungal Proteins metabolism, Galactokinase genetics, Galactokinase metabolism, Galactosephosphates metabolism, Protein Engineering methods, Protein Interaction Mapping methods, Yeasts physiology
- Abstract
The reverse two-hybrid system has been developed to readily identify molecules or mutations that can disrupt protein-protein interactions in vivo. This system is generally based on the interaction-dependent activation of a reporter gene, whose product inhibits the growth of the engineered yeast cell. Thus, disruption of the interaction between the hybrid proteins can be positively selected because, by reducing the expression of the negative marker gene, it allows cell growth. Although several counter-selectable marker genes are currently available, their application in the reverse two-hybrid system is generally confronted with technical and practical problems such as low selectivity and relatively complex experimental procedures. Thus, the characterization of more reliable and simple counter-selection assays for the reverse two-hybrid system continues to be of interest. We have developed a novel counter-selection assay based on the toxicity of intracellular galactose-1-phosphate, which accumulates upon expression of a galactokinase-encoding GAL1 reporter gene in the absence of transferase activity. Decreased GAL1 gene expression upon dissociation of interacting proteins causes reduction of intracellular galactose-1-phosphate concentrations, thus allowing cell growth under selective conditions.
- Published
- 2004
- Full Text
- View/download PDF
39. Organ polarity in Arabidopsis. NOZZLE physically interacts with members of the YABBY family.
- Author
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Sieber P, Petrascheck M, Barberis A, and Schneitz K
- Subjects
- Arabidopsis genetics, Arabidopsis Proteins genetics, Base Sequence, Binding Sites, Cloning, Molecular, DNA Primers, Flowers metabolism, Flowers ultrastructure, Nuclear Proteins genetics, Plasmids genetics, Recombinant Fusion Proteins metabolism, Repressor Proteins genetics, Zinc Fingers, Arabidopsis anatomy & histology, Arabidopsis metabolism, Arabidopsis Proteins metabolism, Nuclear Proteins metabolism, Repressor Proteins metabolism
- Abstract
Plant lateral organs exhibit proximal-distal and adaxial-abaxial polarity. In Arabidopsis, abaxial cell fate is regulated in part by putative transcription factors of the YABBY family, such as FILAMENTOUS FLOWER (FIL) and INNER NO OUTER (INO), by a mechanism that currently is not fully understood. NOZZLE (NZZ) encodes a plant-specific nuclear protein. Genetic evidence has shown that NZZ is involved in the positive feedback regulation of INO, thereby acting both as a temporal and spatial repressor of INO transcription. This mechanism allows the ovule primordium to complete its proximal-distal organization, prior to the onset of adaxial-abaxial development in the chalaza. During our study, we isolated FIL in a yeast two-hybrid screen using NZZ as bait. In vitro pull-down experiments confirmed the NZZ-FIL interaction. NZZ also bound INO and YABBY3, suggesting that NZZ generally interacts with YABBY proteins in vitro. The polar-charged region of NZZ was necessary and sufficient to bind to the zinc finger of INO and to interact with its C terminus carrying the high mobility group-like domain. We suggest that NZZ coordinates proximal-distal patterning and adaxial-abaxial polarity establishment in the developing ovule by directly binding to INO.
- Published
- 2004
- Full Text
- View/download PDF
40. Two-hybrid selection assay to identify proteins interacting with polymerase II transcription factors and regulators.
- Author
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Petrascheck M, Castagna F, and Barberis A
- Subjects
- Animals, Genes, Reporter, Mice, Transcription Factor TFIIA, Transcription Factor TFIID, Yeasts genetics, Proteins metabolism, RNA Polymerase III metabolism, RNA, Small Nuclear genetics, Transcription Factors metabolism, Transcription Factors, TFII metabolism
- Abstract
The RNA polymerase III-based two-hybrid system has been developed to detect interactions between proteins such as RNA polymerase II transcription factors and regulators that cannot be studied by the original RNA polymerase II two-hybrid system. This novel method appears to be most useful for a refined analysis of already known protein-protein interactions. However, the application of this system in library screenings has been impaired by the lack of a suitable assay for the selection of the activated pol III reporter gene in yeast. Here, we describe a novel selection assay for the pol III-based two-hybrid system that makes it readily usable for screening expression libraries to search for interacting partners. Our system utilizes a temperature-sensitive (ts) U6 snRNA, which is synthesized by RNA polymerase III from a mutated SNR6 gene in yeast. In this ts strain, interactions between hybrid proteins activate an artificial pol III reporter construct (UASG-SNR6), which controls expression of wild-type U6 snRNA. This wild-type U6 snRNA can suppress the ts phenotype and allow growth at the nonpermissive temperature of 37 degrees C, thus providing a positive selection system for interacting proteins.
- Published
- 2001
- Full Text
- View/download PDF
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