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1. Examining associations between prenatal biomarkers of oxidative stress and ASD-related outcomes using quantile regression.

Author

Carey, Meghan, Rando, Juliette, Melnyk, Stepan, James, S, Snyder, Nathaniel, Salafia, Carolyn, Croen, Lisa, Fallin, M, Hertz-Picciotto, Irva, Volk, Heather, Newschaffer, Craig, and Lyall, Kristen

Subjects
Autism spectrum disorder, Cohort, Epidemiology, Neurodevelopment, Oxidative stress, Risk factors, Child, Humans, Female, Pregnancy, Autism Spectrum Disorder, Glutathione Disulfide, Vitamins, Oxidative Stress, Biomarkers, Glutathione
Abstract

We examined associations between prenatal oxidative stress (OS) and child autism-related outcomes. Women with an autistic child were followed through a subsequent pregnancy and that younger siblings childhood. Associations between glutathione (GSH), glutathione disulfide (GSSG), 8-oxo-deoxyguanine (8-OHdG), and nitrotyrosine and younger sibling Social Responsiveness Scale (SRS) scores were examined using quantile regression. Increasing GSH:GSSG (suggesting decreasing OS) was associated with minor increases in SRS scores (50th percentile β: 1.78, 95% CI: 0.67, 3.06); no other associations were observed. Results from this cohort with increased risk for autism do not support a strong relationship between OS in late pregnancy and autism-related outcomes. Results may be specific to those with enriched autism risk; future work should consider other timepoints and biomarkers.

Published
2023

2. Acetate controls endothelial-to-mesenchymal transition.

Author

Zhu, Xiaolong, Wang, Yunyun, Soaita, Ioana, Lee, Heon-Woo, Bae, Hosung, Boutagy, Nabil, Bostwick, Anna, Zhang, Rong-Mo, Bowman, Caitlyn, Xu, Yanying, Trefely, Sophie, Chen, Yu, Qin, Lingfeng, Sessa, William, Tellides, George, Jang, Cholsoon, Snyder, Nathaniel, Yu, Luyang, Arany, Zoltan, and Simons, Michael

Subjects
ACSS2, ALK5, PDK4, acetate, acetyl-CoA, atherosclerosis, endfothelial cells, endothelial-to-mesenchymal transition, transforming growth factor beta signaling, Humans, Endothelial Cells, Signal Transduction, Endothelium, Transforming Growth Factor beta, Vascular Diseases
Abstract

Endothelial-to-mesenchymal transition (EndMT), a process initiated by activation of endothelial TGF-β signaling, underlies numerous chronic vascular diseases and fibrotic states. Once induced, EndMT leads to a further increase in TGF-β signaling, thus establishing a positive-feedback loop with EndMT leading to more EndMT. Although EndMT is understood at the cellular level, the molecular basis of TGF-β-driven EndMT induction and persistence remains largely unknown. Here, we show that metabolic modulation of the endothelium, triggered by atypical production of acetate from glucose, underlies TGF-β-driven EndMT. Induction of EndMT suppresses the expression of the enzyme PDK4, which leads to an increase in ACSS2-dependent Ac-CoA synthesis from pyruvate-derived acetate. This increased Ac-CoA production results in acetylation of the TGF-β receptor ALK5 and SMADs 2 and 4 leading to activation and long-term stabilization of TGF-β signaling. Our results establish the metabolic basis of EndMT persistence and unveil novel targets, such as ACSS2, for the potential treatment of chronic vascular diseases.

Published
2023

3. A study on the association of placental and maternal urinary phthalate metabolites

Author

Liang, Hai-Wei, Snyder, Nathaniel, Wang, Jiebiao, Xun, Xiaoshuang, Yin, Qing, LeWinn, Kaja, Carroll, Kecia N, Bush, Nicole R, Kannan, Kurunthachalam, Barrett, Emily S, Mitchell, Rod T, Tylavsky, Fran, and Adibi, Jennifer J

Subjects
Pediatric Research Initiative, Contraception/Reproduction, Urologic Diseases, Pediatric, Clinical Research, Prevention, Conditions Affecting the Embryonic and Fetal Periods, Reproductive health and childbirth, Good Health and Well Being, Humans, Pregnancy, Female, Placenta, Phthalic Acids, Pregnancy Trimesters, Obesity, Environmental Pollutants, Environmental Exposure, Maternal Exposure, Endocrine Disruptors, Epidemiology, Exposure Modeling, Phthalates, Vulnerable Populations, Chemical Sciences, Environmental Sciences, Medical and Health Sciences
Abstract

BackgroundPhthalate exposure in pregnancy is typically estimated using maternal urinary phthalate metabolite levels. Our aim was to evaluate the association of urinary and placental tissue phthalates, and to explore the role of maternal and pregnancy characteristics that may bias estimates.MethodsFifty pregnancies were selected from the CANDLE Study, recruited from 2006 to 2011 in Tennessee. Linear models were used to estimate associations of urinary phthalates (2nd, 3rd trimesters) and placental tissue phthalates (birth). Potential confounders and modifiers were evaluated in categories: temporality (time between urine and placenta sample), fetal sex, demographics, social advantage, reproductive history, medication use, nutrition and adiposity. Molar and quantile normalized phthalates were calculated to facilitate comparison of placental and urinary levels.ResultsMetabolites detectable in >80% of both urine and placental samples were MEP, MnBP, MBzP, MECPP, MEOHP, MEHHP, and MEHP. MEP was most abundant in urine (geometric mean [GM] 7.00 ×102 nmol/l) and in placental tissue (GM 2.56 ×104 nmol/l). MEHP was the least abundant in urine (GM 5.32 ×101 nmol/l) and second most abundant in placental tissue (2.04 ×104 nmol/l). In aggregate, MEHP differed the most between urine and placenta (2.21 log units), and MEHHP differed the least (0.07 log units). MECPP was positively associated between urine and placenta (regression coefficient: 0.31 95% CI 0.09, 0.53). Other urine-placenta metabolite associations were modified by measures of social advantage, reproductive history, medication use, and adiposity.ConclusionPhthalates were ubiquitous in 50 full-term placental samples, as has already been shown in maternal urine. MEP and MEHP were the most abundant. Measurement and comparison of urinary and placental phthalates can advance knowledge on phthalate toxicity in pregnancy and provide insight into the validity and accuracy of relying on maternal urinary concentrations to estimate placental exposures.Impact statementThis is the first report of correlations/associations of urinary and placental tissue phthalates in human pregnancy. Epidemiologists have relied exclusively on maternal urinary phthalate metabolite concentrations to assess exposures in pregnant women and risk to their fetuses. Even though it has not yet been confirmed empirically, it is widely assumed that urinary concentrations are strongly and positively correlated with placental and fetal levels. Our data suggest that may not be the case, and these associations may vary by phthalate metabolite and associations may be modified by measures of social advantage, reproductive history, medication use, and adiposity.

Published
2023

4. Let's Talk Through Physics! Covert Cyber-Physical Data Exfiltration on Air-Gapped Edge Devices

Author

Chan, Matthew, Snyder, Nathaniel, Lucas, Marcus, Garcia, Luis, Sokolsky, Oleg, Weimer, James, Lee, Insup, Tabuada, Paulo, Zonouz, Saman, and Srivastava, Mani

Subjects
Computer Science - Cryptography and Security
Abstract

Although organizations are continuously making concerted efforts to harden their systems against network attacks by air-gapping critical systems, attackers continuously adapt and uncover covert channels to exfiltrate data from air-gapped systems. For instance, attackers have demonstrated the feasibility of exfiltrating data from a computer sitting in a Faraday cage by exfiltrating data using magnetic fields. Although a large body of work has recently emerged highlighting various physical covert channels, these attacks have mostly targeted open-loop cyber-physical systems where the covert channels exist on physical channels that are not being monitored by the victim. Network architectures such as fog computing push sensitive data to cyber-physical edge devices--whose physical side channels are typically monitored via state estimation. In this paper, we formalize covert data exfiltration that uses existing cyber-physical models and infrastructure of individual devices to exfiltrate data in a stealthy manner, i.e., we propose a method to circumvent cyber-physical state estimation intrusion detection techniques while exfiltrating sensitive data from the network. We propose a generalized model for encoding and decoding sensitive data within cyber-physical control loops. We evaluate our approach on a distributed IoT network that includes computation nodes residing on physical drones as well as on an industrial control system for the control of a robotic arm. Unlike prior works, we formalize the constraints of covert cyber-physical channel exfiltration in the presence of a defender performing state estimation.

Published
2022

6. Maternal androgens and autism spectrum disorder in the MARBLES prospective cohort study

Author

Granillo, Lauren, Iosif, Ana-Maria, Goodrich, Amanda, Snyder, Nathaniel W, and Schmidt, Rebecca J

Subjects
Psychology, Clinical and Health Psychology, Applied and Developmental Psychology, Mental Health, Women's Health, Pediatric, Brain Disorders, Pregnancy, Prevention, Intellectual and Developmental Disabilities (IDD), Autism, 2.3 Psychological, social and economic factors, Reproductive health and childbirth, Mental health, Good Health and Well Being, Testosterone, Androstenedione, Prospective study, Specialist Studies in Education, Rehabilitation, Applied and developmental psychology, Clinical and health psychology
Abstract

BackgroundMaternal hormonal risk factors for autism spectrum disorder (ASD) in offspring could intersect genetic and environmental risk factors.ObjectivesThis analysis explored ASD risk in association with maternal testosterone, androstenedione, and dehydroepiandrosterone (DHEA) measured in first, second, and third trimesters of pregnancy.MethodsMARBLES is a prospective pregnancy cohort study based at the MIND Institute in Northern California that enrolls mothers who have at least one child previously diagnosed with ASD and are expecting, or planning to have another child. At 36 months the younger sibling is clinically classified as having ASD, or as non-typically developing (Non-TD), or typically developing (TD). Maternal androgens during pregnancy were measured in serum samples from 196 mothers. Multivariable logistic regression models estimated risk of ASD and Non-TD in offspring compared to TD, in relation to the log-transformed maternal androgen concentrations, at each trimester.ResultsNon-significant associations were observed, and borderline significant associations were only observed in some stratified unadjusted models. Second trimester maternal testosterone was non-significantly associated with ASD in female offspring, although not after adjustment, aRR 1.54 (95% CI 0.71, 3.33), and second trimester maternal DHEA was non-significantly associated with non-TD in male offspring, again not after adjustment, aRR 0.50 (95% CI 0.21, 1.21). Secondary analysis suggested that third trimester androgen concentrations in mothers with male offspring had significant or near significant associations with their child's Social Responsiveness Scale score.ConclusionNo significant associations were found between maternal androgen concentrations and risk of ASD or Non-TD in the child.

Published
2022

7. Integrated landscape of cardiac metabolism in end-stage human nonischemic dilated cardiomyopathy.

Author

Murashige, Danielle, Yang, Yifan, Morley, Michael, Jung, Sunhee, Kantner, Daniel, Pepper, Hannah, Bedi, Kenneth, Brandimarto, Jeff, Prosser, Benjamin, Cappola, Thomas, Snyder, Nathaniel, Rabinowitz, Joshua, Margulies, Kenneth, Arany, Zolt, Flam, Emily, and Jang, Cholsoon

Abstract

Heart failure (HF) is a leading cause of mortality. Failing hearts undergo profound metabolic changes, but a comprehensive evaluation in humans is lacking. We integrate plasma and cardiac tissue metabolomics of 678 metabolites, genome-wide RNA-sequencing, and proteomic studies to examine metabolic status in 87 explanted human hearts from 39 patients with end-stage HF compared with 48 nonfailing donors. We confirm bioenergetic defects in human HF and reveal selective depletion of adenylate purines required for maintaining ATP levels. We observe substantial reductions in fatty acids and acylcarnitines in failing tissue, despite plasma elevations, suggesting defective import of fatty acids into cardiomyocytes. Glucose levels, in contrast, are elevated. Pyruvate dehydrogenase, which gates carbohydrate oxidation, is de-repressed, allowing increased lactate and pyruvate burning. Tricarboxylic acid cycle intermediates are significantly reduced. Finally, bioactive lipids are profoundly reprogrammed, with marked reductions in ceramides and elevations in lysoglycerophospholipids. These data unveil profound metabolic abnormalities in human failing hearts.

Published
2022

8. A subpopulation of lipogenic brown adipocytes drives thermogenic memory

Author

Lundgren, Patrick, Sharma, Prateek V., Dohnalová, Lenka, Coleman, Kyle, Uhr, Giulia T., Kircher, Susanna, Litichevskiy, Lev, Bahnsen, Klaas, Descamps, Hélène C., Demetriadou, Christina, Chan, Jacqueline, Chellappa, Karthikeyani, Cox, Timothy O., Heyman, Yael, Pather, Sarshan R., Shoffler, Clarissa, Petucci, Christopher, Shalem, Ophir, Raj, Arjun, Baur, Joseph A., Snyder, Nathaniel W., Wellen, Kathryn E., Levy, Maayan, Seale, Patrick, Li, Mingyao, and Thaiss, Christoph A.

Published
2023
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9. Direct anabolic metabolism of three-carbon propionate to a six-carbon metabolite occurs in vivo across tissues and species

Author

Doan, Mary T, Neinast, Michael D, Varner, Erika L, Bedi, Kenneth C, Bartee, David, Jiang, Helen, Trefely, Sophie, Xu, Peining, Singh, Jay P, Jang, Cholsoon, Rame, J Eduardo, Brady, Donita C, Meier, Jordan L, Marguiles, Kenneth B, Arany, Zoltan, and Snyder, Nathaniel W

Subjects
Digestive Diseases, Biotechnology, Acetyl Coenzyme A, Acyl Coenzyme A, Animals, Carbon, Liver, Mice, Oxidation-Reduction, Propionates, &nbsp, Metabolism, propionate, anabolism, acetyl-CoA, condensation reaction, stable isotope tracing, LC-MS, HRMS, TCA cycle, valine, 2M2PE-CoA, LC-MS/HRMS, Biochemistry and Cell Biology, Medical Biochemistry and Metabolomics, Biochemistry & Molecular Biology
Abstract

Anabolic metabolism of carbon in mammals is mediated via the one- and two-carbon carriers S-adenosyl methionine and acetyl-coenzyme A. In contrast, anabolic metabolism of three-carbon units via propionate has not been shown to extensively occur. Mammals are primarily thought to oxidize the three-carbon short chain fatty acid propionate by shunting propionyl-CoA to succinyl-CoA for entry into the TCA cycle. Here, we found that this may not be absolute as, in mammals, one nonoxidative fate of propionyl-CoA is to condense to two three-carbon units into a six-carbon trans-2-methyl-2-pentenoyl-CoA (2M2PE-CoA). We confirmed this reaction pathway using purified protein extracts provided limited substrates and verified the product via LC-MS using a synthetic standard. In whole-body in vivo stable isotope tracing following infusion of 13C-labeled valine at steady state, 2M2PE-CoA was found to form via propionyl-CoA in multiple murine tissues, including heart, kidney, and to a lesser degree, in brown adipose tissue, liver, and tibialis anterior muscle. Using ex vivo isotope tracing, we found that 2M2PE-CoA also formed in human myocardial tissue incubated with propionate to a limited extent. While the complete enzymology of this pathway remains to be elucidated, these results confirm the in vivo existence of at least one anabolic three- to six-carbon reaction conserved in humans and mice that utilizes propionate.

Published
2022

14. Lactoylglutathione promotes inflammatory signaling in macrophages through histone lactoylation

Author

Trujillo, Marissa N., Jennings, Erin Q., Hoffman, Emely A., Zhang, Hao, Phoebe, Aiden M., Mastin, Grace E., Kitamura, Naoya, Reisz, Julie A., Megill, Emily, Kantner, Daniel, Marcinkiewicz, Mariola M., Twardy, Shannon M., Lebario, Felicidad, Chapman, Eli, McCullough, Rebecca L., D'Alessandro, Angelo, Snyder, Nathaniel W., Cusanovich, Darren A., and Galligan, James J.

Published
2024
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16. Bempedoic acid suppresses diet-induced hepatic steatosis independently of ATP-citrate lyase

Author

Liu, Joyce Y., Kuna, Ramya S., Pinheiro, Laura V., Nguyen, Phuong T.T., Welles, Jaclyn E., Drummond, Jack M., Murali, Nivitha, Sharma, Prateek V., Supplee, Julianna G., Shiue, Mia, Zhao, Steven, Farria, Aimee T., Kumar, Avi, Ruchhoeft, Mauren L., Demetriadou, Christina, Kantner, Daniel S., Chatoff, Adam, Megill, Emily, Titchenell, Paul M., Snyder, Nathaniel W., Metallo, Christian M., and Wellen, Kathryn E.

Published
2024
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18. Meconium androgens are correlated with ASD-related phenotypic traits in early childhood in a familial enriched risk cohort

Author

Terloyeva, Dina, Frey, Alexander J, Park, Bo Y, Kauffman, Elizabeth M, Mathew, Leny, Bostwick, Anna, Varner, Erika L, Lee, Brian K, Croen, Lisa A, Fallin, Margaret D, Hertz-Picciotto, Irva, Newschaffer, Craig J, Lyall, Kristen, and Snyder, Nathaniel W

Subjects
Reproductive Medicine, Biomedical and Clinical Sciences, Pediatric Research Initiative, Brain Disorders, Perinatal Period - Conditions Originating in Perinatal Period, Pediatric, Clinical Research, Prevention, Intellectual and Developmental Disabilities (IDD), Mental Health, Autism, Reproductive health and childbirth, Androgens, Autism Spectrum Disorder, Child, Child, Preschool, Cohort Studies, Confidence Intervals, Family, Female, Humans, Infant, Newborn, Linear Models, Male, Meconium, Phenotype, Risk Factors, Statistics, Nonparametric, Autism-related traits, Androgen, Sibling, Sex difference, Prenatal exposure, Clinical Sciences, Neurosciences, Clinical sciences, Biological psychology
Abstract

BackgroundPrenatal exposure to increased androgens has been suggested as a risk factor for autism spectrum disorder (ASD). This hypothesis has been examined by measurement of steroids in amniotic fluid, cord blood, saliva, and blood with mixed results.MethodsTo provide an orthogonal measure of fetal exposure, this study used meconium, the first stool of a newborn, to measure prenatal androgen exposure from infants in the Early Autism Risk Longitudinal Investigation (EARLI). EARLI is a familial-enriched risk cohort that enrolled pregnant mothers who already had a child with an ASD diagnosis. In the younger child, we investigated the association between meconium unconjugated (u) and total (t) concentrations of major androgens testosterone (T), dehydroepiandrosterone (DHEA), and androstenedione (A4), and ASD-related traits at 12 and 36 months of age. Traits were measured at 12 months with Autism Observation Scale for Infants (AOSI) and at 36 months with total score on the Social Responsiveness Scale (SRS). One hundred and seventy children had meconium and AOSI, 140 had meconium and SRS, and 137 had meconium and both AOSI and SRS.ResultsSeparate robust linear regressions between each of the log-transformed androgens and log-transformed SRS scores revealed three-way interaction between sex of the child, sex of the proband, and testosterone concentration. In the adjusted analyses, t-T, u-A4, and u-DHEA (P ≤ 0.01) were positively associated with AOSI scores, while u-T (P = 0.004) and u-DHEA (P = 0.007) were positively associated with SRS total score among females with female probands (n = 10). Additionally, higher concentrations of u-T (P = 0.01) and t-T (P = 0.01) predicted higher SRS total score in males with male probands (n = 63). Limitations Since we explored three-way interactions, this resulted in a limited sample size for some analyses. This study was from an enriched-risk cohort which may limit generalizability, and this study used ASD-assessment scales as outcomes instead of diagnostic categories. Additionally, the novel use of meconium in this study limits the ability to compare the results in this cohort to others due to the paucity of research on meconium.ConclusionsThis study supports the utility of meconium for studies of endogenous fetal metabolism and suggests the sex of older siblings with autism should be considered as a biological variable in relevant studies.

Published
2020

22. Dietary fructose feeds hepatic lipogenesis via microbiota-derived acetate.

Author

Zhao, Steven, Jang, Cholsoon, Liu, Joyce, Uehara, Kahealani, Gilbert, Michael, Izzo, Luke, Zeng, Xianfeng, Trefely, Sophie, Fernandez, Sully, Carrer, Alessandro, Miller, Katelyn D, Schug, Zachary T, Snyder, Nathaniel W, Gade, Terence P, Titchenell, Paul M, Rabinowitz, Joshua D, and Wellen, Kathryn E

Subjects
Liver, Hepatocytes, Animals, Mice, Acetates, Citric Acid, Acetyl Coenzyme A, Acetate-CoA Ligase, ATP Citrate (pro-S)-Lyase, Fructose, Fatty Acids, Isotope Labeling, Gene Expression Regulation, Substrate Specificity, Male, Lipogenesis, Gastrointestinal Microbiome, Dietary Sugars, Digestive Diseases, Liver Disease, Nutrition, Obesity, Oral and gastrointestinal, General Science & Technology
Abstract

Consumption of fructose has risen markedly in recent decades owing to the use of sucrose and high-fructose corn syrup in beverages and processed foods1, and this has contributed to increasing rates of obesity and non-alcoholic fatty liver disease2-4. Fructose intake triggers de novo lipogenesis in the liver4-6, in which carbon precursors of acetyl-CoA are converted into fatty acids. The ATP citrate lyase (ACLY) enzyme cleaves cytosolic citrate to generate acetyl-CoA, and is upregulated after consumption of carbohydrates7. Clinical trials are currently pursuing the inhibition of ACLY as a treatment for metabolic diseases8. However, the route from dietary fructose to hepatic acetyl-CoA and lipids remains unknown. Here, using in vivo isotope tracing, we show that liver-specific deletion of Acly in mice is unable to suppress fructose-induced lipogenesis. Dietary fructose is converted to acetate by the gut microbiota9, and this supplies lipogenic acetyl-CoA independently of ACLY10. Depletion of the microbiota or silencing of hepatic ACSS2, which generates acetyl-CoA from acetate, potently suppresses the conversion of bolus fructose into hepatic acetyl-CoA and fatty acids. When fructose is consumed more gradually to facilitate its absorption in the small intestine, both citrate cleavage in hepatocytes and microorganism-derived acetate contribute to lipogenesis. By contrast, the lipogenic transcriptional program is activated in response to fructose in a manner that is independent of acetyl-CoA metabolism. These data reveal a two-pronged mechanism that regulates hepatic lipogenesis, in which fructolysis within hepatocytes provides a signal to promote the expression of lipogenic genes, and the generation of microbial acetate feeds lipogenic pools of acetyl-CoA.

Published
2020

25. Dietary branched-chain amino acids get to the heart of H3K23Pr

Author

Demetriadou, Christina, Kantner, Daniel S., and Snyder, Nathaniel W.

Subjects
Lysine -- Physiological aspects -- Analysis, Branched chain amino acids -- Physiological aspects -- Analysis, Metabolites -- Physiological aspects -- Analysis, Heart -- Analysis -- Physiological aspects, Acylation -- Analysis -- Physiological aspects, Health care industry
Abstract

Cardiac metabolism provides effects that extend beyond the transformation of energy for the heart to operate effectively. Some metabolites also function as signaling molecules and exert transcriptional changes. Heart failure is a progressive pathology in which these metabolite functions falter. In this issue of the JCI, Yang et al. describe a protective effect from a low-branched chain amino acid (BCAA) diet in a mouse model of heart failure. The findings implicate a propionylation mark on histone H3 lysine 23 (H3K23Pr), previously shown to be dependent on the BCAA isoleucine, in transcriptional control of the cardiac stress response. The result underscores the interplay between metabolism and histone acylation, highlighting targeted dietary and pharmacological intervention as a means to decelerate cardiac hypertrophy., Histone lysine acylations and branched-chain amino acid metabolism In eukaryotic cells, the genome is elegantly packed into structured chromatin with DNA wrapped around histone octamers. Covalent posttranslational modifications (PTMs) on [...]

Published
2023
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26. Safety, pharmacodynamics, and potential benefit of omaveloxolone in Friedreich ataxia.

Author

Lynch, David, Farmer, Jennifer, Hauser, Lauren, Blair, Ian, Wang, Qing, Mesaros, Clementina, Snyder, Nathaniel, Boesch, Sylvia, Chin, Melanie, Delatycki, Martin, Giunti, Paola, Goldsberry, Angela, Hoyle, Chad, McBride, Michael, Nachbauer, Wolfgang, OGrady, Megan, Perlman, Susan, Subramony, S, Wilmot, George, Zesiewicz, Theresa, and Meyer, Colin

Subjects
Adolescent, Adult, Dose-Response Relationship, Drug, Female, Friedreich Ataxia, Humans, Male, NF-E2-Related Factor 2, NF-kappa B, Treatment Outcome, Triterpenes, Young Adult
Abstract

OBJECTIVE: Previous studies have demonstrated that suppression of Nrf2 in Friedreich ataxia tissues contributes to excess oxidative stress, mitochondrial dysfunction, and reduced ATP production. Omaveloxolone, an Nrf2 activator and NF-kB suppressor, targets dysfunctional inflammatory, metabolic, and bioenergetic pathways. The dose-ranging portion of this Phase 2 study assessed the safety, pharmacodynamics, and potential benefit of omaveloxolone in Friedreich ataxia patients (NCT02255435). METHODS: Sixty-nine Friedreich ataxia patients were randomized 3:1 to either omaveloxolone or placebo administered once daily for 12 weeks. Patients were randomized in cohorts of eight patients, at dose levels of 2.5-300 mg/day. RESULTS: Omaveloxolone was well tolerated, and adverse events were generally mild. Optimal pharmacodynamic changes (noted by changes in ferritin and GGT) were observed at doses of 80 and 160 mg/day. No significant changes were observed in the primary outcome, peak work load in maximal exercise testing (0.9 ± 2.9 W, placebo corrected). At the 160 mg/day dose, omaveloxolone improved the secondary outcome of the mFARS by 3.8 points versus baseline (P = 0.0001) and by 2.3 points versus placebo (P = 0.06). Omaveloxolone produced greater improvements in mFARS in patients that did not have musculoskeletal foot deformity (pes cavus). In patients without this foot deformity, omaveloxolone improved mFARS by 6.0 points from baseline (P

Published
2019

28. Thymidine rescues ATR kinase inhibitor-induced deoxyuridine contamination in genomic DNA, cell death, and interferon-α/β expression

Author

Sugitani, Norie, Vendetti, Frank P., Cipriano, Andrew J., Pandya, Pinakin, Deppas, Joshua J., Moiseeva, Tatiana N., Schamus-Haynes, Sandra, Wang, Yiyang, Palmer, Drake, Osmanbeyoglu, Hatice U., Bostwick, Anna, Snyder, Nathaniel W., Gong, Yi-Nan, Aird, Katherine M., Delgoffe, Greg M., Beumer, Jan H., and Bakkenist, Christopher J.

Published
2022
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29. O-GlcNAc transferase regulates glioblastoma acetate metabolism via regulation of CDK5-dependent ACSS2 phosphorylation

Author

Ciraku, Lorela, Bacigalupa, Zachary A., Ju, Jing, Moeller, Rebecca A., Le Minh, Giang, Lee, Rusia H., Smith, Michael D., Ferrer, Christina M., Trefely, Sophie, Izzo, Luke T., Doan, Mary T., Gocal, Wiktoria A., D’Agostino, Luca, Shi, Wenyin, Jackson, Joshua G., Katsetos, Christos D., Wellen, Kathryn E., Snyder, Nathaniel W., and Reginato, Mauricio J.

Published
2022
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30. Meconium as an Analyte for Androgen Exposure: Analysis Through Varying Maternal‐Fetal Biomarkers.

Author

Knudsen, Nicole, Tang, Stacey, Lauzon, Sylvie, Dhaurali, Supriya, Snyder, Nathaniel W., and Voegtline, Kristin M.

Abstract

Meconium, the first stool produced by neonates, has been used as an analyte for exogenous fetal exposures. However, few studies have investigated the relationship between meconium and androgen exposure in utero. Here, we examine the associations of testosterone and dehydroepiandrosterone (DHEA) across maternal antenatal salivary testosterone, cord blood, meconium, and infant salivary testosterone. A total of 47 women with singleton, uncomplicated pregnancies, and their infants were included in this study. Participants were recruited from an academic obstetric clinic. Maternal saliva was collected at 36‐weeks' gestation. Cord blood and meconium were collected at birth. Infant salivary testosterone was collected at 1 and 4 weeks of age. Multivariate model results showed that meconium testosterone was associated with neonatal testosterone at 1 (F = 5.62, p = 0.029) and 4 weeks (F = 4.28, p = 0.048) postnatal age; no sex differences were detected. This study suggests meconium is a valuable tool for evaluating endogenous androgen exposure and should be used in future studies to investigate the fetal hormonal milieu. [ABSTRACT FROM AUTHOR]

Published
2024
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31. A Real-Time and Robust Multivariate Estimator for Dynamic Systems with Heavy-Tailed Additive Uncertainties

Author

Snyder, Nathaniel Jeffrey

Subjects
Mechanical engineering, Distributed Computation, Heavy Tailed Densities, Kalman Filtering, Multivariate Dynamic Systems, State Estimation
Abstract

In this dissertation, a real-time, analytic and recursive multivariate state-estimation algorithm is developed for time-invariant, time-varying and nonlinear dynamical systems. Unlike Gaussian based state-estimation algorithms, the proposed state-estimation algorithm uses Cauchy random variables to model the uncertainties in the process and measurement functions. For this reason, it is referred to as the multivariate Cauchy estimator (MCE). The MCE uses a characteristic function representation of the conditional probability density function of the system state vector, given the measurement history, which generates the conditional mean and covariance estimates of the system state vector at each estimation step. The characteristic function of the MCE is enhanced in this dissertation from its previous form by an innovative, computationally tractable, and reduced structure. In particular, the backward recursive, or tree-like, evaluation procedure of the previously-used characteristic function is replaced by a linear parameterization. This linear parameterization compresses the backward recursive characteristic function at each estimation step and allows similar terms of the characteristic function to now be combined together, which was previously not possible. Compressing the characteristic function is shown to lead to the elimination of over 99% of terms that previously comprised it after several estimation steps, although the number of terms after a measurement update still grows. Therefore, a method is developed to run the MCE for arbitrary simulation lengths and for the multivariate setting, despite the growing size of the characteristic function. Furthermore, the estimation structure of the MCE is extended to handle nonlinearities in both the system dynamics and the measurement model, in a fashion similar to that of the extended Kalman filter. It is then shown that the MCE algorithm can achieve real-time computational performance by exploiting the parallel structure of the compressed characteristic function, which is done by distributing the computation onto general-purpose graphical processing units. Through several linear and nonlinear dynamic simulations, the MCE and the extended MCE are shown to outperform the Kalman filter and the extended Kalman filter, respectively, for dynamical systems within heavy-tailed noise environments. Monte Carlo experiments illustrate the exciting robustness properties of the proposed estimator over the class of symmetric alpha-stable probability density functions.

Published
2023

32. The Glucose Transporter 5 Enhances CAR-T Cell Metabolic Function and Anti-tumour Durability

Author

O'Connor, Roddy, primary, Valentić, Bakir, additional, Kelly, Andre, additional, Shestov, Alexander, additional, Gan, Zhiyang, additional, Shen, Feng, additional, Chatoff, Adam, additional, Jaccard, Alison, additional, Crispim, Claudia, additional, Scholler, John, additional, Heeke, Simon, additional, Snyder, Nathaniel, additional, Ghassemi, Saba, additional, Jones, Nicholas, additional, and Gill, Saar, additional

Published
2024
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33. De novo purine metabolism is a metabolic vulnerability of cancers with low p16 expression

Author

Tangudu, Naveen Kumar, primary, Buj, Raquel, additional, Wang, Hui, additional, Wang, Jiefei, additional, Cole, Aidan R, additional, Uboveja, Apoorva, additional, Fang, Richard, additional, Amalric, Amandine, additional, Yang, Baixue, additional, Chatoff, Adam, additional, Crispim, Claudia V, additional, Sajjakulnukit, Peter, additional, Lyons, Maureen A, additional, Cooper, Kristine, additional, Hempel, Nadine, additional, Lyssiotis, Costas A, additional, Chandran, Uma R, additional, Snyder, Nathaniel W., additional, and Aird, Katherine M, additional

Published
2024
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34. WITHDRAWN: SAH is a major metabolic sensor mediating worsening metabolic crosstalk in metabolic syndrome

Author

Cueto, Ramon, primary, Shen, Wen, additional, Liu, Lu, additional, Wang, Xianwei, additional, Wu, Sheng, additional, Mohsin, Sadia, additional, Yang, Ling, additional, Khan, Mohsin, additional, Hu, Wenhui, additional, Snyder, Nathaniel, additional, Wu, Qinghua, additional, Ji, Yong, additional, Yang, Xiao-Feng, additional, and Wang, Hong, additional

Published
2024
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35. Differences in testosterone and its precursors by sex of the offspring in meconium

Author

Frey, Alexander J, Park, Bo Y, Schriver, Emily R, Feldman, Daniel R, Parry, Samuel, Croen, Lisa A, Fallin, Daniele M, Hertz-Picciotto, Irva, Newschaffer, Craig J, and Snyder, Nathaniel W

Subjects
Analytical Chemistry, Chemical Sciences, Pediatric, Brain Disorders, Neurosciences, Androstenedione, Androsterone, Chromatography, Liquid, Cohort Studies, Dehydroepiandrosterone, Female, Humans, Infant, Newborn, Male, Mass Spectrometry, Meconium, Sex Factors, Temperature, Testosterone, Prenatal development, Steroids, Androgens, Mass spectrometry, Sexual differentiation, Biochemistry and Cell Biology, Endocrinology & Metabolism, Biochemistry and cell biology, Analytical chemistry
Abstract

Prenatal metabolism exerts profound effects on development. The first stool of the newborn, meconium, provides a window into the prenatal metabolic environment. The objective of this study was to examine the feasibility of meconium as a novel matrix to quantify prenatal steroid levels. We quantified parameters of analytical interest regarding the use of meconium, including sample stability. We hypothesized that meconium steroid content would differ by sex, prompting analysis of meconium to test effects of prenatal steroid metabolism. Meconium from 193 newborns enrolled in the Early Autism Risk Longitudinal Investigation (EARLI) study, including 107 males, and 86 females, were analyzed by isotope dilution-liquid chromatography-high resolution mass spectrometry (ID-LC-HRMS) while blinded to identity for testosterone (T), androstenedione (AD), and dehydroepiandrosterone (DHEA). Steroid levels were compared by sex, and investigations of potential trends resulting from sample storage or processing was conducted. The unconjugated steroid content of meconium in ng/g (mean, standard deviation) was for males: T (2.67, 8.99), AD (20.01, 28.12), DHEA (13.96, 23.57) and for females: T (0.82, 1.63), AD (22.32, 24.38), DHEA (21.06, 43.49). T was higher in meconium from males (p=0.0333), and DHEA was higher in meconium from females (p=0.0202). 6 female and 3 male T values were below the limit of detection. No extreme variability in hydration or trend in steroid levels by storage time was detected. Sexually dimorphic levels of hormones may reflect gestational differentiation, and future studies should consider meconium analysis.

Published
2017

36. Validation of highly sensitive simultaneous targeted and untargeted analysis of keto-steroids by Girard P derivatization and stable isotope dilution-liquid chromatography-high resolution mass spectrometry

Author

Frey, Alexander J, Wang, Qingqing, Busch, Christine, Feldman, Daniel, Bottalico, Lisa, Mesaros, Clementina A, Blair, Ian A, Vachani, Anil, and Snyder, Nathaniel W

Subjects
Bioengineering, Good Health and Well Being, Androstenedione, Chromatography, Liquid, Dehydroepiandrosterone, Humans, Mass Spectrometry, Serum, Spectrometry, Mass, Electrospray Ionization, Steroids, Testosterone, Girard P, High resolution/accurate mass, Liquid chromatography, Mass spectrometry, Steroid, Clinical Sciences, Endocrinology & Metabolism
Abstract

A multiplexed quantitative method for the analysis of three major unconjugated steroids in human serum by stable isotope dilution liquid chromatography-high resolution mass spectrometry (LC-HRMS) was developed and validated on a Q Exactive Plus hybrid quadrupole/Orbitrap mass spectrometer. This quantification utilized isotope dilution and Girard P derivatization on the keto-groups of testosterone (T), androstenedione (AD) and dehydroepiandrosterone (DHEA) to improve ionization efficiency using electrospray ionization. Major isomeric compounds to T and DHEA; the inactive epimer of testosterone (epiT), and the metabolite of AD, 5α-androstanedione (5α-AD) were completely resolved on a biphenyl column within an 18min method. Inter- and intra-day method validation using LC-HRMS with qualifying product ions was performed and acceptable analytical performance was achieved. The method was further validated by comparing steroid levels from 100μL of serum from young vs older subjects. Since this approach provides high-dimensional HRMS data, untargeted analysis by age group was performed. DHEA and T were detected among the top analytes most significantly different across the two groups after untargeted LC-HRMS analysis, as well as a number of other still unknown metabolites, indicating the potential for combined targeted/untargeted analysis in steroid analysis.

Published
2016

37. Selective and Brain-Penetrant ACSS2 Inhibitors Target Breast Cancer Brain Metastatic Cells

Author

Esquea, Emily, Ciraku, Lorela, Young, Riley, Merzy, Jessica, Talarico, Alexandra, Ahmed, Nusaiba, Karuppiah, Mangalam, Ramesh, Anna, Chatoff, Adam, Crispim, Claudia, Rashad, Adel, Cocklin, Simon, Snyder, Nathaniel, Beld, Joris, Simone, Nicole, Reginato, Mauricio, Dick, Alexej, Esquea, Emily, Ciraku, Lorela, Young, Riley, Merzy, Jessica, Talarico, Alexandra, Ahmed, Nusaiba, Karuppiah, Mangalam, Ramesh, Anna, Chatoff, Adam, Crispim, Claudia, Rashad, Adel, Cocklin, Simon, Snyder, Nathaniel, Beld, Joris, Simone, Nicole, Reginato, Mauricio, and Dick, Alexej

Abstract

Breast cancer brain metastasis (BCBM) typically results in an end-stage diagnosis and is hindered by a lack of brain-penetrant drugs. Tumors in the brain rely on the conversion of acetate to acetyl-CoA by the enzyme acetyl-CoA synthetase 2 (ACSS2), a key regulator of fatty acid synthesis and protein acetylation. Here, we used a computational pipeline to identify novel brain-penetrant ACSS2 inhibitors combining pharmacophore-based shape screen methodology with absorption, distribution, metabolism, and excretion (ADME) property predictions. We identified compounds AD-5584 and AD-8007 that were validated for specific binding affinity to ACSS2. Treatment of BCBM cells with AD-5584 and AD-8007 leads to a significant reduction in colony formation, lipid storage, acetyl-CoA levels and cell survival in vitro. In an ex vivo brain-tumor slice model, treatment with AD-8007 and AD-5584 reduced pre-formed tumors and synergized with irradiation in blocking BCBM tumor growth. Treatment with AD-8007 reduced tumor burden and extended survival in vivo. This study identifies selective brain-penetrant ACSS2 inhibitors with efficacy towards breast cancer brain metastasis.

Published
2024

38. The helminth‐derived peptide, FhHDM‐1, reverses the trained phenotype of NOD bone‐marrow‐derived macrophages and regulates proinflammatory responses.

Author

Quinteros, Susel Loli, Snyder, Nathaniel W., Chatoff, Adam, Ryan, Fiona, O'Brien, Bronwyn, and Donnelly, Sheila

Subjects
PEPTIDES, MACROPHAGES, PHENOTYPES, BONE marrow cells, MACROPHAGE inflammatory proteins
Abstract

This article explores the concept of "trained immunity" in bone-marrow-derived macrophages and its role in the development of type 1 diabetes. The study focuses on macrophages from nonobese diabetic (NOD) mice and finds that they exhibit characteristics of trained immunity, such as increased histone methylation, glycolysis, and proinflammatory cytokine production. The authors suggest that previous infections or changes in gut microbiota may train myeloid cells in the bone marrow, leading to an amplified proinflammatory response and the initiation of autoimmunity in type 1 diabetes. The article also discusses the potential therapeutic effects of a peptide called FhHDM-1, secreted by the parasitic worm Fasciola hepatica, in preventing type 1 diabetes in mice. Administering FhHDM-1 to mice resulted in a reduction in histone methylation, a shift in macrophage metabolism, and a decrease in proinflammatory responses. These findings suggest that FhHDM-1 may alter the epigenetic imprint of macrophages, regulating immune responses and potentially preventing type 1 diabetes and other autoimmune/inflammatory disorders. [Extracted from the article]

Published
2024
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41. αKG-mediated carnitine synthesis promotes homologous recombination via histone acetylation

Author

Uboveja, Apoorva, primary, Huang, Zhentai, additional, Buj, Raquel, additional, Amalric, Amandine, additional, Wang, Hui, additional, Tangudu, Naveen Kumar, additional, Cole, Aidan R., additional, Megill, Emily, additional, Kantner, Daniel, additional, Chatoff, Adam, additional, Ahmad, Hafsah, additional, Marcinkiewicz, Mariola M., additional, Disharoon, Julie A., additional, Graff, Sarah, additional, Dahl, Erika S., additional, Hempel, Nadine, additional, Stallaert, Wayne, additional, Sidoli, Simone, additional, Bitler, Benjamin G., additional, Long, David T., additional, Snyder, Nathaniel W., additional, and Aird, Katherine M., additional

Published
2024
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42. Acyl-CoA thioesterase-2 facilitates β-oxidation in glycolytic skeletal muscle in a lipid supply dependent manner

Author

Bekeova, Carmen, primary, Han, Ji In, additional, Xu, Heli, additional, Kerr, Evan, additional, Blackburne, Brittney, additional, Lynch, Shannon C., additional, Mesaros, Clementina, additional, Murgia, Marta, additional, Vadigepalli, Rajanikanth, additional, Beld, Joris, additional, Leonardi, Roberta, additional, Snyder, Nathaniel W., additional, and Seifert, Erin L., additional

Published
2024
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43. Programmed death ligand-1 expression on donor T cells drives graft-versus-host disease lethality

Author

Saha, Asim, O’Connor, Roddy S, Thangavelu, Govindarajan, Lovitch, Scott B, Dandamudi, Durga Bhavani, Wilson, Caleph B, Vincent, Benjamin G, Tkachev, Victor, Pawlicki, Jan M, Furlan, Scott N, Kean, Leslie S, Aoyama, Kazutoshi, Taylor, Patricia A, Panoskaltsis-Mortari, Angela, Foncea, Rocio, Ranganathan, Parvathi, Devine, Steven M, Burrill, Joel S, Guo, Lili, Sacristan, Catarina, Snyder, Nathaniel W, Blair, Ian A, Milone, Michael C, Dustin, Michael L, Riley, James L, Bernlohr, David A, Murphy, William J, Fife, Brian T, Munn, David H, Miller, Jeffrey S, Serody, Jonathan S, Freeman, Gordon J, Sharpe, Arlene H, Turka, Laurence A, and Blazar, Bruce R

Subjects
Transplantation, Cancer, Rare Diseases, Orphan Drug, Stem Cell Research, Stem Cell Research - Nonembryonic - Non-Human, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Animals, Apoptosis, B7-H1 Antigen, Bone Marrow Cells, Bone Marrow Transplantation, Cytokines, Female, Glucose, Glutamine, Glycolysis, Graft vs Host Disease, Humans, Inflammation, Leukocytes, Mononuclear, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Oxygen, Phosphorylation, Programmed Cell Death 1 Receptor, Signal Transduction, T-Lymphocytes, Treatment Outcome, Medical and Health Sciences, Immunology
Abstract

Programmed death ligand-1 (PD-L1) interaction with PD-1 induces T cell exhaustion and is a therapeutic target to enhance immune responses against cancer and chronic infections. In murine bone marrow transplant models, PD-L1 expression on host target tissues reduces the incidence of graft-versus-host disease (GVHD). PD-L1 is also expressed on T cells; however, it is unclear whether PD-L1 on this population influences immune function. Here, we examined the effects of PD-L1 modulation of T cell function in GVHD. In patients with severe GVHD, PD-L1 expression was increased on donor T cells. Compared with mice that received WT T cells, GVHD was reduced in animals that received T cells from Pdl1-/- donors. PD-L1-deficient T cells had reduced expression of gut homing receptors, diminished production of inflammatory cytokines, and enhanced rates of apoptosis. Moreover, multiple bioenergetic pathways, including aerobic glycolysis, oxidative phosphorylation, and fatty acid metabolism, were also reduced in T cells lacking PD-L1. Finally, the reduction of acute GVHD lethality in mice that received Pdl1-/- donor cells did not affect graft-versus-leukemia responses. These data demonstrate that PD-L1 selectively enhances T cell-mediated immune responses, suggesting a context-dependent function of the PD-1/PD-L1 axis, and suggest selective inhibition of PD-L1 on donor T cells as a potential strategy to prevent or ameliorate GVHD.

Published
2016

44. LC-quadrupole/Orbitrap high-resolution mass spectrometry enables stable isotope-resolved simultaneous quantification and 13C-isotopic labeling of acyl-coenzyme A thioesters

Author

Frey, Alexander J, Feldman, Daniel R, Trefely, Sophie, Worth, Andrew J, Basu, Sankha S, and Snyder, Nathaniel W

Subjects
Bioengineering, Nutrition, Biotechnology, Acyl Coenzyme A, Carbon Isotopes, Cell Line, Tumor, Chromatography, Liquid, Esters, Humans, Isotope Labeling, Bioanalytical methods, Coenzyme A, Mass spectrometry, Metabolism, Stable isotope labeling, Chemical Sciences, Biological Sciences, Engineering, Analytical Chemistry
Abstract

Acyl-coenzyme A (acyl-CoA) thioesters are evolutionarily conserved, compartmentalized, and energetically activated substrates for biochemical reactions. The ubiquitous involvement of acyl-CoA thioesters in metabolism, including the tricarboxylic acid cycle, fatty acid metabolism, amino acid degradation, and cholesterol metabolism highlights the broad applicability of applied measurements of acyl-CoA thioesters. However, quantitation of acyl-CoA levels provides only one dimension of metabolic information and a more complete description of metabolism requires the relative contribution of different precursors to individual substrates and pathways. Using two distinct stable isotope labeling approaches, acyl-CoA thioesters can be labeled with either a fixed [(13)C3(15)N1] label derived from pantothenate into the CoA moiety or via variable [(13)C] labeling into the acyl chain from metabolic precursors. Liquid chromatography-hybrid quadrupole/Orbitrap high-resolution mass spectrometry using parallel reaction monitoring, but not single ion monitoring, allowed the simultaneous quantitation of acyl-CoA thioesters by stable isotope dilution using the [(13)C3(15)N1] label and measurement of the incorporation of labeled carbon atoms derived from [(13)C6]-glucose, [(13)C5(15)N2]-glutamine, and [(13)C3]-propionate. As a proof of principle, we applied this method to human B cell lymphoma (WSU-DLCL2) cells in culture to precisely describe the relative pool size and enrichment of isotopic tracers into acetyl-, succinyl-, and propionyl-CoA. This method will allow highly precise, multiplexed, and stable isotope-resolved determination of metabolism to refine metabolic models, characterize novel metabolism, and test modulators of metabolic pathways involving acyl-CoA thioesters.

Published
2016

45. Regulation of nuclear epigenome by mitochondrial DNA heteroplasmy

Author

Kopinski, Piotr K., Janssen, Kevin A., Schaefer, Patrick M., Trefely, Sophie, Perry, Caroline E., Potluri, Prasanth, Tintos-Hernandez, Jesus A., Singh, Larry N., Karch, Kelly R., Campbell, Sydney L., Doan, Mary T., Jiang, Helen, Nissim, Itzhak, Nakamaru-Ogiso, Eiko, Wellen, Kathryn E., Snyder, Nathaniel W., Garcia, Benjamin A., and Wallace, Douglas C.

Published
2019

46. Gut microbiota modulate dendritic cell antigen presentation and radiotherapy-induced antitumor immune response

Author

Uribe-Herranz, Mireia, Rafail, Stavros, Beghi, Silvia, Gil-de-Gomez, Luis, Verginadis, Ioannis, Bittinger, Kyle, Pustylnikov, Sergey, Pierini, Stefano, Perales-Linares, Renzo, Blair, Ian A., Mesaros, Clementina A., Snyder, Nathaniel W., Bushman, Frederic, Koumenis, Constantinos, and Facciabene, Andrea

Subjects
Thermo Fisher Scientific Inc., Cancer treatment, Antigens, Microbiota (Symbiotic organisms), Tumors, Radiotherapy, Dendritic cells, Immune response, Antibacterial agents, Scientific equipment industry, T cells, Antibiotics, Cancer, Esters, Vancomycin, Diseases, Bacteria, Metabolites, Health care industry, University of Pennsylvania
Abstract

Alterations in gut microbiota impact the pathophysiology of several diseases, including cancer. Radiotherapy (RT), an established curative and palliative cancer treatment, exerts potent immune modulatory effects, inducing tumor- associated antigen (TAA) cross-priming with antitumor [CD8.sup.+] T cell elicitation and abscopal effects. We tested whether the gut microbiota modulates antitumor immune response following RT distal to the gut. Vancomycin, an antibiotic that acts mainly on gram-positive bacteria and is restricted to the gut, potentiated the RT-induced antitumor immune response and tumor growth inhibition. This synergy was dependent on TAA cross presentation to cytolytic [CD8.sup.+] T cells and on IFN-[gamma]. Notably, butyrate, a metabolite produced by the vancomycin-depleted gut bacteria, abrogated the vancomycin effect. In conclusion, depletion of vancomycin-sensitive bacteria enhances the antitumor activity of RT, which has important clinical ramifications., Introduction Radiotherapy (RT) is a well-established antitumor treatment, with more than 50% of newly diagnosed cancer patients with solid tumors receiving RT at some point during their treatment, usually in [...]

Published
2020
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50. Selective and brain-penetrant ACSS2 inhibitors target breast cancer brain metastatic cells.

Author

Esquea, Emily M., Ciraku, Lorela, Young, Riley G., Merzy, Jessica, Talarico, Alexandra N., Ahmed, Nusaiba N., Karuppiah, Mangalam, Ramesh, Anna, Chatoff, Adam, Crispim, Claudia V., Rashad, Adel A., Cocklin, Simon, Snyder, Nathaniel W., Beld, Joris, Simone, Nicole L., Reginato, Mauricio J., and Dick, Alexej

Subjects
ACETYLCOENZYME A, TUMOR growth, CELL survival, BRAIN tumors, PROTEIN synthesis, FATTY acids
Abstract

Breast cancer brain metastasis (BCBM) typically results in an end-stage diagnosis and is hindered by a lack of brain-penetrant drugs. Tumors in the brain rely on the conversion of acetate to acetyl-CoA by the enzyme acetyl-CoA synthetase 2 (ACSS2), a key regulator of fatty acid synthesis and protein acetylation. Here, we used a computational pipeline to identify novel brain-penetrant ACSS2 inhibitors combining pharmacophore-based shape screen methodology with absorption, distribution, metabolism, and excretion (ADME) property predictions. We identified compounds AD-5584 and AD-8007 that were validated for specific binding affinity to ACSS2. Treatment of BCBM cells with AD-5584 and AD-8007 leads to a significant reduction in colony formation, lipid storage, acetyl-CoA levels and cell survival in vitro. In an ex vivo brain-tumor slice model, treatment with AD-8007 and AD-5584 reduced pre-formed tumors and synergized with irradiation in blocking BCBM tumor growth. Treatment with AD-8007 reduced tumor burden and extended survival in vivo. This study identifies selective brain-penetrant ACSS2 inhibitors with efficacy towards breast cancer brain metastasis. [ABSTRACT FROM AUTHOR]

Published
2024
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