Your search keyword '"Gerszten, Robert E."' showing total 29 results

1. Proteomic signature of HIV-associated subclinical left atrial remodeling and incident heart failure.

Author

Peterson, Tess E., Hahn, Virginia S., Moaddel, Ruin, Zhu, Min, Haberlen, Sabina A., Palella, Frank J., Plankey, Michael, Bader, Joel S., Lima, Joao A. C., Gerszten, Robert E., Rotter, Jerome I., Rich, Stephen S., Heckbert, Susan R., Kirk, Gregory D., Piggott, Damani A., Ferrucci, Luigi, Margolick, Joseph B., Brown, Todd T., Wu, Katherine C., and Post, Wendy S.

Subjects

CARDIAC magnetic resonance imaging, IMMUNE checkpoint proteins, TUMOR necrosis factors, HEART failure, LEFT heart atrium

Abstract

People living with HIV are at higher risk of heart failure and associated left atrial remodeling compared to people without HIV. Mechanisms are unclear but have been linked to inflammation and premature aging. Here we obtain plasma proteomics concurrently with cardiac magnetic resonance imaging in two independent study populations to identify parallels between HIV-related and aging-related immune dysfunction that could contribute to atrial remodeling and clinical heart failure. We discover a plasma proteomic signature that may in part reflect or contribute to HIV-associated atrial remodeling, many features of which are associated with older age and time to incident heart failure among an independent community-based cohort without HIV. This proteomic profile was statistically enriched for immune checkpoint proteins, tumor necrosis factor signaling, ephrin signaling, and extracellular matrix organization, identifying possible shared pathways in HIV and aging that may contribute to risk of heart failure. Mechanisms underlying excess risk of heart failure among people with HIV are unclear. Here, the authors identify a proteomic signature enriched in immune activation and extracellular matrix remodeling that may reflect shared pathways in HIV and aging that contribute to risk of heart failure. [ABSTRACT FROM AUTHOR]

Published

2025

2. Identification of proteins associated with type 2 diabetes risk in diverse racial and ethnic populations.

Author

Liu, Shuai, Zhu, Jingjing, Zhong, Hua, Wu, Chong, Xue, Haoran, Darst, Burcu F., Guo, Xiuqing, Durda, Peter, Tracy, Russell P., Liu, Yongmei, Johnson, W. Craig, Taylor, Kent D., Manichaikul, Ani W., Goodarzi, Mark O., Gerszten, Robert E., Clish, Clary B., Chen, Yii-Der Ida, Highland, Heather, Haiman, Christopher A., and Gignoux, Christopher R.

Abstract

Aims/hypothesis: Several studies have reported associations between specific proteins and type 2 diabetes risk in European populations. To better understand the role played by proteins in type 2 diabetes aetiology across diverse populations, we conducted a large proteome-wide association study using genetic instruments across four racial and ethnic groups: African; Asian; Hispanic/Latino; and European. Methods: Genome and plasma proteome data from the Multi-Ethnic Study of Atherosclerosis (MESA) study involving 182 African, 69 Asian, 284 Hispanic/Latino and 409 European individuals residing in the USA were used to establish protein prediction models by using potentially associated cis- and trans-SNPs. The models were applied to genome-wide association study summary statistics of 250,127 type 2 diabetes cases and 1,222,941 controls from different racial and ethnic populations. Results: We identified three, 44 and one protein associated with type 2 diabetes risk in Asian, European and Hispanic/Latino populations, respectively. Meta-analysis identified 40 proteins associated with type 2 diabetes risk across the populations, including well-established as well as novel proteins not yet implicated in type 2 diabetes development. Conclusions/interpretation: Our study improves our understanding of the aetiology of type 2 diabetes in diverse populations. Data availability: The summary statistics of multi-ethnic type 2 diabetes GWAS of MVP, DIAMANTE, Biobank Japan and other studies are available from The database of Genotypes and Phenotypes (dbGaP) under accession number phs001672.v3.p1. MESA genetic, proteome and covariate data can be accessed through dbGaP under phs000209.v13.p3. All code is available on GitHub (https://github.com/Arthur1021/MESA-1K-PWAS). [ABSTRACT FROM AUTHOR]

Published

2024

3. Analysis of plasma metabolomes from 11 309 subjects in five population-based cohorts.

Author

Ghosh, Nilanjana, Lejonberg, Carl, Czuba, Tomasz, Dekkers, Koen, Robinson, Richard, Ärnlöv, Johan, Melander, Olle, Smith, Maya Landenhed, Evans, Anne M., Gidlöf, Olof, Gerszten, Robert E., Lind, Lars, Engström, Gunnar, Fall, Tove, and Smith, J. Gustav

Subjects

LIQUID chromatography-mass spectrometry, METABOLOMICS, CLINICAL chemistry, XENOBIOTICS, LOGNORMAL distribution

Abstract

Plasma metabolomics holds potential for precision medicine, but limited information is available to compare the performance of such methods across multiple cohorts. We compared plasma metabolite profiles after an overnight fast in 11,309 participants of five population-based Swedish cohorts (50–80 years, 52% women). Metabolite profiles were uniformly generated at a core laboratory (Metabolon Inc.) with untargeted liquid chromatography mass spectrometry and a comprehensive reference library. Analysis of a second sample obtained one year later was conducted in a subset. Of 1629 detected metabolites, 1074 (66%) were detected in all cohorts while only 10% were unique to one cohort, most of which were xenobiotics or uncharacterized. The major classes were lipids (28%), xenobiotics (22%), amino acids (14%), and uncharacterized (19%). The most abundant plasma metabolome components were the major dietary fatty acids and amino acids, glucose, lactate and creatinine. Most metabolites displayed a log-normal distribution. Temporal variability was generally similar to clinical chemistry analytes but more pronounced for xenobiotics. Extensive metabolite-metabolite correlations were observed but mainly restricted to within each class. Metabolites were broadly associated with clinical factors, particularly body mass index, sex and renal function. Collectively, our findings inform the conduct and interpretation of metabolite association and precision medicine studies. [ABSTRACT FROM AUTHOR]

Published

2024

4. Proteomics and Population Biology in the Cardiovascular Health Study (CHS): design of a study with mentored access and active data sharing.

Author

Austin, Thomas R., McHugh, Caitlin P., Brody, Jennifer A., Bis, Joshua C., Sitlani, Colleen M., Bartz, Traci M., Biggs, Mary L., Bansal, Nisha, Buzkova, Petra, Carr, Steven A., deFilippi, Christopher R., Elkind, Mitchell S. V., Fink, Howard A., Floyd, James S., Fohner, Alison E., Gerszten, Robert E., Heckbert, Susan R., Katz, Daniel H., Kizer, Jorge R., and Lemaitre, Rozenn N.

Subjects

POPULATION biology, PROTEOMICS, INFORMATION sharing, OLDER people, EXPERIMENTAL design

Abstract

Background: In the last decade, genomic studies have identified and replicated thousands of genetic associations with measures of health and disease and contributed to the understanding of the etiology of a variety of health conditions. Proteins are key biomarkers in clinical medicine and often drug-therapy targets. Like genomics, proteomics can advance our understanding of biology. Methods and Results: In the setting of the Cardiovascular Health Study (CHS), a cohort study of older adults, an aptamer-based method that has high sensitivity for low-abundance proteins was used to assay 4979 proteins in frozen, stored plasma from 3188 participants (61% women, mean age 74 years). CHS provides active support, including central analysis, for seven phenotype-specific working groups (WGs). Each CHS WG is led by one or two senior investigators and includes 10 to 20 early or mid-career scientists. In this setting of mentored access, the proteomic data and analytic methods are widely shared with the WGs and investigators so that they may evaluate associations between baseline levels of circulating proteins and the incidence of a variety of health outcomes in prospective cohort analyses. We describe the design of CHS, the CHS Proteomics Study, characteristics of participants, quality control measures, and structural characteristics of the data provided to CHS WGs. We additionally highlight plans for validation and replication of novel proteomic associations. Conclusion: The CHS Proteomics Study offers an opportunity for collaborative data sharing to improve our understanding of the etiology of a variety of health conditions in older adults. [ABSTRACT FROM AUTHOR]

Published

2022

5. Exerkines in health, resilience and disease.

Author

Chow, Lisa S., Gerszten, Robert E., Taylor, Joan M., Pedersen, Bente K., van Praag, Henriette, Trappe, Scott, Febbraio, Mark A., Galis, Zorina S., Gao, Yunling, Haus, Jacob M., Lanza, Ian R., Lavie, Carl J., Lee, Chih-Hao, Lucia, Alejandro, Moro, Cedric, Pandey, Ambarish, Robbins, Jeremy M., Stanford, Kristin I., Thackray, Alice E., and Villeda, Saul

Subjects

*WHITE adipose tissue, *BROWN adipose tissue, *HEART cells, *FAT cells, *NERVOUS system, *TYPE 2 diabetes, *ENDOCRINE glands, *CARDIOVASCULAR diseases, *OBESITY, *SKELETAL muscle, *EXERCISE, *RESEARCH funding, *PEPTIDE hormones

Abstract

The health benefits of exercise are well-recognized and are observed across multiple organ systems. These beneficial effects enhance overall resilience, healthspan and longevity. The molecular mechanisms that underlie the beneficial effects of exercise, however, remain poorly understood. Since the discovery in 2000 that muscle contraction releases IL-6, the number of exercise-associated signalling molecules that have been identified has multiplied. Exerkines are defined as signalling moieties released in response to acute and/or chronic exercise, which exert their effects through endocrine, paracrine and/or autocrine pathways. A multitude of organs, cells and tissues release these factors, including skeletal muscle (myokines), the heart (cardiokines), liver (hepatokines), white adipose tissue (adipokines), brown adipose tissue (baptokines) and neurons (neurokines). Exerkines have potential roles in improving cardiovascular, metabolic, immune and neurological health. As such, exerkines have potential for the treatment of cardiovascular disease, type 2 diabetes mellitus and obesity, and possibly in the facilitation of healthy ageing. This Review summarizes the importance and current state of exerkine research, prevailing challenges and future directions. [ABSTRACT FROM AUTHOR]

Published

2022

6. Lymphocyte activation gene-3-associated protein networks are associated with HDL-cholesterol and mortality in the Trans-omics for Precision Medicine program.

Author

Manichaikul, Ani, Lin, Honghuang, Kang, Chansuk, Yang, Chaojie, Rich, Stephen S., Taylor, Kent D., Guo, Xiuqing, Rotter, Jerome I., Craig Johnson, W., Cornell, Elaine, Tracy, Russell P., Peter Durda, J., Liu, Yongmei, Vasan, Ramachandran S., Adrienne Cupples, L., Gerszten, Robert E., Clish, Clary B., Jain, Deepti, Conomos, Matthew P., and Blackwell, Thomas

Subjects

LYMPHOCYTE transformation, INDIVIDUALIZED medicine, HIGH density lipoproteins, BLOOD proteins, IMMUNE checkpoint proteins, HDL cholesterol

Abstract

Deficiency of the immune checkpoint lymphocyte activation gene-3 (LAG3) protein is significantly associated with both elevated HDL-cholesterol (HDL-C) and myocardial infarction risk. We determined the association of genetic variants within ±500 kb of LAG3 with plasma LAG3 and defined LAG3-associated plasma proteins with HDL-C and clinical outcomes. Whole genome sequencing and plasma proteomics were obtained from the Multi-Ethnic Study of Atherosclerosis (MESA) and the Framingham Heart Study (FHS) cohorts as part of the Trans-Omics for Precision Medicine program. In situ Hi-C chromatin capture was performed in EBV-transformed cell lines isolated from four MESA participants. Genetic association analyses were performed in MESA using multivariate regression models, with validation in FHS. A LAG3-associated protein network was tested for association with HDL-C, coronary heart disease, and all-cause mortality. We identify an association between the LAG3 rs3782735 variant and plasma LAG3 protein. Proteomics analysis reveals 183 proteins significantly associated with LAG3 with four proteins associated with HDL-C. Four proteins discovered for association with all-cause mortality in FHS shows nominal associations in MESA. Chromatin capture analysis reveals significant cis interactions between LAG3 and C1S, LRIG3, TNFRSF1A, and trans interactions between LAG3 and B2M. A LAG3-associated protein network has significant associations with HDL-C and mortality. Rodriguez et al. use whole genome sequencing and plasma proteomics from the Multi-Ethnic Study of Atherosclerosis (MESA) and the Framingham Heart Study (FHS) cohorts of the Trans-Omics for Precision Medicine program and perform in situ Hi-C chromatin capture in cell lines isolated from four MESA participants. They demonstrate that lymphocyte activation gene-3 protein networks are associated with HDL-cholesterol and mortality, which could guide the development of precision medicine. [ABSTRACT FROM AUTHOR]

Published

2022

7. Genomics and transcriptomics landscapes associated to changes in insulin sensitivity in response to endurance exercise training.

Author

Takeshita, Louise Y., Davidsen, Peter K., Herbert, John M., Antczak, Philipp, Hesselink, Matthijs K. C., Schrauwen, Patrick, Weisnagel, S. John, Robbins, Jeremy M., Gerszten, Robert E., Ghosh, Sujoy, Sarzynski, Mark A., Bouchard, Claude, and Falciani, Francesco

Subjects

INSULIN sensitivity, EXERCISE therapy, LANDSCAPE changes, GENETIC variation, GENOMICS

Abstract

Despite good adherence to supervised endurance exercise training (EET), some individuals experience no or little improvement in peripheral insulin sensitivity. The genetic and molecular mechanisms underlying this phenomenon are currently not understood. By investigating genome-wide variants associated with baseline and exercise-induced changes (∆) in insulin sensitivity index (Si) in healthy volunteers, we have identified novel candidate genes whose mouse knockouts phenotypes were consistent with a causative effect on Si. An integrative analysis of functional genomic and transcriptomic profiles suggests genetic variants have an aggregate effect on baseline Si and ∆Si, focused around cholinergic signalling, including downstream calcium and chemokine signalling. The identification of calcium regulated MEF2A transcription factor as the most statistically significant candidate driving the transcriptional signature associated to ∆Si further strengthens the relevance of calcium signalling in EET mediated Si response. [ABSTRACT FROM AUTHOR]

Published

2021

8. The genetic architecture of plasma kynurenine includes cardiometabolic disease mechanisms associated with the SH2B3 gene.

Author

Bagheri, Minoo, Wang, Chuan, Shi, Mingjian, Manouchehri, Ali, Murray, Katherine T., Murphy, Matthew B., Shaffer, Christian M., Singh, Kritika, Davis, Lea K., Jarvik, Gail P., Stanaway, Ian B., Hebbring, Scott, Reilly, Muredach P., Gerszten, Robert E., Wang, Thomas J., Mosley, Jonathan D., and Ferguson, Jane F.

Subjects

KYNURENINE, HEART metabolism disorders, INFLAMMATION, BIOMARKERS, SINGLE nucleotide polymorphisms

Abstract

Inflammation increases the risk of cardiometabolic disease. Delineating specific inflammatory pathways and biomarkers of their activity could identify the mechanistic underpinnings of the increased risk. Plasma levels of kynurenine, a metabolite involved in inflammation, associates with cardiometabolic disease risk. We used genetic approaches to identify inflammatory mechanisms associated with kynurenine variability and their relationship to cardiometabolic disease. We identified single-nucleotide polymorphisms (SNPs) previously associated with plasma kynurenine, including a missense-variant (rs3184504) in the inflammatory gene SH2B3/LNK. We examined the association between rs3184504 and plasma kynurenine in independent human samples, and measured kynurenine levels in SH2B3-knock-out mice and during human LPS-evoked endotoxemia. We conducted phenome scanning to identify clinical phenotypes associated with each kynurenine-related SNP and with a kynurenine polygenic score using the UK-Biobank (n = 456,422), BioVU (n = 62,303), and Electronic Medical Records and Genetics (n = 32,324) databases. The SH2B3 missense variant associated with plasma kynurenine levels and SH2B3−/− mice had significant tissue-specific differences in kynurenine levels.LPS, an acute inflammatory stimulus, increased plasma kynurenine in humans. Mendelian randomization showed increased waist-circumference, a marker of central obesity, associated with increased kynurenine, and increased kynurenine associated with C-reactive protein (CRP). We found 30 diagnoses associated (FDR q < 0.05) with the SH2B3 variant, but not with SNPs mapping to genes known to regulate tryptophan-kynurenine metabolism. Plasma kynurenine may be a biomarker of acute and chronic inflammation involving the SH2B3 pathways. Its regulation lies upstream of CRP, suggesting that kynurenine may be a biomarker of one inflammatory mechanism contributing to increased cardiometabolic disease risk. [ABSTRACT FROM AUTHOR]

Published

2021

9. The choline transporter Slc44a2 controls platelet activation and thrombosis by regulating mitochondrial function.

Author

Bennett, J. Allen, Mastrangelo, Michael A., Ture, Sara K., Smith, Charles O., Loelius, Shannon G., Berg, Rachel A., Shi, Xu, Burke, Ryan M., Spinelli, Sherry L., Cameron, Scott J., Carey, Thomas E., Brookes, Paul S., Gerszten, Robert E., Sabater-Lleal, Maria, de Vries, Paul S., Huffman, Jennifer E., Smith, Nicholas L., Morrell, Craig N., and Lowenstein, Charles J.

Subjects

BLOOD platelet activation, THROMBOTIC thrombocytopenic purpura, CHOLINE, LOCUS (Genetics), OXYGEN consumption, THROMBOSIS

Abstract

Genetic factors contribute to the risk of thrombotic diseases. Recent genome wide association studies have identified genetic loci including SLC44A2 which may regulate thrombosis. Here we show that Slc44a2 controls platelet activation and thrombosis by regulating mitochondrial energetics. We find that Slc44a2 null mice (Slc44a2(KO)) have increased bleeding times and delayed thrombosis compared to wild-type (Slc44a2(WT)) controls. Platelets from Slc44a2(KO) mice have impaired activation in response to thrombin. We discover that Slc44a2 mediates choline transport into mitochondria, where choline metabolism leads to an increase in mitochondrial oxygen consumption and ATP production. Platelets lacking Slc44a2 contain less ATP at rest, release less ATP when activated, and have an activation defect that can be rescued by exogenous ADP. Taken together, our data suggest that mitochondria require choline for maximum function, demonstrate the importance of mitochondrial metabolism to platelet activation, and reveal a mechanism by which Slc44a2 influences thrombosis. Genetic association studies have identified loci including the choline transporter SLC44A2 as a potential regulator of thrombosis. Here the authors report that loss of SLC44A2 impairs platelet activation and thrombosis in mice via a reduction of mitochondrial ATP production. [ABSTRACT FROM AUTHOR]

Published

2020

10. Changes in Citric Acid Cycle and Nucleoside Metabolism Are Associated with Anthracycline Cardiotoxicity in Patients with Breast Cancer.

Author

Asnani, Aarti, Shi, Xu, Farrell, Laurie, Lall, Rahul, Sebag, Igal A., Plana, Juan Carlos, Gerszten, Robert E., and Scherrer-Crosbie, Marielle

Abstract

Anthracyclines and HER2-targeted antibodies are very effective for the treatment of breast cancer, but their use is limited by cardiotoxicity. In this nested case-control study, we assessed the role of intermediary metabolism in 38 women with breast cancer treated with anthracyclines and trastuzumab. Using targeted mass spectrometry to measure 71 metabolites in the plasma, we identified changes in citric acid and aconitic acid that differentiated patients who developed cardiotoxicity from those who did not. In patients with cardiotoxicity, the magnitude of change in citric acid at three months correlated with the change in left ventricular ejection fraction (LVEF) and absolute LVEF at nine months. Patients with cardiotoxicity also demonstrated more pronounced changes in purine and pyrimidine metabolism. Early metabolic changes may therefore provide insight into the mechanisms associated with the development of chemotherapy-associated cardiotoxicity. [ABSTRACT FROM AUTHOR]

Published

2020

11. Profiling of the plasma proteome across different stages of human heart failure.

Author

Egerstedt, Anna, Berntsson, John, Smith, Maya Landenhed, Gidlöf, Olof, Nilsson, Roland, Benson, Mark, Wells, Quinn S., Celik, Selvi, Lejonberg, Carl, Farrell, Laurie, Sinha, Sumita, Shen, Dongxiao, Lundgren, Jakob, Rådegran, Göran, Ngo, Debby, Engström, Gunnar, Yang, Qiong, Wang, Thomas J., Gerszten, Robert E., and Smith, J. Gustav

Subjects

PROTEOMICS, HEART failure treatment, PATHOLOGICAL physiology, COHORT analysis, IMMUNOLOGY

Abstract

Heart failure (HF) is a major public health problem characterized by inability of the heart to maintain sufficient output of blood. The systematic characterization of circulating proteins across different stages of HF may provide pathophysiological insights and identify therapeutic targets. Here we report application of aptamer-based proteomics to identify proteins associated with prospective HF incidence in a population-based cohort, implicating modulation of immunological, complement, coagulation, natriuretic and matrix remodeling pathways up to two decades prior to overt disease onset. We observe further divergence of these proteins from the general population in advanced HF, and regression after heart transplantation. By leveraging coronary sinus samples and transcriptomic tools, we describe likely cardiac and specific cellular origins for several of the proteins, including Nt-proBNP, thrombospondin-2, interleukin-18 receptor, gelsolin, and activated C5. Our findings provide a broad perspective on both cardiac and systemic factors associated with HF development. Heart failure is a major health issue worldwide. Here, Egerstedt et al. perform proteomic profiling of human plasma at different stages of heart failure, providing a comprehensive analysis of changes in the plasma proteome during disease progression. [ABSTRACT FROM AUTHOR]

Published

2019

12. Metabolomics insights into early type 2 diabetes pathogenesis and detection in individuals with normal fasting glucose.

Author

Merino, Jordi, Leong, Aaron, Liu, Ching-Ti, Porneala, Bianca, Walford, Geoffrey A., von Grotthuss, Marcin, Wang, Thomas J., Flannick, Jason, Dupuis, Josée, Levy, Daniel, Gerszten, Robert E., Florez, Jose C., and Meigs, James B.

Abstract

Aims/hypothesis: Identifying the metabolite profile of individuals with normal fasting glucose (NFG [<5.55 mmol/l]) who progressed to type 2 diabetes may give novel insights into early type 2 diabetes disease interception and detection.Methods: We conducted a population-based prospective study among 1150 Framingham Heart Study Offspring cohort participants, age 40-65 years, with NFG. Plasma metabolites were profiled by LC-MS/MS. Penalised regression models were used to select measured metabolites for type 2 diabetes incidence classification (training dataset) and to internally validate the discriminatory capability of selected metabolites beyond conventional type 2 diabetes risk factors (testing dataset).Results: Over a follow-up period of 20 years, 95 individuals with NFG developed type 2 diabetes. Nineteen metabolites were selected repeatedly in the training dataset for type 2 diabetes incidence classification and were found to improve type 2 diabetes risk prediction beyond conventional type 2 diabetes risk factors (AUC was 0.81 for risk factors vs 0.90 for risk factors + metabolites, p = 1.1 × 10−4). Using pathway enrichment analysis, the nitrogen metabolism pathway, which includes three prioritised metabolites (glycine, taurine and phenylalanine), was significantly enriched for association with type 2 diabetes risk at the false discovery rate of 5% (p = 0.047). In adjusted Cox proportional hazard models, the type 2 diabetes risk per 1 SD increase in glycine, taurine and phenylalanine was 0.65 (95% CI 0.54, 0.78), 0.73 (95% CI 0.59, 0.9) and 1.35 (95% CI 1.11, 1.65), respectively. Mendelian randomisation demonstrated a similar relationship for type 2 diabetes risk per 1 SD genetically increased glycine (OR 0.89 [95% CI 0.8, 0.99]) and phenylalanine (OR 1.6 [95% CI 1.08, 2.4]).Conclusions/interpretation: In individuals with NFG, information from a discrete set of 19 metabolites improved prediction of type 2 diabetes beyond conventional risk factors. In addition, the nitrogen metabolism pathway and its components emerged as a potential effector of earliest stages of type 2 diabetes pathophysiology. [ABSTRACT FROM AUTHOR]

Published

2018

13. Atherosclerotic Coronary Disease.

Author

Runge, Marschall S., Patterson, Cam, Gerszten, Robert E., and Rosenzweig, Anthony

Abstract

Atherosclerotic coronary artery disease is a complex biological process resulting in narrowing of the arterial vessels that supply the heart muscle with oxygen and nutrients. Despite major advances in the understanding of this process and its clinical management, it remains a major cause of morbidity and mortality throughout the world. In the United States, coronary artery disease accounts for about 500,000 deaths each year, of which about half are sudden. This chapter reviews the clinical presentation and treatment of this condition, focusing on advances and the biological insights they provide. Some of the leading hypotheses regarding the molecular mechanisms underlying this incompletely understood condition are considered. [ABSTRACT FROM AUTHOR]

Published

2006

14. Reply to 'Lactate as a major myokine and exerkine'.

Author

Chow, Lisa S., Gerszten, Robert E., Taylor, Joan M., Pedersen, Bente K., van Praag, Henriette, Trappe, Scott, Febbraio, Mark A., Galis, Zorina S., Gao, Yunling, Haus, Jacob M., Lanza, Ian R., Lavie, Carl J., Lee, Chih-Hao, Lucia, Alejandro, Moro, Cedric, Pandey, Ambarish, Robbins, Jeremy M., Stanford, Kristin I., Thackray, Alice E., and Villeda, Saul

Subjects

*SKELETAL muscle, *MYOKINES, *RESEARCH funding, *LACTIC acid

Published

2022

15. Programming human pluripotent stem cells into white and brown adipocytes.

Author

Ahfeldt, Tim, Schinzel, Robert T., Lee, Youn-Kyoung, Hendrickson, David, Kaplan, Adam, Lum, David H., Camahort, Raymond, Xia, Fang, Shay, Jennifer, Rhee, Eugene P., Clish, Clary B., Deo, Rahul C., Shen, Tony, Lau, Frank H., Cowley, Alicia, Mowrer, Greg, Al-Siddiqi, Heba, Nahrendorf, Matthias, Musunuru, Kiran, and Gerszten, Robert E.

Subjects

PLURIPOTENT stem cells, FAT cells, MESENCHYMAL stem cells, TRANSGENE expression, LIPID metabolism, LABORATORY mice

Abstract

The utility of human pluripotent stem cells is dependent on efficient differentiation protocols that convert these cells into relevant adult cell types. Here we report the robust and efficient differentiation of human pluripotent stem cells into white or brown adipocytes. We found that inducible expression of PPARG2 alone or combined with CEBPB and/or PRDM16 in mesenchymal progenitor cells derived from pluripotent stem cells programmed their development towards a white or brown adipocyte cell fate with efficiencies of 85%-90%. These adipocytes retained their identity independent of transgene expression, could be maintained in culture for several weeks, expressed mature markers and had mature functional properties such as lipid catabolism and insulin-responsiveness. When transplanted into mice, the programmed cells gave rise to ectopic fat pads with the morphological and functional characteristics of white or brown adipose tissue. These results indicate that the cells could be used to faithfully model human disease. [ABSTRACT FROM AUTHOR]

Published

2012

16. A pipeline that integrates the discovery and verification of plasma protein biomarkers reveals candidate markers for cardiovascular disease.

Author

Addona, Terri A, Shi, Xu, Keshishian, Hasmik, Mani, D R, Burgess, Michael, Gillette, Michael A, Clauser, Karl R, Shen, Dongxiao, Lewis, Gregory D, Farrell, Laurie A, Fifer, Michael A, Sabatine, Marc S, Gerszten, Robert E, and Carr, Steven A

Subjects

PROTEOMICS, BIOMARKERS, MYOCARDIAL infarction, CARDIOMYOPATHIES, CARDIOVASCULAR diseases

Abstract

We developed a pipeline to integrate the proteomic technologies used from the discovery to the verification stages of plasma biomarker identification and applied it to identify early biomarkers of cardiac injury from the blood of patients undergoing a therapeutic, planned myocardial infarction (PMI) for treatment of hypertrophic cardiomyopathy. Sampling of blood directly from patient hearts before, during and after controlled myocardial injury ensured enrichment for candidate biomarkers and allowed patients to serve as their own biological controls. LC-MS/MS analyses detected 121 highly differentially expressed proteins, including previously credentialed markers of cardiovascular disease and >100 novel candidate biomarkers for myocardial infarction (MI). Accurate inclusion mass screening (AIMS) qualified a subset of the candidates based on highly specific, targeted detection in peripheral plasma, including some markers unlikely to have been identified without this step. Analyses of peripheral plasma from controls and patients with PMI or spontaneous MI by quantitative multiple reaction monitoring mass spectrometry or immunoassays suggest that the candidate biomarkers may be specific to MI. This study demonstrates that modern proteomic technologies, when coherently integrated, can yield novel cardiovascular biomarkers meriting further evaluation in large, heterogeneous cohorts. [ABSTRACT FROM AUTHOR]

Published

2011

17. Metabolite profiles and the risk of developing diabetes.

Author

Wang, Thomas J., Larson, Martin G., Vasan, Ramachandran S., Cheng, Susan, Rhee, Eugene P., McCabe, Elizabeth, Lewis, Gregory D., Fox, Caroline S., Jacques, Paul F., Fernandez, Céline, O'Donnell, Christopher J., Carr, Stephen A., Mootha, Vamsi K., Florez, Jose C., Souza, Amanda, Melander, Olle, Clish, Clary B., and Gerszten, Robert E.

Subjects

METABOLITES, DIABETES risk factors, TANDEM mass spectrometry, LIQUID chromatography, AMINO acid metabolism, PHENYLALANINE

Abstract

Emerging technologies allow the high-throughput profiling of metabolic status from a blood specimen (metabolomics). We investigated whether metabolite profiles could predict the development of diabetes. Among 2,422 normoglycemic individuals followed for 12 years, 201 developed diabetes. Amino acids, amines and other polar metabolites were profiled in baseline specimens by liquid chromatography-tandem mass spectrometry (LC-MS). Cases and controls were matched for age, body mass index and fasting glucose. Five branched-chain and aromatic amino acids had highly significant associations with future diabetes: isoleucine, leucine, valine, tyrosine and phenylalanine. A combination of three amino acids predicted future diabetes (with a more than fivefold higher risk for individuals in top quartile). The results were replicated in an independent, prospective cohort. These findings underscore the potential key role of amino acid metabolism early in the pathogenesis of diabetes and suggest that amino acid profiles could aid in diabetes risk assessment. [ABSTRACT FROM AUTHOR]

Published

2011

18. The M2 splice isoform of pyruvate kinase is important for cancer metabolism and tumour growth.

Author

Christofk, Heather R., Vander Heiden, Matthew G., Harris, Marian H., Ramanathan, Arvind, Gerszten, Robert E., Wei, Ru, Fleming, Mark D., Schreiber, Stuart L., and Cantley, Lewis C.

Subjects

CANCER cells, PHOSPHORYLATION, PYRUVATE kinase, GENOTYPE-environment interaction, PHOTOSYNTHETIC oxygen evolution, GLYCOLYSIS, CELL lines, MOLECULAR genetics, MOLECULAR biology

Abstract

Many tumour cells have elevated rates of glucose uptake but reduced rates of oxidative phosphorylation. This persistence of high lactate production by tumours in the presence of oxygen, known as aerobic glycolysis, was first noted by Otto Warburg more than 75 yr ago. How tumour cells establish this altered metabolic phenotype and whether it is essential for tumorigenesis is as yet unknown. Here we show that a single switch in a splice isoform of the glycolytic enzyme pyruvate kinase is necessary for the shift in cellular metabolism to aerobic glycolysis and that this promotes tumorigenesis. Tumour cells have been shown to express exclusively the embryonic M2 isoform of pyruvate kinase. Here we use short hairpin RNA to knockdown pyruvate kinase M2 expression in human cancer cell lines and replace it with pyruvate kinase M1. Switching pyruvate kinase expression to the M1 (adult) isoform leads to reversal of the Warburg effect, as judged by reduced lactate production and increased oxygen consumption, and this correlates with a reduced ability to form tumours in nude mouse xenografts. These results demonstrate that M2 expression is necessary for aerobic glycolysis and that this metabolic phenotype provides a selective growth advantage for tumour cells in vivo. [ABSTRACT FROM AUTHOR]

Published

2008

19. The search for new cardiovascular biomarkers.

Author

Gerszten, Robert E. and Wang, Thomas J.

Subjects

*CORONARY heart disease prevention, *BIOMARKERS, *CARDIOVASCULAR diseases, *HEART disease risk factors, *BLOOD pressure, *DIABETES, *BIOINDICATORS, *HEART diseases, *THERAPEUTICS, *BLOOD

Abstract

Despite considerable advances in the treatment of cardiovascular disease, it remains the leading cause of death in developed countries. Assessment of classic cardiovascular risk factors — including high blood pressure, diabetes and smoking — has a central role in disease prevention. However, many individuals with coronary heart disease (a narrowing of the blood vessels that supply the heart) have only one, or none, of the classic risk factors. Thus, new biomarkers are needed to augment the information obtained from traditional indicators and to illuminate disease mechanisms. [ABSTRACT FROM AUTHOR]

Published

2008

20. Leukotriene B4 receptor BLT1 mediates early effector T cell recruitment.

Author

Tager, Andrew M., Bromley, Shannon K., Medoff, Benjamin D., Islam, Sabina A., Bercury, Scott D., Friedrich, Erik B., Carafone, Andrew D., Gerszten, Robert E., and Luster, Andrew D.

Subjects

LEUKOTRIENES, LEUCOCYTES, T cells, CELL adhesion, BIOCHEMISTRY

Abstract

Leukotriene B4 (LTB4) was originally described as a potent lipid myeloid cell chemoattractant, rapidly generated from innate immune cells, that activates leukocytes through the G protein-coupled receptor BLT1. We report here that BLT1 is expressed on effector CD4+ T cells generated in vitro as well as in vivo when effector T cells migrate out of the lymphoid compartment and are recruited into peripheral tissues. BLT1 mediated LTB4-induced T helper type 1 (TH1) and TH2 cell chemotaxis and firm adhesion to endothelial cells under flow, as well as early CD4+ and CD8+ T cell recruitment into the airway in an asthma model. Our findings show that the LTB4-BLT1 pathway is involved in linking early immune system activation and early effector T cell recruitment. [ABSTRACT FROM AUTHOR]

Published

2003

21. MCP-1 and IL-8 trigger firm adhesion of monocytes to vascular endothelium under flow conditions.

Author

Gerszten, Robert E., Garcia-Zepeda, Eduardo A., Yaw-Chyn Lim, Yoshida, Masayuki, Ding, Han A., Gimbrone Jr., Michael A., Luster, Andrew D., Luscinskas, Francis W., and Rosenzweig, Anthony

Subjects

*CHEMOKINES, *MONOCYTES, *LEUCOCYTES, *VASCULAR endothelium, *PHYSIOLOGY, *CYTOCHEMISTRY

Abstract

Presents research which studied the ability of chemokines to control monocytes under flow conditions with vascular endothelium that has been transduced to express specific leukocyte-adherence receptors. Role of monocytes in the development of atherosclerotic lesions; Effects of monocyte chemoattractant protein-1 (MCP-1) and interleukin-8 (IL-8) on monocytes; Chemokines in monocyte recruitment.

Published

1999

22. Specificity of the thrombin receptor for agonist peptide is defined by its extracellular surface.

Author

Gerszten, Robert E. and Chen, Ji

Subjects

*THROMBIN, *PEPTIDES

Abstract

Explores the specificity of the thrombin receptor for agonist peptide. Activation of G-protein-coupled receptors for catecholamines and other small ligands; Docking interactions of peptide agonists; Activation of human and Xenopus thrombin receptor homologues; Switching of receptor specificity from Xenopus to human.

Published

1994

23. An exome array study of the plasma metabolome.

Author

Rhee, Eugene P., Yang, Qiong, Yu, Bing, Liu, Xuan, Cheng, Susan, Deik, Amy, Pierce, Kerry A., Bullock, Kevin, Ho, Jennifer E., Levy, Daniel, Florez, Jose C., Kathiresan, Sek, Larson, Martin G., Vasan, Ramachandran S., Clish, Clary B., Wang, Thomas J., Boerwinkle, Eric, O'Donnell, Christopher J., and Gerszten, Robert E.

Published

2016

24. Erratum: Distinct metabolomic signatures are associated with longevity in humans.

Author

Cheng, Susan, Larson, Martin G., McCabe, Elizabeth L., Murabito, Joanne M., Rhee, Eugene P., Ho, Jennifer E., Jacques, Paul F., Ghorbani, Anahita, Magnusson, Martin, Souza, Amanda L., Deik, Amy A., Pierce, Kerry A., Bullock, Kevin, O'Donnell, Christopher J., Melander, Olle, Clish, Clary B., Vasan, Ramachandran S., Gerszten, Robert E., and Wang, Thomas J.

Published

2015

25. Distinct metabolomic signatures are associated with longevity in humans.

Author

Cheng, Susan, Larson, Martin G., McCabe, Elizabeth L., Murabito, Joanne M., Rhee, Eugene P., Ho, Jennifer E., Jacques, Paul F., Ghorbani, Anahita, Magnusson, Martin, Souza, Amanda L., Deik, Amy A., Pierce, Kerry A., Bullock, Kevin, O'Donnell, Christopher J., Melander, Olle, Clish, Clary B., Vasan, Ramachandran S., Gerszten, Robert E., and Wang, Thomas J.

Published

2015

26. Metabolic profiling of the human response to a glucose challenge reveals distinct axes of insulin sensitivity.

Author

Shaham, Oded, Wei, Ru, Wang, Thomas J, Ricciardi, Catherine, Lewis, Gregory D, Vasan, Ramachandran S, Carr, Steven A, Thadhani, Ravi, Gerszten, Robert E, and Mootha, Vamsi K

Abstract

Glucose ingestion after an overnight fast triggers an insulin-dependent, homeostatic program that is altered in diabetes. The full spectrum of biochemical changes associated with this transition is currently unknown. We have developed a mass spectrometry-based strategy to simultaneously measure 191 metabolites following glucose ingestion. In two groups of healthy individuals (n=22 and 25), 18 plasma metabolites changed reproducibly, including bile acids, urea cycle intermediates, and purine degradation products, none of which were previously linked to glucose homeostasis. The metabolite dynamics also revealed insulin’s known actions along four key axes—proteolysis, lipolysis, ketogenesis, and glycolysis—reflecting a switch from catabolism to anabolism. In pre-diabetics (n=25), we observed a blunted response in all four axes that correlated with insulin resistance. Multivariate analysis revealed that declines in glycerol and leucine/isoleucine (markers of lipolysis and proteolysis, respectively) jointly provide the strongest predictor of insulin sensitivity. This observation indicates that some humans are selectively resistant to insulin’s suppression of proteolysis, whereas others, to insulin’s suppression of lipolysis. Our findings lay the groundwork for using metabolic profiling to define an individual’s ‘insulin response profile’, which could have value in predicting diabetes, its complications, and in guiding therapy. [ABSTRACT FROM AUTHOR]

Published

2008

27. Lac-Phe mediates the effects of metformin on food intake and body weight.

Author

Xiao S, Li VL, Lyu X, Chen X, Wei W, Abbasi F, Knowles JW, Tung AS, Deng S, Tiwari G, Shi X, Zheng S, Farrell L, Chen ZZ, Taylor KD, Guo X, Goodarzi MO, Wood AC, Chen YI, Lange LA, Rich SS, Rotter JI, Clish CB, Tahir UA, Gerszten RE, Benson MD, and Long JZ

Subjects

Animals, Humans, Mice, Male, Hypoglycemic Agents pharmacology, Hypoglycemic Agents therapeutic use, Phenylalanine pharmacology, Phenylalanine metabolism, Dipeptides pharmacology, Metformin pharmacology, Body Weight drug effects, Eating drug effects

Abstract

Metformin is a widely prescribed anti-diabetic medicine that also reduces body weight. There is ongoing debate about the mechanisms that mediate metformin's effects on energy balance. Here, we show that metformin is a powerful pharmacological inducer of the anorexigenic metabolite N-lactoyl-phenylalanine (Lac-Phe) in cells, in mice and two independent human cohorts. Metformin drives Lac-Phe biosynthesis through the inhibition of complex I, increased glycolytic flux and intracellular lactate mass action. Intestinal epithelial CNDP2 + cells, not macrophages, are the principal in vivo source of basal and metformin-inducible Lac-Phe. Genetic ablation of Lac-Phe biosynthesis in male mice renders animals resistant to the effects of metformin on food intake and body weight. Lastly, mediation analyses support a role for Lac-Phe as a downstream effector of metformin's effects on body mass index in participants of a large population-based observational cohort, the Multi-Ethnic Study of Atherosclerosis. Together, these data establish Lac-Phe as a critical mediator of the body weight-lowering effects of metformin., (© 2024. The Author(s), under exclusive licence to Springer Nature Limited.)

Published

2024

28. Author Correction: Human plasma proteomic profiles indicative of cardiorespiratory fitness.

Author

Robbins JM, Peterson B, Schranner D, Tahir UA, Rienmüller T, Deng S, Keyes MJ, Katz DH, Beltran PMJ, Barber JL, Baumgartner C, Carr SA, Ghosh S, Shen C, Jennings LL, Ross R, Sarzynski MA, Bouchard C, and Gerszten RE

Published

2021

29. Human plasma proteomic profiles indicative of cardiorespiratory fitness.

Author

Robbins JM, Peterson B, Schranner D, Tahir UA, Rienmüller T, Deng S, Keyes MJ, Katz DH, Beltran PMJ, Barber JL, Baumgartner C, Carr SA, Ghosh S, Shen C, Jennings LL, Ross R, Sarzynski MA, Bouchard C, and Gerszten RE

Subjects

Biomarkers, Exercise, Humans, Life Style, Metabolic Networks and Pathways, Oxygen Consumption, Blood Proteins, Cardiorespiratory Fitness, Proteome, Proteomics methods

Abstract

Maximal oxygen uptake (VO 2 max) is a direct measure of human cardiorespiratory fitness and is associated with health. However, the molecular determinants of interindividual differences in baseline (intrinsic) VO 2 max, and of increases of VO 2 max in response to exercise training (ΔVO 2 max), are largely unknown. Here, we measure ~5,000 plasma proteins using an affinity-based platform in over 650 sedentary adults before and after a 20-week endurance-exercise intervention and identify 147 proteins and 102 proteins whose plasma levels are associated with baseline VO 2 max and ΔVO 2 max, respectively. Addition of a protein biomarker score derived from these proteins to a score based on clinical traits improves the prediction of an individual's ΔVO 2 max. We validate findings in a separate exercise cohort, further link 21 proteins to incident all-cause mortality in a community-based cohort and reproduce the specificity of ~75% of our key findings using antibody-based assays. Taken together, our data shed light on biological pathways relevant to cardiorespiratory fitness and highlight the potential additive value of protein biomarkers in identifying exercise responsiveness in humans.

Published

2021