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1. APOL1 Risk Variants Associate With the Prevalence of Stroke in African American Current and Past Smokers

Author

Rakic, Jelena Mustra, Pullinger, Clive R, Van Blarigan, Erin L, Movsesyan, Irina, Stock, Eveline Oestreicher, Malloy, Mary J, and Kane, John P

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Clinical Research, Tobacco, Prevention, Stroke, Brain Disorders, Genetics, Genetic Testing, Tobacco Smoke and Health, Human Genome, 2.1 Biological and endogenous factors, Aetiology, Cancer, Good Health and Well Being, Adult, Humans, Genetic Predisposition to Disease, Apolipoprotein L1, Smokers, Black or African American, Cross-Sectional Studies, Prevalence, Genotype, Risk Factors, Apolipoproteins, African American adults, APOL1, cross-sectional design, smoking history, stroke, cross‐sectional design, Cardiorespiratory Medicine and Haematology, Cardiovascular medicine and haematology
Abstract

BackgroundAfrican American smokers have 2.5 times higher risk for stroke compared with nonsmokers (higher than other races). About 50% of the African American population carry 1 or 2 genetic variants (G1 and G2; rare in other races) of the apolipoprotein L1 gene (APOL1). Studies showed these variants may be associated with stroke. However, the role of the APOL1 risk variants in tobacco-related stroke is unknown.Methods and resultsIn a cross-sectional study, we examined whether APOL1 risk variants modified the relationship between tobacco smoking and stroke prevalence in 513 African American adults recruited at University of California, San Francisco. Using DNA, plasma, and questionnaires we determined APOL1 variants, smoking status, and stroke prevalence. Using logistic regression models, we examined the association between smoking (ever versus never smokers) and stroke overall, and among carriers of APOL1 risk variants (1 or 2 risk alleles), and noncarriers, separately. Among participants, 41% were ever (current and past) smokers, 54% were carriers of the APOL1 risk variants, and 41 had a history of stroke. The association between smoking and stroke differed by APOL1 genotype (Pinteraction term=0.014). Among carriers, ever versus never smokers had odds ratio (OR) 2.46 (95% CI, 1.08-5.59) for stroke (P=0.034); OR 2.00 (95% CI, 0.81-4.96) among carriers of 1 risk allele, and OR 4.72 (95% CI, 0.62-36.02) for 2 risk alleles. Among noncarriers, smoking was not associated with a stroke.ConclusionsCurrent and past smokers who carry APOL1 G1 and/or G2 risk variants may be more susceptible to stroke among the African American population.

Published
2023

2. Whole-exome sequencing reveals damaging gene variants associated with hypoalphalipoproteinemia

Author

Dong, Weilai, Wong, Karen HY, Liu, Youbin, Levy-Sakin, Michal, Hung, Wei-Chien, Li, Mo, Li, Boyang, Jin, Sheng Chih, Choi, Jungmin, Lopez-Giraldez, Francesc, Vaka, Dedeepya, Poon, Annie, Chu, Catherine, Lao, Richard, Balamir, Melek, Movsesyan, Irina, Malloy, Mary J, Zhao, Hongyu, Kwok, Pui-Yan, Kane, John P, Lifton, Richard P, and Pullinger, Clive R

Subjects
Biological Sciences, Biomedical and Clinical Sciences, Genetics, Heart Disease, Biotechnology, Human Genome, Atherosclerosis, Cardiovascular, Clinical Research, 2.1 Biological and endogenous factors, Aetiology, Cholesterol, HDL, Genome-Wide Association Study, Heterozygote, Humans, Hypoalphalipoproteinemias, Exome Sequencing, dyslipidemia, genetics, HDL, LDL, lipoproteins, prebeta-1 HDL, reverse cholesterol transport, triglycerides, Biochemistry and Cell Biology, Medical Biochemistry and Metabolomics, Biochemistry & Molecular Biology, Biochemistry and cell biology, Medical biochemistry and metabolomics
Abstract

Low levels of high density lipoprotein-cholesterol (HDL-C) are associated with an elevated risk of arteriosclerotic coronary heart disease. Heritability of HDL-C levels is high. In this research discovery study, we used whole-exome sequencing to identify damaging gene variants that may play significant roles in determining HDL-C levels. We studied 204 individuals with a mean HDL-C level of 27.8 ± 6.4 mg/dl (range: 4-36 mg/dl). Data were analyzed by statistical gene burden testing and by filtering against candidate gene lists. We found 120 occurrences of probably damaging variants (116 heterozygous; four homozygous) among 45 of 104 recognized HDL candidate genes. Those with the highest prevalence of damaging variants were ABCA1 (n = 20), STAB1 (n = 9), OSBPL1A (n = 8), CPS1 (n = 8), CD36 (n = 7), LRP1 (n = 6), ABCA8 (n = 6), GOT2 (n = 5), AMPD3 (n = 5), WWOX (n = 4), and IRS1 (n = 4). Binomial analysis for damaging missense or loss-of-function variants identified the ABCA1 and LDLR genes at genome-wide significance. In conclusion, whole-exome sequencing of individuals with low HDL-C showed the burden of damaging rare variants in the ABCA1 and LDLR genes is particularly high and revealed numerous occurrences in HDL candidate genes, including many genes identified in genome-wide association study reports. Many of these genes are involved in cancer biology, which accords with epidemiologic findings of the association of HDL deficiency with increased risk of cancer, thus presenting a new area of interest in HDL genomics.

Published
2022

3. KIBRA, MTNR1B, and FKBP5 genotypes are associated with decreased odds of incident delirium in elderly post-surgical patients.

Author

Terrelonge, Mark, LaHue, Sara C, Tang, Christopher, Movsesyan, Irina, Pullinger, Clive R, Dubal, Dena B, Leung, Jacqueline, and Douglas, Vanja C

Subjects
Genotype, Genetics, Aging, Brain Disorders, Acquired Cognitive Impairment, Clinical Research, Mental Health
Abstract

Despite the association between cognitive impairment and delirium, little is known about whether genetic differences that confer cognitive resilience also confer resistance to delirium. To investigate whether older adults without postoperative delirium, compared with those with postoperative delirium, are more likely to have specific single nucleotide polymorphisms (SNPs) in the FKBP5, KIBRA, KLOTHO, MTNR1B, and SIRT1 genes known to be associated with cognition or delirium. This prospective nested matched exploratory case-control study included 94 older adults who underwent orthopedic surgery and screened for postoperative delirium. Forty-seven subjects had incident delirium, and 47 age-matched controls were not delirious. The primary study outcome was genotype frequency for the five SNPs. Compared with participants with delirium, those without delirium had higher adjusted odds of KIBRA SNP rs17070145 CT/TT [vs. CC; adjusted odds ratio (aOR) 2.80, 95% confidence interval (CI) 1.03, 7.54; p = 0.04] and MTNR1B SNP rs10830963 CG/GG (vs. CC; aOR 4.14, 95% CI 1.36, 12.59; p = 0.01). FKBP5 SNP rs1360780 CT/TT (vs. CC) demonstrated borderline increased adjusted odds of not developing delirium (aOR 2.51, 95% CI 1.00, 7.34; p = 0.05). Our results highlight the relevance of KIBRA, MTNR1B, and FKBP5 in understanding the complex relationship between delirium, cognition, and sleep, which warrant further study in larger, more diverse populations.

Published
2022

4. Aberrant activation of TCL1A promotes stem cell expansion in clonal haematopoiesis

Author

Weinstock, Joshua S., Gopakumar, Jayakrishnan, Burugula, Bala Bharathi, Uddin, Md Mesbah, Jahn, Nikolaus, Belk, Julia A., Bouzid, Hind, Daniel, Bence, Miao, Zhuang, Ly, Nghi, Mack, Taralynn M., Luna, Sofia E., Prothro, Katherine P., Mitchell, Shaneice R., Laurie, Cecelia A., Broome, Jai G., Taylor, Kent D., Guo, Xiuqing, Sinner, Moritz F., von Falkenhausen, Aenne S., Kääb, Stefan, Shuldiner, Alan R., O’Connell, Jeffrey R., Lewis, Joshua P., Boerwinkle, Eric, Barnes, Kathleen C., Chami, Nathalie, Kenny, Eimear E., Loos, Ruth J. F., Fornage, Myriam, Hou, Lifang, Lloyd-Jones, Donald M., Redline, Susan, Cade, Brian E., Psaty, Bruce M., Bis, Joshua C., Brody, Jennifer A., Silverman, Edwin K., Yun, Jeong H., Qiao, Dandi, Palmer, Nicholette D., Freedman, Barry I., Bowden, Donald W., Cho, Michael H., DeMeo, Dawn L., Vasan, Ramachandran S., Yanek, Lisa R., Becker, Lewis C., Kardia, Sharon L. R., Peyser, Patricia A., He, Jiang, Rienstra, Michiel, Van der Harst, Pim, Kaplan, Robert, Heckbert, Susan R., Smith, Nicholas L., Wiggins, Kerri L., Arnett, Donna K., Irvin, Marguerite R., Tiwari, Hemant, Cutler, Michael J., Knight, Stacey, Muhlestein, J. Brent, Correa, Adolfo, Raffield, Laura M., Gao, Yan, de Andrade, Mariza, Rotter, Jerome I., Rich, Stephen S., Tracy, Russell P., Konkle, Barbara A., Johnsen, Jill M., Wheeler, Marsha M., Smith, J. Gustav, Melander, Olle, Nilsson, Peter M., Custer, Brian S., Duggirala, Ravindranath, Curran, Joanne E., Blangero, John, McGarvey, Stephen, Williams, L. Keoki, Xiao, Shujie, Yang, Mao, Gu, C. Charles, Chen, Yii-Der Ida, Lee, Wen-Jane, Marcus, Gregory M., Kane, John P., Pullinger, Clive R., Shoemaker, M. Benjamin, Darbar, Dawood, Roden, Dan M., Albert, Christine, Kooperberg, Charles, Zhou, Ying, Manson, JoAnn E., Desai, Pinkal, Johnson, Andrew D., Mathias, Rasika A., Blackwell, Thomas W., Abecasis, Goncalo R., Smith, Albert V., Kang, Hyun M., Satpathy, Ansuman T., Natarajan, Pradeep, Kitzman, Jacob O., Whitsel, Eric A., Reiner, Alexander P., Bick, Alexander G., and Jaiswal, Siddhartha

Published
2023
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5. Separation of postprandial lipoproteins: improved purification of chylomicrons using an ApoB100 immunoaffinity method

Author

Jones, Grace Marie, Caccavello, Russell, Palii, Sergiu P, Pullinger, Clive R, Kane, John P, Mulligan, Kathleen, Gugliucci, Alejandro, and Schwarz, Jean-Marc

Subjects
Biomedical and Clinical Sciences, Nutrition and Dietetics, Prevention, Cardiovascular, Nutrition, Digestive Diseases, Atherosclerosis, Apolipoprotein B-100, Chromatography, Affinity, Chylomicrons, Female, Healthy Volunteers, Humans, Immunoprecipitation, Lipoproteins, Male, Postprandial Period, Triglycerides, triacylglycerol, stable-isotope tracer, mass spectrometry, immunoaffinity, apolipoprotein B100, chylomicrons, Biochemistry and Cell Biology, Medical Biochemistry and Metabolomics, Biochemistry & Molecular Biology, Biochemistry and cell biology, Medical biochemistry and metabolomics
Abstract

Elevated levels of triglyceride-rich lipoproteins (TRLs), both fasting and postprandial, are associated with increased risk for atherosclerosis. However, guidelines for treatment are defined solely by fasting lipid levels, even though postprandial lipids may be more informative. In the postprandial state, circulating lipids consist of dietary fat transported from the intestine in chylomicrons (CMs; containing ApoB48) and fat transported from the liver in VLDL (containing ApoB100). Research into the roles of endogenous versus dietary fat has been hindered because of the difficulty in separating these particles by ultracentrifugation. CM fractions have considerable contamination from VLDL (purity, 10%). To separate CMs from VLDL, we produced polyclonal antibodies against ApoB100 and generated immunoaffinity columns. TRLs isolated by ultracentrifugation of plasma were applied to these columns, and highly purified CMs were collected (purity, 90-94%). Overall eight healthy unmedicated adult volunteers (BMI, 27.2 ± 1.4 kg/m2; fasting triacylglycerol, 102.6 ± 19.5 mg/dl) participated in a feeding study, which contained an oral stable-isotope tracer (1-13C acetate). We then used this technique on plasma samples freshly collected during an 8 h human feeding study from a subset of four subjects. We analyzed fractionated lipoproteins by Western blot, isolated and derivatized triacylglycerols, and calculated fractional de novo lipogenesis. The results demonstrated effective separation of postprandial lipoproteins and substantially improved purity compared with ultracentrifugation protocols, using the immunoaffinity method. This method can be used to better delineate the role of dietary sugar and fat on postprandial lipids in cardiovascular risk and explore the potential role of CM remnants in atherosclerosis.

Published
2020

6. Three patients with homozygous familial hypercholesterolemia: Genomic sequencing and kindred analysis

Author

Wong, Karen HY, Levy‐Sakin, Michal, Ma, Walfred, Gonzaludo, Nina, Mak, Angel CY, Vaka, Dedeepya, Poon, Annie, Chu, Catherine, Lao, Richard, Balamir, Melek, Grenville, Zoe, Wong, Nicolas, Kane, John P, Kwok, Pui‐Yan, Malloy, Mary J, and Pullinger, Clive R

Subjects
Biological Sciences, Genetics, Atherosclerosis, Clinical Research, Biotechnology, Cardiovascular, Human Genome, Rare Diseases, Minority Health, 2.1 Biological and endogenous factors, Base Sequence, Child, Preschool, Cholesterol, LDL, Chromosome Mapping, Cohort Studies, Frameshift Mutation, Genetic Variation, Genome, Human, Heterozygote, Homozygote, Humans, Hyperlipoproteinemia Type II, Infant, Lipoproteins, LDL, Pedigree, Phenotype, Receptors, LDL, Sequence Analysis, DNA, Exome Sequencing, 10xG linked-reads whole genome sequencing, dyslipidemia, LDL, whole exome sequencing, Medicinal and Biomolecular Chemistry, Clinical Sciences, Medicinal and biomolecular chemistry
Abstract

BackgroundHomozygous Familial Hypercholesterolemia (HoFH) is an inherited recessive condition associated with extremely high levels of low-density lipoprotein (LDL) cholesterol in affected individuals. It is usually caused by homozygous or compound heterozygous functional mutations in the LDL receptor (LDLR). A number of mutations causing FH have been reported in literature and such genetic heterogeneity presents great challenges for disease diagnosis.ObjectiveWe aim to determine the likely genetic defects responsible for three cases of pediatric HoFH in two kindreds.MethodsWe applied whole exome sequencing (WES) on the two probands to determine the likely functional variants among candidate FH genes. We additionally applied 10x Genomics (10xG) Linked-Reads whole genome sequencing (WGS) on one of the kindreds to identify potentially deleterious structural variants (SVs) underlying HoFH. A PCR-based screening assay was also established to detect the LDLR structural variant in a cohort of 641 patients with elevated LDL.ResultsIn the Caucasian kindred, the FH homozygosity can be attributed to two compound heterozygous LDLR damaging variants, an exon 12 p.G592E missense mutation and a novel 3kb exon 1 deletion. By analyzing the 10xG phased data, we ascertained that this deletion allele was most likely to have originated from a Russian ancestor. In the Mexican kindred, the strikingly elevated LDL cholesterol level can be attributed to a homozygous frameshift LDLR variant p.E113fs.ConclusionsWhile the application of WES can provide a cost-effective way of identifying the genetic causes of FH, it often lacks sensitivity for detecting structural variants. Our finding of the LDLR exon 1 deletion highlights the broader utility of Linked-Read WGS in detecting SVs in the clinical setting, especially when HoFH patients remain undiagnosed after WES.

Published
2019

9. Autoantibodies against GPIHBP1 as a Cause of Hypertriglyceridemia

Author

Beigneux, Anne P, Miyashita, Kazuya, Ploug, Michael, Blom, Dirk J, Ai, Masumi, Linton, MacRae F, Khovidhunkit, Weerapan, Dufour, Robert, Garg, Abhimanyu, McMahon, Maureen A, Pullinger, Clive R, Sandoval, Norma P, Hu, Xuchen, Allan, Christopher M, Larsson, Mikael, Machida, Tetsuo, Murakami, Masami, Reue, Karen, Tontonoz, Peter, Goldberg, Ira J, Moulin, Philippe, Charrière, Sybil, Fong, Loren G, Nakajima, Katsuyuki, and Young, Stephen G

Subjects
Biotechnology, 2.1 Biological and endogenous factors, Aetiology, Adult, Autoantibodies, Female, Humans, Hyperlipoproteinemia Type I, Immunoassay, Lipolysis, Lipoprotein Lipase, Male, Middle Aged, Protein Binding, Protein Transport, Receptors, Lipoprotein, Medical and Health Sciences, General & Internal Medicine
Abstract

BackgroundA protein that is expressed on capillary endothelial cells, called GPIHBP1 (glycosylphosphatidylinositol-anchored high-density lipoprotein binding protein 1), binds lipoprotein lipase and shuttles it to its site of action in the capillary lumen. A deficiency in GPIHBP1 prevents lipoprotein lipase from reaching the capillary lumen. Patients with GPIHBP1 deficiency have low plasma levels of lipoprotein lipase, impaired intravascular hydrolysis of triglycerides, and severe hypertriglyceridemia (chylomicronemia). During the characterization of a monoclonal antibody-based immunoassay for GPIHBP1, we encountered two plasma samples (both from patients with chylomicronemia) that contained an interfering substance that made it impossible to measure GPIHBP1. That finding raised the possibility that those samples might contain GPIHBP1 autoantibodies.MethodsUsing a combination of immunoassays, Western blot analyses, and immunocytochemical studies, we tested the two plasma samples (as well as samples from other patients with chylomicronemia) for the presence of GPIHBP1 autoantibodies. We also tested the ability of GPIHBP1 autoantibodies to block the binding of lipoprotein lipase to GPIHBP1.ResultsWe identified GPIHBP1 autoantibodies in six patients with chylomicronemia and found that these autoantibodies blocked the binding of lipoprotein lipase to GPIHBP1. As in patients with GPIHBP1 deficiency, those with GPIHBP1 autoantibodies had low plasma levels of lipoprotein lipase. Three of the six patients had systemic lupus erythematosus. One of these patients who had GPIHBP1 autoantibodies delivered a baby with plasma containing maternal GPIHBP1 autoantibodies; the infant had severe but transient chylomicronemia. Two of the patients with chylomicronemia and GPIHBP1 autoantibodies had a response to treatment with immunosuppressive agents.ConclusionsIn six patients with chylomicronemia, GPIHBP1 autoantibodies blocked the ability of GPIHBP1 to bind and transport lipoprotein lipase, thereby interfering with lipoprotein lipase-mediated processing of triglyceride-rich lipoproteins and causing severe hypertriglyceridemia. (Funded by the National Heart, Lung, and Blood Institute and the Leducq Foundation.).

Published
2017

10. Cytokine polymorphisms are associated with daytime napping in adults living with HIV.

Author

Byun, Eeeseung, Gay, Caryl L, Portillo, Carmen J, Pullinger, Clive R, Aouizerat, Bradley E, and Lee, Kathryn A

Subjects
Humans, HIV Infections, Cytokines, Longitudinal Studies, Cross-Sectional Studies, Sleep, Polymorphism, Single Nucleotide, Adult, Aged, Middle Aged, Female, Male, Young Adult, Actigraphy, Fitness Trackers, Cytokine, Daytime napping, Genetic, HIV, Inflammation, Mental Health, Infectious Diseases, Genetics, Clinical Research, Prevention, HIV/AIDS, Aetiology, 2.1 Biological and endogenous factors, Good Health and Well Being, Clinical Sciences, Psychology, Neurology & Neurosurgery
Abstract

Objective/backgroundDaytime napping longer than one hour has been associated with an increased risk for all-cause mortality. Associations between cytokine polymorphisms and daytime napping in chronic illnesses such as HIV, however, have not been well described. The purpose of this study was to examine cytokine polymorphisms associated with long daytime napping in adults living with HIV.MethodsA cross-sectional analysis was conducted using a convenience sample of 257 adults living with HIV. Daytime napping was assessed with wrist actigraphy data collected over three days. Participants categorized as long nappers (≥60 min) were compared to short nappers and non-nappers (

Published
2017

12. Circadian regulation gene polymorphisms are associated with sleep disruption and duration, and circadian phase and rhythm in adults with HIV

Author

Lee, Kathryn A, Gay, Caryl, Byun, Eeeseung, Lerdal, Anners, Pullinger, Clive R, and Aouizerat, Bradley E

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Genetics, Behavioral and Social Science, Neurosciences, Clinical Research, Sleep Research, HIV/AIDS, Mental Health, Activity Cycles, Adult, Aged, CLOCK Proteins, Circadian Rhythm Signaling Peptides and Proteins, Cryptochromes, Female, Genetic Predisposition to Disease, HIV Infections, Habits, Humans, Longitudinal Studies, Male, Middle Aged, Period Circadian Proteins, Phenotype, Polymorphism, Genetic, Risk Factors, San Francisco, Sleep, Sleep Wake Disorders, Time Factors, Wakefulness, Young Adult, Acrophase, actigraphy, autocorrelation, chronotype, circadian, genetic, HIV, mesor, Biological Sciences, Medical and Health Sciences, Physiology, Biological sciences, Biomedical and clinical sciences, Health sciences
Abstract

Genes involved in circadian regulation, such as circadian locomotor output cycles kaput [CLOCK], cryptochrome [CRY1] and period [PER], have been associated with sleep outcomes in prior animal and human research. However, it is unclear whether polymorphisms in these genes are associated with the sleep disturbances commonly experienced by adults living with human immunodeficiency virus/acquired immunodeficiency syndrome (HIV/AIDS). Thus, the purpose of this study was to describe polymorphisms in selected circadian genes that are associated with sleep duration or disruption as well as the sleep-wake rhythm strength and phase timing among adults living with HIV/AIDS. A convenience sample of 289 adults with HIV/AIDS was recruited from HIV clinics and community sites in the San Francisco Bay Area. A wrist actigraph was worn for 72 h on weekdays to estimate sleep duration or total sleep time (TST), sleep disruption or percentage of wake after sleep onset (WASO) and several circadian rhythm parameters: mesor, amplitude, the ratio of mesor to amplitude (circadian quotient), and 24-h autocorrelation. Circadian phase measures included clock time for peak activity (acrophase) from actigraphy movement data, and bed time and final wake time from actigraphy and self-report. Genotyping was conducted for polymorphisms in five candidate genes involved in circadian regulation: CLOCK, CRY1, PER1, PER2 and PER3. Demographic and clinical variables were evaluated as potential covariates. Interactions between genotype and HIV variables (i.e. viral load, years since HIV diagnosis) were also evaluated. Controlling for potentially confounding variables (e.g. race, gender, CD4+ T-cell count, waist circumference, medication use, smoking and depressive symptoms), CLOCK was associated with WASO, 24-h autocorrelation and objectively-measured bed time; CRY1 was associated with circadian quotient; PER1 was associated with mesor and self-reported habitual wake time; PER2 was associated with TST, mesor, circadian quotient, 24-h autocorrelation and bed and wake times; PER3 was associated with amplitude, 24-h autocorrelation, acrophase and bed and wake times. Most of the observed associations involved a significant interaction between genotype and HIV. In this chronic illness population, polymorphisms in several circadian genes were associated with measures of sleep disruption and timing. These findings extend the evidence for an association between genetic variability in circadian regulation and sleep outcomes to include the sleep-wake patterns experienced by adults living with HIV/AIDS. These results provide direction for future intervention research related to circadian sleep-wake behavior patterns.

Published
2015

13. Cytokine polymorphisms and plasma levels are associated with sleep onset insomnia in adults living with HIV/AIDS

Author

Gay, Caryl L, Zak, Rochelle S, Lerdal, Anners, Pullinger, Clive R, Aouizerat, Bradley E, and Lee, Kathryn A

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Clinical Research, Genetics, Sleep Research, Prevention, Aetiology, 2.1 Biological and endogenous factors, Good Health and Well Being, Acquired Immunodeficiency Syndrome, Adult, Aged, Cytokines, Female, Genotype, HIV Infections, Humans, Male, Middle Aged, Polymorphism, Single Nucleotide, Sleep, Sleep Initiation and Maintenance Disorders, Young Adult, Sleep onset latency, Insomnia, Cytokine, Inflammation, Genetic, Biomarker, HIV, Immunology, Neurosciences, Psychology, Neurology & Neurosurgery, Biological psychology
Abstract

Sleep disturbance has been associated with inflammation and cytokine activity, and we previously described genetic associations between cytokine polymorphisms and sleep maintenance and duration among adults with HIV/AIDS. Although sleep onset insomnia (SOI) is also a commonly reported sleep problem, associations between cytokine biomarkers and SOI have not been adequately studied. The purpose of this study was to describe SOI in relation to cytokine plasma concentrations and gene polymorphisms in a convenience sample of 307 adults (212 men, 72 women, and 23 transgender) living with HIV/AIDS. Based on the Pittsburgh Sleep Quality Index item that asks the time it usually took to fall asleep in the past month, participants were categorized as either >30min to fall asleep (n=70, 23%) or 30min or less to fall asleep (n=237). Plasma cytokines were analyzed, and genotyping was conducted for 15 candidate genes involved in cytokine signaling: interferon-gamma (IFNG), IFNG receptor 1 (IFNGR1), interleukins (IL1R2, IL2, IL4, IL6, IL8, IL10, IL13, IL17A), nuclear factor of kappa light polypeptide gene enhancer in B cells (NFKB1 and NFKB2), and tumor necrosis factor alpha (TNFA). Demographic and clinical variables were evaluated as potential covariates. After adjusting for genomic estimates of ancestry, self-reported race/ethnicity and viral load, SOI was associated with higher IL-13 plasma levels and with six single nucleotide polymorphisms (SNPs): IL1B rs1143642 and rs1143623, IL6 rs4719714, IL13 rs1295686, NFKB1 rs4648110, and TNFA rs2857602. In addition, the IL1B rs1143642 polymorphism was associated with plasma levels of IL-1β in adjusted analyses. This study strengthens the evidence for an association between inflammation and sleep disturbance, particularly self-report of habitual SOI. In this chronic illness population, the cytokine polymorphisms associated with SOI provide direction for future personalized medicine intervention research.

Published
2015

14. Exome Sequencing in Suspected Monogenic Dyslipidemias

Author

Stitziel, Nathan O, Peloso, Gina M, Abifadel, Marianne, Cefalu, Angelo B, Fouchier, Sigrid, Motazacker, M Mahdi, Tada, Hayato, Larach, Daniel B, Awan, Zuhier, Haller, Jorge F, Pullinger, Clive R, Varret, Mathilde, Rabès, Jean-Pierre, Noto, Davide, Tarugi, Patrizia, Kawashiri, Masa-Aki, Nohara, Atsushi, Yamagishi, Masakazu, Risman, Marjorie, Deo, Rahul, Ruel, Isabelle, Shendure, Jay, Nickerson, Deborah A, Wilson, James G, Rich, Stephen S, Gupta, Namrata, Farlow, Deborah N, Neale, Benjamin M, Daly, Mark J, Kane, John P, Freeman, Mason W, Genest, Jacques, Rader, Daniel J, Mabuchi, Hiroshi, Kastelein, John JP, Hovingh, G Kees, Averna, Maurizio R, Gabriel, Stacey, Boileau, Catherine, and Kathiresan, Sekar

Subjects
Clinical Research, Human Genome, Atherosclerosis, Genetics, Aetiology, 2.1 Biological and endogenous factors, Dyslipidemias, Exome, Female, High-Throughput Nucleotide Sequencing, Humans, Male, Metabolism, Inborn Errors, DNA sequencing, exome, genetics, human, lipids, Medical Biotechnology, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology
Abstract

BackgroundExome sequencing is a promising tool for gene mapping in Mendelian disorders. We used this technique in an attempt to identify novel genes underlying monogenic dyslipidemias.Methods and resultsWe performed exome sequencing on 213 selected family members from 41 kindreds with suspected Mendelian inheritance of extreme levels of low-density lipoprotein cholesterol (after candidate gene sequencing excluded known genetic causes for high low-density lipoprotein cholesterol families) or high-density lipoprotein cholesterol. We used standard analytic approaches to identify candidate variants and also assigned a polygenic score to each individual to account for their burden of common genetic variants known to influence lipid levels. In 9 families, we identified likely pathogenic variants in known lipid genes (ABCA1, APOB, APOE, LDLR, LIPA, and PCSK9); however, we were unable to identify obvious genetic etiologies in the remaining 32 families, despite follow-up analyses. We identified 3 factors that limited novel gene discovery: (1) imperfect sequencing coverage across the exome hid potentially causal variants; (2) large numbers of shared rare alleles within families obfuscated causal variant identification; and (3) individuals from 15% of families carried a significant burden of common lipid-related alleles, suggesting complex inheritance can masquerade as monogenic disease.ConclusionsWe identified the genetic basis of disease in 9 of 41 families; however, none of these represented novel gene discoveries. Our results highlight the promise and limitations of exome sequencing as a discovery technique in suspected monogenic dyslipidemias. Considering the confounders identified may inform the design of future exome sequencing studies.

Published
2015

16. Effects of the Absence of Apolipoprotein E on Lipoproteins, Neurocognitive Function, and Retinal Function

Author

Mak, Angel CY, Pullinger, Clive R, Tang, Ling Fung, Wong, Jinny S, Deo, Rahul C, Schwarz, Jean-Marc, Gugliucci, Alejandro, Movsesyan, Irina, Ishida, Brian Y, Chu, Catherine, Poon, Annie, Kim, Phillip, Stock, Eveline O, Schaefer, Ernst J, Asztalos, Bela F, Castellano, Joseph M, Wyss-Coray, Tony, Duncan, Jacque L, Miller, Bruce L, Kane, John P, Kwok, Pui-Yan, and Malloy, Mary J

Subjects
Biomedical and Clinical Sciences, Ophthalmology and Optometry, Neurodegenerative, Dementia, Alzheimer's Disease, Neurosciences, Aging, Genetics, Cardiovascular, Atherosclerosis, Brain Disorders, Clinical Research, Acquired Cognitive Impairment, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Eye Disease and Disorders of Vision, Aetiology, 2.1 Biological and endogenous factors, Neurological, Adult, Apolipoproteins A, Apolipoproteins C, Apolipoproteins E, Carotid Artery Diseases, Exercise Test, Exome, Frameshift Mutation, Genotype, High-Density Lipoproteins, Pre-beta, Humans, Hyperlipoproteinemia Type III, Lipase, Lipid Metabolism, Lipoproteins, HDL, Lipoproteins, LDL, Lipoproteins, VLDL, Male, Multidrug Resistance-Associated Protein 2, Multidrug Resistance-Associated Proteins, Phenotype, Retina, Sequence Analysis, DNA, Severity of Illness Index, Skin Diseases, Triglycerides, Ultrasonography, Xanthomatosis
Abstract

ImportanceThe identification of a patient with a rare form of severe dysbetalipoproteinemia allowed the study of the consequences of total absence of apolipoprotein E (apoE).ObjectivesTo discover the molecular basis of this rare disorder and to determine the effects of complete absence of apoE on neurocognitive and visual function and on lipoprotein metabolism.Design, setting, and participantsWhole-exome sequencing was performed on the patient's DNA. He underwent detailed neurological and visual function testing and lipoprotein analysis. Lipoprotein analysis was also performed in the Cardiovascular Research Institute, University of California, San Francisco, on blood samples from the proband's mother, wife, 2 daughters, and normolipidemic control participants.Main outcome measuresWhole-exome sequencing, lipoprotein analysis, and neurocognitive function.ResultsThe patient was homozygous for an ablative APOE frameshift mutation (c.291del, p.E97fs). No other mutations likely to contribute to the phenotype were discovered, with the possible exception of two, in ABCC2 (p.I670T) and LIPC (p.G137R). Despite complete absence of apoE, he had normal vision, exhibited normal cognitive, neurological, and retinal function, had normal findings on brain magnetic resonance imaging, and had normal cerebrospinal fluid levels of β-amyloid and tau proteins. He had no significant symptoms of cardiovascular disease except a suggestion of myocardial ischemia on treadmill testing and mild atherosclerosis noted on carotid ultrasonography. He had exceptionally high cholesterol content (760 mg/dL; to convert to millimoles per liter, multiply by 0.0259) and a high cholesterol to triglycerides ratio (1.52) in very low-density lipoproteins with elevated levels of small-diameter high-density lipoproteins, including high levels of prebeta-1 high-density lipoprotein. Intermediate-density lipoproteins, low-density lipoproteins, and very low-density lipoproteins contained elevated apoA-I and apoA-IV levels. The patient's apoC-III and apoC-IV levels were decreased in very low-density lipoproteins. Electron microscopy revealed large lamellar particles having electron-opaque cores attached to electron-lucent zones in intermediate-density and low-density lipoproteins. Low-density lipoprotein particle diameters were distributed bimodally.Conclusions and relevanceDespite a profound effect on lipoprotein metabolism, detailed neurocognitive and retinal studies failed to demonstrate any defects. This suggests that functions of apoE in the brain and eye are not essential or that redundant mechanisms exist whereby its role can be fulfilled. Targeted knockdown of apoE in the central nervous system might be a therapeutic modality in neurodegenerative disorders.

Published
2014

17. Aberrant Hetero-Disulfide Bond Formation by the Hypertriglyceridemia-Associated p.Gly185Cys APOA5 Variant (rs2075291)

Author

Sharma, Vineeta, Witkowski, Andrzej, Witkowska, H Ewa, Dykstra, Andrew, Simonsen, Jens B, Nelbach, Lisa, Beckstead, Jennifer A, Pullinger, Clive R, Kane, John P, Malloy, Mary J, Watson, Gordon, Forte, Trudy M, and Ryan, Robert O

Subjects
Medical Biotechnology, Biomedical and Clinical Sciences, Genetics, Aetiology, 2.1 Biological and endogenous factors, Animals, Apolipoprotein A-V, Apolipoproteins, Apolipoproteins A, Biomarkers, Case-Control Studies, Dependovirus, Disease Models, Animal, Disulfides, Gene Transfer Techniques, Genetic Vectors, HEK293 Cells, Humans, Hypertriglyceridemia, Male, Mice, Mice, Knockout, Polymorphism, Single Nucleotide, Protein Binding, Transduction, Genetic, Transfection, Triglycerides, genetic therapy, lipoproteins, polymorphism, single nucleotide, triglycerides, Cardiorespiratory Medicine and Haematology, Clinical Sciences, Cardiovascular System & Hematology, Cardiovascular medicine and haematology, Clinical sciences
Abstract

ObjectiveApolipoprotein A-V (apoA-V) is a low-abundance plasma protein that modulates triacylglycerol homeostasis. Gene transfer studies were undertaken in apoa5 (-/-) mice to define the mechanism underlying the correlation between the single-nucleotide polymorphism c.553G>T in APOA5 and hypertriglyceridemia.Approach and resultsAdeno-associated virus (AAV) 2/8-mediated gene transfer of wild-type apoA-V induced a dramatic lowering of plasma triacylglycerol in apoa5 (-/-) mice, whereas AAV2/8-Gly162Cys apoA-V (corresponding to the c.553G>T single-nucleotide polymorphism: rs2075291; p.Gly185Cys when numbering includes signal sequence) had a modest effect. Characterization studies revealed that plasma levels of wild-type and G162C apoA-V in transduced mice were similar and within the physiological range. Fractionation of plasma from mice transduced with AAV2/8-G162C apoA-V indicated that, unlike wild-type apoA-V, >50% of G162C apoA-V was recovered in the lipoprotein-free fraction. Nonreducing SDS-PAGE immunoblot analysis provided evidence that G162C apoA-V present in the lipoprotein-free fraction, but not that portion associated with lipoproteins, displayed altered electrophoretic mobility consistent with disulfide-linked heterodimer formation. Immunoprecipitation followed by liquid chromatography/mass spectrometry of human plasma from subjects homozygous for wild-type APOA5 and c.553G>T APOA5 revealed that G162C apoA-V forms adducts with extraneous plasma proteins including fibronectin, kininogen-1, and others.ConclusionsSubstitution of Cys for Gly at position 162 of mature apoA-V introduces a free cysteine that forms disulfide bonds with plasma proteins such that its lipoprotein-binding and triacylglycerol-modulation functions are compromised.

Published
2014

18. Cytokine polymorphisms are associated with fatigue in adults living with HIV/AIDS

Author

Lee, Kathryn A, Gay, Caryl L, Lerdal, Anners, Pullinger, Clive R, and Aouizerat, Bradley E

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, HIV/AIDS, Clinical Research, Genetics, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system, Good Health and Well Being, Acquired Immunodeficiency Syndrome, Adult, Aged, Cytokines, Fatigue, Female, HIV Infections, Humans, Male, Middle Aged, Polymorphism, Single Nucleotide, Young Adult, Cytokine, Inflammation, Genetic, Biomarker, HIV, Immunology, Neurosciences, Psychology, Neurology & Neurosurgery, Biological psychology
Abstract

Fatigue has been associated with inflammation and cytokine activity among adults, but this relationship has not been evaluated among adults living with HIV. Diurnal patterns of fatigue have been previously identified in adults with HIV/AIDS. Thus, the purpose of this study was to describe these fatigue patterns in relation to cytokine plasma concentrations and gene polymorphisms. A convenience sample of 317 adults living with HIV/AIDS completed a measure of fatigue in the morning and evening for three consecutive days; participants reporting low levels of both morning and evening fatigue (n=110) or high levels of fatigue in the morning and evening (n=114) were included in the analysis, resulting in a final sample of 224 adults (151 men, 55 women, and 18 transgender). Plasma cytokines were analyzed, and genotyping was conducted for 15 candidate genes involved in cytokine signaling: interferon-gamma (IFNG), IFNG receptor 1 (IFNGR1), interleukins (IL), nuclear factor of kappa light polypeptide gene enhancer in B cells (NFKB-1 and -2), and tumor necrosis factor alpha (TNFA). Demographic and clinical variables were evaluated as potential covariates. Controlling for genomic estimates of ancestry and self-reported race/ethnicity and gender, the high fatigue pattern was associated with five single nucleotide polymorphisms (SNPs): IL1B rs1071676 and rs1143627, IL4 rs2243274, and TNFA rs1800683 and rs1041981. The IL1B and TNFA polymorphisms were not associated with plasma levels of IL-1β or TNFα, respectively. This study strengthens the evidence for an association between inflammation and fatigue. In this chronic illness population, the cytokine polymorphisms associated with high levels of morning and evening fatigue provide direction for future personalized medicine intervention research.

Published
2014

19. Polymorphisms of Interleukin-1 Beta and Interleukin-17Alpha Genes Are Associated With Restless Legs Syndrome

Author

Hennessy, Mary Dawn, Zak, Rochelle S, Gay, Caryl L, Pullinger, Clive R, Lee, Kathryn A, and Aouizerat, Bradley E

Subjects
Nursing, Health Sciences, Brain Disorders, Genetics, Aetiology, 2.1 Biological and endogenous factors, Infection, Adult, Biomarkers, Female, Genetic Predisposition to Disease, HIV Infections, Humans, Interleukin-17, Interleukin-1beta, Male, Middle Aged, Polymorphism, Genetic, Restless Legs Syndrome, inflammation, HIV/AIDS, genes, restless legs syndrome
Abstract

ObjectiveDopamine, iron, and inflammatory pathways are considered important to the development of restless legs syndrome (RLS). Recent genetic studies support involvement of dopamine and iron; however, cytokine gene variation in the inflammatory component remains unexplored. A recent study reported a high prevalence of RLS among HIV-infected adults. We estimate occurrence of RLS in an ethnically diverse sample of HIV-infected adults and examine differences in demographic factors, clinical characteristics, and biomarkers relating to dopamine, iron, and inflammation between adults with and without RLS symptoms.DesignA prospective longitudinal study aimed at identifying biomarkers of RLS symptom experience among HIV-infected adults.Method316 HIV-positive adults were evaluated using International RLS Study Group criteria. Genes were chosen for hypothesized relationships to dopamine (NOS1, NOS2), iron (HFE) or inflammation-mediated by cytokine genes (interferon [IFN], interleukin [IL], nuclear factor kappa-B [NFKB], and tumor necrosis factor alpha [TNFA]).ResultsSimilar to general population estimates, 11% of the sample met all four RLS diagnostic criteria. Controlling for race, gender, and hemoglobin, carrying two copies of the minor allele for IL1B rs1143643, rs1143634, or rs1143633 or carrying the minor allele for IL17A rs8193036 was associated with increased likelihood of meeting RLS diagnostic criteria.ConclusionThis study provides preliminary evidence of a genetic association between IL1B and IL17A genes and RLS.

Published
2014

20. Association of CASQ2 polymorphisms with sudden cardiac arrest and heart failure in patients with coronary artery disease

Author

Refaat, Marwan M, Aouizerat, Bradley E, Pullinger, Clive R, Malloy, Mary, Kane, John, and Tseng, Zian H

Subjects
Medical Physiology, Biomedical and Clinical Sciences, Cardiovascular, Heart Disease - Coronary Heart Disease, Clinical Research, Prevention, Genetics, Heart Disease, 2.1 Biological and endogenous factors, Aetiology, Aged, Arrhythmias, Cardiac, Calsequestrin, Coronary Disease, Death, Sudden, Cardiac, Female, Heart Failure, Humans, Hypertension, Logistic Models, Male, Middle Aged, Polymorphism, Single Nucleotide, Sudden cardiac arrest, Ventricular arrhythmias, Ventricular tachycardia, Coronary artery disease, Congestive heart failure, Calsequestrin 2, Biomedical Engineering, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology, Cardiovascular medicine and haematology
Abstract

BackgroundAbnormal calcium handling plays a crucial role in arrhythmias, sudden cardiac arrest (SCA), and congestive heart failure (CHF). Calsequestrin 2 (CASQ2) mutations affect calcium release and initiate malignant ventricular arrhythmias (VAs) and SCA syndromes. Common single nucleotide polymorphisms (SNPs) in CASQ2 may be associated with SCA in patients with coronary artery disease (CAD).ObjectiveThe purpose of this study was to examine the association of common CASQ2 SNPs with the risk of SCA in patients with CAD.MethodsCASQ2 SNPs (n = 14) were genotyped and analyzed in a case control study comparing 114 patients with CAD and SCA due to VA to 311 CAD controls without VA or SCA.ResultsMultivariate logistic regression adjusting for age and CHF status identified an association between rs7521023 with SCA (odds ratio [OR] 2.72, 95% confidence interval [CI] 1.44-5.13, P = .002). The substantial impact of CHF on SCA in the model (OR 26.6, 95% CI 13.40-52.70, P

Published
2014

21. Cytokine Polymorphisms are Associated with Poor Sleep Maintenance in Adults Living with Human Immunodeficiency Virus/Acquired Immunodeficiency Syndrome

Author

Lee, Kathryn A, Gay, Caryl, Pullinger, Clive R, Hennessy, Mary Dawn, Zak, Rochelle S, and Aouizerat, Bradley E

Subjects
Genetics, Clinical Research, Sleep Research, HIV/AIDS, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Acquired Immunodeficiency Syndrome, Adult, Aged, CD4 Lymphocyte Count, Cross-Sectional Studies, Cytokines, Female, Genotype, HIV Infections, Humans, Interleukins, Male, Middle Aged, Polymorphism, Genetic, Polymorphism, Single Nucleotide, San Francisco, Sleep, Sleep Initiation and Maintenance Disorders, Transgender Persons, Tumor Necrosis Factor-alpha, Wakefulness, Young Adult, Actigraphy, cytokine, genetic, HIV, inflammation, sleep maintenance, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Neurology & Neurosurgery
Abstract

Study objectivesCytokine activity and polymorphisms have been associated with sleep outcomes in prior animal and human research. The purpose of this study was to determine whether circulating plasma cytokines and cytokine polymorphisms are associated with the poor sleep maintenance commonly experienced by adults living with human immunodeficiency virus/acquired immunodeficiency syndrome (HIV/AIDS).DesignCross-sectional descriptive study.SettingHIV clinics and community sites in the San Francisco Bay area.ParticipantsA convenience sample of 289 adults (193 men, 73 women, and 23 transgender) living with HIV/AIDS.InterventionsNone.Measurements and resultsA wrist actigraph was worn for 72 h to estimate the percentage of wake after sleep onset (WASO%) and total sleep time (TST), plasma cytokines were analyzed, and genotyping was conducted for 15 candidate genes involved in cytokine signaling: interferon-gamma (IFNG), IFNG receptor 1 (IFNGR1), interleukins (IL1B, IL1R2, IL1R2, IL2, IL4, IL6, IL8, IL10, IL13, IL17A), nuclear factor of kappa light polypeptide gene enhancer in B cells (NFKB1 and NFKB2), and tumor necrosis factor-alpha (TNFA). Controlling for demographic variables such as race and sex, and clinical variables such as CD4+ count and medications, higher WASO% was associated with single nucleotide polymorphisms (SNPs) of IL1R2 rs11674595 and TNFA rs1041981 and less WASO% was associated with IL2 rs2069776. IL1R2 rs11674595 and TNFA rs1041981 were also associated with short sleep duration.ConclusionsThis study strengthens the evidence for an association between inflammation and sleep maintenance problems. In this chronic illness population, cytokine polymorphisms associated with wake after sleep onset provide direction for intervention research aimed at comparing anti-inflammatory mechanisms with hypnotic agents for improving sleep maintenance and total sleep time.

Published
2014

22. Impact of a 4q25 Genetic Variant in Atrial Flutter and on the Risk of Atrial Fibrillation After Cavotricuspid Isthmus Ablation

Author

Roberts, Jason D, Hsu, Jonathan C, Aouizerat, Bradley E, Pullinger, Clive R, Malloy, Mary J, Kane, John P, Olgin, Jeffrey E, and Marcus, Gregory M

Subjects
Biomedical and Clinical Sciences, Cardiovascular Medicine and Haematology, Heart Disease, Clinical Research, Genetics, Cardiovascular, Aetiology, 2.1 Biological and endogenous factors, Adult, Aged, Atrial Fibrillation, Atrial Flutter, Catheter Ablation, Chromosomes, Human, Pair 4, Female, Follow-Up Studies, Genetic Association Studies, Genetic Variation, Humans, Male, Middle Aged, Polymorphism, Single Nucleotide, Risk Factors, Treatment Outcome, Tricuspid Valve, atrial fibrillation, atrial flutter, catheter ablation, genetics, molecular biology, Cardiorespiratory Medicine and Haematology, Cardiovascular System & Hematology, Cardiovascular medicine and haematology
Abstract

BackgroundThe prediction of atrial fibrillation (AF) following catheter ablation of atrial flutter (Afl) would be helpful to facilitate targeted arrhythmia monitoring and anti-coagulation strategies. A single nucleotide polymorphism, rs2200733, is strongly associated with AF. We sought to characterize the association between rs2200733 and prevalent Afl and to determine if the variant could predict AF after cavotricuspid isthmus ablation.Methods and resultsWe performed a genetic association study of 295 patients with Afl and/or AF and 469 controls using multivariable logistic regression. The variant was then assessed as a predictor of incident AF after cavotricuspid isthmus ablation in 87 consecutive typical Afl patients with Cox proportional hazards models. The rs2200733 rare allele was associated with an adjusted 2.06-fold increased odds of isolated Afl (95% CI: 1.13-3.76, P = 0.019) and an adjusted 2.79-fold increased odds of a combined phenotype of AF and Afl (95% CI: 1.81-4.28, P < 0.001). Following catheter ablation for Afl, carrier status of rs2200733 failed to predict an increased risk of AF either among all subjects (adjusted HR: 0.94; 95% CI: 0.58-1.53, P = 0.806) or among those with isolated Afl (adjusted HR: 1.29; 95% CI: 0.51-3.26, P = 0.585).ConclusionsOur study demonstrates that Afl, whether occurring in isolation or along with AF, is associated with the rs2200733 AF risk allele. Genetic carrier status of rs2200733 failed to predict an increased risk of incident or recurrent AF following catheter ablation for Afl. These findings suggest that the causal mechanism associated with rs2200733 is germane to both AF and Afl.

Published
2014

23. Telomere Length is Associated with Sleep Duration But Not Sleep Quality in Adults with Human Immunodeficiency Virus

Author

Lee, Kathryn A, Gay, Caryl, Humphreys, Janice, Portillo, Carmen J, Pullinger, Clive R, and Aouizerat, Bradley E

Subjects
Clinical and Health Psychology, Psychology, Behavioral and Social Science, Sexually Transmitted Infections, Aging, Sleep Research, Neurosciences, Infectious Diseases, Good Health and Well Being, Actigraphy, Adult, Aged, Anxiety Disorders, Body Mass Index, Cellular Senescence, Chronic Disease, Cross-Sectional Studies, Depression, Female, HIV Infections, Hormones, Humans, Leukocytes, Male, Middle Aged, Racial Groups, San Francisco, Self Report, Sex Characteristics, Sleep, Telomere, Time Factors, Wakefulness, Young Adult, body mass index, HIV, metabolic hormones, telomere, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Neurology & Neurosurgery, Biological sciences, Biomedical and clinical sciences
Abstract

Background and study objectiveTelomere length provides an estimate of cellular aging and is influenced by oxidative stress and health behaviors such as diet and exercise. This article describes relationships between telomere length and sleep parameters that included total sleep time (TST), wake after sleep onset (WASO), and self-reported sleep quality in a sample of adults with chronic illness.Design and participantsCross-sectional study of 283 adults (74% male, 42% Caucasian) infected with human immunodeficiency virus (HIV) while living in the San Francisco Bay area, CA, USA. Ages ranged from 22-77 y.Measurements and resultsTST and WASO were estimated with wrist actigraphy across 72 h; self-reported sleep quality was assessed with the Pittsburgh Sleep Quality Index. Relative telomere length (RTL) in leukocytes was estimated by quantitative polymerase chain reaction assays. Shorter RTL was associated with older age, and RTL was shorter in males than females. RTL was unrelated to HIV disease characteristics. RTL was not associated with WASO or self-reported sleep quality. Participants with at least 7 h sleep had longer RTL than those with less than 7 h, even after controlling for the effects of age, sex, race, education, body mass index, metabolic hormones (i.e., leptin, ghrelin, adiponectin, and resistin), depression and anxiety, and sleep quality.ConclusionResults suggest that sleep duration is associated with preserving telomere length in a population of human immunodeficiency virus-infected adults. Getting at least 7 hours of sleep at night may either protect telomeres from damage or restore them on a nightly basis.

Published
2014

25. Epigenetic Regulation and Measurement of Epigenetic Changes

Author

Stephens, Kimberly E, Miaskowski, Christine A, Levine, Jon D, Pullinger, Clive R, and Aouizerat, Bradley E

Subjects
Nursing, Health Sciences, Genetics, Human Genome, Generic health relevance, Chromatin, DNA Methylation, Epigenesis, Genetic, Histones, Humans, Phenotype, RNA, Small Untranslated, epigenetics, DNA methylation, histone modification, small untranslated RNA
Abstract

Epigenetic mechanisms provide an adaptive layer of control in the regulation of gene expression that enables an organism to adjust to a changing environment. Epigenetic regulation increases the functional complexity of deoxyribonucleic acid (DNA) by altering chromatin structure, nuclear organization, and transcript stability. These changes may additively or synergistically influence gene expression and result in long-term molecular and functional consequences independent of the DNA sequence that may ultimately define an individual's phenotype. This article (1) describes histone modification, DNA methylation, and expression of small noncoding RNA species; (2) reviews the most common methods used to measure these epigenetic changes; and (3) presents factors that need to be considered when choosing a specific tissue to evaluate for epigenetic changes.

Published
2013

26. Association between regulator of G protein signaling 9-2 and body weight.

Author

Waugh, Jeffrey L, Celver, Jeremy, Sharma, Meenakshi, Dufresne, Robert L, Terzi, Dimitra, Risch, S Craig, Fairbrother, William G, Neve, Rachael L, Kane, John P, Malloy, Mary J, Pullinger, Clive R, Gu, Harvest F, Tsatsanis, Christos, Hamilton, Steven P, Gold, Stephen J, Zachariou, Venetia, and Kovoor, Abraham

Subjects
Nucleus Accumbens, Adipose Tissue, Adipocytes, Animals, Mice, Knockout, Humans, Mice, Rats, Body Weight, Weight Loss, RGS Proteins, Body Mass Index, Motor Activity, RNA Splicing, Sequence Deletion, Base Sequence, Genes, Reporter, Introns, Molecular Sequence Data, Female, Male, Intra-Abdominal Fat, Genetic Association Studies, Genes, Reporter, Knockout, General Science & Technology
Abstract

Regulator of G protein signaling 9-2 (RGS9-2) is a protein that is highly enriched in the striatum, a brain region that mediates motivation, movement and reward responses. We identified a naturally occurring 5 nucleotide deletion polymorphism in the human RGS9 gene and found that the mean body mass index (BMI) of individuals with the deletion was significantly higher than those without. A splicing reporter minigene assay demonstrated that the deletion had the potential to significantly decrease the levels of correctly spliced RGS9 gene product. We measured the weights of rats after virally transduced overexpression of RGS9-2 or the structurally related RGS proteins, RGS7, or RGS11, in the nucleus accumbens (NAc) and observed a reduction in body weight after overexpression of RGS9-2 but not RGS7 or 11. Conversely, we found that the RGS9 knockout mice were heavier than their wild-type littermates and had significantly higher percentages of abdominal fat. The constituent adipocytes were found to have a mean cross-sectional area that was more than double that of corresponding cells from wild-type mice. However, food intake and locomotion were not significantly different between the two strains. These studies with humans, rats and mice implicate RGS9-2 as a factor in regulating body weight.

Published
2011

29. Lack of Support for the Association Between GAD2 Polymorphisms and Severe Human Obesity

Author

Swarbrick, Michael M., Waldenmaier, Bjorn, Pennacchio, Len A., Lind, Denise L., Cavazos, Martha M., Geller, Frank, Merriman, Raphael, Ustaszewska, Anna, Malloy, Mary, Scherag, Andre, Hsueh, Wen-Chi, Rief, Winfried, Mauvais-Jarvis, Franck, Pullinger, Clive R., Kane, John P., Dent, Robert, McPherson, Ruth, Kwok, Pui-Yan, Hinney, Anke, Hebebrand, Johannes, and Vaisse, Christian

Subjects
Applied life sciences
Abstract

Demonstration of association between common genetic variants and chronic human diseases such as obesity could have profound implications for the prediction, prevention and treatment of these conditions. Unequivocal proof of such an association, however, requires adherence to established methodological guidelines, which include independent replication of initial positive findings. Recently, single nucleotide polymorphisms (SNPs) within GAD2 were found to be associated with class III obesity (BMI > 40 kg/m2) in 188 families (612 individuals) segregating the condition and a case-control study of 575 cases and 646 lean controls. Functional data supporting a pathophysiological role for one of the SNPs (-243A>G) were also presented. In the present study, we attempted to replicate this association in larger groups of subjects, and to extend the functional studies of the -243A>G SNP. In 2,327 subjects comprising 692 German nuclear families with severe, early-onset obesity, we found no evidence for a relationship between the three GAD2 SNPs and obesity, whether SNPs were studied individually or as haplotypes. In two independent case-control studies (a total of 680 class III obesity cases and 1,186 lean controls), there was no significant relationship between the -243A>G SNP and obesity (odds ratio (OR) = 0.99, 95 percent CI 0.83 - 1.18, in the pooled sample). These negative findings were reinforced by a meta-analysis for the association between the 243G allele and class III obesity, which yielded an OR of 1.11 (95 percent CI 0.90 - 1.36) in a total sample of 1,252 class III obese cases and 1,800 lean controls. Finally, we were unable to confirm or extend the functional data pertaining to th e -243A>G variant. Potential confounding variables in association studies invo lving common variants and complex diseases (low power to detect modest genetic effects, over-interpretation of marginal data, population stratification and biological plausibility) are also discussed in the context of GAD2 and severe obesity.

Published
2004

30. Multi-ethnic genome-wide association study for atrial fibrillation

Author

Roselli, Carolina, Chaffin, Mark D., Weng, Lu-Chen, Aeschbacher, Stefanie, Ahlberg, Gustav, Albert, Christine M., Almgren, Peter, Alonso, Alvaro, Anderson, Christopher D., Aragam, Krishna G., Arking, Dan E., Barnard, John, Bartz, Traci M., Benjamin, Emelia J., Bihlmeyer, Nathan A., Bis, Joshua C., Bloom, Heather L., Boerwinkle, Eric, Bottinger, Erwin B., Brody, Jennifer A., Calkins, Hugh, Campbell, Archie, Cappola, Thomas P., Carlquist, John, Chasman, Daniel I., Chen, Lin Y., Chen, Yii-Der Ida, Choi, Eue-Keun, Choi, Seung Hoan, Christophersen, Ingrid E., Chung, Mina K., Cole, John W., Conen, David, Cook, James, Crijns, Harry J., Cutler, Michael J., Damrauer, Scott M., Daniels, Brian R., Darbar, Dawood, Delgado, Graciela, Denny, Joshua C., Dichgans, Martin, Dörr, Marcus, Dudink, Elton A., Dudley, Samuel C., Esa, Nada, Esko, Tonu, Eskola, Markku, Fatkin, Diane, Felix, Stephan B., Ford, Ian, Franco, Oscar H., Geelhoed, Bastiaan, Grewal, Raji P., Gudnason, Vilmundur, Guo, Xiuqing, Gupta, Namrata, Gustafsson, Stefan, Gutmann, Rebecca, Hamsten, Anders, Harris, Tamara B., Hayward, Caroline, Heckbert, Susan R., Hernesniemi, Jussi, Hocking, Lynne J., Hofman, Albert, Horimoto, Andrea R. V. R., Huang, Jie, Huang, Paul L., Huffman, Jennifer, Ingelsson, Erik, Ipek, Esra Gucuk, Ito, Kaoru, Jimenez-Conde, Jordi, Johnson, Renee, Jukema, J. Wouter, Kääb, Stefan, Kähönen, Mika, Kamatani, Yoichiro, Kane, John P., Kastrati, Adnan, Kathiresan, Sekar, Katschnig-Winter, Petra, Kavousi, Maryam, Kessler, Thorsten, Kietselaer, Bas L., Kirchhof, Paulus, Kleber, Marcus E., Knight, Stacey, Krieger, Jose E., Kubo, Michiaki, Launer, Lenore J., Laurikka, Jari, Lehtimäki, Terho, Leineweber, Kirsten, Lemaitre, Rozenn N., Li, Man, Lim, Hong Euy, Lin, Henry J., Lin, Honghuang, Lind, Lars, Lindgren, Cecilia M., Lokki, Marja-Liisa, London, Barry, Loos, Ruth J. F., Low, Siew-Kee, Lu, Yingchang, Lyytikäinen, Leo-Pekka, Macfarlane, Peter W., Magnusson, Patrik K., Mahajan, Anubha, Malik, Rainer, Mansur, Alfredo J., Marcus, Gregory M., Margolin, Lauren, Margulies, Kenneth B., März, Winfried, McManus, David D., Melander, Olle, Mohanty, Sanghamitra, Montgomery, Jay A., Morley, Michael P., Morris, Andrew P., Müller-Nurasyid, Martina, Natale, Andrea, Nazarian, Saman, Neumann, Benjamin, Newton-Cheh, Christopher, Niemeijer, Maartje N., Nikus, Kjell, Nilsson, Peter, Noordam, Raymond, Oellers, Heidi, Olesen, Morten S., Orho-Melander, Marju, Padmanabhan, Sandosh, Pak, Hui-Nam, Paré, Guillaume, Pedersen, Nancy L., Pera, Joanna, Pereira, Alexandre, Porteous, David, Psaty, Bruce M., Pulit, Sara L., Pullinger, Clive R., Rader, Daniel J., Refsgaard, Lena, Ribasés, Marta, Ridker, Paul M., Rienstra, Michiel, Risch, Lorenz, Roden, Dan M., Rosand, Jonathan, Rosenberg, Michael A., Rost, Natalia, Rotter, Jerome I., Saba, Samir, Sandhu, Roopinder K., Schnabel, Renate B., Schramm, Katharina, Schunkert, Heribert, Schurman, Claudia, Scott, Stuart A., Seppälä, Ilkka, Shaffer, Christian, Shah, Svati, Shalaby, Alaa A., Shim, Jaemin, Shoemaker, M. Benjamin, Siland, Joylene E., Sinisalo, Juha, Sinner, Moritz F., Slowik, Agnieszka, Smith, Albert V., Smith, Blair H., Smith, J. Gustav, Smith, Jonathan D., Smith, Nicholas L., Soliman, Elsayed Z., Sotoodehnia, Nona, Stricker, Bruno H., Sun, Albert, Sun, Han, Svendsen, Jesper H., Tanaka, Toshihiro, Tanriverdi, Kahraman, Taylor, Kent D., Teder-Laving, Maris, Teumer, Alexander, Thériault, Sébastien, Trompet, Stella, Tucker, Nathan R., Tveit, Arnljot, Uitterlinden, Andre G., Van Der Harst, Pim, Van Gelder, Isabelle C., Van Wagoner, David R., Verweij, Niek, Vlachopoulou, Efthymia, Völker, Uwe, Wang, Biqi, Weeke, Peter E., Weijs, Bob, Weiss, Raul, Weiss, Stefan, Wells, Quinn S., Wiggins, Kerri L., Wong, Jorge A., Woo, Daniel, Worrall, Bradford B., Yang, Pil-Sung, Yao, Jie, Yoneda, Zachary T., Zeller, Tanja, Zeng, Lingyao, Lubitz, Steven A., Lunetta, Kathryn L., and Ellinor, Patrick T.

Published
2018
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39. Clonal hematopoiesis is driven by aberrant activation of TCL1A

Author

Weinstock, Joshua S., primary, Gopakumar, Jayakrishnan, additional, Burugula, Bala Bharathi, additional, Uddin, Md Mesbah, additional, Jahn, Nikolaus, additional, Belk, Julia A., additional, Daniel, Bence, additional, Ly, Nghi, additional, Mack, Taralyn M., additional, Laurie, Cecelia A., additional, Broome, Jai G., additional, Taylor, Kent D., additional, Guo, Xiuqing, additional, Sinner, Moritz F., additional, von Falkenhausen, Aenne S., additional, Kääb, Stefan, additional, Shuldiner, Alan R., additional, O’Connell, Jeffrey R., additional, Lewis, Joshua P., additional, Boerwinkle, Eric, additional, Barnes, Kathleen C., additional, Chami, Nathalie, additional, Kenny, Eimear E., additional, Loos, Ruth J., additional, Fornage, Myriam, additional, Hou, Lifang, additional, Lloyd-Jones, Donald M., additional, Redline, Susan, additional, Cade, Brian E., additional, Psaty, Bruce M., additional, Bis, Joshua C., additional, Brody, Jennifer A., additional, Silverman, Edwin K., additional, Yun, Jeong H., additional, Qiao, Dandi, additional, Palmer, Nicholette D., additional, Freedman, Barry I., additional, Bowden, Donald W., additional, Cho, Michael H., additional, DeMeo, Dawn L., additional, Vasan, Ramachandran S., additional, Yanek, Lisa R., additional, Becker, Lewis C., additional, Kardia, Sharon, additional, Peyser, Patricia A., additional, He, Jiang, additional, Rienstra, Michiel, additional, Harst, Pim Van der, additional, Kaplan, Robert, additional, Heckbert, Susan R., additional, Smith, Nicholas L., additional, Wiggins, Kerri L., additional, Arnett, Donna K., additional, Irvin, Marguerite R., additional, Tiwari, Hemant, additional, Cutler, Michael J., additional, Knight, Stacey, additional, Muhlestein, J Brent., additional, Correa, Adolfo, additional, Raffield, Laura M., additional, Gao, Yan, additional, Andrade, Mariza de, additional, Rotter, Jerome I., additional, Rich, Stephen S., additional, Tracy, Russell P., additional, Konkle, Barbara A., additional, Johnsen, Jill M., additional, Wheeler, Marsha M., additional, Smith, J. Gustav, additional, Melander, Olle, additional, Nilsson, Peter M., additional, Custer, Brian S., additional, Duggirala, Ravindranath, additional, Curran, Joanne E., additional, Blangero, John, additional, McGarvey, Stephen, additional, Williams, L. Keoki, additional, Xiao, Shujie, additional, Yang, Mao, additional, Gu, C. Charles., additional, Chen, Yii-Der Ida., additional, Lee, Wen-Jane, additional, Marcus, Gregory M., additional, Kane, John P., additional, Pullinger, Clive R., additional, Shoemaker, M. Benjamin, additional, Darbar, Dawood, additional, Roden, Dan, additional, Albert, Christine, additional, Kooperberg, Charles, additional, Zhou, Ying, additional, Manson, JoAnn E., additional, Desai, Pinkal, additional, Johnson, Andrew, additional, Mathias, Rasika, additional, Blackwell, Thomas W., additional, Abecasis, Goncalo R., additional, Smith, Albert V., additional, Kang, Hyun M., additional, Satpathy, Ansuman T., additional, Natarajan, Pradeep, additional, Kitzman, Jacob, additional, Whitsel, Eric, additional, Reiner, Alexander P., additional, Bick, Alexander G., additional, and Jaiswal, Sidd, additional

Published
2021
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44. WW-domain-containing oxidoreductase is associated with low plasma HDL-C-levels

Author

Lee, Jenny C., Weissglas-Volkov, Daphna, Kyttala, Mira, Dastani, Zari, Cantor, Rita M., Sobel, Eric M., Plaisier, Christopher L., Engert, James C., van Greevenborek, Marleen M.J., Kane, John P., Malloy, Mary J., Pullinger, Clive R., Huertas-Vazquez, Adriana, Aguilar-Salinas, Carlos A., Tusie-Luna, Teresa, de Bruin, Tjerk W.A., Aouizerat, Bradley E., van der Kallen, Carla C.J., Croce, Carlo M., Aqeilan, Rami I., Marcil, Michel, Viikari, Jorma S.A., Lehtimaki, Terho, Raitakari, Olli T., Kuusisto, Johanna, Laakso, Markku, Taskinen, Marja-Riitta, Genest, Jacques, and Pajukanta, Paivi

Subjects
Gene expression -- Analysis, Cholesterol, HDL -- Evaluation, Oxidoreductases -- Genetic aspects, Population genetics -- Research, Biological sciences
Abstract

Several Mexican and European families are examined to prove that the WW-domain-containing oxidoreductase (WWOX) gene often leads to low plasma serum HDL-cholesterol (HDL-C) in humans. The WWOX region is shown to function as a cis-regulatory element and also forms an allele-specific DNA-nuclear-factor complex, hence causing the disorder.

Published
2008

45. Identification of four gene variants associated with myocardial infarction

Author

Shiffman, Dov, Ellis, Stephen G., Rowland, Charles M., Malloy, Mary J., Luke, May M., Iakoubova, Olga A., Pullinger, Clive R., Cassano, June, Aouizerat, Bradley E., Fenwick, Raymond G., Reitz, Richard E., Catanese, Joseph J., Leong, Diane U., Zellner, Christian, Sninsky, John J., Topol, Eric J., Devlin, James J., and Kane, John P.

Subjects
Heart attack -- Genetic aspects, Heart attack -- Research, Heart attack -- Statistics, Biological sciences
Published
2005

48. Polymorphisms and Noncardioembolic Stroke in Three Case-Control Studies

Author

Luke, May M., Berger, Klaus, Rowland, Charles M., Catanese, Joseph J., Tong, Carmen H., Ross, David A., Garcia, Veronica, Kuhlenbaeumer, Gregor, Ringelstein, Bernd E., Pullinger, Clive R., Malloy, Mary J., Deedwania, Prakash, Ellis, Stephen G., Kane, John P., Devlin, James J., Lalouschek, Wolfgang, and Mannhalter, Christine

Published
2012
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49. Functional Variants of the HMGA1 Gene and Type 2 Diabetes Mellitus

Author

Chiefari, Eusebio, Tanyolaç, Sinan, Paonessa, Francesco, Pullinger, Clive R., Capula, Carmelo, Iiritano, Stefania, Mazza, Tommaso, Forlin, Michele, Fusco, Alfredo, Durlach, Vincent, Durlach, Anne, Malloy, Mary J., Kane, John P., Heiner, Steven W., Filocamo, Mirella, Foti, Daniela P., Goldfine, Ira D., and Brunetti, Antonio

Published
2011
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