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1. Exercise training and high‐sensitivity cardiac troponin‐I in patients with heart failure with reduced ejection fraction

Author

Egil Riveland, Torstein Valborgland, Anastasia Ushakova, Øyvind Skadberg, Trine Karlsen, Torstein Hole, Asbjørn Støylen, Håvard Dalen, Vibeke Videm, Elias Koppen, Axel Linke, Charles Delagardelle, Emeline M. Van Craenenbroeck, Paul Beckers, Eva Prescott, Martin Halle, Torbjørn Omland, Øyvind Ellingsen, Alf Inge Larsen, and the SMARTEX‐HF Study Group

Subjects
Biomarkers, Cardiac rehabilitation, Chronic heart failure, HFrEF, Troponin I, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Abstract Aims The aims of this sub‐study of the SMARTEX trial were (1) to evaluate the effects of a 12‐week exercise training programme on serum levels of high sensitivity cardiac troponin I (hs‐cTnI) in patients with moderate chronic heart failure (CHF), in New York Heart Association class II‐III with reduced ejection fraction (HFrEF) and (2) to explore the associations with left ventricular remodelling, functional capacity and filling pressures measured with N‐terminal pro brain natriuretic peptide (NT‐proBNP). Methods and results In this sub‐study, 196 patients were randomly assigned to high intensity interval training (HIIT, n = 70), moderate continuous training (MCT, n = 59) or recommendation of regular exercise (RRE), (n = 67) for 12 weeks. To reveal potential difference between structured intervention and control, HIIT and MCT groups were merged and named supervised exercise training (SET) group. The RRE group constituted the control group (CG). To avoid contributing factors to myocardial injury, we also evaluated changes in patients without additional co‐morbidities (atrial fibrillation, hypertension, diabetes mellitus, and chronic obstructive pulmonary disease). The relationship between hs‐cTnI and left ventricular end‐diastolic diameter (LVEDD), VO2peak, and NT‐proBNP was analysed by linear mixed models. At 12 weeks, Hs‐cTnI levels were modestly but significantly reduced in the SET group from median 11.9 ng/L (interquartile ratio, IQR 7.1–21.8) to 11.5 ng/L (IQR 7.0–20.7), P = 0.030. There was no between‐group difference (SET vs. CG, P = 0.116). There was a numerical but not significant reduction in hs‐cTnI for the whole population (P = 0.067) after 12 weeks. For the sub‐group of patients without additional co‐morbidities, there was a significant between‐group difference: SET group (delta −1.2 ng/L, IQR −2.7 to 0.1) versus CG (delta −0.1 ng/L, IQR −0.4 to 0.7), P = 0.007. In the SET group, hs‐cTnI changed from 10.9 ng/L (IQR 6.0–22.7) to 9.2 ng/L (IQR 5.2–20.5) (P = 0.002), whereas there was no change in the CG (6.4 to 5.8 ng/L, P = 0.64). Changes in hs‐cTnI (all patients) were significantly associated with changes in; LVEDD, VO2peak, and NT‐proBNP, respectively. Conclusions In patients with stable HFrEF, 12 weeks of structured exercise intervention was associated with a modest, but significant reduction of hs‐cTnI. There was no significant difference between intervention group and control group. In the sub‐group of patients without additional co‐morbidities, this difference was highly significant. The alterations in hs‐cTnI were associated with reduction of LVEDD and natriuretic peptide concentrations as well as improved functional capacity.

Published
2024
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4. Filaggrin Mutation Status and Prevention of Atopic Dermatitis with Maternal Probiotic Supplementation

Author

Dinastry Pramadita Zakiudin, Jacob P. Thyssen, Claus Zachariae, Vibeke Videm, Torbjørn Øien, and Melanie Rae Simpson

Subjects
atopic dermatitis, child, preschool, filaggrin, gene, probiotic, Dermatology, RL1-803
Abstract

The World Allergy Organization recommends probiotics in the prevention of atopic dermatitis in high-risk populations. Mutations in the filaggrin gene (FLG) result in an increased risk of atopic dermatitis through disruption of the skin keratin layer. This exploratory study investigated whether the preventive effect of maternal probiotics was evident in children with and without FLG mutations. DNA was collected from children (n = 228) from the Probiotic in the Prevention of Allergy among Children in Trondheim (ProPACT) study. Samples were analysed for 3 common FLG mutations (R501X, R2447X, and 2282del4). Overall, 7% of children had heterozygous FLG mutations; each child had only one of the 3 mutations. Mutation status had no association with atopic dermatitis (RR = 1.1; 95% CI 0.5 to 2.3). The risk ratio (RR) for having atopic dermatitis following maternal probiotics was 0.6 (95% CI 0.4 to 0.9) and RR was similar if the child expressed an FLG mutation (RR = 0.6; 95% CI 0.1 to 4.1) or wildtype FLG (RR = 0.6; 95% CI 0.4 to 0.9). The preventive effect of probiotics for atopic dermatitis was also evident in children without FLG mutation. Larger confirmatory studies are needed.

Published
2024
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6. Systemic inflammatory proteins in offspring following maternal probiotic supplementation for atopic dermatitis prevention

Author

Dinastry Pramadita Zakiudin, Anne Dorthea Bjerkenes Rø, Vibeke Videm, Torbjørn Øien, and Melanie Rae Simpson

Subjects
Atopic dermatitis, Biomarkers, Children, Plasma, Probiotics, Immunologic diseases. Allergy, RC581-607
Abstract

Abstract Background Maternal probiotic supplementation has a promising effect on atopic dermatitis (AD) prevention in infancy. In the randomised controlled study, Probiotics in the Prevention of Allergy among Children in Trondheim (ProPACT), maternal probiotics reduced the cumulative incidence of AD in their offspring by 40% at 2 years of age. However, our understanding on how probiotics prevented AD is still limited, and the role of inflammatory proteins in infants following maternal probiotic supplementation is unclear. We hypothesised that maternal probiotics lowered pro-inflammatory proteins and increased anti-inflammatory proteins in their 2-year-old children as a mechanism of AD prevention. We aimed to explore this hypothesis and the association between these proteins and the presence of AD, severity of AD, and the degree of preventive effect of probiotics. Methods Plasma samples were collected from 2-year-old children (n = 202) during the ProPACT study, a randomised placebo-controlled trial of maternal probiotic supplementation. These samples were analysed for 92 inflammatory proteins using a multiplex proximity extension assay. Associations between inflammatory proteins and the presence and severity of AD, and the degree of preventive effect, was estimated individually using regression analysis and then collectively using unsupervised cluster analysis. Results Several proteins were observed to differ between the groups. The probiotic group had lower CCL11 and IL-17C, while children with AD had higher IL-17C, MCP-4, uPA, and CD6. Cytokine CCL20 and IL-18 had moderate correlation (r = 0.35 and r = 0.46) with the severity of AD. The cluster analysis revealed that children in the cluster of samples with the highest value of immune checkpoint receptors and inflammatory suppressor enzymes showed the greatest AD preventive effect from probiotics. Conclusions The proteins associated with both maternal probiotic supplementation and the presence and severity of AD warrant attention because of their potential biological relevance. Cluster analysis may provide a new insight when considering which subgroups benefit from probiotic supplementation. Larger studies are needed to confirm the results. Trial registration number: The study was retrospectively registered at ClinicalTrials.gov (NCT00159523) on 12nd September 2005.

Published
2023
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7. Rheumatoid arthritis, disease-modifying antirheumatic drugs and risk of major osteoporotic fracture: prospective data from the HUNT Study, Norway

Author

Tom Ivar Lund Nilsen, Mari Hoff, Vibeke Videm, Arnulf Langhammer, Jonas Johansson, Julie Horn, Ingebjørg Tronstad, and Sigrid Anna Aalberg Vikjord

Subjects
Medicine
Abstract

Objectives Rheumatoid arthritis has been associated with increased fracture risk. New treatments have improved the course of the disease substantially, but it is not clear if this influences fracture risk. We examined if rheumatoid arthritis, overall and according to disease-modifying antirheumatic drugs (DMARDs), is associated with a risk of major osteoporotic fractures.Methods Overall, 92 285 participants in the population-based Nord-Trndelag Health Study (HUNT), Norway were included and linked with hospital records for a validated rheumatoid arthritis diagnosis (n=605), type of DMARD treatment and fracture diagnosis. Participants were followed up until the first major osteoporotic fracture, death, emigration or end of follow-up. Cox regression was used to estimate HRs for fractures among individuals with rheumatoid arthritis, overall and by DMARD treatment, compared with participants without rheumatoid arthritis.Results A total of 9670 fractures were observed during follow-up, of which 88 were among those with rheumatoid arthritis. Compared with the reference group of participants without rheumatoid arthritis, those with the disease had an HR of fracture of 1.41 (95% CI 1.13 to 1.74). The association was largely similar for users of csDMARDs (HR 1.44; 95% CI 1.15 to 1.81), whereas the association for bDMARD users was weaker and less precise (HR 1.19; 95% CI 0.64 to 2.21).Conclusion Participants with rheumatoid arthritis had a 40% higher risk of fracture than participants without the disease. A similar fracture risk was observed for conventional synthetic DMARD use, whereas there was weak evidence that the use of biological DMARDs may be associated with a somewhat lower fracture risk.

Published
2024
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10. Validation in Indonesia of two published scores for mortality prediction after cardiac surgery

Author

Yunita Widyastuti, Cindy E Boom, I Made A. Parmana, Juni Kurniawaty, Akhmad Y Jufan, Dudy A Hanafy, and Vibeke Videm

Subjects
acef score, cardiac surgery, euroscore ii, in-hospital mortality, recalibration, risk prediction, Anesthesiology, RD78.3-87.3, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Introduction: No mortality risk prediction model has previously been validated for cardiac surgery in Indonesia. This study aimed at validating the EuroSCORE II and Age Creatinine Ejection Fraction (ACEF) score as predictors for in-hospital mortality after cardiac surgery a in tertiary center, and if necessary, to recalibrate the EuroSCORE II model to our population. Methods: This study was a single-center observational study from prospectively collected data on adult patients undergoing cardiac surgery from January 2006 to December 2011 (n = 1833). EuroSCORE II and ACEF scores were calculated for all patients to predict in-hospital mortality. Discrimination was assessed using the area under the curve (AUC) with a 95% confidence interval. Calibration was assessed with the Hosmer–Lemeshow test (HL test). Multivariable analysis was performed to recalibrate the EuroSCORE II; variables with P < 0.2 entered the final model. Results: The in-hospital mortality rate was 3.8%, which was underestimated by the EuroSCORE II (2.1%) and the ACEF score (2.4%). EuroSCORE II (AUC 0.774 (0.714–0.834)) showed good discrimination, whereas the ACEF score (AUC 0.638 [0.561–0.718]) showed poor discrimination. The differences in AUC were significant (P = 0.002). Both scores were poorly calibrated (EuroSCORE II: HL test P < 0.001, ACEF score: HL test P < 0.001) and underestimated mortality in all risk groups. After recalibration, EuroSCORE II showed good discrimination (AUC 0.776 [0.714– 0.840]) and calibration (HL test P = 0.79). Conclusions: EuroSCORE II and the ACEF score were unsuitable for risk prediction of in-hospital mortality after cardiac surgery in our center. Following recalibration, the calibration of the EuroSCORE II was greatly improved.

Published
2023
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12. Inflammation mediates approximately one quarter of excess relative all-cause mortality in persons with rheumatoid arthritis: the Trøndelag Health Study

Author

Vibeke Videm, Ingrid Sæther Houge, Marthe Halsan Liff, and Mari Hoff

Subjects
Medicine, Science
Abstract

Abstract Inflammation may contribute to excess mortality in rheumatoid arthritis (RA) patients. We investigated associations to all-cause mortality of the inflammation markers high-sensitivity C-reactive protein (CRP), lactoferrin (neutrophil activation marker), and neopterin (monocyte activation marker). From the population-based Trøndelag Health Study (3rd wave 2006–2008), 316 RA patients and 43,579 controls were included. Lactoferrin and neopterin were quantified in a nested cohort (n = 283 RA patients, n = 3698 controls). Follow-up was until death found by linkage to the Norwegian Cause of Death Registry or 31.12.2018. All-cause mortality was analyzed using Cox regression and Cox regression-based mediation analysis. Having RA (hazard ratio (HR): 1.25, 95%CI: 1.00, 1.56, p = 0.048), and CRP ≥ 3 mg/L (HR: 1.50, 95%CI: 1.41, 1.60, p

Published
2022
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13. Relative importance of inflammation and cardiorespiratory fitness for all-cause mortality risk in persons with rheumatoid arthritis: the population-based Trøndelag Health Study

Author

Mari Hoff, Marthe Halsan Liff, and Vibeke Videm

Subjects
Medicine
Abstract

Objective Inflammation and reduced cardiorespiratory fitness (CRF) are associated with increased mortality rates in rheumatoid arthritis (RA). We aimed at directly comparing the relative importance of inflammation and reduced CRF as mediators of all-cause mortality in persons with RA compared with controls, quantifying direct and indirect (mediated) effects.Methods Persons with (n=223, cases) and without (n=31 684, controls) RA from the third survey of the Trøndelag Health Study (HUNT3, 2006–2008) were included. Inflammation was quantified using C reactive protein (CRP) and estimated CRF (eCRF) was calculated using published formulae. All-cause mortality was found by linkage to the Norwegian Cause of Death Registry, with follow-up from inclusion in HUNT3 until death or 31 December 2018. Data were analysed using standardised equation modelling, permitting complex correlations among variables.Results Persons with RA had increased all-cause mortality rates (24.1% vs 9.9%, p

Published
2023
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15. Moderate continuous or high intensity interval exercise in heart failure with reduced ejection fraction: Differences between ischemic and non-ischemic etiology

Author

Martin Halle, Eva Prescott, Emeline M. Van Craenenbroeck, Paul Beckers, Vibeke Videm, Trine Karlsen, Patrick Feiereisen, Ephraim B. Winzer, Norman Mangner, Martin Snoer, Jeffrey W. Christle, Håvard Dalen, Asbjørn Støylen, Katrin Esefeld, Melanie Heitkamp, Bianca Spanier, Axel Linke, Øyvind Ellingsen, and Charles Delagardelle

Subjects
Exercise intensity, Training, HIIT, Heart failure, Etiology, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Background: Exercise for heart failure (HF) with reduced ejection fraction (HFrEF) is recommended by guidelines, but exercise mode and intensities are not differentiated between HF etiologies. We, therefore, investigated the effect of moderate or high intensity exercise on left ventricular end-diastolic diameter (LVEDD), left ventricular ejection fraction (LVEF) and maximal exercise capacity (peak VO2) in patients with ischemic cardiomyopathy (ICM) and non-ischemic cardiomyopathy (NICM). Methods: The Study of Myocardial Recovery after Exercise Training in Heart Failure (SMARTEX-HF) consecutively enrolled 231 patients with HFrEF (LVEF ≤ 35 %, NYHA II-III) in a 12-weeks supervised exercise program. Patients were stratified for HFrEF etiology (ICM versus NICM) and randomly assigned (1:1:1) to supervised exercise thrice weekly: a) moderate continuous training (MCT) at 60–70 % of peak heart rate (HR), b) high intensity interval training (HIIIT) at 90–95 % peak HR, or c) recommendation of regular exercise (RRE) according to guidelines. LVEDD, LVEF and peak VO2 were assessed at baseline, after 12 and 52 weeks. Results: 215 patients completed the intervention. ICM (59 %; n = 126) compared to NICM patients (41 %; n = 89) had significantly lower peak VO2 values at baseline and after 12 weeks (difference in peak VO2 2.2 mL/(kg*min); p

Published
2022
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16. Safety and efficacy of plasma transfusion from exercise-trained donors in patients with early Alzheimer’s disease: protocol for the ExPlas study

Author

Ulrik Wisløff, Vibeke Videm, Håvard Dalen, Stian Lydersen, Atefe R Tari, Espen Holte, Linda R White, Geir Bråthen, Geir Selbaek, Helene Haugen Berg, Ragnhild Nyhus Røsbjørgen, Katja Scheffler, Asta K Haberg, Emrah Duezel, Sverre Bergh, Kjell Rune Logan-Halvorsrud, and Sigrid Botne Sando

Subjects
Medicine
Abstract

Introduction Given that exercise training reduces the risk of developing Alzheimer’s disease (AD), induces changes in the blood composition and has widespread systemic benefits, it is reasonable to hypothesise that exercised plasma (ExPlas) may have rejuvenative properties. The main objective is to test safety and tolerability of transfusing ExPlas from young, healthy, fit adults to patients with mild cognitive impairment (MCI) or early AD. The study is a pilot for a future efficacy study. The key secondary objectives are examining the effect of plasma transfusions on cognitive function, fitness level, vascular risk profile, assessment of cerebral blood flow and hippocampal volume, quality of life, functional connectivity assessed by resting state functional MRI and biomarkers in blood and cerebrospinal fluid.Methods and analysis ExPlas is a double-blinded, randomised controlled clinical single-centre trial. Patients up to 75 years of age with diagnosis early symptomatic phase AD will be recruited from two Norwegian hospitals. ExPlas is plasma drawn by plasmapheresis once a month for 4 months, from a total of 30 fit male donors (aged 18–40, BMI≤27 kg/m2 and maximal oxygen uptake>55 mL/kg/min). All units will be virus inactivated by the Intercept method in accordance with procedures at St. Olavs University Hospital. Comparison with isotonic saline allows differentiation from a non-blood product. The main study consists of 6 rounds of examinations in addition to 12 plasma transfusions divided over three 4-week periods during study year-1. It is also planned to conduct follow-up examinations 2 and 5 years after baselineEthics and dissemination Written informed consent will be obtained from all participants and participation is voluntary. All participants have a next of kin who will follow them throughout the study to represent the patient’s interest. The study is approved by the Regional Committee for Medical and Health Research Ethics (REK 2018/702) and the Norwegian Medicines Agency (EudraCT No. 2018-000148-24). The study will be published in an open access journal and results will be presented at numerous national and international meetings as well as on social media platforms.Trial registration number EudraCT No. 2018-000148-24. ClinicalTrials.gov, NCT05068830

Published
2022
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17. Inflammatory markers and risk of cardiovascular mortality in relation to diabetes status in the HUNT study

Author

Lena Løfblad, Gunhild Garmo Hov, Arne Åsberg, and Vibeke Videm

Subjects
Medicine, Science
Abstract

Abstract Inflammatory markers have been associated with increased risk of cardiovascular mortality in general populations. We assessed whether these associations differ by diabetes status. From a population-based cohort study (n = 62,237) we included all participants with diabetes (n = 1753) and a control group without diabetes (n = 1818). Cox regression models were used to estimate hazard ratios (HRs) with 95% confidence intervals (CI) for possible associations with cardiovascular mortality of 4 different inflammatory markers; C-reactive protein (CRP), calprotectin, neopterin and lactoferrin. During a median follow-up of 13.9 years, 728 (20.4%) died from cardiovascular disease (CVD). After adjustment for age, sex and diabetes, the associations of all inflammatory markers with risk of cardiovascular mortality were log-linear (all P ≤ 0.017 for trend) and did not differ according to diabetes status (all P ≥ 0.53 for interaction). After further adjustments for established risk factors, only CRP remained independently associated with cardiovascular mortality. HRs were 1.22 (1.12–1.32) per standard deviation higher loge CRP concentration and 1.91 (1.50–2.43) when comparing individuals in the top versus bottom quartile. The associations of CRP, calprotectin, lactoferrin and neopterin with cardiovascular mortality did not differ by diabetes, suggesting that any potential prognostic value of these markers is independent of diabetes status.

Published
2021
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18. Exercise training and high‐sensitivity cardiac troponin T in patients with heart failure with reduced ejection fraction

Author

Elias Koppen, Torbjørn Omland, Alf Inge Larsen, Trine Karlsen, Axel Linke, Eva Prescott, Martin Halle, Håvard Dalen, Charles Delagardelle, Torstein Hole, Emeline M. vanCraenenbroeck, Paul Beckers, Øyvind Ellingsen, Patrick Feiereisen, Torstein Valborgland, Vibeke Videm, and SMARTEX‐HF Study Group

Subjects
Heart failure, Troponin T, Cardiorespiratory fitness, Exercise training interventions, Training intensity, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Abstract Aims Whether an exercise training intervention is associated with reduction in long‐term high‐sensitivity cardiac troponin T (hs‐cTnT) concentration (a biomarker of subclinical myocardial injury) in patients with heart failure with reduced ejection fraction (HFrEF) is unknown. The aims were to determine (i) the effect of a 12 week endurance exercise training intervention with different training intensities on hs‐cTnT in stable patients with HFrEF (left ventricular ejection fraction ≤ 35%) and (ii) associations between hs‐cTnT and peak oxygen uptake (VO2peak). Methods and results In this sub‐study of the SMARTEX‐HF trial originally including 261 patients from nine European centres, 213 eligible patients were included after withdrawals and appropriate exclusions [19% women, mean age 61.2 years (standard deviation: 11.9)], randomized to high‐intensity interval training (HIIT; n = 77), moderate continuous training (MCT; n = 63), or a recommendation of regular exercise (RRE; n = 73). Hs‐cTnT measurements and clinical data acquired before (BL) and after a 12 week exercise training intervention (12 weeks) and at 1 year follow‐up (1 year) were analysed using multivariable mixed models. Baseline hs‐cTnT was above the 99th percentile upper reference limit of 14 ng/L in 35 (48%), 35 (56%), and 49 (64%) patients in the RRE, MCT, and HIIT groups, respectively. Median hs‐cTnT was 16 ng/L at BL, 14 ng/L at 12 weeks, and 14 ng/L at 1 year. Hs‐cTnT was statistically significantly reduced at 12 weeks in a model adjusted for randomization group, centre and VO2peak, and after further adjustment in the final model that also included age, sex, creatinine concentrations, N‐terminal pro‐brain natriuretic peptide, smoking, and heart failure treatment. The mean reduction from BL to 12 weeks in the final model was 1.1 ng/L (95% confidence interval: 1.0–1.2 ng/L, P

Published
2021
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21. Genetic risk score associations for myocardial infarction are comparable in persons with and without rheumatoid arthritis: the population-based HUNT study

Author

S. Rostami, M. Hoff, H. Dalen, K. Hveem, and V. Videm

Subjects
Medicine, Science
Abstract

Abstract Persons with rheumatoid arthritis (RA) have increased risk of myocardial infarction (MI). Overlapping associations with MI of weighted genetic risk scores (wGRS) for coronary artery disease (CAD) and RA is unknown in a population-based setting. Data from the prospective Nord-Trøndelag Health Study (HUNT2: 1995–1997 and HUNT3: 2006–2008) were used. wGRS added each participant’s carriage of all risk variants weighted by the coefficient from published association studies. Published wGRS for CAD and RA were analysed in Cox regression with MI as outcome, age as analysis time, and censoring at the first MI, death, or 31.12.2017. 2609 of 61,465 participants developed MI during follow-up (mean 17.7 years). The best-fitting wGRS for CAD and RA included 157 and 27 single-nucleotide polymorphisms, respectively. In multivariable analysis including traditional CAD risk factors, the CAD wGRS was associated with MI [hazard ratio = 1.23 (95% CI 1.18–1.27) for each SD increase, p

Published
2020
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23. Reduced cardiorespiratory fitness is a mediator of excess all-cause mortality in rheumatoid arthritis: the Trøndelag Health Study

Author

Mari Hoff, Marthe Halsan Liff, Ulrik Wisløff, and Vibeke Videm

Subjects
Medicine
Abstract

Objectives Investigate if low cardiorespiratory fitness (CRF) was associated with and acted as a mediator of excess all-cause mortality rate in persons suffering from rheumatoid arthritis (RA) compared with the general population.Methods All-cause mortality was analysed using Cox regression modelling in patients with RA (n=348) and controls (n=60 938) who took part in the second (1995–1997) and third (2006–2008) waves of the longitudinal population-based Trøndelag Health Study in Norway. A mediation analysis was performed to investigate if excess relative risk of mortality in RA was mediated by low estimated CRF (eCRF).Results During the follow-up until 31 December 2018 (mean 19.3 years), the mortality rate among patients with RA (n=127, 36.5%) was higher than among controls (n=12 942, 21.2%) (p

Published
2021
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29. Symptoms of Depression and Risk of Abdominal Aortic Aneurysm: A HUNT Study

Author

Linn Åldstedt Nyrønning, Malin Stenman, Rebecka Hultgren, Grethe Albrektsen, Vibeke Videm, and Erney Mattsson

Subjects
abdominal aortic aneurysm, depression, depressive symptoms, risk factors, HADS score, HUNT study, Diseases of the circulatory (Cardiovascular) system, RC666-701
Abstract

Background Depression is associated with cardiovascular diseases, but the evidence is scarce regarding depression and risk of abdominal aortic aneurysms (AAA). The aim was to determine whether individuals with depressive symptoms have increased risk of AAA. Methods and Results This population‐based prospective study included 59 136 participants (52.4% women) aged 50 to 106 years from the HUNT (Norwegian Nord‐Trøndelag Health Study). Symptoms of depression were assessed using the depression subscale of the Hospital Anxiety and Depression Scale (HADS). During a median follow‐up of 13 years, there were 742 incident cases of AAA (201 women). A total of 6401 individuals (12.3%) reported depressive symptoms (defined as HADS depression scale [HADS‐D]) ≥8) (52.5% women). The annual incidence rate of AAA was 1.0 per 1000 individuals. At all ages, the estimated proportion of individuals diagnosed with AAA was higher among those with depressive symptoms (log‐rank test, P

Published
2019
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30. Cardiorespiratory fitness in patients with rheumatoid arthritis is associated with the patient global assessment but not with objective measurements of disease activity

Author

Mari Hoff, Ranjeny Thomas, Marthe Halsan Liff, Thomas Fremo, Ulrik Wisløff, and Vibeke Videm

Subjects
Medicine
Abstract

Objective Patients with rheumatoid arthritis (RA) suffer from more cardiovascular disease (CVD), and develop cardiovascular risk factors at an earlier age than the general population. Cardiorespiratory fitness (CRF) is an important predictor of cardiovascular health. There are few data regarding CRF of RA patients, measured as peak oxygen uptake (VO2peak) by the gold standard method; cardiopulmonary exercise testing. We compared CRF in RA patients to those from a healthy population, and investigated if risk factors for CVD and RA-specific variables including subjective and objective disease activity measures were associated with CRF in RA patients.Methods VO2peak tests of RA patients (n=93) were compared to those of an age-matched and gender-matched healthy population (n=4631) from the Nord-Trøndelag Health Study. Predictors of VO2peak were found using Lasso (least absolute shrinkage and selection operator) regression, followed by standardised multiple linear regression.Results Women with RA ≥40 years and men with RA aged 40–49 years or 60–69 years had up to 20% lower CRF than the healthy population in the same age groups. By relative importance, body mass index (standardised coefficient=−0.25, p

Published
2019
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32. The Galaxy platform for accessible, reproducible and collaborative biomedical analyses: 2022 update

Author

Ostrovsky, AE, Mahmoud, A, Lonie, AJ, Syme, A, Fouilloux, A, Bretaudeau, A, Nekrutenko, A, Kumar, A, Eschenlauer, AC, DeSanto, AD, Guerler, A, Serrano-Solano, B, Batut, B, Gruening, BA, Langhorst, BW, Carr, B, Raubenolt, BA, Hyde, CJ, Bromhead, CJ, Barnett, CB, Royaux, C, Gallardo, C, Blankenberg, D, Fornika, DJ, Baker, D, Bouvier, D, Clements, D, Morais, DADL, Tabernero, DL, Lariviere, D, Nasr, E, Afgan, E, Zambelli, F, Heyl, F, Psomopoulos, F, Coppens, F, Price, GR, Cuccuru, G, Le Corguille, G, Von Kuster, G, Akbulut, GG, Rasche, H, Hans-Rudolf, H, Eguinoa, I, Makunin, I, Ranawaka, IJ, Taylor, JP, Joshi, J, Hillman-Jackson, J, Goecks, J, Chilton, JM, Kamali, K, Suderman, K, Poterlowicz, K, Yvan, LB, Lopez-Delisle, L, Sargent, L, Bassetti, ME, Tangaro, MA, van den Beek, M, Cech, M, Bernt, M, Fahrner, M, Tekman, M, Foell, MC, Schatz, MC, Crusoe, MR, Roncoroni, M, Kucher, N, Coraor, N, Stoler, N, Rhodes, N, Soranzo, N, Pinter, N, Goonasekera, NA, Moreno, PA, Videm, P, Melanie, P, Mandreoli, P, Jagtap, PD, Gu, Q, Weber, RJM, Lazarus, R, Vorderman, RHP, Hiltemann, S, Golitsynskiy, S, Garg, S, Bray, SA, Gladman, SL, Leo, S, Mehta, SP, Griffin, TJ, Jalili, V, Yves, V, Wen, V, Nagampalli, VK, Bacon, WA, de Koning, W, Maier, W, Briggs, PJ, Ostrovsky, AE, Mahmoud, A, Lonie, AJ, Syme, A, Fouilloux, A, Bretaudeau, A, Nekrutenko, A, Kumar, A, Eschenlauer, AC, DeSanto, AD, Guerler, A, Serrano-Solano, B, Batut, B, Gruening, BA, Langhorst, BW, Carr, B, Raubenolt, BA, Hyde, CJ, Bromhead, CJ, Barnett, CB, Royaux, C, Gallardo, C, Blankenberg, D, Fornika, DJ, Baker, D, Bouvier, D, Clements, D, Morais, DADL, Tabernero, DL, Lariviere, D, Nasr, E, Afgan, E, Zambelli, F, Heyl, F, Psomopoulos, F, Coppens, F, Price, GR, Cuccuru, G, Le Corguille, G, Von Kuster, G, Akbulut, GG, Rasche, H, Hans-Rudolf, H, Eguinoa, I, Makunin, I, Ranawaka, IJ, Taylor, JP, Joshi, J, Hillman-Jackson, J, Goecks, J, Chilton, JM, Kamali, K, Suderman, K, Poterlowicz, K, Yvan, LB, Lopez-Delisle, L, Sargent, L, Bassetti, ME, Tangaro, MA, van den Beek, M, Cech, M, Bernt, M, Fahrner, M, Tekman, M, Foell, MC, Schatz, MC, Crusoe, MR, Roncoroni, M, Kucher, N, Coraor, N, Stoler, N, Rhodes, N, Soranzo, N, Pinter, N, Goonasekera, NA, Moreno, PA, Videm, P, Melanie, P, Mandreoli, P, Jagtap, PD, Gu, Q, Weber, RJM, Lazarus, R, Vorderman, RHP, Hiltemann, S, Golitsynskiy, S, Garg, S, Bray, SA, Gladman, SL, Leo, S, Mehta, SP, Griffin, TJ, Jalili, V, Yves, V, Wen, V, Nagampalli, VK, Bacon, WA, de Koning, W, Maier, W, and Briggs, PJ

Abstract

Galaxy is a mature, browser accessible workbench for scientific computing. It enables scientists to share, analyze and visualize their own data, with minimal technical impediments. A thriving global community continues to use, maintain and contribute to the project, with support from multiple national infrastructure providers that enable freely accessible analysis and training services. The Galaxy Training Network supports free, self-directed, virtual training with >230 integrated tutorials. Project engagement metrics have continued to grow over the last 2 years, including source code contributions, publications, software packages wrapped as tools, registered users and their daily analysis jobs, and new independent specialized servers. Key Galaxy technical developments include an improved user interface for launching large-scale analyses with many files, interactive tools for exploratory data analysis, and a complete suite of machine learning tools. Important scientific developments enabled by Galaxy include Vertebrate Genome Project (VGP) assembly workflows and global SARS-CoV-2 collaborations.

Published
2022

33. Community-driven ELIXIR activities in single-cell omics [version 1; peer review: awaiting peer review]

Author

Czarnewski, P., Mahfouz, Ahmed, Calogero, R. A., Palagi, P. M., Portell-Silva, L., Gonzalez-Uriarte, A., Soneson, C., Burdett, T., Szomolay, B., Videm, P., Hotz, H. R., Papatheodorou, I., Hancock, J. M., Gruening, B., Haerty, W., Krause, Roland, Capella-Gutierrez, S., Lesko?ek, B., Alessandri, L., Arigoni, M., Rezen, T., Botzki, A., Ferk, P., Lindvall, J., Heil, Katharina, Ishaque, N., Korpelainen, E., Czarnewski, P., Mahfouz, Ahmed, Calogero, R. A., Palagi, P. M., Portell-Silva, L., Gonzalez-Uriarte, A., Soneson, C., Burdett, T., Szomolay, B., Videm, P., Hotz, H. R., Papatheodorou, I., Hancock, J. M., Gruening, B., Haerty, W., Krause, Roland, Capella-Gutierrez, S., Lesko?ek, B., Alessandri, L., Arigoni, M., Rezen, T., Botzki, A., Ferk, P., Lindvall, J., Heil, Katharina, Ishaque, N., and Korpelainen, E.

Published
2022

34. Reduced Long-Term Relative Survival in Females and Younger Adults Undergoing Cardiac Surgery: A Prospective Cohort Study.

Author

Tone Bull Enger, Hilde Pleym, Roar Stenseth, Guri Greiff, Alexander Wahba, and Vibeke Videm

Subjects
Medicine, Science
Abstract

OBJECTIVES:To assess long-term survival and mortality in adult cardiac surgery patients. METHODS:8,564 consecutive patients undergoing cardiac surgery in Trondheim, Norway from 2000 until censoring 31.12.2014 were prospectively followed. Observed long-term mortality following surgery was compared to the expected mortality in the Norwegian population, matched on gender, age and calendar year. This enabled assessment of relative survival (observed/expected survival rates) and relative mortality (observed/expected deaths). Long-term mortality was compared across gender, age and surgical procedure. Predictors of reduced survival were assessed with multivariate analyses of observed and relative mortality. RESULTS:During follow-up (median 6.4 years), 2,044 patients (23.9%) died. The observed 30-day, 1-, 3- and 5-year mortality rates were 2.2%, 4.4%, 8.2% and 13.8%, respectively, and remained constant throughout the study period. Comparing observed mortality to that expected in a matched sample from the general population, patients undergoing cardiac surgery showed excellent survival throughout the first seven years of follow-up (relative survival ≥ 1). Subsequently, survival decreased, which was more pronounced in females and patients undergoing other procedures than isolated coronary artery bypass grafting (CABG). Relative mortality was higher in younger age groups, females and patients undergoing aortic valve replacement (AVR). The female survival advantage in the general population was obliterated (relative mortality ratio (RMR) 1.35 (1.19-1.54), p

Published
2016
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35. MOF-associated complexes ensure stem cell identity and Xist repression

Author

Tomasz Chelmicki, Friederike Dündar, Matthew James Turley, Tasneem Khanam, Tugce Aktas, Fidel Ramírez, Anne-Valerie Gendrel, Patrick Rudolf Wright, Pavankumar Videm, Rolf Backofen, Edith Heard, Thomas Manke, and Asifa Akhtar

Subjects
D. melanogaster, epigenetic, chromatin, transcription, acetylation, X inactivation, Medicine, Science, Biology (General), QH301-705.5
Abstract

Histone acetyl transferases (HATs) play distinct roles in many cellular processes and are frequently misregulated in cancers. Here, we study the regulatory potential of MYST1-(MOF)-containing MSL and NSL complexes in mouse embryonic stem cells (ESCs) and neuronal progenitors. We find that both complexes influence transcription by targeting promoters and TSS-distal enhancers. In contrast to flies, the MSL complex is not exclusively enriched on the X chromosome, yet it is crucial for mammalian X chromosome regulation as it specifically regulates Tsix, the major repressor of Xist lncRNA. MSL depletion leads to decreased Tsix expression, reduced REX1 recruitment, and consequently, enhanced accumulation of Xist and variable numbers of inactivated X chromosomes during early differentiation. The NSL complex provides additional, Tsix-independent repression of Xist by maintaining pluripotency. MSL and NSL complexes therefore act synergistically by using distinct pathways to ensure a fail-safe mechanism for the repression of X inactivation in ESCs.

Published
2014
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36. Mannose-binding lectin deficiency is associated with myocardial infarction: the HUNT2 study in Norway.

Author

Inga Thorsen Vengen, Hans O Madsen, Peter Garred, Carl Platou, Lars Vatten, and Vibeke Videm

Subjects
Medicine, Science
Abstract

OBJECTIVES: Mannose-binding lectin (MBL) and ficolins activate the complement cascade, which is involved in atherogenesis. Based on a pilot study, we hypothesized that functional polymorphisms in the MBL gene (MBL2) leading to dysfunctional protein are related to development of myocardial infarction (MI). The aim of the present study was to study polymorphisms in MBL2 and ficolin genes in relation to the risk of MI. METHODS AND RESULTS: Using the population-based HUNT Study in Norway, 57,133 persons were followed up for a first-time MI from 1995-1997 until the end of 2008. The 370 youngest MI patients were matched by age (range 29-62 years) and gender to 370 controls. A younger population was selected because disease in this group might be less dependent on non-genetic risk factors. The study size was based on power calculation. Polymorphisms in MBL2 and in the genes of ficolin-1, ficolin-2 and ficolin-3 were genotyped by pyrosequencing and related to the risk of MI, estimated as odds ratios (OR). Functional haplotypes were analyzed and stringent alpha levels of significance were set by permutation testing. Variant MBL2 haplotypes causing MBL deficiency were associated with a two-fold higher risk of MI (OR 2.04, 95%CI 1.29-3.24). Adjustments for conventional cardiovascular risk factors did not substantially influence the association. The ficolins were not associated with MI risk. CONCLUSION: In a young to middle aged and relatively healthy Caucasian population, MBL2 variants related to functional MBL deficiency were associated with a doubling of the risk for MI, independent of conventional risk factors. This supports that MBL deficiency may lead to increased atherosclerosis or development of vulnerable plaques.

Published
2012
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39. The RNA workbench 2.0: next generation RNA data analysis

Author

Fallmann, J, Videm, P, Bagnacani, A, Batut, B, Doyle, MA, Klingstrom, T, Eggenhofer, F, Stadler, PF, Backofen, R, Gruening, B, Fallmann, J, Videm, P, Bagnacani, A, Batut, B, Doyle, MA, Klingstrom, T, Eggenhofer, F, Stadler, PF, Backofen, R, and Gruening, B

Abstract

RNA has become one of the major research topics in molecular biology. As a central player in key processes regulating gene expression, RNA is in the focus of many efforts to decipher the pathways that govern the transition of genetic information to a fully functional cell. As more and more researchers join this endeavour, there is a rapidly growing demand for comprehensive collections of tools that cover the diverse layers of RNA-related research. However, increasing amounts of data, from diverse types of experiments, addressing different aspects of biological questions need to be consolidated and integrated into a single framework. Only then is it possible to connect findings from e.g. RNA-Seq experiments and methods for e.g. target predictions. To address these needs, we present the RNA Workbench 2.0 , an updated online resource for RNA related analysis. With the RNA Workbench we created a comprehensive set of analysis tools and workflows that enables researchers to analyze their data without the need for sophisticated command-line skills. This update takes the established framework to the next level, providing not only a containerized infrastructure for analysis, but also a ready-to-use platform for hands-on training, analysis, data exploration, and visualization. The new framework is available at https://rna.usegalaxy.eu , and login is free and open to all users. The containerized version can be found at https://github.com/bgruening/galaxy-rna-workbench.

Published
2019

40. Community-Driven Data Analysis Training for Biology

Author

Batut, B. (Bérénice), Hiltemann, S. (Saskia), Bagnacani, A. (Andrea), Baker, D. (Dannon), Bhardwaj, V. (Vivek), Blank, C. (Clemens), Bretaudeau, A. (Anthony), Brillet-Guéguen, L. (Loraine), Čech, M. (Martin), Chilton, J. (John), Clements, D. (Dave), Doppelt-Azeroual, O. (Olivia), Erxleben, A. (Anika), Freeberg, M.A. (Mallory Ann), Gladman, S. (Simon), Hoogstrate, Y. (Youri), Hotz, H.-R. (Hans-Rudolf), Houwaart, T. (Torsten), Jagtap, P. (Pratik), Larivière, D. (Delphine), Le Corguillé, G. (Gildas), Manke, T. (Thomas), Mareuil, F. (Fabien), Ramírez, F. (Fidel), Ryan, D. (Devon), Sigloch, F.C. (Florian Christoph), Soranzo, N. (Nicola), Wolff, J. (Joachim), Videm, P. (Pavankumar), Wolfien, M. (Markus), Wubuli, A. (Aisanjiang), Yusuf, D. (Dilmurat), Taylor, J. (James), Backofen, R. (Rolf), Nekrutenko, A. (Anton), Grüning, B. (Björn), Batut, B. (Bérénice), Hiltemann, S. (Saskia), Bagnacani, A. (Andrea), Baker, D. (Dannon), Bhardwaj, V. (Vivek), Blank, C. (Clemens), Bretaudeau, A. (Anthony), Brillet-Guéguen, L. (Loraine), Čech, M. (Martin), Chilton, J. (John), Clements, D. (Dave), Doppelt-Azeroual, O. (Olivia), Erxleben, A. (Anika), Freeberg, M.A. (Mallory Ann), Gladman, S. (Simon), Hoogstrate, Y. (Youri), Hotz, H.-R. (Hans-Rudolf), Houwaart, T. (Torsten), Jagtap, P. (Pratik), Larivière, D. (Delphine), Le Corguillé, G. (Gildas), Manke, T. (Thomas), Mareuil, F. (Fabien), Ramírez, F. (Fidel), Ryan, D. (Devon), Sigloch, F.C. (Florian Christoph), Soranzo, N. (Nicola), Wolff, J. (Joachim), Videm, P. (Pavankumar), Wolfien, M. (Markus), Wubuli, A. (Aisanjiang), Yusuf, D. (Dilmurat), Taylor, J. (James), Backofen, R. (Rolf), Nekrutenko, A. (Anton), and Grüning, B. (Björn)

Abstract

The primary problem with the explosion of biomedical datasets is not the data, not computational resources, and not the required storage space, but the general lack of trained and skilled researchers to manipulate and analyze these data. Eliminating this problem requires development of comprehensive educational resources. Here we present a community-driven framework that enables modern, interactive teaching of data analytics in life sciences and facilitates the development of training materials. The key feature of our system is that it is not a static but a continuously improved collection of tutorials. By coupling tutorials with a web-based analysis framework, biomedical researchers can learn by performing computation themselves through a web browser without the need to install software or search for example datasets. Our ultimate goal is to expand the breadth of training materials to include fundamental statistical and data science topics and to precipitate a complete re-engineering of undergraduate and graduate curricula in life sciences. This project is accessible at https://training.galaxyproject.org. We developed an infrastructure that facilitates data analysis training in life sciences. It is an interactive learning platform tuned for current types of data and research problems. Importantly, it provides a means for community-wide content creation and maintenance and, finally, enables trainers and trainees to use the tutorials in a variety of situations, such as those where reliable Internet access is unavailable.

Published
2018
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41. Community-Driven Data Analysis Training for Biology

Author

Batut, B, Hiltemann, Saskia, Bagnacani, A, Baker, D, Bhardwaj, V, Blank, C, Bretaudeau, A, Brillet-Gueguen, L, Cech, M, Chilton, J, Clements, D, Doppelt-Azeroual, O, Erxleben, A, Freeberg, MA, Gladman, S, Hoogstrate, Youri, Hotz, HR, Houwaart, T, Jagtap, P, Lariviere, D, Le Corguille, G, Manke, T, Mareuil, F, Ramirez, F, Ryan, D, Sigloch, FC, Soranzo, N, Wolff, J, Videm, P, Wolfien, M, Wubuli, A, Yusuf, D, Taylor, J, Backofen, R, Nekrutenko, A, Gruning, B, Batut, B, Hiltemann, Saskia, Bagnacani, A, Baker, D, Bhardwaj, V, Blank, C, Bretaudeau, A, Brillet-Gueguen, L, Cech, M, Chilton, J, Clements, D, Doppelt-Azeroual, O, Erxleben, A, Freeberg, MA, Gladman, S, Hoogstrate, Youri, Hotz, HR, Houwaart, T, Jagtap, P, Lariviere, D, Le Corguille, G, Manke, T, Mareuil, F, Ramirez, F, Ryan, D, Sigloch, FC, Soranzo, N, Wolff, J, Videm, P, Wolfien, M, Wubuli, A, Yusuf, D, Taylor, J, Backofen, R, Nekrutenko, A, and Gruning, B

Published
2018

43. Perioperative Factors Associated With Changes in Troponin T During Coronary Artery Bypass Grafting.

Author

Koppen, Elias, Madsen, Erik, Greiff, Guri, Stenseth, Roar, Pleym, Hilde, Wiseth, Rune, Wahba, Alexander, and Videm, Vibeke

Abstract

Investigate important clinical and operative variables associated with increases in cardiac troponin T (cTnT) as indicators of myocardial injury after coronary artery bypass grafting (CABG). Prospective cohort study. Single university hospital. The study comprised 626 patients undergoing isolated CABG from April 2008 through April 2010 with a validation cohort (n = 686) from 2015-2017. None. Perioperative variables were registered prospectively. The extent of diffuse coronary atherosclerosis and significant stenoses were assessed with preoperative coronary angiography. Mixed model analysis was used to construct a statistical model explaining the course of cTnT concentrations. The model was adjusted for preoperative and intraoperative/postoperative myocardial infarction (MI) for independent assessment of additional variables. Clinical factors associated with increased cTnT concentrations during and after CABG were longer duration of cardiopulmonary bypass (p < 0.001), higher preoperative creatinine (p < 0.001), New York Heart Association functional classification IV (p = 0.006), reduced LVEF (p = 0.034), higher preoperative C-reactive protein (p = 0.049), and intraoperative/postoperative MI (p < 0.001). Factors associated with decreasing cTnT concentrations during CABG were higher BSA (p < 0.001) and a recent preoperative MI (p < 0.001). The extent of diffuse coronary atherosclerosis and significant stenoses were not associated with changes in cTnT (p = 0.35). Results were similar in the validation cohort. Left ventricular ejection fraction, New York Heart Association classification, kidney function, inflammation status, duration of cardiopulmonary bypass, body surface area, and preoperative MI were associated with the cTnT rise-and-fall pattern related to myocardial injury after CABG. Information regarding these variables may be valuable when using cTnT in the diagnostic workup of postoperative MI. [ABSTRACT FROM AUTHOR]

Published
2019
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44. The RNA workbench: Best practices for RNA and high-throughput sequencing bioinformatics in Galaxy

Author

Grüning, B.A. (Björn A.), Fallmann, J. (Jörg), Yusuf, D. (Dilmurat), Will, S. (Sebastian), Erxleben, A. (Anika), Eggenhofer, F. (Florian), Houwaart, T. (Torsten), Batut, B. (Bérénice), Videm, P. (Pavankumar), Bagnacani, A. (Andrea), Wolfien, M. (Markus), Lott, S.C. (Steffen C.), Hoogstrate, Y. (Youri), Hess, W.R. (Wolfgang R.), Wolkenhauer, O. (Olaf), Hoffmann, S. (Steve), Akalin, A. (Altuna), Ohler, U. (Uwe), Stadler, P.F. (Peter F.), Backofen, R. (Rolf), Grüning, B.A. (Björn A.), Fallmann, J. (Jörg), Yusuf, D. (Dilmurat), Will, S. (Sebastian), Erxleben, A. (Anika), Eggenhofer, F. (Florian), Houwaart, T. (Torsten), Batut, B. (Bérénice), Videm, P. (Pavankumar), Bagnacani, A. (Andrea), Wolfien, M. (Markus), Lott, S.C. (Steffen C.), Hoogstrate, Y. (Youri), Hess, W.R. (Wolfgang R.), Wolkenhauer, O. (Olaf), Hoffmann, S. (Steve), Akalin, A. (Altuna), Ohler, U. (Uwe), Stadler, P.F. (Peter F.), and Backofen, R. (Rolf)

Abstract

RNA-based regulation has become a major research topic in molecular biology. The analysis of epigenetic and expression data is therefore incomplete if RNA-based regulation is not taken into account. Thus, it is increasingly important but not yet standard to combine RNA-centric data and analysis tools with other types of experimental data such as RNA-seq or ChIP-seq. Here, we present the RNA workbench, a comprehensive set of analysis tools and consolidated workflows that enable the researcher to combine these two worlds. Based on the Galaxy framework the workbench guarantees simple access, easy extension, flexible adaption to personal and security needs, and sophisticated analyses that are independent of command-line knowledge. Currently, it includes more than 50 bioinformatics tools that are dedicated to different research areas of RNA biology including RNA structure analysis, RNA alignment, RNA annotation, RNA-protein interaction, ribosome profiling, RNA-seq analysis and RNA target prediction. The workbench is developed and maintained by experts in RNA bioinformatics and the Galaxy framework. Together with the growing community evolving around this workbench, we are committed to keep the workbench up-to-date for future standards and needs, providing researchers with a reliable and robust framework for RNA data analysis.

Published
2017
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45. The RNA workbench: best practices for RNA and high-throughput sequencing bioinformatics in Galaxy

Author

Gruning, BA, Fallmann, J, Yusuf, D, Will, S, Erxleben, A, Eggenhofer, F, Houwaart, T, Batut, B, Videm, P, Bagnacani, A, Wolfien, M, Lott, SC, Hoogstrate, Youri, Hess, WR, Wolkenhauer, O, Hoffmann, S, Akalin, A, Ohler, U, Stadler, PF, Backofen, R, Gruning, BA, Fallmann, J, Yusuf, D, Will, S, Erxleben, A, Eggenhofer, F, Houwaart, T, Batut, B, Videm, P, Bagnacani, A, Wolfien, M, Lott, SC, Hoogstrate, Youri, Hess, WR, Wolkenhauer, O, Hoffmann, S, Akalin, A, Ohler, U, Stadler, PF, and Backofen, R

Published
2017

46. EXPLORING THE MENTAL HEALTH AND SPIRITUAL RECOVERY OF AN EXPERT-BY-EXPERIENCE: A DISCUSSION OF THE UNIQUE CONTRIBUTION SOCIAL WORKERS CAN MAKE TO SUPPORT THIS JOURNEY.

Author

Fox, Joanna and Videmšek, Petra

Subjects
SOCIAL workers, CULTURAL pluralism, MENTAL health, ACTIVE recovery, SOCIAL work education, CULTURAL competence
Abstract

Copyright of Ljetopis Socijalnog Rada / Annual of Social Work is the property of Pravni Fakultet Sveucilista u Zagrebu, Studijski Centar Socijalnog Rada and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published
2019
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47. Influence of Storage and Inter- and Intra-Assay Variability on the Measurement of Inflammatory Biomarkers in Population-Based Biobanking.

Author

van Waateringe, Robert P., Muller Kobold, Anneke C., van Vliet-Ostaptchouk, Jana V., van der Klauw, Melanie M., Koerts, Jan, Anton, Gabriele, Peters, Annette, Trischler, Gerlinde, Kvaløy, Kirsti, Naess, Marit, Videm, Vibeke, Hveem, Kristian, Waldenberger, Melanie, Koenig, Wolfgang, and Wolffenbuttel, Bruce H.R.

Abstract

Background: In the present study, we examined the effect of sample storage on the reproducibility of several inflammatory biomarkers, including high-sensitivity C-reactive protein (hsCRP), high-sensitivity interleukin-6 (hsIL6), and high-sensitivity tumor necrosis factor alpha (hsTNFα). In addition, we assessed inter- and intra-assay variability between collaborating biobanks. Methods: In total, 240 fasting plasma samples were obtained from the LifeLines biobank. Samples had been stored for less than 2 or more than 4 years at −80°C. Measurements were performed at three different laboratories. hsCRP was measured by immunonephelometry and ELISA, hsIL6, and hsTNFα samples were measured with ELISAs from two different manufacturers. For confirmation, similar analyses were performed on samples obtained from a subpopulation of 80 obese individuals. Passing-Bablok regression analysis and Bland-Altman plots were used to compare the results. Results: We observed good stability of samples stored at −80°C. hsCRP measured on the day of blood draw was similar to levels measured after more than 4 years of storage. There were small interlaboratory differences with the R&D ELISAs for hsIL6 and hsTNFα. We found a linear correlation between the Bender Medsystems ELISA and the R&D ELISA for hsIL6, with significantly higher levels measured with the R&D ELISA. Over 90% of hsTNFα samples measured with the IBL ELISA were below the detection limit of 0.13 ng/L, rendering this assay unsuitable for large-scale analysis. Similar results were found in the confirmation study. Conclusion: In summary, plasma hsCRP showed good stability in samples stored for either less than 2 years or more than 4 years at −80°C. Both the R&D and Bender Medsystems for hsIL6 measurement yielded similar results. The IBL hsTNFα assay is not suited for use in biobanking samples. Assays for the measurement of inflammatory biomarker assays should be rigorously tested before large sample sets are measured. [ABSTRACT FROM AUTHOR]

Published
2017
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48. Inflammation Is Strongly Associated With Cardiorespiratory Fitness, Sex, BMI, and the Metabolic Syndrome in a Self-reported Healthy Population: HUNT3 Fitness Study

Author

Madssen, Erik, Skaug, Eli-Anne, Wisløff, Ulrik, Ellingsen, Øyvind, and Videm, Vibeke

Abstract

To investigate whether C-reactive protein (CRP, a general marker of inflammation), neopterin (activated macrophages), lactoferrin (activated neutrophils), and endothelial function (flow-mediated vasodilation [FMD]) are associated with cardiorespiratory fitness (peak oxygen uptake [VO2peak]), sex, body mass index (BMI), and the metabolic syndrome (MetSyn) in a healthy adult population.

Published
2019
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49. Annotations of selected papers by foreign scientists

Author

Auerbach, T., Chernick, J., Julien, J., Lellouche, G., Zinn, W., Hummel, H. H., Cohn, C. E., Fischer, G. J., Kate, W. Y., Martens, F. H., Meneghettl, D., Toppel, B. I., Blomberg, P., Hellstr, E., Korner, S., Brlmberg, S., Dalstrom, I., Simon, Albert, Post, R. F., Damm, C. C., Howard, J. C., Wharton, C. B., Spitzer, Jr., Lyman, Colmer, F. C. W., Gallic, R. R., Gott, H. H., McNelly, M. J., Shoults, D. R., Levy, S., Voorhees, B. G., Aline, P. G., Cohen, K. P., Humphreys, Jr., I. R., Glbrat, R., Rtcard, J., Balke, S., Wivstad, I., Mileikowsky, C., Howells, G. R., Hughes, T. G., Mackey, D. R., Saddington, K., Huber, A. P., Dykstra, J., Thompson, B. H., Lewis, W. H., Flanary, R., Brooksbank, R. E., Leuze, R. E., Baybarz, R. D., Waldron, M. B., Garston, J., Lee, J. A., Mardon, P. G., Marples, J. A. C., Poole, D. M., Wtlllamson, G. K., Videm, K., Hayward, B. R., Hotley, C. E., Mulford, R. N. R., Huber, Jr., E. J., Head, E. L., Borklund, K. V., Chiswik, H. H., Oosthuizen, S. A., Pyne-Mercler, W. G., Fichardt, T., and Savage, D.

Published
1958
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