318 results on '"Postma, Dirkje"'
Search Results
2. Integrated proteogenomic approach identifying a protein signature of COPD and a new splice variant of SORBS1.
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Brandsma, Corry-Anke, Guryev, Victor, Timens, Wim, Ciconelle, Ana, Postma, Dirkje S., Bischoff, Rainer, Johansson, Maria, Ovchinnikova, Ekaterina S., Malm, Johan, Marko-Varga, Gyorgy, Fehniger, Thomas E., van den Berge, Maarten, and Horvatovich, Peter
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RNA sequencing ,OBSTRUCTIVE lung diseases ,PROTEINS - Abstract
Translation of genomic alterations to protein changes in chronic obstructive pulmonary disease (COPD) is largely unexplored. Using integrated proteomic and RNA sequencing analysis of COPD and control lung tissues, we identified a protein signature in COPD characterised by extracellular matrix changes and a potential regulatory role for SUMO2. Furthermore, we identified 61 differentially expressed novel, non-reference, peptides in COPD compared with control lungs. This included two peptides encoding for a new splice variant of SORBS1, of which the transcript usage was higher in COPD compared with control lungs. These explorative findings and integrative proteogenomic approach open new avenues to further unravel the pathology of COPD. [ABSTRACT FROM AUTHOR]
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- 2020
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3. Nasal gene expression changes with inhaled corticosteroid treatment in asthma.
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Boudewijn, Ilse M., Lan, Andy, Faiz, Alen, Cox, Claire A., Brouwer, Sharon, Schokker, Siebrig, Vroegop, Sebastiaan J., Nawijn, Martijn C., Woodruff, Prescott G., Christenson, Stephanie A., Hagedoorn, Paul, Frijlink, Henderik W., Choy, David F., Brouwer, Uilke, Wisman, Marissa, Postma, Dirkje S., Fingleton, James, Beasley, Richard, van den Berge, Maarten, and Guryev, Victor
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GENE expression ,FLUTICASONE propionate ,WHEEZE ,ASTHMA ,GENE expression profiling - Abstract
C and E, Genes upregulated in nasal brushes after ICS treatment are significantly enriched among genes upregulated in bronchial biopsies of asthma patients after ICS treatment (both FDR < 0.01). D and F, Genes downregulated in nasal brushes after ICS treatment are significantly enriched among genes downregulated in bronchial biopsies of asthma patients after ICS treatment (both FDR < 0.01). In summary, we show that nasal gene expression is dynamic, changes with ICS treatment in asthma patients and can be used as a proxy for the lower airways to investigate ICS-induced gene expression changes. [Extracted from the article]
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- 2020
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4. Occupational exposure to gases/fumes and mineral dust affect DNA methylation levels of genes regulating expression.
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Plaat, Diana A van der, Vonk, Judith M, Terzikhan, Natalie, Jong, Kim de, Vries, Maaike de, Gemert, Sacha La Bastide-van, Diemen, Cleo C van, Lahousse, Lies, Brusselle, Guy G, Nedeljkovic, Ivana, Amin, Najaf, Consortium, BIOS, Kromhout, Hans, Vermeulen, Roel C H, Postma, Dirkje S, Duijn, Cornelia M van, and Boezen, H Marike
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- 2019
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5. Diagnosis and management of asthma, COPD and asthma‐COPD overlap among primary care physicians and respiratory/allergy specialists: A global survey.
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Jenkins, Christine, FitzGerald, J. Mark, Martinez, Fernando J., Postma, Dirkje S., Rennard, Stephen, Molen, Thys, Gardev, Asparuh, Genofre, Eduardo, and Calverley, Peter
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ASTHMA diagnosis ,ASTHMA treatment ,OBSTRUCTIVE lung diseases ,PRIMARY care ,PHYSICIANS ,RESPIRATORY therapists ,DECISION making in clinical medicine ,DIFFERENTIAL diagnosis - Abstract
Introduction: Asthma‐chronic obstructive pulmonary disease (COPD) overlap (ACO) is a heterogenous condition with clinical features shared by both asthma and COPD. Objectives: This online global survey of respiratory/allergy specialists and primary care practitioners (PCPs) was performed to understand current clinical approaches to the differential diagnosis and management of asthma, COPD and ACO. Methods: Respondents were recruited through: (a) a global online physician respondent community (49,980 PCPs and 7205 specialists); (b) market research agents; (c) experts; (d) professional societies; (e) colleague invitation. Respondents were presented with a survey including hypothetical clinical scenarios of diagnostic uncertainty to identify management approaches. Results: 891 responses (447 PCPs and 444 specialists) were collected across 13 countries. Reported features used for diagnosis of asthma and COPD were consistent with practice guidelines, but there was variability in those selected for ACO diagnosis. Features typically selected by specialists focused on spirometry/history, while PCPs focused on previous treatment/symptoms. Most respondents could correctly diagnose patients with features of ACO; however, features selected for theoretical diagnosis were often different to those selected in the case scenarios. Additionally, treatment selection was often inconsistent with guidelines, with over half of respondents not recommending inhaled corticosteroids in a patient with ACO and dominant features of asthma. Conclusion: While most PCPs and respiratory/allergy specialists can reach a working diagnosis of ACO, there remains uncertainty around which diagnostic features are most important and what constitutes optimal management. It is imperative that clinical studies including patients with ACO are initiated, allowing the generation of evidence‐based management strategies. [ABSTRACT FROM AUTHOR]
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- 2019
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6. Predictive value of eosinophils and neutrophils on clinical effects of ICS in COPD.
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Hartjes, Floor J., Vonk, Judith M., Faiz, Alen, Hiemstra, Pieter S., Lapperre, Thérèse S., Kerstjens, Huib A.M., Postma, Dirkje S., and van den Berge, Maarten
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EOSINOPHILS ,NEUTROPHILS ,ADRENOCORTICAL hormones ,OBSTRUCTIVE lung diseases ,BIOMARKERS - Abstract
Background and objective: Inflammation is present to a variable degree and composition in patients with COPD. This study investigates associations between both eosinophils and neutrophils in blood, sputum, airway wall biopsies and bronchoalveolar lavage (BAL) and their potential use as biomarkers for clinical response to inhaled corticosteroids (ICS). Methods: In total, 114 steroid‐naïve COPD patients of the Groningen Leiden Universities Corticosteroids in Obstructive Lung Disease (GLUCOLD) study using ICS or placebo during 30‐month follow‐up were included. Cell counts in blood, sputum, biopsies and BAL were evaluated at baseline. In addition, at baseline, 6 and 30 months, forced expiratory flow in 1 s (FEV1), residual volume/total lung capacity (hyperinflation) and Clinical COPD Questionnaire were evaluated. Results: Cross‐sectional analyses at baseline showed that higher blood eosinophils were significantly associated with higher eosinophil counts in sputum, biopsies and BAL. However, blood neutrophils did not significantly correlate with neutrophil counts in the other compartments. Baseline eosinophils and neutrophils, in whichever compartment measured, did not predict longitudinal FEV1 changes. Higher baseline biopsy eosinophils were associated with an increase in symptoms during 6‐ and 30‐month ICS treatment. In addition, higher biopsy neutrophils were associated with a more marked reduction in hyperinflation during 6‐month ICS treatment compared with placebo. Conclusion: Our findings indicate that blood eosinophils reflect eosinophils in other compartments, in contrast to neutrophils, in ICS‐naïve COPD patients. Both baseline eosinophils and neutrophils do not predict ICS‐induced lung function changes over a period of 6–30 months. The associations of biopsy eosinophils with worsening respiratory symptoms and biopsy neutrophils with improvement in hyperinflation during ICS treatment deserve further investigation. See Letter Blood eosinophils, in contrast to neutrophils, reflect eosinophils in sputum, biopsies and bronchoalveolar lavage (BAL), in inhaled corticosteroids (ICS)‐naïve COPD patients. However, both baseline eosinophils and neutrophils, whether measured in blood, sputum, biopsies and BAL, insufficiently predict lung function response to ICS in COPD over a period of 6–30 months. [ABSTRACT FROM AUTHOR]
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- 2018
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7. Lung tissue gene-expression signature for the ageing lung in COPD.
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de Vries, Maaike, Faiz, Alen, Woldhuis, Roy R., Postma, Dirkje S., de Jong, Tristan V., Sin, Don D., Bossé, Yohan, Nickle, David C., Guryev, Victor, Timens, Wim, Van den Berge, Maarten, and Brandsma, Corry-Anke
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RIBOSOMAL proteins ,MYOSIN ,GUANINE nucleotide exchange factors ,LUNGS - Published
- 2018
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8. Occupational exposure to pesticides is associated with differential DNA methylation.
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van der Plaat, Diana A., de Jong, Kim, de Vries, Maaike, van Diemen, Cleo C., Nedeljković, Ivana, Amin, Najaf, Kromhout, Hans, Vermeulen, Roel, Postma, Dirkje S., van Duijn, Cornelia M., Boezen, H. Marike, Vonk, Judith M., and Biobank-based Integrative Omics Study Consortium
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Objectives: Occupational pesticide exposure is associated with a wide range of diseases, including lung diseases, but it is largely unknown how pesticides influence airway disease pathogenesis. A potential mechanism might be through epigenetic mechanisms, like DNA methylation. Therefore, we assessed associations between occupational exposure to pesticides and genome-wide DNA methylation sites.Methods: 1561 subjects of LifeLines were included with either no (n=1392), low (n=108) or high (n=61) exposure to any type of pesticides (estimated based on current or last held job). Blood DNA methylation levels were measured using Illumina 450K arrays. Associations between pesticide exposure and 420 938 methylation sites (CpGs) were assessed using robust linear regression adjusted for appropriate confounders. In addition, we performed genome-wide stratified and interaction analyses by gender, smoking and airway obstruction status, and assessed associations between gene expression and methylation for genome-wide significant CpGs (n=2802).Results: In total for all analyses, high pesticide exposure was genome-wide significantly (false discovery rate P<0.05) associated with differential DNA methylation of 31 CpGs annotated to 29 genes. Twenty of these CpGs were found in subjects with airway obstruction. Several of the identified genes, for example, RYR1, ALLC, PTPRN2, LRRC3B, PAX2 and VTRNA2-1, are genes previously linked to either pesticide exposure or lung-related diseases. Seven out of 31 CpGs were associated with gene expression levels.Conclusions: We show for the first time that occupational exposure to pesticides is genome-wide associated with differential DNA methylation. Further research should reveal whether this differential methylation plays a role in the airway disease pathogenesis induced by pesticides. [ABSTRACT FROM AUTHOR]- Published
- 2018
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9. A Genome-Wide Linkage Study for Chronic Obstructive Pulmonary Disease in a Dutch Genetic Isolate Identifies Novel Rare Candidate Variants.
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Nedeljkovic, Ivana, Terzikhan, Natalie, Vonk, Judith M., van der Plaat, Diana A., Lahousse, Lies, van Diemen, Cleo C., Hobbs, Brian D., Qiao, Dandi, Cho, Michael H., Brusselle, Guy G., Postma, Dirkje S., Boezen, H. M., van Duijn, Cornelia M., and Amin, Najaf
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OBSTRUCTIVE lung diseases ,REPRODUCTIVE isolation ,METALLOTHIONEIN - Abstract
Chronic obstructive pulmonary disease (COPD) is a complex and heritable disease, associated with multiple genetic variants. Specific familial types of COPD may be explained by rare variants, which have not been widely studied. We aimed to discover rare genetic variants underlying COPD through a genome-wide linkage scan. Affectedonly analysis was performed using the 6K Illumina Linkage IV Panel in 142 cases clustered in 27 families from a genetic isolate, the Erasmus Rucphen Family (ERF) study. Potential causal variants were identified by searching for shared rare variants in the exome-sequence data of the affected members of the families contributing most to the linkage peak. The identified rare variants were then tested for association with COPD in a large meta-analysis of several cohorts. Significant evidence for linkage was observed on chromosomes 15q14-15q25 [logarithm of the odds (LOD) score = 5.52], 11p15.4-11q14.1 (LOD = 3.71) and 5q14.3-5q33.2 (LOD = 3.49). In the chromosome 15 peak, that harbors the known COPD locus for nicotinic receptors, and in the chromosome 5 peak we could not identify shared variants. In the chromosome 11 locus, we identified four rare (minor allele frequency (MAF) <0.02), predicted pathogenic, missense variants. These were shared among the affected family members. The identified variants localize to genes including neuroblast differentiation-associated protein (AHNAK), previously associated with blood biomarkers in COPD, phospholipase C Beta 3 (PLCB3), shown to increase airway hyper-responsiveness, solute carrier family 22-A11 (SLC22A11), involved in amino acid metabolism and ion transport, and metallothionein-like protein 5 (MTL5), involved in nicotinate and nicotinamide metabolism. Association of SLC22A11 and MTL5 variants were confirmed in the meta-analysis of 9,888 cases and 27,060 controls. In conclusion, we have identified novel rare variants in plausible genes related to COPD. Further studies utilizing large sample whole-genome sequencing should further confirm the associations at chromosome 11 and investigate the chromosome 15 and 5 linked regions. [ABSTRACT FROM AUTHOR]
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- 2018
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10. SIRT1/FoxO3 axis alteration leads to aberrant immune responses in bronchial epithelial cells.
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Di Vincenzo, Serena, Heijink, Irene H., Noordhoek, Jacobien A., Cipollina, Chiara, Siena, Liboria, Bruno, Andreina, Ferraro, Maria, Postma, Dirkje S., Gjomarkaj, Mark, and Pace, Elisabetta
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OBSTRUCTIVE lung diseases ,AGING ,FORKHEAD transcription factors ,SMALL interfering RNA ,HISTONE deacetylase ,SIRTUINS ,GENETICS - Abstract
Abstract: Inflammation and ageing are intertwined in chronic obstructive pulmonary disease (COPD). The histone deacetylase SIRT1 and the related activation of FoxO3 protect from ageing and regulate inflammation. The role of SIRT1/FoxO3 in COPD is largely unknown. This study evaluated whether cigarette smoke, by modulating the SIRT1/FoxO3 axis, affects airway epithelial pro‐inflammatory responses. Human bronchial epithelial cells (16HBE) and primary bronchial epithelial cells (PBECs) from COPD patients and controls were treated with/without cigarette smoke extract (CSE), Sirtinol or FoxO3 siRNA. SIRT1, FoxO3 and NF‐κB nuclear accumulation, SIRT1 deacetylase activity, IL‐8 and CCL20 expression/release and the release of 12 cytokines, neutrophil and lymphocyte chemotaxis were assessed. In PBECs, the constitutive FoxO3 expression was lower in patients with COPD than in controls. Furthermore, CSE reduced FoxO3 expression only in PBECs from controls. In 16HBE, CSE decreased SIRT1 activity and nuclear expression, enhanced NF‐κB binding to the IL‐8 gene promoter thus increasing IL‐8 expression, decreased CCL20 expression, increased the neutrophil chemotaxis and decreased lymphocyte chemotaxis. Similarly, SIRT1 inhibition reduced FoxO3 expression and increased nuclear NF‐κB. FoxO3 siRNA treatment increased IL‐8 and decreased CCL20 expression in 16HBE. In conclusion, CSE impairs the function of SIRT1/FoxO3 axis in bronchial epithelium, dysregulating NF‐κB activity and inducing pro‐inflammatory responses. [ABSTRACT FROM AUTHOR]
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- 2018
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11. Long-term Air Pollution Exposure, Genome-wide DNA Methylation and Lung Function in the LifeLines Cohort Study.
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de F. C. Lichtenfels, Ana Julia, van der Plaat, Diana A., Kim de Jong, van Diemen, Cleo C., Postma, Dirkje S., Nedeljkovic, Ivana, van Duijn, Cornelia M., Amin, Najaf, la Bastide-van Gemert, Sacha, de Vries, Maaike, Ward-Caviness, Cavin K., Wolf, Kathrin, Waldenberger, Melanie, Peters, Annette, Stolk, Ronald P., Brunekreef, Bert, Boezen, H. Marike, and Vonk, Judith M.
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AIR pollution ,CONFIDENCE intervals ,METHYLATION ,RESEARCH funding ,PULMONARY function tests ,STATISTICS ,DATA analysis ,ENVIRONMENTAL exposure ,SECONDARY analysis ,DATA analysis software ,DESCRIPTIVE statistics - Abstract
BACKGROUND: Long-term air pollution exposure is negatively associated with lung function, yet the mechanisms underlying this association are not fully clear. Differential DNA methylation may explain this association. OBJECTIVES: Our main aim was to study the association between long-term air pollution exposure and DNA methylation. METHODS: We performed a genome-wide methylation study using robust linear regression models in 1,017 subjects from the LifeLines cohort study to analyze the association between exposure to nitrogen dioxide (NO
2 ) and particulate matter (PM2.5 , fine particulate matter with aerodynamic diameter ≤2.5 µm; PM10 , particulate matter with aerodynamic diameter ≤10 µm) and PM2.5absorbance , indicator of elemental carbon content (estimated with land-use-regression models) with DNA methylation in whole blood (Illumina® HumanMethylation450K BeadChip). Replication of the top hits was attempted in two independent samples from the population-based Cooperative Health Research in the Region of Augsburg studies (KORA). RESULTS: Depending on the p-value threshold used, we found significant associations between NO2 exposure and DNA methylation for seven CpG sites (Bonferroni corrected threshold p < 1.19 X 10-7 ) or for 4,980 CpG sites (False Discovery Rate <0.05). The top associated CpG site was annotated to the PSMB9 gene (i.e., cg04908668). None of the seven Bonferroni significant CpG-sites were significantly replicated in the two KORA-cohorts. No associations were found for PM exposure. CONCLUSIONS: Long-term NO2 exposure was genome-wide significantly associated with DNA methylation in the identification cohort but not in the replication cohort. Future studies are needed to further elucidate the potential mechanisms underlying NO2 -exposure-related respiratory disease. [ABSTRACT FROM AUTHOR]- Published
- 2018
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12. COPD GWAS variant at 19q13.2 in relation with DNA methylation and gene expression.
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Nedeljkovic, Ivana, Lahousse, Lies, Carnero-Montoro, Elena, Faiz, Alen, Vonk, Judith M., Jong, Kim de, van der Plaat, Diana A., van Diemen, Cleo C., Berge, Maarten van den, Obeidat, Ma'en, Bossé, Yohan, Nickle, David C., Consortium, BIOS, Uitterlinden, Andre G., van Meurs, Joyce B.J., Stricker, Bruno H.C., Brusselle, Guy G., Postma, Dirkje S., Boezen, H. Marike, and van Duijn, Cornelia M.
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- 2018
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13. Integrative Genomics of Emphysema-Associated Genes Reveals Potential Disease Biomarkers.
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Obeidat, Ma'en, Yunlong Nie, Fishbane, Nick, Xuan Li, Bossé, Yohan, Joubert, Philippe, Nickle, David C., Ke Hao, Postma, Dirkje S., Timens, Wim, Sze, Marc A., Shannon, Casey P., Hollander, Zsuzsanna, Ng, Raymond T., McManus, Bruce, Miller, Bruce E., Rennard, Stephen, Spira, Avrum, Hackett, Tillie-Louise, and Wan Lam
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- 2017
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14. Identification of transforming growth factor-beta-regulated microRNAs and the microRNA-targetomes in primary lung fibroblasts.
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Ong, Jennie, Timens, Wim, Rajendran, Vijay, Algra, Arjan, Spira, Avrum, Lenburg, Marc E., Campbell, Joshua D., van den Berge, Maarten, Postma, Dirkje S., van den Berg, Anke, Kluiver, Joost, and Brandsma, Corry-Anke
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FIBROBLASTS ,HOMEOSTASIS ,TRANSFORMING growth factors-beta ,LUNG disease treatment ,MICRORNA ,GENE expression ,THERAPEUTICS - Abstract
Background: Lung fibroblasts are involved in extracellular matrix homeostasis, which is mainly regulated by transforming growth factor-beta (TGF-β), and are therefore crucial in lung tissue repair and remodeling. Abnormal repair and remodeling has been observed in lung diseases like COPD. As miRNA levels can be influenced by TGF-β, we hypothesized that TGF-β influences miRNA expression in lung fibroblasts, thereby affecting their function. Materials and methods: We investigated TGF-β1-induced miRNA expression changes in 9 control primary parenchymal lung fibroblasts using miRNA arrays. TGF-β1-induced miRNA expression changes were validated and replicated in an independent set of lung fibroblasts composted of 10 controls and 15 COPD patients using qRT-PCR. Ago2-immunoprecipitation followed by mRNA expression profiling was used to identify the miRNA-targetomes of unstimulated and TGF-β1-stimulated primary lung fibroblasts (n = 2). The genes affected by TGF-β1-modulated miRNAs were identified by comparing the miRNA targetomes of unstimulated and TGF-β1-stimulated fibroblasts. Results: Twenty-nine miRNAs were significantly differentially expressed after TGF-β1 stimulation (FDR<0.05). The TGF-β1-induced miR-455-3p and miR-21-3p expression changes were validated and replicated, with in addition, lower miR-455-3p levels in COPD (p<0.05). We identified 964 and 945 genes in the miRNA-targetomes of unstimulated and TGF-β1-stimulated lung fibroblasts, respectively. The TGF-β and Wnt pathways were significantly enriched among the Ago2-IP enriched and predicted targets of miR-455-3p and miR-21-3p. The miR-455-3p target genes HN1, NGF, STRADB, DLD and ANO3 and the miR-21-3p target genes HHEX, CHORDC1 and ZBTB49 were consistently more enriched after TGF-β1 stimulation. Conclusion: Two miRNAs, miR-455-3p and miR-21-3p, were induced by TGF-β1 in lung fibroblasts. The significant Ago2-IP enrichment of targets of these miRNAs related to the TGF-β and/or Wnt pathways (NGF, DLD, HHEX) in TGF-β1-stimulated fibroblasts suggest a role for these miRNAs in lung diseases by affecting lung fibroblast function. [ABSTRACT FROM AUTHOR]
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- 2017
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15. Risk of pneumonia in obstructive lung disease: A real-life study comparing extra-fine and fine-particle inhaled corticosteroids.
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Sonnappa, Samatha, Martin, Richard, Israel, Elliot, Postma, Dirkje, van Aalderen, Wim, Burden, Annie, Usmani, Omar S., Price, David B., and null, null
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CORTICOSTEROIDS ,OBSTRUCTIVE lung disease treatment ,RISK factors of pneumonia ,RESPIRATORY diseases ,LOGISTIC regression analysis ,PATIENTS - Abstract
Background: Regular use of inhaled corticosteroids (ICS) in patients with obstructive lung diseases has been associated with a higher risk of pneumonia, particularly in COPD. The risk of pneumonia has not been previously evaluated in relation to ICS particle size and dose used. Methods: Historical cohort, UK database study of 23,013 patients with obstructive lung disease aged 12–80 years prescribed extra-fine or fine-particle ICS. The endpoints assessed during the outcome year were diagnosis of pneumonia, acute exacerbations and acute respiratory events in relation to ICS dose. To determine the association between ICS particle size, dose and risk of pneumonia in unmatched and matched treatment groups, logistic and conditional logistic regression models were used. Results: 14788 patients were stepped-up to fine-particle ICS and 8225 to extra-fine ICS. On unmatched analysis, patients stepping-up to extra-fine ICS were significantly less likely to be coded for pneumonia (adjusted odds ratio [aOR] 0.60; 95% CI 0.37, 0.97]); experience acute exacerbations (adjusted risk ratio [aRR] 0.91; 95%CI 0.85, 0.97); and acute respiratory events (aRR 0.90; 95%CI 0.86, 0.94) compared with patients stepping-up to fine-particle ICS. Patients prescribed daily ICS doses in excess of 700 mcg (fluticasone propionate equivalent) had a significantly higher risk of pneumonia (OR [95%CI] 2.38 [1.17, 4.83]) compared with patients prescribed lower doses, irrespective of particle size. Conclusions: These findings suggest that patients with obstructive lung disease on extra-fine particle ICS have a lower risk of pneumonia than those on fine-particle ICS, with those receiving higher ICS doses being at a greater risk. [ABSTRACT FROM AUTHOR]
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- 2017
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16. Computational analysis of multimorbidity between asthma, eczema and rhinitis.
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Aguilar, Daniel, Pinart, Mariona, Koppelman, Gerard H., Saeys, Yvan, Nawijn, Martijn C., Postma, Dirkje S., Akdis, Mübeccel, Auffray, Charles, Ballereau, Stéphane, Benet, Marta, García-Aymerich, Judith, González, Juan Ramón, Guerra, Stefano, Keil, Thomas, Kogevinas, Manolis, Lambrecht, Bart, Lemonnier, Nathanael, Melen, Erik, Sunyer, Jordi, and Valenta, Rudolf
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COMORBIDITY ,ECZEMA ,ASTHMA ,RHINITIS ,ALLERGIES - Abstract
Background: The mechanisms explaining the co-existence of asthma, eczema and rhinitis (allergic multimorbidity) are largely unknown. We investigated the mechanisms underlying multimorbidity between three main allergic diseases at a molecular level by identifying the proteins and cellular processes that are common to them. Methods: An in silico study based on computational analysis of the topology of the protein interaction network was performed in order to characterize the molecular mechanisms of multimorbidity of asthma, eczema and rhinitis. As a first step, proteins associated to either disease were identified using data mining approaches, and their overlap was calculated. Secondly, a functional interaction network was built, allowing to identify cellular pathways involved in allergic multimorbidity. Finally, a network-based algorithm generated a ranked list of newly predicted multimorbidity-associated proteins. Results: Asthma, eczema and rhinitis shared a larger number of associated proteins than expected by chance, and their associated proteins exhibited a significant degree of interconnectedness in the interaction network. There were 15 pathways involved in the multimorbidity of asthma, eczema and rhinitis, including IL4 signaling and GATA3-related pathways. A number of proteins potentially associated to these multimorbidity processes were also obtained. Conclusions: These results strongly support the existence of an allergic multimorbidity cluster between asthma, eczema and rhinitis, and suggest that type 2 signaling pathways represent a relevant multimorbidity mechanism of allergic diseases. Furthermore, we identified new candidates contributing to multimorbidity that may assist in identifying new targets for multimorbid allergic diseases. [ABSTRACT FROM AUTHOR]
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- 2017
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17. Cohort Analysis of Exacerbation Rates in Adolescent and Adult Patients Initiating Inhaled Corticosteroids for Asthma: Different Dose-Response Profile by Particle Size.
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Postma, Dirkje, Kaplan, Alan, Soriano, Joan, Grigg, Jonathon, Guilbert, Theresa, Aalderen, Wim, Roche, Nicolas, Burden, Anne, Hillyer, Elizabeth, Israel, Elliot, and Price, David
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DOSE-effect relationship in pharmacology ,BECLOMETHASONE dipropionate ,ASTHMA diagnosis ,ASTHMA treatment ,INHALATION anesthetics ,PATIENT satisfaction - Abstract
Introduction: Targeting small airway inflammation could lead to improved clinical outcomes in asthma. Previous observational studies concluded that therapy with extrafine-particle [mass median aerodynamic diameter (MMAD) <2 µm] inhaled corticosteroids (ICS) is associated with similar or better odds of achieving asthma control at lower prescribed doses than fine-particle ICS (MMAD = 2-5 µm). However, while it is believed that the dose-response for ICS reaches a plateau at sub-maximal doses, it is not clear whether such a plateau occurs with extrafine-particle ICS. Methods: To evaluate the potential effect of ICS particle size on dose-response of asthma-related outcomes, we studied severe exacerbation rates in a historical patient cohort of UK adults and adolescents with asthma initiating extrafine- or fine-particle ICS. We extracted electronic medical record data centralized at primary care practices, where information from secondary care and hospitalizations is also aggregated. Data were collected over one baseline (pre-initiation) and one outcome year. Results: Of 32,235 patients with asthma (aged 12-80 years), 54% initiated ICS with extrafine-particle ICS and 46% with fine-particle ICS. Overall, mean age (SD) was 41 (17) years; 60% female; 24% current and 20% ex-smokers. We found a greater ( P < 0.001) reduction in exacerbation rate at higher as compared with lower doses of extrafine-particle ICS: for patients initiating on ≤125 µg/day the reduction was −0.016 (95% CI −0.038, 0.006) exacerbations per year and for those initiating on >250 µg/day the reduction was −0.072 (−0.095, −0.049). No significant dose-response relationship was observed for patients initiating on fine-particle ICS [reduction in exacerbations per year: −0.041 (−0.070, −0.012) at the lowest doses and 0.009 (−0.017, 0.036) at the highest, P = 0.856, despite similar exacerbation rates in the baseline period for both cohorts ( P = 0.40)]. Conclusion: Our findings suggest that extrafine-particle ICS is associated with a reduction in exacerbation rates in a dose-dependent fashion in an adult asthma population. This dose-response relationship was not observed with fine-particle ICS. ENCePP Trial Registration: EUPAS8840. [ABSTRACT FROM AUTHOR]
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- 2017
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18. Sex-Related Allergic Rhinitis Prevalence Switch from Childhood to Adulthood: A Systematic Review and Meta-Analysis.
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Pinart, Mariona, Keller, Theresa, Reich, andreas, Fröhlich, Matthias, Cabieses, Báltica, Hohmann, Cynthia, Postma, Dirkje S., Bousquet, Jean, antó, Josep M., and Keil, Thomas
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ALLERGIC rhinitis ,DISEASE prevalence ,REGRESSION analysis ,ASTHMA in children ,META-analysis ,DISEASE risk factors ,ASTHMA risk factors - Abstract
Background: A sex-related switch in the prevalence of asthma from childhood (male predominance) to adulthood (female predominance) has been described, but for allergic rhinitis this remains unclear. We aimed to examine sex- and age-group-specific differences in allergic rhinitis prevalence by systematically evaluating studies from across the globe. Methods: A systematic search of MEDLINE and Embase for population-based cross-sectional studies was performed regardless of the language of publication. The search was restricted to the present millennium (2000 to June 2014). Study quality was defined by the sampling method, response rate, sample size, and data collection method. To assess sex differences in the prevalence of self- or parent-reported symptoms of rhinitis, calculated pooled estimates of the male-female ratio (MFR) were obtained using random-effects model metaanalyses due to heterogeneity. A meta-regression analysis was also performed. Results: Out of 6,539 publications identified, 67 cross-sectional population-based studies (291,726 males and 301,781 females) were included in our meta-analysis. In children (<11 years of age) significantly more boys than girls had rhinitis symptoms (MFR 1.21, 95% CI 1.17-1.25), whereas in adolescents (11 to <18 years of age) males were significantly less often affected than females (MFR 0.90, 95% CI 0.85-0.95). No sex-specific prevalence difference was observed in adults (MFR 0.96, 95% CI 0.83-1.17). These findings were consistent in all continents except in Asia, where the male predominance remained beyond childhood. Conclusions: The male predominance of rhinitis prevalence in child- hood changed towards a female predominance in adolescence across the globe, except in Asia. Longitudinal studies are needed to confirm these cross-sectional data and examine possible determinants and underlying mechanisms. [ABSTRACT FROM AUTHOR]
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- 2017
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19. The effect of COPD severity and study duration on exacerbation outcome in randomized controlled trials.
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Eriksson, Göran, Calverley, Peter M., Jenkins, Christine R., Anzueto, Antonio R., Make, Barry J., Lindberg, Magnus, Fagerås, Malin, and Postma, Dirkje S.
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- 2017
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20. Sulfatase modifying factor 1 (SUMF1) is associated with Chronic Obstructive Pulmonary Disease.
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Weidner, Julie, Jarenbäck, Linnea, de Jong, Kim, Vonk, Judith M., van den Berge, Maarten, Brandsma, Corry-Anke, Marike Boezen, H., Sin, Don, Bossé, Yohan, Nickle, David, Ankerst, Jaro, Bjermer, Leif, Postma, Dirkje S., Faiz, Alen, Tufvesson, Ellen, and Boezen, H Marike
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OBSTRUCTIVE lung diseases ,LABORATORY mice ,PHENOTYPES ,GENE expression ,SINGLE nucleotide polymorphisms ,GENOTYPES ,DISEASE susceptibility ,ESTERASES ,GENETIC polymorphisms ,GENETIC techniques ,RESEARCH evaluation ,SMOKING ,SPUTUM ,GENETIC markers ,DISEASE prevalence - Abstract
Background: It has been observed that mice lacking the sulfatase modifying factor (Sumf1) developed an emphysema-like phenotype. However, it is unknown if SUMF1 may play a role in Chronic Obstructive Pulmonary Disease (COPD) in humans. The aim was to investigate if the expression and genetic regulation of SUMF1 differs between smokers with and without COPD.Methods: SUMF1 mRNA was investigated in sputum cells and whole blood from controls and COPD patients (all current or former smokers). Expression quantitative trait loci (eQTL) analysis was used to investigate if single nucleotide polymorphisms (SNPs) in SUMF1 were significantly associated with SUMF1 expression. The association of SUMF1 SNPs with COPD was examined in a population based cohort, Lifelines. SUMF1 mRNA from sputum cells, lung tissue, and lung fibroblasts, as well as lung function parameters, were investigated in relation to genotype.Results: Certain splice variants of SUMF1 showed a relatively high expression in lung tissue compared to many other tissues. SUMF1 Splice variant 2 and 3 showed lower levels in sputum cells from COPD patients as compared to controls. Twelve SNPs were found significant by eQTL analysis and overlapped with the array used for genotyping of Lifelines. We found alterations in mRNA expression in sputum cells and lung fibroblasts associated with SNP rs11915920 (top hit in eQTL), which validated the results of the lung tissue eQTL analysis. Of the twelve SNPs, two SNPs, rs793391 and rs308739, were found to be associated with COPD in Lifelines. The SNP rs793391 was also confirmed to be associated with lung function changes.Conclusions: We show that SUMF1 expression is affected in COPD patients compared to controls, and that SNPs in SUMF1 are associated with an increased risk of COPD. Certain COPD-associated SNPs have effects on either SUMF1 gene expression or on lung function. Collectively, this study shows that SUMF1 is associated with an increased risk of developing COPD. [ABSTRACT FROM AUTHOR]- Published
- 2017
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21. An evaluation of exact matching and propensity score methods as applied in a comparative effectiveness study of inhaled corticosteroids in asthma.
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Burden, Anne, Roche, Nicolas, Miglio, Cristiana, Hillyer, Elizabeth V., Postma, Dirkje S., Herings, Ron M. C., Overbeek, Jetty A., Khalid, Javaria Mona, van Eickels, Daniela, and Price, David B.
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- 2017
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22. Control of moderate-to-severe asthma with randomized ciclesonide doses of 160, 320 and 640 μg/day.
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Pedersen, Søren E., Prasad, Niyati, Goehring, Udo-Michael, Andersson, Henrik, and Postma, Dirkje S.
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STEROID receptors ,ADRENOCORTICAL hormones ,ASTHMATICS ,ASTHMA treatment ,DRUG therapy for asthma - Abstract
Background: The inhaled corticosteroid (ICS) ciclesonide (Cic), controls asthma symptoms in the majority of patients at the recommended dose of 160 µg/day. However, the relationship between the level of asthma control and increasing doses of Cic is unknown. This study investigated whether long-term treatment with higher doses of Cic would further improve asthma symptoms in patients with uncontrolled asthma despite ICS use. Patients and methods: In a double-blind, randomized, parallel-group study, 367 patients were allocated to one of three treatment arms (Cic 160, 320 and 640 µg/day). After a singleblind, 3-week baseline period with Cic 160 µg/day, eligible patients were randomized to receive 52 weeks of treatment with Cic 160, 320 or 640 µg/day (double-blind period) during which forced expiratory volume in 1 second (FEV
1 ), exacerbations and Asthma Control Questionnaire (ACQ) scores were measured. Results: Treatment with all the three doses was associated with significant improvements in ACQ scores, FEV1 and asthma symptoms (P<0.01). There were no statistically significant differences between the three doses. The results of the primary end point analysis showed a numerical improvement in the ACQ score with Cic 640 µ g/day compared with Cic 160 µg/day (least square [LS] mean: -0.122; two-sided P-value: 0.30). Post hoc subgroup analyses showed that the improvement in the ACQ score with Cic 640 µ g/day compared with Cic 160 µ g/day was statistically significant in subjects who experience at least one exacerbation per year (LS mean: -0.586; 95% confidence interval: -1.110, -0.062, P=0.0285). Adverse events were low and consistent with the known safety profile of Cic. Conclusion: In patients with persistent, uncontrolled asthma, increasing the Cic dose from 160 to 640 µg/day provided no clear additional effect. Patients who experience more than one exacerbation per year may benefit from higher doses; however, further studies are necessary to confirm this. All Cic doses were well tolerated. [ABSTRACT FROM AUTHOR]- Published
- 2017
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23. TRPA1 gene polymorphisms and childhood asthma.
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Gallo, Valentina, Dijk, F. Nicole, Holloway, John W., Ring, Susan M., Koppelman, Gerard H., Postma, Dirkje S., Strachan, David P., Granell, Raquel, Jongste, Johan C., Jaddoe, Vincent W. V., Dekker, Herman T., Duijts, Liesbeth, Henderson, A. John, and Shaheen, Seif O.
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ASTHMA in children ,GENETIC polymorphisms ,ACETAMINOPHEN ,ALLERGIES ,SINGLE nucleotide polymorphisms - Abstract
Background Animal data have suggested that the transient receptor potential ankyrin-1 ( TRPA1) ion channel plays a key role in promoting airway inflammation in asthma and may mediate effects of paracetamol on asthma, yet confirmatory human data are lacking. To study associations of TRPA1 gene variants with childhood asthma and total IgE concentration, and interactions between TRPA1 and prenatal paracetamol exposure on these outcomes. Methods We analysed associations between 31 TRPA1 single nucleotide polymorphisms ( SNPs) and current doctor-diagnosed asthma and total IgE concentration at 7.5 years in the Avon Longitudinal Study of Parents and Children ( ALSPAC) birth cohort. We sought to confirm the most significant associations with comparable outcomes in the Prevention and Incidence of Asthma and Mite Allergy ( PIAMA) and Generation R birth cohorts. In ALSPAC, we explored interactions with prenatal paracetamol exposure. Results In ALSPAC, there was strong evidence for association between six SNPs and asthma: rs959974 and rs1384001 (per-allele odds ratio for both: 1.30 (95% CI: 1.15-1.47), p = 0.00001), rs7010969 ( OR 1.28 (1.13-1.46), p = 0.00004), rs3735945 ( OR 1.30 (1.09-1.55), p = 0.003), rs920829 ( OR 1.30 (1.09-1.54), p = 0.004) and rs4738202 ( OR 1.22 (1.07-1.39), p = 0.004). In a meta-analysis across the three cohorts, the pooled effect estimates confirmed that all six SNPs were significantly associated with asthma. In ALSPAC, TRPA1 associations with asthma were not modified by prenatal paracetamol, although associations with IgE concentration were. Conclusion This study suggests that TRPA1 may play a role in the development of childhood asthma. (249 words) [ABSTRACT FROM AUTHOR]
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- 2017
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24. Airway wall thickness on HRCT scans decreases with age and increases with smoking.
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Telenga, Eef D., Oudkerk, Matthijs, van Ooijen, Peter M. A., Vliegenthart, Rozemarijn, ten Hacken, Nick H. T., Postma, Dirkje S., and van den Berge, Maarten
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AIRWAY (Anatomy) ,COMPUTED tomography ,PHYSIOLOGICAL effects of tobacco ,PULMONARY function tests ,INFLAMMATION ,AGING ,BRONCHI ,LONGITUDINAL method ,MULTIVARIATE analysis ,REFERENCE values ,REGRESSION analysis ,RESPIRATORY measurements ,SMOKING ,SPIROMETRY ,VITAL capacity (Respiration) ,CASE-control method - Abstract
Background: To investigate if age, gender and smoking are associated with airway wall thickness (AWT) measured by high resolution computed tomography (HRCT) and if higher AWT is associated with lower levels of pulmonary function in healthy current- and never-smokers with a wide age range.Methods: HRCT scans were performed in 99 subjects (48 never- and 51 current-smokers, median age 39 years [IQR 22 - 54], 57% males). The AWT at an internal perimeter of 10 mm (AWT Pi10) was calculated as an overall measurement of AWT, based on all measurements throughout the lungs. Extensive pulmonary function testing was performed in all subjects.Results: Higher age was associated with a lower AWT Pi10 (b = -0.003, p < 0.001). Current-smokers had a higher AWT Pi10 than never-smokers (mean 0.49 mm versus 0.44 mm, p = 0.022). In multivariate analysis, age and current-smoking were independently associated with AWT Pi10 (age b = -0.002, p < 0.001, current-smoking b = 0.041, p = 0.021), whereas gender was not (b = 0.011, p = 0.552). Higher AWT Pi10 was associated with a lower FEV1, FEV1/FVC, FEF25-75 and higher R5, R20 and X5.Conclusions: AWT decreases with higher age, possibly reflecting structural changes of the airways. Additionally, current-smokers have a higher AWT, possibly due to remodeling or inflammation. Finally, higher AWT is associated with a lower level of pulmonary function, even in this population of healthy subjects.Trial Registration: This Study was registered at www.clinicaltrials.gov with number NCT00848406 on 19 February 2009. [ABSTRACT FROM AUTHOR]- Published
- 2017
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25. Early efficacy of budesonide/formoterol in patients with moderate-to-very-severe COPD.
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Calverley, Peter M., Eriksson, Göran, Jenkins, Christine R., Anzueto, Antonio R., Make, Barry J., Persson, Anders, Fagerås, Malin, and Postma, Dirkje S.
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- 2017
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26. Targeting the small airways with dry powder adenosine: a challenging concept.
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van der Wiel, Erica, Lexmond, Anne J., van den Berge, Maarten, Postma, Dirkje S., Hagedoorn, Paul, Frijlink, Henderik W., Farenhorst, Martijn P., de Boer, Anne H., and ten Hacken, Nick H. T.
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- 2017
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27. Eosinophil Count Is a Common Factor for Complex Metabolic and Pulmonary Traits and Diseases: The LifeLines Cohort Study.
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Amini, Marzyeh, Bashirova, Dinara, Prins, Bram P., Corpeleijn, Eva, null, null, Bruinenberg, Marcel, Franke, Lude, Harst, Pim van der, Navis, Gerjan, Wolffenbuttel, Bruce H. R., Stolk, Ronald P., Wijmenga, Cisca, Postma, Dirkje S., Koppelman, Gerard H., Boezen, H. Marike, Vonk, Judith, Snieder, Harold, and Alizadeh, Behrooz Z.
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EOSINOPHILS ,OBESITY treatment ,LUNG disease diagnosis ,OBSTRUCTIVE lung disease treatment ,LUNG disease treatment ,BODY mass index - Abstract
There is ongoing debate on the association between eosinophil count and diseases, as previous studies were inconsistent. We studied the relationship of eosinophil count with 22 complex metabolic, cardiac, and pulmonary traits and diseases. From the population-based LifeLines Cohort Study (N = 167,729), 13,301 individuals were included. We focused on relationship of eosinophil count with three classes of metabolic (7 traits, 2 diseases), cardiac (6 traits, 2 diseases), and pulmonary (2 traits, 2 diseases) outcomes. Regression analyses were applied in overall, women and men, while adjusted for age, sex, BMI and smoking. A p-value of <0.00076 was considered statistically significant. 58.2% of population were women (mean±SD 51.3±11.1 years old). In overall, one-SD higher of ln-eosinophil count was associated with a 0.04 (±SE ±0.002;p = 6.0×10
−6 ) SD higher levels in ln-BMI, 0.06 (±0.007;p = 3.1×10−12 ) SD in ln-TG, 0.04 (±0.003;p = 7.0×10−6 ) SD in TC, 0.04 (±0.004;p = 6.3×10−7 ) SD in LDL, 0.04 (±0.006;p = 6.0×10−6 ) SD in HbA1c; and with a 0.05 (±0.004;p = 1.7×10−8 ) SD lower levels in HDL, 0.05 (±0.007;p = 3.4×10−23 ) SD in FEV1, and 0.09 (±0.001;p = 6.6×10−28 ) SD in FEV1/FVC. A higher ln-eosinophil count was associated with 1.18 (95%CI 1.09–1.28;p = 2.0×10−5 ) odds ratio of obesity, 1.29 (1.19–1.39;p = 1.1×10−10 ) of metabolic syndrome, 1.40 (1.25–1.56;p = 2.7×10−9 ) of COPD and 1.81 (1.61–2.03;p = 1.0×10−23 ) of asthma. Similar results were found in women. We found no association between ln-eosinophil count either with blood pressure indices in overall, women and men; or with BMI, LDL, HbA1c and obesity in men. In a large population based cohort, we confirmed eosinophil count as a potential factor implicated in metabolic and pulmonary outcomes. [ABSTRACT FROM AUTHOR]- Published
- 2016
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28. The Well-Known Gene HHIP and Novel Gene MECR Are Implicated in Small Airway Obstruction.
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van der Plaat, Diana A., Jong, Kim de, Lahousse, Lies, Faiz, Alen, Vonk, Judith M., van Diemen, Cleo C., Nedeljkovic, Ivana, Amin, Najaf, Obeidat, Ma’en, van Duijn, Cornelia M., Boezen, H. Marike, Postma, Dirkje S., de Jong, Kim, and Obeidat, Ma'en
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- 2016
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29. Targeted high-throughput sequencing of candidate genes for chronic obstructive pulmonary disease.
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Matsson, Hans, Söderhäll, Cilla, Einarsdottir, Elisabet, Lamontagne, Maxime, Gudmundsson, Sanna, Backman, Helena, Lindberg, Anne, Rönmark, Eva, Kere, Juha, Sin, Don, Postma, Dirkje S., Bossé, Yohan, Lundbäck, Bo, and Klar, Joakim
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OBSTRUCTIVE lung diseases patients ,OBSTRUCTIVE lung disease treatment ,NUCLEOTIDE sequencing ,PUBLIC health ,CHOLINERGIC receptors - Abstract
Background: Reduced lung function in patients with chronic obstructive pulmonary disease (COPD) is likely due to both environmental and genetic factors. We report here a targeted high-throughput DNA sequencing approach to identify new and previously known genetic variants in a set of candidate genes for COPD. Methods: Exons in 22 genes implicated in lung development as well as 61 genes and 10 genomic regions previously associated with COPD were sequenced using individual DNA samples from 68 cases with moderate or severe COPD and 66 controls matched for age, gender and smoking. Cases and controls were selected from the Obstructive Lung Disease in Northern Sweden (OLIN) studies. Results: In total, 37 genetic variants showed association with COPD (p < 0.05, uncorrected). Several variants previously discovered to be associated with COPD from genetic genome-wide analysis studies were replicated using our sample. Two high-risk variants were followed-up for functional characterization in a large eQTL mapping study of 1,111 human lung specimens. The C allele of a synonymous variant, rs8040868, predicting a p.(S45=) in the gene for cholinergic receptor nicotinic alpha 3 (CHRNA3) was associated with COPD (p = 8.8 x 10-3). This association remained (p = 0.003 and OR = 1.4, 95 % CI 1.1-1.7) when analysing all available cases and controls in OLIN (n = 1,534). The rs8040868 variant is in linkage disequilibrium with rs16969968 previously associated with COPD and altered expression of the CHRNA5 gene. A follow-up analysis for detection of expression quantitative trait loci revealed that rs8040868-C was found to be significantly associated with a decreased expression of the nearby gene cholinergic receptor, nicotinic, alpha 5 (CHRNA5) in lung tissue. Conclusion: Our data replicate previous result suggesting CHRNA5 as a candidate gene for COPD and rs8040868 as a risk variant for the development of COPD in the Swedish population. [ABSTRACT FROM AUTHOR]
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- 2016
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30. Protocadherin-1 Localization and Cell-Adhesion Function in Airway Epithelial Cells in Asthma.
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Faura Tellez, Grissel, Willemse, Brigitte W. M., Brouwer, Uilke, Nijboer-Brinksma, Susan, Vandepoele, Karl, Noordhoek, Jacobien A., Heijink, Irene, de Vries, Maaike, Smithers, Natalie P., Postma, Dirkje S., Timens, Wim, Wiffen, Laura, van Roy, Frans, Holloway, John W., Lackie, Peter M., Nawijn, Martijn C., and Koppelman, Gerard H.
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GENETICS of asthma ,CADHERINS ,EPITHELIAL cells ,CELL adhesion molecules ,GENE expression ,CONFOCAL fluorescence microscopy - Abstract
Background: The asthma gene PCDH1 encodes Protocadherin-1, a putative adhesion molecule of unknown function expressed in the airway epithelium. Here, we characterize the localization, differential expression, homotypic adhesion specificity and function of PCDH1 in airway epithelial cells in asthma. Methods: We performed confocal fluorescence microscopy to determine subcellular localization of PCDH1 in 16HBE cells and primary bronchial epithelial cells (PBECs) grown at air-liquid interface. Next, to compare PCDH1 expression and localization in asthma and controls we performed qRT-PCR and fluorescence microscopy in PBECs and immunohistochemistry on airway wall biopsies. We examined homotypic adhesion specificity of HEK293T clones overexpressing fluorescently tagged-PCDH1 isoforms. Finally, to evaluate the role for PCDH1 in epithelial barrier formation and repair, we performed siRNA knockdown-studies and measured epithelial resistance. Results: PCDH1 localized to the cell membrane at cell-cell contact sites, baso-lateral to adherens junctions, with increasing expression during epithelial differentiation. No differences in gene expression or localization of PCDH1 isoforms expressing the extracellular domain were observed in either PBECs or airway wall biopsies between asthma patients and controls. Overexpression of PCDH1 mediated homotypic interaction, whereas downregulation of PCDH1 reduced epithelial barrier formation, and impaired repair after wounding. Conclusions: In conclusion, PCDH1 is localized to the cell membrane of bronchial epithelial cells baso-lateral to the adherens junction. Expression of PCDH1 is not reduced nor delocalized in asthma even though PCDH1 contributes to homotypic adhesion, epithelial barrier formation and repair. [ABSTRACT FROM AUTHOR]
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- 2016
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31. Individualized prediction of lung-function decline in chronic obstructive pulmonary disease.
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Zafari, Zafar, Sin, Don D., Postma, Dirkje S., Löfdahl, Claes-Göran, Vonk, Judith, Bryan, Stirling, Lam, Stephen, Tammemagi, Martin, Khakban, Rahman, Paul Man, S. F., Tashkin, Donald, Wise, Robert A., Connett, John E., McManus, Bruce, Ng, Raymond, Hollander, Zsuszanna, Sadatsafavi, Mohsen, Tammemagi, C Martin, and Man, S F Paul
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OBSTRUCTIVE lung disease diagnosis ,OBSTRUCTIVE lung disease treatment ,HEALTH of cigarette smokers ,CIGARETTE smokers ,PUBLIC health ,MEDICAL care ,MANAGEMENT - Abstract
Background: The rate of lung-function decline in chronic obstructive pulmonary disease (COPD) varies substantially among individuals. We sought to develop and validate an individualized prediction model for forced expiratory volume at 1 second (FEV1) in current smokers with mild-to-moderate COPD.Methods: Using data from a large long-term clinical trial (the Lung Health Study), we derived mixed-effects regression models to predict future FEV1 values over 11 years according to clinical traits. We modelled heterogeneity by allowing regression coefficients to vary across individuals. Two independent cohorts with COPD were used for validating the equations.Results: We used data from 5594 patients (mean age 48.4 yr, 63% men, mean baseline FEV1 2.75 L) to create the individualized prediction equations. There was significant between-individual variability in the rate of FEV1 decline, with the interval for the annual rate of decline that contained 95% of individuals being -124 to -15 mL/yr for smokers and -83 to 15 mL/yr for sustained quitters. Clinical variables in the final model explained 88% of variation around follow-up FEV1. The C statistic for predicting severity grades was 0.90. Prediction equations performed robustly in the 2 external data sets.Interpretation: A substantial part of individual variation in FEV1 decline can be explained by easily measured clinical variables. The model developed in this work can be used for prediction of future lung health in patients with mild-to-moderate COPD.Trial Registration: Lung Health Study - ClinicalTrials.gov, no. NCT00000568; Pan-Canadian Early Detection of Lung Cancer Study - ClinicalTrials.gov, no. NCT00751660. [ABSTRACT FROM AUTHOR]- Published
- 2016
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32. Novel Genetic Susceptibility Loci for FEV1 in the Context of Occupational Exposure in Never-Smokers.
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Kim de Jong, Vonk, Judith M., Faiz, Alen, van der Plaat, Diana A., Timens, Wim, Bossé, Yohan, Kromhout, Hans, Nedeljkovic, Ivana, Postma, Dirkje S., and Boezen, H. Marike
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- 2016
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33. Novel Genetic Susceptibility Loci for FEV1 in the Context of Occupational Exposure in Never-Smokers.
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de Jong, Kim, Vonk, Judith M, Faiz, Alen, van der Plaat, Diana A, Timens, Wim, Bossé, Yohan, Kromhout, Hans, Nedeljkovic, Ivana, Postma, Dirkje S, and Boezen, H Marike
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- 2016
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34. Atopy and Inhaled Corticosteroid Use Associate with Fewer IL-17+ Cells in Asthmatic Airways.
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Fattahi, Fatemeh, Brandsma, Corry-Anke, Lodewijk, Monique, Reinders-Luinge, Marjan, Postma, Dirkje S., Timens, Wim, Hylkema, Machteld N., and ten Hacken, Nick H. T.
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ATOPY ,INTERLEUKIN-17 ,CORTICOSTEROIDS ,ASTHMA ,AIRWAY (Anatomy) ,IMMUNOSTAINING - Abstract
Background: Interleukin (IL)-17 plays a critical role in numerous immune and inflammatory responses and was recently suggested to contribute to the pathogenesis of nonatopic (non-eosinophil/neutrophil-dominant) asthma. We aimed to compare expression of IL-17 in bronchial airways between atopic and nonatopic asthmatics, with/without inhaled corticosteroid (ICS) use and to identify its major cellular source. Methods: Bronchial biopsies from 114 patients with mild-to-moderate asthma were investigated: 33 nonatopic, 63 non-corticosteroid users, 90 nonsmokers. IL-17 expression was correlated with atopy and inflammatory cell counts (EPX, NP57, CD3, CD4, CD8, CD20, CD68), taking ICS use and smoking into account. Multiple linear regression analyses were used to determine the independent factors as well as the most relevant inflammatory cells contributing to IL-17 expression. Double immunostainings were performed to confirm the major cellular source of IL-17. Results: In non-ICS users, nonatopic asthmatics had more IL-17
+ cells in the airway wall than atopic asthmatics. In both atopic and nonatopic asthmatics, ICS use was associated with lower numbers of IL-17+ cells, independent of smoking. The number of IL-17+ cells was associated with the number of neutrophils (B: 0.26, 95% CI: 0.17–0.35) and eosinophils (B: 0.18, 95% CI: 0.07–0.29). The majority of IL-17+ cells were neutrophils, as confirmed by double immunostaining. Conclusions: We show for the first time that atopy and ICS use are associated with lower numbers of IL-17+ cells in asthmatic airways. Importantly, IL-17+ cells were mostly neutrophils which conflicts with the paradigm that lymphocytes (Th17) are the main source of IL-17. [ABSTRACT FROM AUTHOR]- Published
- 2016
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35. Cost-Effectiveness of Asthma Step-Up Therapy as an Increased Dose of Extrafine-Particle Inhaled Corticosteroid or Add-On Long-Acting Beta-Agonist.
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Roche, Nicolas, Colice, Gene, Israel, Elliot, Martin, Richard, Dorinsky, Paul, Postma, Dirkje, Guilbert, Theresa, Grigg, Jonathan, Aalderen, Willem, Barion, Francesca, Hillyer, Elizabeth, Thomas, Victoria, Burden, Anne, Brett McQueen, R., and Price, David
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ASTHMA ,BECLOMETHASONE dipropionate ,BUDESONIDE ,CORTICOSTEROIDS ,FLUTICASONE propionate ,SALMETEROL - Abstract
Introduction: Data from different healthcare systems on relative cost-effectiveness of asthma step-up therapy strategies are required to inform decision-makers and clinicians. Our objective was to compare cost-effectiveness from the United Kingdom National Health Service perspective of three step-up strategies for patients with asthma uncontrolled by inhaled corticosteroid (ICS) monotherapy. Methods: This was a historical matched cohort cost-effectiveness analysis of anonymized medical records for patients with asthma of age 12-80 years. We conducted two-way comparisons of step-up therapy using increased dose (≥50%) of extrafine-particle ICS or add-on long-acting β-agonist (LABA) via fixed-dose combination (FDC) ICS/LABA inhaler or via separate inhaler. The incremental cost-effectiveness ratio (ICER) was calculated using asthma-related direct costs during one outcome year and a composite measure of risk-domain asthma control (no asthma-related hospital attendance, acute oral corticosteroids, or consultation for lower respiratory tract infection). Results: Patients prescribed ICS dose step-up ( n = 3036) had significantly lower baseline-adjusted, mean asthma-related healthcare costs during the outcome year than those prescribed FDC ICS/LABA ( n = 3036; mean difference, £124/year). ICS dose step-up had 56% probability of being less costly and marginally less effective (a trade-off), with ICER of £51,449 per additional patient controlled with FDC; and ICS dose step-up had 44% probability of being the preferred treatment strategy (less costly and more effective). In a second comparison, ICS step-up ( n = 3232) had 100% probability of being cheaper and more effective than adding LABA to ICS via separate inhalers ( n = 6464). Conclusion: For asthma step-up therapy, increasing ICS dose using extrafine-particle ICS is significantly less costly from the payer perspective and marginally (non-significantly) less effective than FDC ICS/LABA therapy containing standard fine-particle ICS. These findings apply primarily to the UK healthcare system but warrant consideration when developing guidelines in settings with strong economic constraints. Trial Registration: ClinicalTrials.gov identifier: NCT01697722. Funding: Teva Pharmaceuticals Limited, Petach Tikva, Israel. [ABSTRACT FROM AUTHOR]
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- 2016
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36. Effectiveness of initiating extrafine-particle versus fine-particle inhaled corticosteroids as asthma therapy in the Netherlands.
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van der Molen, Thys, Postma, Dirkje S., Martin, Richard J., Herings, Ron M. C., Overbeek, Jetty A., Thomas, Victoria, Miglio, Cristiana, Dekhuijzen, Richard, Roche, Nicolas, Guilbert, Theresa, Israel, Elliot, van Aalderen, Wim, Hillyer, Elizabeth V., van Rysewyk, Simon, and Price, David B.
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ASTHMA treatment ,ANTIASTHMATIC agents ,CORTICOSTEROIDS ,BECLOMETHASONE dipropionate ,LOGISTIC regression analysis ,THERAPEUTICS ,DRUG therapy for asthma ,BRONCHODILATOR agents ,COMPARATIVE studies ,DATABASES ,LONGITUDINAL method ,RESEARCH methodology ,MEDICAL cooperation ,PARTICLES ,RESEARCH ,STEROIDS ,EVALUATION research ,TREATMENT effectiveness ,INHALATION administration - Abstract
Background: Most randomised clinical trials typically exclude a significant proportion of asthma patients, including those at higher risk of adverse events, with comorbidities, obesity, poor inhaler technique and adherence, or smokers. However, these patients might differentially benefit from extrafine-particle inhaled corticosteroids (ICS). This matched cohort, database study, compared the effectiveness of extrafine-particle with fine-particle ICS in a real-life population initiating ICS therapy in the Netherlands.Methods: Data were from the Pharmo Database Network, comprising pharmacy and hospital discharge records, representative of 20 % of the Dutch population. The study population included patients aged 12 - 60, with a General Practice-recorded diagnosis for asthma (International Classification of Primary Care code R96), when available, ≥2 prescriptions for asthma therapy at any time in their recorded history, and receiving first prescription of ICS therapy as either extrafine-particle (ciclesonide or hydrofluoroalkane beclomethasone dipropionate [BDP]) or fine-particle ICS (fluticasone propionate or non-extrafine-particle-BDP). Patients were matched (1:1) on relevant demographic and clinical characteristics over 1-year baseline. Primary outcomes were severe exacerbation rates, risk domain asthma control and overall asthma control during the year following first ICS prescription. Secondary outcomes, treatment stability and being prescribed higher versus lower category of short-acting β2 agonists (SABA) dose, were compared over a 1-year outcome period using conditional logistic regression models.Results: Following matching, 1399 patients were selected in each treatment cohort (median age: 43 years; males: 34 %). Median (interquartile range) initial ICS doses (fluticasone-equivalents in μg) were 160 (160 - 320) for extrafine-particle versus 500 (250 - 500) for fine-particle ICS (p < 0.001). Following adjustment for residual confounders, matched patients prescribed extrafine-particle ICS had significantly lower rates of exacerbations (adjusted rate ratio [95 % CI], 0.59 [0.47-0.73]), and significantly higher odds of achieving asthma control and treatment stability in the year following initiation than those prescribed fine-particle ICS, and this occurred at lower prescribed doses. Patients prescribed extrafine-particle ICS had lower odds of being prescribed higher doses of SABA (0.50 [0.44-0.57]).Conclusion: In this historical, matched study, extrafine-particle ICS was associated with better odds of asthma control than fine-particle ICS in patients prescribed their first ICS therapy in the Netherlands. Of importance, this was reached at significantly lower prescribed dose. [ABSTRACT FROM AUTHOR]- Published
- 2016
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37. TGF-β-induced profibrotic signaling is regulated in part by the WNT receptor Frizzled-8.
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Spanjer, Anita I. R., Baarsma, Hoeke A., Oostenbrink, Lisette M., Jansen, Sepp R., Kuipers, Christine C., Lindner, Michael, Postma, Dirkje S., Meurs, Herman, Heijink, Irene H., Gosens, Reinoud, and Königshoff, Melanie
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TRANSFORMING growth factors ,CELLULAR signal transduction ,WNT genes ,LUNG injuries ,PULMONARY fibrosis ,LABORATORY mice - Abstract
TGF-β is important in lung injury and remodeling processes. TGF-β and Wingless/integrase-1 (WNT) signaling are interconnected; however, the WNT ligand-receptor complexes involved are unknown. Thus, we aimed to identify Frizzled (FZD) receptors that mediate TGF-β-induced profibrotic signaling. MRC-5 and primary human lung fibroblasts were stimulated with TGF-β
1 , WNT-5A, or WNT-5B in the presence and absence of specific pathway inhibitors. Specific small interfering RNA was used to knock down FZD8.In vivostudies using bleomycin-induced lung fibrosis were performed in wild-type and FZD8-deficient mice. TGF-β1 induced FZD8 specifically viaSmad3-dependent signaling in MRC-5 and primary human lung fibroblasts. It is noteworthy that FZD8 knockdown reduced TGF-β1 -induced collagen Iα1, fibronectin, versican, α-smooth muscle (sm)-actin, and connective tissue growth factor. Moreover, bleomycin-induced lung fibrosis was attenuated in FZD8-deficient mice in vivo. Although inhibition of canonical WNT signaling did not affect TGF-β1 -induced gene expression in vitro, noncanonical WNT-5B mimicked TGF-β1 -induced fibroblast activation. FZD8knockdown reduced both WNT-5B-induced gene expression of fibronectin and α-sm-actin, as well as WNT-5B-induced changes in cellular impedance. Collectively, our findings demonstrate a role for FZD8 in TGF-β-induced profibrotic signaling and imply that WNT-5B may be the ligand for FZD8 in these responses. [ABSTRACT FROM AUTHOR]- Published
- 2016
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38. Advanced glycation endproducts and their receptor in different body compartments in COPD.
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Hoonhorst, Susan J. M., Lo Tam Loi, Adéle T., Pouwels, Simon D., Faiz, Alen, Telenga, Eef D., van den Berge, Maarten, Koenderman, Leo, Lammers, Jan-Willem J., Boezen, H. Marike, van Oosterhout, Antoon J. M., Lodewijk, Monique E., Timens, Wim, Postma, Dirkje S., ten Hacken, Nick H. T., and Lo Tam Loi, Adèle T
- Subjects
ANTI-inflammatory agents ,GAS laws (Physical chemistry) ,COMBUSTION ,OBSTRUCTIVE lung diseases ,COLLOIDS - Abstract
Background: Chronic obstructive pulmonary disease (COPD) is a chronic lung disease characterized by chronic airway inflammation and emphysema, and is caused by exposure to noxious particles or gases, e.g. cigarette smoke. Smoking and oxidative stress lead to accelerated formation and accumulation of advanced glycation end products (AGEs), causing local tissue damage either directly or by binding the receptor for AGEs (RAGE). This study assessed the association of AGEs or RAGE in plasma, sputum, bronchial biopsies and skin with COPD and lung function, and their variance between these body compartments.Methods: Healthy smoking and never-smoking controls (n = 191) and COPD patients (n = 97, GOLD stage I-IV) were included. Autofluorescence (SAF) was measured in the skin, AGEs (pentosidine, CML and CEL) and sRAGE in blood and sputum by ELISA, and in bronchial biopsies by immunohistochemistry. eQTL analysis was performed in bronchial biopsies.Results: COPD patients showed higher SAF values and lower plasma sRAGE levels compared to controls and these values associated with decreased lung function (p <0.001; adjusting for relevant covariates). Lower plasma sRAGE levels significantly and independently predicted higher SAF values (p < 0.001). One SNP (rs2071278) was identified within a region of 50 kB flanking the AGER gene, which was associated with the gene and protein expression levels of AGER and another SNP (rs2071278) which was associated with the accumulation of AGEs in the skin.Conclusion: In COPD, AGEs accumulate differentially in body compartments, i.e. they accumulate in the skin, but not in plasma, sputum and bronchial biopsies. The association between lower sRAGE and higher SAF levels supports the hypothesis that the protective mechanism of sRAGE as a decoy-receptor is impaired in COPD. [ABSTRACT FROM AUTHOR]- Published
- 2016
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39. A pro-inflammatory role for the Frizzled-8 receptor in chronic bronchitis.
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Spanjer, Anita I. R., Menzen, Mark H., Dijkstra, Akkelies E., van den Berge, Maarten, Boezen, H. Marike, Nickle, David C., Sin, Don D., Bossé, Yohan, Brandsma, Corry-Anke, Timens, Wim, Postma, Dirkje S., Meurs, Herman, Heijink, Irene H., and Gosens, Reinoud
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CHRONIC bronchitis ,APTERYGOTA ,PHYSIOLOGICAL effects of tobacco ,SINGLE nucleotide polymorphisms ,LABORATORY mice ,ANIMAL experimentation ,BIOLOGICAL models ,CELL receptors ,CELLULAR signal transduction ,CYTOKINES ,EPITHELIAL cells ,FIBROBLASTS ,GENETIC polymorphisms ,GLYCOPROTEINS ,INFLAMMATION ,LUNGS ,OBSTRUCTIVE lung diseases ,MICE ,GENETIC markers ,IN vitro studies ,GENOTYPES - Abstract
Rationale: We have previously shown increased expression of the Frizzled-8 receptor of the Wingless/integrase-1 (WNT) signalling pathway in COPD. Here, we investigated if the Frizzled-8 receptor has a functional role in airway inflammation associated with chronic bronchitis.Methods: Acute cigarette-smoke-induced airway inflammation was studied in wild-type and Frizzled-8-deficient mice. Genetic association studies and lung expression quantitative trait loci (eQTL) analyses for Frizzled-8 were performed to evaluate polymorphisms in FZD8 and their relationship to tissue expression in chronic bronchitis. Primary human lung fibroblasts and primary human airway epithelial cells were used for in vitro studies.Results: Cigarette-smoke-exposure induced airway inflammation in wild-type mice, which was prevented in Frizzled-8-deficient mice, suggesting a crucial role for Frizzled-8 in airway inflammation. Furthermore, we found a significant genetic association (p=0.009) between single nucleotide polymorphism (SNP) rs663700 in the FZD8 region and chronic mucus hypersecretion, a characteristic of chronic bronchitis, in a large cohort of smoking individuals. We found SNP rs663700 to be a cis-eQTL regulating Frizzled-8 expression in lung tissue. Functional data link mesenchymal Frizzled-8 expression to inflammation as its expression in COPD-derived lung fibroblasts was regulated by pro-inflammatory cytokines in a genotype-dependent manner. Moreover, Frizzled-8 regulates inflammatory cytokine secretion from human lung fibroblasts, which in turn promoted MUC5AC expression by differentiated human airway epithelium.Conclusions: These findings indicate an important pro-inflammatory role for Frizzled-8 and suggest that its expression is related to chronic bronchitis. Furthermore, our findings indicate an unexpected role for fibroblasts in regulating airway inflammation in COPD. [ABSTRACT FROM AUTHOR]- Published
- 2016
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40. Association of Forced Vital Capacity with the Developmental Gene NCOR2.
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Minelli, Cosetta, Dean, Charlotte H., Hind, Matthew, Alves, Alexessander Couto, Amaral, André F. S., Siroux, Valerie, Huikari, Ville, Soler Artigas, María, Evans, David M., Loth, Daan W., Bossé, Yohan, Postma, Dirkje S., Sin, Don, Thompson, John, Demenais, Florence, Henderson, John, null, null, Bouzigon, Emmanuelle, Jarvis, Deborah, and Järvelin, Marjo-Riitta
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VITAL capacity (Respiration) ,DEVELOPMENTAL genetics ,EPIDEMIOLOGY ,MORTALITY ,LUNG development ,MORPHOGENESIS ,DEVELOPMENTAL biology ,COMPUTATIONAL biology - Abstract
Background: Forced Vital Capacity (FVC) is an important predictor of all-cause mortality in the absence of chronic respiratory conditions. Epidemiological evidence highlights the role of early life factors on adult FVC, pointing to environmental exposures and genes affecting lung development as risk factors for low FVC later in life. Although highly heritable, a small number of genes have been found associated with FVC, and we aimed at identifying further genetic variants by focusing on lung development genes. Methods: Per-allele effects of 24,728 SNPs in 403 genes involved in lung development were tested in 7,749 adults from three studies (NFBC1966, ECRHS, EGEA). The most significant SNP for the top 25 genes was followed-up in 46,103 adults (CHARGE and SpiroMeta consortia) and 5,062 children (ALSPAC). Associations were considered replicated if the replication p-value survived Bonferroni correction (p<0.002; 0.05/25), with a nominal p-value considered as suggestive evidence. For SNPs with evidence of replication, effects on the expression levels of nearby genes in lung tissue were tested in 1,111 lung samples (Lung eQTL consortium), with further functional investigation performed using public epigenomic profiling data (ENCODE). Results: NCOR2-rs12708369 showed strong replication in children (p = 0.0002), with replication unavailable in adults due to low imputation quality. This intronic variant is in a strong transcriptional enhancer element in lung fibroblasts, but its eQTL effects could not be tested due to low imputation quality in the eQTL dataset. SERPINE2-rs6754561 replicated at nominal level in both adults (p = 0.036) and children (p = 0.045), while WNT16-rs2707469 replicated at nominal level only in adults (p = 0.026). The eQTL analyses showed association of WNT16-rs2707469 with expression levels of the nearby gene CPED1. We found no statistically significant eQTL effects for SERPINE2-rs6754561. Conclusions: We have identified a new gene, NCOR2, in the retinoic acid signalling pathway pointing to a role of vitamin A metabolism in the regulation of FVC. Our findings also support SERPINE2, a COPD gene with weak previous evidence of association with FVC, and suggest WNT16 as a further promising candidate. [ABSTRACT FROM AUTHOR]
- Published
- 2016
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41. Early response to inhaled bronchodilators and corticosteroids as a predictor of 12-month treatment responder status and COPD exacerbations.
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Calverley, Peter M., Postma, Dirkje S., Anzueto, Antonio R., Make, Barry J., Eriksson, Göran, Peterson, Stefan, and Jenkins, Christine R.
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- 2016
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42. Sexual maturation protects against development of lung inflammation through estrogen.
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Draijer, Christina, Hylkema, Machteld N., Boorsma, Carian E., Klok, Pieter A., Robbe, X. Patricia, Timens, Wim, Postma, Dirkje S., Greene, Catherine M., and Melgert, Barbro N.
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LUNG diseases ,INFLAMMATION ,ASTHMA ,PHYSIOLOGICAL effects of estrogen ,SEXUAL dimorphism ,INTERLEUKIN-33 - Abstract
Increasing levels of estrogen and progesterone are suggested to play a role in the gender switch in asthma prevalence during puberty. We investigated whether the process of sexual maturation in mice affects the development of lung inflammation in adulthood and the contributing roles of estrogen and progesterone during this process. By inducing ovalbumin-induced lung inflammation in sexually mature and immature (ovariectomized before sexual maturation) adult mice, we showed that sexually immature adult mice developed more eosinophilic lung inflammation. This protective effect of "puberty" appears to be dependent on estrogen, as estrogen supplementation at the time of ovariectomy protected against development of lung inflammation in adulthood whereas progesterone supplementation did not. Investigating the underlying mechanism of estrogen-mediated protection, we found that estrogen-treated mice had higher expression of the anti-inflammatory mediator secretory leukoprotease inhibitor (SLPI) and lower expression of the proasthmatic cytokine IL-33 in parenchymal lung tissue and that their expressions colocalized with type II alveolar epithelial cells (AECII). Treating AECII directly with SLPI significantly inhibited IL-33 production upon stimulation with ATP. Our data suggest that estrogen during puberty has a protective effect on asthma development, which is accompanied by induction of anti-inflammatory SLPI production and inhibition of proinflammatory IL-33 production by AECII. [ABSTRACT FROM AUTHOR]
- Published
- 2016
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43. Prediction of Long-Term Benefits of Inhaled Steroids by Phenotypic Markers in Moderate-to-Severe COPD: A Randomized Controlled Trial.
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Snoeck-Stroband, Jiska B., Lapperre, Therese S., Sterk, Peter J., Hiemstra, Pieter S., Thiadens, Henk A., Boezen, H. Marike, ten Hacken, Nick H. T., Kerstjens, Huib A. M., Postma, Dirkje S., Timens, Wim, Sont, Jacob K., and null, null
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OBSTRUCTIVE lung diseases ,PHENOTYPES ,RANDOMIZED controlled trials ,BIOMARKERS ,STEROIDS ,PULMONARY function tests - Abstract
Background: The decline in lung function can be reduced by long-term inhaled corticosteroid (ICS) treatment in subsets of patients with chronic obstructive pulmonary disease (COPD). We aimed to identify which clinical, physiological and non-invasive inflammatory characteristics predict the benefits of ICS on lung function decline in COPD. Methods: Analysis was performed in 50 steroid-naive compliant patients with moderate to severe COPD (postbronchodilator forced expiratory volume in one second (FEV
1 ), 30–80% of predicted, compatible with GOLD stages II-III), age 45–75 years, >10 packyears smoking and without asthma. Patients were treated with fluticasone propionate (500 μg bid) or placebo for 2.5 years. Postbronchodilator FEV1 , dyspnea and health status were measured every 3 months; lung volumes, airway hyperresponsiveness (PC20 ), and induced sputum at 0, 6 and 30 months. A linear mixed effect model was used for analysis of this hypothesis generating study. Results: Significant predictors of attenuated FEV1 -decline by fluticasone treatment compared to placebo were: fewer packyears smoking, preserved diffusion capacity, limited hyperinflation and lower inflammatory cell counts in induced sputum (p<0.04). Conclusions: Long-term benefits of ICS on lung function decline in patients with moderate-to-severe COPD are most pronounced in patients with fewer packyears, and less severe emphysema and inflammation. These data generate novel hypotheses on phenotype-driven therapy in COPD. Trial Registration: ClinicalTrials.gov [ABSTRACT FROM AUTHOR]- Published
- 2015
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44. Impact of Statins on Gene Expression in Human Lung Tissues.
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Lane, Jérôme, van Eeden, Stephan F., Obeidat, Ma’en, Sin, Don D., Tebbutt, Scott J., Timens, Wim, Postma, Dirkje S., Laviolette, Michel, Paré, Peter D., and Bossé, Yohan
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STATINS (Cardiovascular agents) ,GENE expression ,LUNG anatomy ,REDUCTASE inhibitors ,CHOLESTEROL ,HEALTH outcome assessment - Abstract
Statins are 3-hydroxy-3-methylglutaryl-coenzyme A reductase inhibitors that alter the synthesis of cholesterol. Some studies have shown a significant association of statins with improved respiratory health outcomes of patients with asthma, chronic obstructive pulmonary disease and lung cancer. Here we hypothesize that statins impact gene expression in human lungs and may reveal the pleiotropic effects of statins that are taking place directly in lung tissues. Human lung tissues were obtained from patients who underwent lung resection or transplantation. Gene expression was measured on a custom Affymetrix array in a discovery cohort (n = 408) and two replication sets (n = 341 and 282). Gene expression was evaluated by linear regression between statin users and non-users, adjusting for age, gender, smoking status, and other covariables. The results of each cohort were combined in a meta-analysis and biological pathways were studied using Gene Set Enrichment Analysis. The discovery set included 141 statin users. The lung mRNA expression levels of eighteen and three genes were up-regulated and down-regulated in statin users (FDR < 0.05), respectively. Twelve of the up-regulated genes were replicated in the first replication set, but none in the second (p-value < 0.05). Combining the discovery and replication sets into a meta-analysis improved the significance of the 12 up-regulated genes, which includes genes encoding enzymes and membrane proteins involved in cholesterol biosynthesis. Canonical biological pathways altered by statins in the lung include cholesterol, steroid, and terpenoid backbone biosynthesis. No genes encoding inflammatory, proteases, pro-fibrotic or growth factors were altered by statins, suggesting that the direct effect of statin in the lung do not go beyond its antilipidemic action. Although more studies are needed with specific lung cell types and different classes and doses of statins, the improved health outcomes and survival observed in statin users with chronic lung diseases do not seem to be mediated through direct regulation of gene expression in the lung. [ABSTRACT FROM AUTHOR]
- Published
- 2015
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45. Old dilemma: asthma with irreversible airway obstruction or COPD.
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Fattahi, Fatemeh, Vonk, Judith, Bulkmans, Nicole, Fleischeuer, Ruth, Gouw, Annette, Grünberg, Katrien, Mauad, Thais, Popper, Helmut, Felipe-Silva, Aloisio, Vrugt, Bart, Wright, Joanne, Yang, Hui-Min, Kocks, Janwillem, Hylkema, Machteld, Postma, Dirkje, Timens, Wim, Hacken, Nick, Vonk, Judith M, Grünberg, Katrien, and Wright, Joanne L
- Abstract
Older asthmatic patients may develop fixed airway obstruction and clinical signs of chronic obstructive pulmonary disease (COPD). We investigated the added value of pathological evaluation of bronchial biopsies to help differentiate asthma from COPD, taking into account smoking, age, and inhaled corticosteroid (ICS) use. Asthma and COPD patients (24 of each category) were matched for ICS use, age, FEV(1), and smoking habits. Five pulmonary and five general pathologists examined bronchial biopsies using an interactive website, without knowing patient information. They were asked to diagnose asthma or COPD on biopsy findings in both a pairwise and randomly mixed order of cases during four different phases, with intervals of 4-6 weeks, covering a maximal period of 36 weeks. Clinically concordant diagnoses of asthma or COPD varied between 63 %-73 %, without important differences between pairwise vs randomly mixed examination or between general vs pulmonary pathologists. The highest percentage of concordant diagnoses was in young asthmatic patients without ICS use and in COPD patients with ICS use. In non ICS users with fixed airway obstruction, a COPD diagnosis was favored if abnormal presence of glands, squamous metaplasia, and submucosal infiltrate was present and an asthma diagnosis in case of abnormal presence of goblet cells. In ICS users with fixed airway obstruction, abnormal presence of submucosal infiltrates, basement membrane thickening, eosinophils, and glands was associated with asthma. Histological characteristics in bronchial biopsies are reproducibly recognized by pathologists, yet the differentiation by histopathology between asthma and COPD is difficult without information about ICS use. [ABSTRACT FROM AUTHOR]
- Published
- 2015
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46. Polymorphisms associated with expression of BPIFA1/BPIFB1 and lung disease severity in cystic fibrosis.
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Saferali, Aabida, Obeidat, Ma'en, Bérubé, Jean-Christophe, Lamontagne, Maxime, Bossé, Yohan, Laviolette, Michel, Ke Hao, Nickle, David C., Timens, Wim, Sin, Don D., Postma, Dirkje S., Strug, Lisa J., Gallins, Paul J., Paré, Peter D., Bingle, Colin D., and Sandford, Andrew J.
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- 2015
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47. Polymorphisms Associated with Expression of BPIFA1/BPIFB1 and Lung Disease Severity in Cystic Fibrosis.
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Saferali, Aabida, Obeidat, Ma'en, Bérubé, Jean-Christophe, Lamontagne, Maxime, Bossé, Yohan, Laviolette, Michel, Ke Hao, Nickle, David C., Timens, Wim, Sin, Don D., Postma, Dirkje S., Strug, Lisa J., Gallins, Paul J., Paré, Peter D., Bingle, Colin D., and Sandford, Andrew J.
- Published
- 2015
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48. A score to predict short-term risk of COPD exacerbations (SCOPEX).
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Make, Barry J., Eriksson, Göran, Calverley, Peter M., Jenkins, Christine R., Postma, Dirkje S., Peterson, Stefan, Östlund, Ollie, and Anzueto, Antonio
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- 2015
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49. Nocturnal dry cough in the first 7 years of life is associated with asthma at school age.
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Boudewijn, Ilse M., Savenije, Olga E.M., Koppelman, Gerard H., Wijga, Alet H., Smit, Henriëtte A., de Jongste, Johan C., Gehring, Ulrike, Postma, Dirkje S., and Kerkhof, Marjan
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- 2015
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50. Low levels of vitamin D are associated with multimorbidity: Results from the LifeLines Cohort Study.
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Meems, Laura M. G., de Borst, Martin H., Postma, Dirkje S., Vonk, Judith M., Kremer, Hubertus P. H., Schuttelaar, Marie-Louise A., Rosmalen, Judith G. M., Weersma, Rinse K., Wolffenbuttel, Bruce H. R., Scholtens, Salome, Stolk, Ronald P., Kema, Ido P., Navis, Gerjan, Khan, Mohsin A. F., van der Harst, Pim, and de Boer, Rudolf A.
- Abstract
Background. The prevalence of multimorbidity (≥ 1 disease within an individual) is rapidly increasing. So far, studies on the relationship between vitamin D and morbidity are mainly focusing on effects on single disease domains only, while vitamin D biology is associated with several diseases throughout the human body. Methods. We studied 8,726 participants from the LifeLines Cohort Study (a cross-sectional, population-based cohort study) and used the self-developed composite morbidity score to study the association between vitamin D levels and multimorbidity. Results. Study participants (mean age 45 ± 13 years, 73% females) had a mean plasma vitamin D level of 59 ± 22 nmol/L. In participants aged between 50 and 60 years, 58% had ≥ 2 affected disease domains, while morbidity score increased with age (70–80 years: 82% morbidity score > 1; > 80 years: 89% morbidity score > 1). Each incremental reduction by 1 standard deviation (SD) of vitamin D level was associated with an 8% higher morbidity score (full model OR 0.92, 95% CI 0.88–0.97, P = 0.001). Participants with vitamin D levels < 25 nmol/L were at highest risk for increasing morbidity prevalence (versus > 80 nmol/L, OR 1.34, 95% CI 1.07–1.67, P = 0.01). Conclusions. Low levels of vitamin D are associated with higher prevalence of multimorbidity, especially in participants with vitamin D levels < 25 nmol/L. Collectively, our results favor a general, rather than an organ-specific, approach when assessing the impact of vitamin D deficiency. [ABSTRACT FROM AUTHOR]
- Published
- 2015
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