40 results on '"Postma, Dirkje"'
Search Results
2. Adenosine receptors in COPD and asymptomatic smokers: effects of smoking cessation
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Versluis, Mieke, ten Hacken, Nick, Postma, Dirkje, Barroso, Begona, Rutgers, Bea, Geerlings, Marie, Willemse, Brigitte, Timens, Wim, and Hylkema, Machteld
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- 2009
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3. Genetic landscape of chronic obstructive pulmonary disease identifies heterogeneous cell-type and phenotype associations
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Sakornsakolpat, Phuwanat, Prokopenko, Dmitry, Lamontagne, Maxime, Reeve, Nicola F., Guyatt, Anna L., Jackson, Victoria E., Shrine, Nick, Qiao, Dandi, Bartz, Traci M., Kim, Deog Kyeom, Lee, Mi Kyeong, Latourelle, Jeanne C., Li, Xingnan, Morrow, Jarrett D., Obeidat, Ma’en, Wyss, Annah B., Bakke, Per, Barr, R. Graham, Beaty, Terri H., Belinsky, Steven A., Brusselle, Guy G., Crapo, James D., de Jong, Kim, DeMeo, Dawn L., Fingerlin, Tasha E., Gharib, Sina A., Gulsvik, Amund, Hall, Ian P., Hokanson, John E., Kim, Woo Jin, Lomas, David A., London, Stephanie J., Meyers, Deborah A., O’Connor, George T., Rennard, Stephen I., Schwartz, David A., Sliwinski, Pawel, Sparrow, David, Strachan, David P., Tal-Singer, Ruth, Tesfaigzi, Yohannes, Vestbo, Jørgen, Vonk, Judith M., Yim, Jae-Joon, Zhou, Xiaobo, Bossé, Yohan, Manichaikul, Ani, Lahousse, Lies, Silverman, Edwin K., Boezen, H. Marike, Wain, Louise V., Tobin, Martin D., Hobbs, Brian D., Cho, Michael H., Batini, Chiara, Zhao, Jing Hua, Wielscher, Matthias, Weiss, Stefan, Kentistou, Katherine A., Cook, James P., Hui, Jennie, Karrasch, Stefan, Imboden, Medea, Harris, Sarah E., Marten, Jonathan, Enroth, Stefan, Kerr, Shona M., Surakka, Ida, Vitart, Veronique, Lehtimäki, Terho, Ewert, Ralf, Gieger, Christian, Homuth, Georg, Joshi, Peter K., Langenberg, Claudia, Lind, Lars, Luan, Jian’an, Mahajan, Anubha, Murray, Alison, Porteous, David J., Rawal, Rajesh, Smith, Blair H., Timmers, Paul R. H. J., Raitakari, Olli T., Kähönen, Mika, Polasek, Ozren, Gyllensten, Ulf, Rudan, Igor, Deary, Ian J., Probst-Hensch, Nicole M., Schulz, Holger, James, Alan L., Wilson, James F., Stubbe, Beate, Zeggini, Eleftheria, Jarvelin, Marjo-Riitta, Wareham, Nick, Hayward, Caroline, Morris, Andrew P., Agusti, Alvar, Anderson, Wayne, Bakerly, Nawar, Bals, Robert, Barnes, Kathleen C., Bleecker, Eugene R., Bowler, Russell, Brightling, Christopher, de Bruijne, Marleen, Castaldi, Peter J., Celli, Bartolome, Coxson, Harvey O., Crystal, Ron, de Jong, Pim, Dirksen, Asger, Dy, Jennifer, Foreman, Marilyn, Garcia-Aymerich, Judith, Gevenois, Pierre, Ghosh, Soumitra, Gietema, Hester, Hansel, Nadia, Hersh, Craig P., Hoffman, Eric, Kalsheker, Noor, Kauczor, Hans-Ulrich, Laitinen, Tarja, Lambrechts, Diether, Lee, Sang-Do, Litonjua, Augusto A., Loth, Daan W., Lutz, Sharon M., Lynch, David, MacNee, William, McDonald, Merry-Lynn, Newell, John D., Nordestgaard, Borge G., Oh, Yeon-Mok, Paré, Peter D., Pistolesi, Massimo, Postma, Dirkje S., Puhan, Milo, Regan, Elizabeth, Rich, Stephen S., Seo, Joon Beom, Short, Andrea, Stoel, Berend, Sverzellati, Nicola, ter Riet, Gerben, Van Beek, Edwin J. R., van Ginneken, Bram, Vogelmeier, Claus F., Wanner, Adam, Washko, George, Wauters, Els, Wouters, Emiel F. M., Young, Robert P., Zeigler-Heitbrock, Loems, SpiroMeta Consortium, Understanding Society Scientific Group, International COPD Genetics Consortium, Institute for Molecular Medicine Finland, Groningen Research Institute for Asthma and COPD (GRIAC), Life Course Epidemiology (LCE), Beeldvorming, MUMC+: DA BV Medisch Specialisten Radiologie (9), MUMC+: MA Longziekten (3), RS: NUTRIM - R3 - Respiratory & Age-related Health, Pulmonologie, General practice, APH - Aging & Later Life, APH - Personalized Medicine, ACS - Diabetes & metabolism, Epidemiology, Pulmonary Medicine, Medical Informatics, and Radiology & Nuclear Medicine
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Male ,Lydia Becker Institute ,Pulmonary Fibrosis ,LD SCORE REGRESSION ,Gene Expression ,Genome-wide association study ,Pulmonary Disease, Chronic Obstructive ,0302 clinical medicine ,Pulmonary fibrosis ,GWAS ,Lung ,GENOME-WIDE ASSOCIATION ,ACIDIC-MAMMALIAN-CHITINASE ,LUNG-FUNCTION ,EXTRACELLULAR-MATRIX ,PREDOMINANT EMPHYSEMA ,CONNECTIVITY MAP ,ATOPIC ASTHMA ,RISK LOCI ,0303 health sciences ,COPD ,education.field_of_study ,Smoking ,1184 Genetics, developmental biology, physiology ,Middle Aged ,3. Good health ,Phenotype ,medicine.anatomical_structure ,Medical genetics ,Female ,Rare cancers Radboud Institute for Health Sciences [Radboudumc 9] ,Adult ,medicine.medical_specialty ,Population ,Biology ,Polymorphism, Single Nucleotide ,Article ,03 medical and health sciences ,All institutes and research themes of the Radboud University Medical Center ,ResearchInstitutes_Networks_Beacons/lydia_becker_institute_of_immunology_and_inflammation ,Genetics ,medicine ,Genetic predisposition ,Humans ,Genetic Predisposition to Disease ,education ,Aged ,030304 developmental biology ,Asthma ,medicine.disease ,respiratory tract diseases ,Genetic Loci ,Case-Control Studies ,Immunology ,3111 Biomedicine ,030217 neurology & neurosurgery ,Genome-Wide Association Study - Abstract
Chronic obstructive pulmonary disease (COPD) is the leading cause of respiratory mortality worldwide. Genetic risk loci provide novel insights into disease pathogenesis. We performed a genome-wide association study in 35,735 cases and 222,076 controls from the UK Biobank and additional studies from the International COPD Genetics Consortium. We identified 82 loci with P-value < 5 × 10−8; 47 were previously described in association with either COPD or population-based lung function. Of the remaining 35 novel loci, 13 were associated with lung function in 79,055 individuals from the SpiroMeta consortium. Using gene expression and regulation data, we identified enrichment for loci in lung tissue, smooth muscle and several lung cell types. We found 14 COPD loci shared with either asthma or pulmonary fibrosis. COPD genetic risk loci clustered into groups of quantitative imaging features and comorbidity associations. Our analyses provide further support to the genetic susceptibility and heterogeneity of COPD., Editorial summary Genome-wide analysis of chronic obstructive pulmonary disease identifies 82 loci, 35 of which are new. Integration of gene expression and genomic annotation data shows enrichment of signals in lung tissue, smooth muscle and several lung cell types.
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- 2019
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4. Air pollution exposure is associated with restrictive ventilatory patterns
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de Jong, Kim, Vonk, Judith M, Zijlema, Wilma L, Stolk, Ronald P, van der Plaat, Diana A, Hoek, Gerard, Brunekreef, Bert, Postma, Dirkje S, Boezen, H Marike, dIRAS RA-2, Risk Assessment, Groningen Research Institute for Asthma and COPD (GRIAC), Life Course Epidemiology (LCE), and Lifestyle Medicine (LM)
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Pulmonary and Respiratory Medicine ,Adult ,Male ,medicine.medical_specialty ,Adolescent ,Air pollution exposure ,Nitrogen Dioxide ,Vital Capacity ,CHILDREN ,ESCAPE ,Cohort Studies ,03 medical and health sciences ,Young Adult ,0302 clinical medicine ,Environmental health ,Air Pollution ,Forced Expiratory Volume ,medicine ,Humans ,COPD ,030212 general & internal medicine ,Intensive care medicine ,Lung function ,Aged ,Netherlands ,Aged, 80 and over ,Ambient air pollution ,business.industry ,Environmental Exposure ,Middle Aged ,respiratory system ,medicine.disease ,Asthma ,respiratory tract diseases ,LUNG-FUNCTION ,030228 respiratory system ,Linear Models ,Female ,Particulate Matter ,Tobacco Smoke Pollution ,business ,circulatory and respiratory physiology - Abstract
Exposure to ambient air pollution is associated with a substantial burden of morbidity and mortality worldwide [1]. In a recent paper, Adam et al. [2] showed significantly impaired levels of forced expiratory volume in 1 s (FEV1) and forced vital capacity (FVC) associated with exposure to the ambient air pollutants nitrogen dioxide (NO2) and particles with a 50% cut-off aerodynamic diameter of 10 μm (PM10) in 7613 adults included in the European Study of Cohorts for Air Pollution Effects (ESCAPE). Effect estimates for FVC were of similar magnitude (for NO2) or larger (for PM10) than those for FEV1. In line with these findings, Forbes et al. [3] showed negative associations of PM10 and NO2 with the level of FEV1 in 40 329 adults included in the Health Survey for England between 1995 and 2001, whereas no significant associations with FEV1/FVC were observed. In 1997, the Swiss Study on Air Pollution and Lung Disease in Adults (SAPALDIA), including 9651 adults, showed negative associations of ambient air pollutants NO2 and PM10 with both FEV1 and FVC [4]. The effect estimates for FVC were stronger than for FEV1 for various pollutants, and this was consistently the case in most subgroups (according to smoking status and respiratory symptoms). Reduced FVC, with FEV1 being normal or reduced to a lesser degree than FVC, suggests restrictive rather than obstructive lung disease (in which FEV1 specifically is reduced, resulting in a low FEV1/FVC ratio). Thus, findings from several European studies suggest that restrictive rather than obstructive ventilatory patterns associate with long-term low levels of exposure to ambient air pollution. A study with slightly different findings is the German Study on the influence of Air Pollution on Lung Function, Inflammation and Ageing (SALIA), including 2593 women. This study also found negative associations of NO2 and PM10 exposure with both FEV1 and FVC, yet the effects estimates for FEV1 were stronger than for FVC, and consequently there were small significant negative associations with the FEV1/FVC ratio [5]. A review article concluded that despite biological plausible mechanisms, there is suggestive, but not conclusive evidence that chronic exposure to air pollution is associated with the prevalence and incidence of chronic obstructive pulmonary disease (COPD), a disease characterised by airway obstruction [6]. Thus far, no studies have focused explicitly on whether air pollution exposure is associated with obstructive or restrictive ventilatory patterns.
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- 2016
5. Prediction and course of symptoms and lung function around an exacerbation in chronic obstructive pulmonary disease
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van den Berge Maarten, Hop Wim CJ, van der Molen Thys, van Noord Jan A, Creemers Jacques PHM, Schreurs Ad JM, Wouters Emiel FM, and Postma Dirkje S
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COPD ,Exacerbations ,CCQ ,Symptoms ,Diseases of the respiratory system ,RC705-779 - Abstract
Abstract Background Frequent exacerbations induce a high burden to Chronic Obstructive Pulmonary Disease (COPD). We investigated the course of exacerbations in the published COSMIC study that investigated the effects of 1-year withdrawal of fluticasone after a 3-month run-in treatment period with salmeterol/fluticasone in patients with COPD. Methods In 373 patients, we evaluated diary cards for symptoms, Peak Expiratory Flow (PEF), and salbutamol use and assessed their course during exacerbations. Results There were 492 exacerbations in 224 patients. The level of symptoms of cough, sputum, dyspnea and nocturnal awakening steadily increased from 2 weeks prior to exacerbation, with a sharp rise during the last week. Symptoms of cough, sputum, and dyspnea reverted to baseline values at different rates (after 4, 4, and 7 weeks respectively), whereas symptoms of nocturnal awakening were still increased after eight weeks. The course of symptoms was similar around a first and second exacerbation. Increases in symptoms and salbutamol use and decreases in PEF were associated with a higher risk to develop an exacerbation, but with moderate predictive values, the areas under the receiver operating curves ranging from 0.63 to 0.70. Conclusions Exacerbations of COPD are associated with increased symptoms that persist for weeks and the course is very similar between a first and second exacerbation. COPD exacerbations are preceded by increased symptoms and salbutamol use and lower PEF, yet predictive values are too low to warrant daily use in clinical practice.
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- 2012
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6. Systemic Inflammation in Patients with Chronic Obstructive Pulmonary Disease: Results from the Cosmic Study
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Wouters Emiel F. M., Spruit Martijn A., Hop Wim C. J., Breyer Marie-Kathrin, Rutten Eric P. A., and Postma Dirkje S.
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medicine.medical_specialty ,Pathology ,COPD ,business.industry ,Adipokine ,Fibrinogen ,Systemic inflammation ,medicine.disease ,Gastroenterology ,Obesity ,Internal medicine ,Medicine ,Tumor necrosis factor alpha ,Mass index ,medicine.symptom ,business ,Body mass index ,medicine.drug - Abstract
Objective: The study aims to elucidate the association of host-related factors on systemic inflammation in COPD patients. Methods: In 295 clinically stable and optimally treated COPD patients from 39 outpatient centers, age, gender, and body composition (body mass index, BMI; fat-free mass index, FFMI; fat mass index, FMI) were related to inflammatory biomarkers: CRP, fibrinogen, TNFα, and its soluble receptors (s)TNFαR1 and sTNFαR2. Furthermore, forced expiratory volume in the first second (FEV1), BMI, FFMI, and FMI were stratified by quartiles to elucidate the influence on inflammatory biomarkers. Monovariate and multivariate regression analyses were performed for associations between inflammatory biomarkers. Results: Positive correlations were found for FFMI with sTNFαR1, FMI with CRP and age with TNFα, sTNFαR1 and sTNFαR2 (p < 0.01). FEV1 was not correlated with body composition and inflammatory markers. Mono- and multivariate analysis showed weak correlations between the acute phase markers and the TNFα system after correcting for multiple co-variants. Conclusions: This study highlights the modest role of age and body composition on levels of systemic inflammatory biomarkers in COPD. Results show the degree of airflow limitation does not affect systemic inflammation. Last, a weak relationship between acute phase markers and markers of the TNFα system is present in COPD.
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- 2012
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7. Genome-wide interaction study of gene-by-occupational exposure and effects on FEV1 levels
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de Jong, Kim, Vonk, Judith M, Timens, Wim, Bossé, Yohan, Sin, Don D, Hao, Ke, Kromhout, Hans, Vermeulen, Roel, Postma, Dirkje S, Boezen, H Marike, Risk Assessment, Infection & Immunity, dIRAS RA-2, dIRAS RA-I&I RA, LS IRAS EEPI EXAS (Arb.hyg+bl.st.kar.), LS IRAS EEPI GRA (Gezh.risico-analyse), Groningen Research Institute for Asthma and COPD (GRIAC), Guided Treatment in Optimal Selected Cancer Patients (GUTS), Life Course Epidemiology (LCE), Risk Assessment, Infection & Immunity, dIRAS RA-2, dIRAS RA-I&I RA, LS IRAS EEPI EXAS (Arb.hyg+bl.st.kar.), and LS IRAS EEPI GRA (Gezh.risico-analyse)
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Male ,Genome-wide association study ,Bioinformatics ,Cohort Studies ,Forced Expiratory Volume ,Immunology and Allergy ,Lung ,POPULATION ,Netherlands ,Aged, 80 and over ,COPD ,education.field_of_study ,Dust ,ASSOCIATION ,Middle Aged ,Cohort ,Female ,Gases ,Adult ,Adolescent ,Genotype ,LIFELINES ,Immunology ,Population ,Quantitative Trait Loci ,Single-nucleotide polymorphism ,Air Pollutants, Occupational ,occupational exposures ,Quantitative trait locus ,Biology ,Polymorphism, Single Nucleotide ,OBSTRUCTIVE PULMONARY-DISEASE ,DENDRITIC CELLS ,NUCLEOTIDE PHOSPHODIESTERASE PDE4D ,Young Adult ,Occupational Exposure ,LUNG-FUNCTION DECLINE ,medicine ,Genetics ,Humans ,Genetic Predisposition to Disease ,RNA, Messenger ,METAANALYSES ,education ,Genetic association ,Aged ,Gene Expression Profiling ,lung function ,interactions ,medicine.disease ,respiratory tract diseases ,Expression quantitative trait loci ,gene expression ,ASTHMA ,Genome-Wide Association Study - Abstract
Background: Chronic obstructive pulmonary disease (COPD) is a complex disease characterized by impaired lung function and airway obstruction resulting from interactions between multiple genes and multiple environmental exposures. Thus far, genome-wide association studies have largely disregarded environmental factors that might trigger the development of lung function impairment and COPD, such as occupational exposures, which are thought to contribute to 15% to 20% of the COPD prevalence.Objectives: We performed a genome-wide interaction study to identify novel susceptibility loci for occupational exposure to biological dust, mineral dust, and gases and fumes in relation to FEV1 levels.Methods: We performed an identification analysis in 12,400 subjects from the LifeLines cohort study and verified our findings in 1436 subjects from a second independent cohort, the Vlagtwedde-Vlaardingen cohort. Additionally, we assessed whether replicated single nucleotide polymorphisms (SNPs) were cis-acting expression (mRNA) quantitative trait loci in lung tissue.Results: Of the 7 replicated SNPs that interacted with one of the occupational exposures, several identified loci were plausible candidates that might be involved in biological pathways leading to lung function impairment, such as PCDH9 and GALNT13. Two of the 7 replicated SNPs were cis-acting expression quantitative trait loci associated with gene expression of PDE4D and TMEM176A in lung tissue.Conclusion: This genome-wide interaction study on occupational exposures in relation to the level of lung function identified several novel genes. Further research should determine whether the identified genes are true susceptibility loci for occupational exposures and whether these SNP-by-exposure interactions consequently contribute to the development of COPD.
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- 2015
8. Dissecting the genetics of chronic mucus hypersecretion in smokers with and without COPD
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Dijkstra, Akkelies E., Boezen, H. Marike, Van Den Berge, Maarten, Vonk, Judith M., Hiemstra, Pieter S., Barr, R. Graham, Burkart, Kirsten M., Manichaikul, Ani, Pottinger, Tess D., Silverman, Edward K., Cho, Michael H., Crapo, James D., Beaty, Terri H., Bakke, Per, Gulsvik, Amund, Lomas, David A., Bossé, Yohan, Nickle, David C., Paré, Peter D., De Koning, Harry J., Lammers, Jan Willem, Zanen, Pieter, Smolonska, Joanna, Wijmenga, Ciska, Brandsma, Corry Anke, Groen, Harry J M, Postma, Dirkje S., Alizadeh, B. Z., De Boer, R. A., Boezen, H. M., Bruinenberg, M., Franke, L., Van Der Harst, P., Hillege, H. L., Van Der Klauw, M. M., Navis, G., Ormel, J., Postma, D. S., Rosmalen, J. G M, Slaets, J. P., Snieder, H., Stolk, R. P., Wolffenbuttel, B. H R, Wijmenga, C., Life Course Epidemiology (LCE), Groningen Research Institute for Asthma and COPD (GRIAC), Groningen Institute for Gastro Intestinal Genetics and Immunology (3GI), Damage and Repair in Cancer Development and Cancer Treatment (DARE), Guided Treatment in Optimal Selected Cancer Patients (GUTS), and Public Health
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Pulmonary and Respiratory Medicine ,Pathology ,medicine.medical_specialty ,Chronic bronchitis ,Population ,Single-nucleotide polymorphism ,Genome-wide association study ,Gastroenterology ,OBSTRUCTIVE PULMONARY-DISEASE ,DESIGN ,Internal medicine ,Genetic model ,Medicine ,EPIDEMIOLOGY ,Respiratory system ,education ,POPULATION ,education.field_of_study ,COPD ,Lung ,business.industry ,ASSOCIATION ,respiratory system ,medicine.disease ,respiratory tract diseases ,medicine.anatomical_structure ,CHRONIC-BRONCHITIS ,RISK-FACTORS ,ECLIPSE ,SMOKING ,business - Abstract
Smoking is a notorious risk factor for chronic mucus hypersecretion (CMH). CMH frequently occurs in chronic obstructive pulmonary disease (COPD). The question arises whether the same single-nucleotide polymorphisms (SNPs) are related to CMH in smokers with and without COPD.We performed two genome-wide association studies of CMH under an additive genetic model in male heavy smokers (≥20 pack-years) with COPD (n=849, 39.9% CMH) and without COPD (n=1348, 25.4% CMH), followed by replication and meta-analysis in comparable populations, and assessment of the functional relevance of significantly associated SNPs.Genome-wide association analysis of CMH in COPD and non-COPD subjects yielded no genome-wide significance after replication. In COPD, our top SNP (rs10461985, p=5.43×10−5) was located in the GDNF-AS1 gene that is functionally associated with the GDNF gene. Expression of GDNF in bronchial biopsies of COPD patients was significantly associated with CMH (p=0.007). In non-COPD subjects, four SNPs had a p-value −5 in the meta-analysis, including a SNP (rs4863687) in the MAML3 gene, the T-allele showing modest association with CMH (p=7.57×10−6, OR 1.48) and with significantly increased MAML3 expression in lung tissue (p=2.59×10−12).Our data suggest the potential for differential genetic backgrounds of CMH in individuals with and without COPD.
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- 2015
9. Asthma and Chronic Obstructive Pulmonary Disease: Similarities and Differences
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Postma, Dirkje S., Reddel, Helen K., ten Hacken, Nicolaas, van den Berge, Maarten, Groningen Research Institute for Asthma and COPD (GRIAC), and Lifestyle Medicine (LM)
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Inflammation ,Overlap phenotype ,RANDOMIZED CONTROLLED-TRIALS ,AIR-FLOW LIMITATION ,INHALED CORTICOSTEROIDS ,Asthma ,Remodeling ,respiratory tract diseases ,RESPIRATORY SYMPTOMS ,immune system diseases ,MUCUS HYPERSECRETION ,LUNG-FUNCTION DECLINE ,VENTILATION HETEROGENEITY ,COPD ,SPUTUM-EOSINOPHILIA ,BRONCHODILATOR RESPONSIVENESS ,SMALL-AIRWAYS - Abstract
Asthma and CORD are both heterogeneous lung diseases including many different phenotypes. The classical asthma and CORD phenotypes are easy to discern because they reflect extremes of a phenotypical spectrum. Thus asthma in childhood and CORD in smokers have their own phenotypic expression with underlying pathophysiological mechanisms that differ importantly. In older adults, asthma and CORD are more difficult to differentiate and there exists a bronchodilator response in most but not all patients with asthma and persistent airway obstruction in most but not all patients with CORD where even up to 50% have been reported to have some bronchodilator response as assessed with FEVi. Airway obstruction is generated in the large and small airways both in asthma and CORD, and this small airway obstruction is located more proximally in asthma, yet is found more distally in severe and older individuals with asthma, comparable to CORD. Though the underlying inflammation and remodelling processes in asthma and COPD are different in their extreme phenotypes, there are overlap phenotypes with eosinophilic inflammation even in stable COPD and neutrophilic inflammation in longstanding and severe asthma.
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- 2014
10. Glycogen synthase kinase-3 (GSK-3) regulates TGF-1-induced differentiation of pulmonary fibroblasts
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Baarsma, Hoeke A., Engelbertink, Lilian H. J. M., van Hees, Lonneke J., Menzen, Mark H., Meurs, Herman, Timens, Wim, Postma, Dirkje S., Kerstjens, Huib A. M., Gosens, Reinoud, Molecular Pharmacology, Groningen Research Institute of Pharmacy, Groningen Research Institute for Asthma and COPD (GRIAC), and Guided Treatment in Optimal Selected Cancer Patients (GUTS)
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GROWTH-FACTOR-BETA ,NF-KAPPA-B ,TGF-BETA ,macromolecular substances ,PROTEIN-KINASE ,DISEASE ,sm-actin ,fibronectin ,AIRWAY SMOOTH-MUSCLE ,LUNG FIBROBLASTS ,CELLS ,EXTRACELLULAR-MATRIX ,COPD ,SB216763 ,cAMP response element-binding protein (CREB) ,GENE-EXPRESSION - Abstract
Background Chronic lung diseases such as asthma, COPD and pulmonary fibrosis are characterized by abnormal extracellular matrix (ECM) turnover. TGF- is a key mediator stimulating ECM production by recruiting and activating lung fibroblasts and initiating their differentiation process into more active myofibroblasts. Glycogen synthase kinase-3 (GSK-3) regulates various intracellular signalling pathways; its role in TGF-1-induced myofibroblast differentiation is currently largely unknown. Purpose To determine the contribution of GSK-3 signalling in TGF-1-induced myofibroblast differentiation. Experimental Approach We used MRC5 human lung fibroblasts and primary pulmonary fibroblasts of individuals with and without COPD. Protein and mRNA expression were determined by immunoblotting and RT-PCR analysis respectively. Results Stimulation of MRC5 and primary human lung fibroblasts with TGF-1 resulted in time- and dose-dependent increases of -sm-actin and fibronectin expression, indicative of myofibroblast differentiation. Pharmacological inhibition of GSK-3 by SB216763 dose-dependently attenuated TGF-1-induced expression of these myofibroblasts markers. Moreover, silencing of GSK-3 by siRNA or pharmacological inhibition by CT/CHIR99021 fully inhibited the TGF-1-induced expression of -sm-actin and fibronectin. The effect of GSK-3 inhibition on -sm-actin expression was similar in fibroblasts from individuals with and without COPD. Neither smad, NF-B nor ERK1/2 were involved in the inhibitory actions of GSK-3 inhibition by SB126763 on myofibroblast differentiation. Rather, SB216763 increased the phosphorylation of CREB, which in its phosphorylated form acts as a functional antagonist of TGF-/smad signalling. Conclusion and Implication We demonstrate that GSK-3 signalling regulates TGF-1-induced myofibroblast differentiation by regulating CREB phosphorylation. GSK-3 may constitute a useful target for treatment of chronic lung diseases.
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- 2013
11. 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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12. Toll-Like Receptor (TLR2 and TLR4) Polymorphisms and Chronic Obstructive Pulmonary Disease
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Budulac, Simona E., Boezen, H. Marike, Hiemstra, Pieter S., Lapperre, Therese S., Vonk, Judith M., Timens, Wim, Postma, Dirkje S., Kauffman, H. F., de Reus, D., Jansen, D. F., Barentsen, M. D.W., Zeinstra-Smit, M., Luteijn, A. J., van der Molen, T., ter Veen, G., Gosman, M. M.E., ten Hacken, N. H.T., Kerstjens, H. A.M., van Maaren, M. S., Veltman, C. A., Verbokkem, A., Verhage, I., Vink-Klooster, H. K., Snoeck-Stroband, J. B., Thiadens, H., Sont, J. K., Bajema, I., Gast-Strookman, J., Janssen, K., Rabe, K. F., van Schadewijk, A., Smit-Bakker, J., Stolk, J., Tire', A. C.J.A., van der Veen, H., Wijffels, M. M.E., Willems, L. N.A., Sterk, P. J., Mauad, T., GLUCOLD Study Grp, Groningen Research Institute for Asthma and COPD (GRIAC), Life Course Epidemiology (LCE), Guided Treatment in Optimal Selected Cancer Patients (GUTS), Erasmus School of Economics, Internal Medicine, Epidemiology, Surgery, Erasmus MC other, Pharmacy, Department of Strategic Management and Entrepreneurship, AII - Amsterdam institute for Infection and Immunity, and Pulmonology
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Male ,Pulmonology ,Chronic Obstructive Pulmonary Diseases ,Pulmonary function testing ,Pulmonary Disease, Chronic Obstructive ,Pathology ,Longitudinal Studies ,TOLL-LIKE-RECEPTOR-2 EXPRESSION ,Lung ,SNPS ,COPD ,Multidisciplinary ,Middle Aged ,medicine.anatomical_structure ,Medicine ,Female ,medicine.symptom ,Engineering sciences. Technology ,Research Article ,Clinical Research Design ,Science ,Inflammation ,Single-nucleotide polymorphism ,Models, Biological ,Polymorphism, Single Nucleotide ,SALMETEROL ,Diagnostic Medicine ,Genetics ,medicine ,Humans ,Biology ,Aged ,Polymorphism, Genetic ,business.industry ,Sputum ,Immunity ,medicine.disease ,GENE ,Toll-Like Receptor 2 ,respiratory tract diseases ,Toll-Like Receptor 4 ,TLR2 ,Gene Expression Regulation ,CIGARETTE-SMOKE ,Genetics of Disease ,Immunology ,CELLS ,Genetic Polymorphism ,TLR4 ,Clinical Immunology ,business ,Population Genetics ,Biomarkers ,General Pathology - Abstract
Toll-like receptors (TLRs) participate in the defence against bacterial infections that are common in patients with Chronic Obstructive Pulmonary Disease (COPD). We studied all tagging SNPs in TLR2 and TLR4 and their associations with the level and change over time of both FEV1 and sputum inflammatory cells in moderate-to-severe COPD. Nine TLR2 SNPs and 17 TLR4 SNPs were genotyped in 110 COPD patients. Associations of SNPs with lung function and inflammatory cells in induced sputum were analyzed cross-sectionally with linear regression and longitudinally with linear mixed-effect models. Two SNPs in TLR2 (rs1898830 and rs11938228) were associated with a lower level of FEV1 and accelerated decline of FEV1 and higher numbers of sputum inflammatory cells. None of the TLR4 SNPs was associated with FEV1 level. Eleven out of 17 SNPs were associated with FEV1 decline, including rs12377632 and rs10759931, which were additionally associated with higher numbers of sputum inflammatory cells at baseline and with increase over time. This is the first longitudinal study showing that tagging SNPs in TLR2 and TLR4 are associated with the level and decline of lung function as well as with inflammatory cell numbers in induced sputum in COPD patients, suggesting a role in the severity and progression of COPD.
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- 2012
13. Oral or IV prednisolone in the treatment of COPD exacerbations - A randomized, controlled, double-blind study
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de Jong, Ynze P., Uil, Steven M., Grotjohan, Hans P., Postma, Dirkje S., Kerstjens, Huib A. M., van den Berg, Jan W. K., and Groningen Research Institute for Asthma and COPD (GRIAC)
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METHYLPREDNISOLONE ,CONTROLLED CLINICAL-TRIAL ,OBSTRUCTIVE PULMONARY-DISEASE ,THERAPY ,INTRAVENOUS CORTICOSTEROIDS ,exacerbation ,CHRONIC-BRONCHITIS ,MANAGEMENT ,COPD ,IV prednisolone ,oral prednisolone ,STRATEGY ,RESPIRATORY QUESTIONNAIRE ,EMERGENCY TREATMENT - Abstract
Background: Treatment with systemic corticosteroids for exacerbations of COPD results in improvement in clinical outcomes. On hospitalization, corticosteroids are generally administered IV. It has not been established whether oral administration is equally effective. We conducted a study to demonstrate that therapy with oral prednisolone was not inferior to therapy with IN prednisolone using a double-blind, double-dummy design. Methods: Patients hospitalized for an exacerbation of COPD were randomized to receive 5 days of therapy with prednisolone, 60 mg IV or orally. Treatment failure, the primary outcome, was defined as death, admission to the ICU, readmission to the ICU because of COPD, or the intensification of pharmacologic therapy during a 90-day follow-up period. Results: A total of 435 patients were referred for a COPD exacerbation warranting hospitalization; 107 patients were randomized to receive IV therapy, and 103 to receive oral therapy. Overall treatment failure within 90 days was similar, as follows: IV prednisolone, 61.7%; oral prednisolone, 56.3% (one-sided lower bound of the 95% confidence interval [CI], -5.8%). There were also no differences in early (ie, within 2 weeks) treatment failure (17.8% and 18.4%, respectively; one-sided lower bound of the 95% CI, -9.4%), late (ie, after 2 weeks) treatment failure (54.0% and 47.0%, respectively; one-sided lower bound of the 95% CI, -5.6%), and mean (+/- SD) length of hospital stay (11.9 +/- 8.6 and 11.2 +/- 6.7 days, respectively). Over I week, clinically relevant improvements were found in spirometry and health-related quality of life, without significant differences between the two treatment groups. Conclusion: Therapy with oral prednisolone is not inferior to IV treatment in the first 90 days after starting therapy. We suggest that the oral route is preferable in the treatment of COPD exacerbations. Trial registration: Clinicaltrials.gov Identifier: NCT00311961.
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- 2007
14. Smoking cessation and bronchial epithelial remodelling in COPD
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Lapperre, Therese, Sont, Jacob K., van Schadewijk, Annemarie, Gosman, Margot M. E., Postma, Dirkje S., Bajema, Ingeborg M., Timens, Wim, Mauad, Thais, Hiemstra, Pieter S., Kauffman, H. F., de Reus, D., Boezen, H. M., Jansen, D. F., Vonk, J., Barentsen, M. D. W., Timens, W., Zeinstra-Smit, M., Luteijn, A. J., van der Molen, T., ter Veen, G., Gosman, M. M. E., ten Hacken, N. H. T., Kerstjens, H. A. M., van Maaren, M. S., Postma, D. S., Veltman, C. A., Verbokkem, A., Verhage, I., Vink-Kloosters, H. K., Snoeck-Stroband, J. B., Thiadens, H., Sont, J. K., Bajema, I., Gast-Strookman, J., Hiemstra, P. S., Janssen, K., Lapperre, T. S., Rabe, K. F., van Schadewijk, A., Schrumpf, J. A., Smit-Bakker, J., Stolk, J., Tire, A. C. J. A., van der Veen, H., Wijffels, M. M. E., Willems, L. N. A., Sterk, P. J., Mauad, T., Groningen Research Institute for Asthma and COPD (GRIAC), Guided Treatment in Optimal Selected Cancer Patients (GUTS), Life Course Epidemiology (LCE), Lifestyle Medicine (LM), and GLUCOLD Study Grp
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Respiratory Mucosa ,Pulmonary and Respiratory Medicine ,Male ,Pathology ,medicine.medical_specialty ,CHRONIC MUCUS HYPERSECRETION ,Bronchi ,LUNG HEALTH ,GOBLET CELL ,PERIPHERAL AIRWAYS ,OBSTRUCTIVE PULMONARY-DISEASE ,Epithelial squamous cell ,AIR-FLOW OBSTRUCTION ,Pulmonary Disease, Chronic Obstructive ,Metaplasia ,medicine ,EX-SMOKERS ,Humans ,Respiratory system ,Aged ,Cell Proliferation ,lcsh:RC705-779 ,Goblet cell ,COPD ,business.industry ,Cell growth ,Research ,CURRENT SMOKERS ,Cell Differentiation ,lcsh:Diseases of the respiratory system ,Middle Aged ,HUMAN NEUTROPHIL DEFENSINS ,medicine.disease ,Epithelium ,respiratory tract diseases ,medicine.anatomical_structure ,Cross-Sectional Studies ,Female ,Smoking Cessation ,Human medicine ,medicine.symptom ,business ,GROWTH-FACTOR RECEPTOR - Abstract
Background Chronic Obstructive Pulmonary Disease (COPD) is associated with bronchial epithelial changes, including squamous cell metaplasia and goblet cell hyperplasia. These features are partially attributed to activation of the epidermal growth factor receptor (EGFR). Whereas smoking cessation reduces respiratory symptoms and lung function decline in COPD, inflammation persists. We determined epithelial proliferation and composition in bronchial biopsies from current and ex-smokers with COPD, and its relation to duration of smoking cessation. Methods 114 COPD patients were studied cross-sectionally: 99 males/15 females, age 62 ± 8 years, median 42 pack-years, no corticosteroids, current (n = 72) or ex-smokers (n = 42, median cessation duration 3.5 years), postbronchodilator FEV1 63 ± 9% predicted. Squamous cell metaplasia (%), goblet cell (PAS/Alcian Blue+) area (%), proliferating (Ki-67+) cell numbers (/mm basement membrane), and EGFR expression (%) were measured in intact epithelium of bronchial biopsies. Results Ex-smokers with COPD had significantly less epithelial squamous cell metaplasia, proliferating cell numbers, and a trend towards reduced goblet cell area than current smokers with COPD (p = 0.025, p = 0.001, p = 0.081, respectively), but no significant difference in EGFR expression. Epithelial features were not different between short-term quitters ( Conclusion Ex-smokers with COPD had less bronchial epithelial remodelling than current smokers, which was only observed after long-term smoking cessation (>3.5 years). Trial registration NCT00158847
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- 2007
15. Reduced inflammatory response in cigarette smoke exposed MrpI/MdrIa/Ib deficient mice
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van der Deen, Margaretha, Timens, Wim, Timmer-Bosscha, Hetty, van der Strate, Barry W., Scheper, Rik J., Postma, Dirkje S., Kerstjens, Huib A., Groningen Research Institute for Asthma and COPD (GRIAC), and Guided Treatment in Optimal Selected Cancer Patients (GUTS)
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INCREASED SENSITIVITY ,BRONCHIAL EPITHELIUM ,LACKING ,MULTIDRUG-RESISTANCE PROTEIN-1 ,COPD ,MRP1 ,INDUCED PULMONARY-EMPHYSEMA ,DENDRITIC CELLS ,GENE ,LUNG - Abstract
Background: Tobacco smoke is the principal risk factor for chronic obstructive pulmonary disease (COPD), though the mechanisms of its toxicity are still unclear. The ABC transporters multidrug resistance-associated protein 1 (MRP1) and P-glycoprotein (P-gp/MDR1) extrude a wide variety of toxic substances across cellular membranes and are highly expressed in bronchial epithelium. Their impaired function may contribute to COPD development by diminished detoxification of noxious compounds in cigarette smoke. Methods: We examined whether triple knock-out (TKO) mice lacking the genes for Mrp1 and Mdr1a/1b are more susceptible to develop COPD features than their wild-type (WT) littermates. TKO and WT mice (six per group) were exposed to 2 cigarettes twice daily by nose-only exposure or room air for 6 months. Inflammatory infiltrates were analyzed in lung sections, cytokines and chemokines in whole lung homogenates, emphysema by mean linear intercept. Multiple linear regression analysis with an interaction term was used to establish the statistical significances of differences. Results: TKO mice had lower levels of interleukin (IL)-7, KC (mouse IL-8), IL-12p70, IL-17, TNF-alpha, G-CSF, GM-CSF and MIP-1-alpha than WT mice independent of smoke exposure (P
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- 2007
16. Mitochondrial localization and function of heme oxygenase-7 in cigarette smoke-induced cell death
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Slebos, Dirk-Jan, Ryter, Stefan W., van der Toorn, Marco, Liu, Fang, Guo, Fengli, Baty, Catherine J., Karlsson, Jenny M., Watkins, Simon C., Kim, Hong Pyo, Wang, Xue, Lee, Janet S., Postma, Dirkje S., Kauffman, Henk F., Choi, Augustine M. K., and Groningen Research Institute for Asthma and COPD (GRIAC)
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TOBACCO-SMOKE ,EXPRESSION ,cigarette smoke ,NECROSIS ,heme oxygenase-1 ,EMPHYSEMA ,CDNA ,OBSTRUCTIVE PULMONARY-DISEASE ,ENDOTHELIAL-CELLS ,APOPTOSIS ,mitochondria ,COPD ,RESPIRATORY-CHAIN ,CARBON-MONOXIDE - Abstract
Cigarette smoke-induced apoptosis and necrosis contribute to the pathogenesis of chronic obstructive pulmonary disease. The induction of heme oxygenase-1 provides cytoprotection against oxidative stress, and may protect in smoking-related disease. Since mitochondria regulate cellular death, we examined the functional expression and mitochondrial localization of heme oxygenase-1 in pulmonary epithelial cells exposed to cigarette smoke extract (CSE), and its role in modulating cell death. Heme oxygenase-1 expression increased dramatically in cytosolic and mitochondrial fractions of human alveolar (A549), or bronchial epithelial cells (Beas-2b) exposed to either hemin, lipopolysaccharide, or CSE. Mitochondrial localization of heme oxygenase-1 was also observed in a primary culture of human small airway epithelial cells. Furthermore, heme oxygenase activity increased dramatically in mitochondrial fractions, and in whole cell extracts of Beas-2b after exposure to hemin and CSE. The mitochondrial localization of heme oxygenase-1 in Beas-2b was confirmed using immunogold-electron microscopy and immunofluorescence labeling on confocal laser microscopy. CSE caused loss of cellular ATP and rapid depolarization of mitochondrial membrane potential. Apoptosis occurred in Beas-2b at low concentrations of cigarette smoke extract, whereas necrosis occurred at high concentrations. Overexpression of heme oxygenase-1 inhibited CSE-induced Beas-2b cell death and preserved cellular ATP levels. Finally, heme oxygenase-1 mRNA expression was elevated in the lungs of mice chronically exposed to cigarette smoke. We demonstrate the functional compartmentalization of heme oxygenase-1 in the mitochondria of lung epithelial cells, and its potential role in defense against mitochondria-mediated cell death during CSE exposure.
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- 2007
17. 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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18. 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
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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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19. 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]
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- 2015
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20. Reliever salbutamol use as a measure of exacerbation risk in chronic obstructive pulmonary disease.
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Jenkins, Christine R., Postma, Dirkje S., Anzueto, Antonio R., Make, Barry J., Peterson, Stefan, Eriksson, Göran, and Calverley, Peter M.
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OBSTRUCTIVE lung diseases ,DISEASE exacerbation ,ALBUTEROL ,BUDESONIDE ,FORMOTEROL - Abstract
Background: Debate exists regarding which endpoints most sensitively reflect day-to-day variation in chronic obstructive pulmonary disease (COPD) symptoms and are most useful in clinical practice to predict COPD exacerbations. We hypothesized that short-acting β2-agonist (SABA) reliever use would predict short- and long-term exacerbation risk in COPD patients. Methods: We performed a retrospective analysis of data from a study (ClinicalTrials.gov registration: NCT00419744) comparing budesonide/formoterol 320/9 μg with formoterol 9 μg (both twice daily) in patients with moderate-to-verysevere COPD; reliever salbutamol 90 μg was provided. First occurrence of reliever use >4 (low), >10 (medium), and >20 (high) inhalations/day was assessed as a predictor of short-term (3-week) exacerbation risk. Mean daily reliever use in the week preceding the 2-month visit was investigated as a predictor of the long-term (10-month) exacerbation risk, using intervals of 2-5, 6-9, and ≥10 inhalations/day. Results: Overall, 810 patients were included (61 % male; mean age 63.2 years; post-bronchodilator forced expiratory volume in 1 s 37.7 % of predicted). First occurrence of low, medium, or high reliever use was predictive of an exacerbation within the following 3 weeks; exacerbation risk increased significantly with increasing reliever use. Mean reliever use over 1 week was predictive of long-term exacerbation risk. Patients with mean use of 2-5, 6-9, and ≥10 inhalations/day exhibited 21 %, 67 %, and 135 % higher exacerbation rates, respectively, in the following 10 months, compared with <2 inhalations/day. Budesonide/formoterol was associated with lower short- and long-term exacerbation risk than formoterol in all reliever-use groups. Conclusions: SABA reliever use is a predictor of short- and long-term exacerbation risk in moderate-to-very-severe COPD patients with a history of exacerbations receiving budesonide/formoterol or formoterol.- [ABSTRACT FROM AUTHOR]
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- 2015
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21. Genome-Wide Association Study Identification of Novel Loci Associated with Airway Responsiveness in Chronic Obstructive Pulmonary Disease.
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Hansel, Nadia N., Paré, Peter D., Rafaels, Nicholas, Sin, Don D., Sandford, Andrew, Daley, Denise, Vergara, Candelaria, Huang, Lili, Elliott, W. Mark, Pascoe, Chris D., Arsenault, Bryna A., Postma, Dirkje S., Boezen, H. Marike, Bossé, Yohan, van den Berge, Maarten, Hiemstra, Pieter S., Cho, Michael H., Litonjua, Augusto A., Sparrow, David, and Ober, Carole
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- 2015
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22. Novel Genes for Airway Wall Thickness Identified with Combined Genome-Wide Association and Expression Analyses.
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Dijkstra, Akkelies E., Postma, Dirkje S., van Ginneken, Bram, Wielpütz, Mark O., Schmidt, Michael, Becker, Nikolaus, Owsijewitsch, Michael, Kauczor, Hans-Ulrich, de Koning, Harry J., Lammers, Jan W., Oudkerk, Matthijs, Brandsma, Corry-Anke, Bossé, Yohan, Nickle, David C., Sin, Don D., Hiemstra, Pieter S., Wijmenga, Ciska, Smolonska, Joanna, Zanen, Pieter, and Vonk, Judith M.
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- 2015
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23. Increased activation of blood neutrophils after cigarette smoking in young individuals susceptible to COPD.
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Hoonhorst, Susan J. M., Timens, Wim, Koenderman, Leo, Lo Tam Loi, Adèle T., Lammers, Jan-Willem J., Marike Boezen, H., Van Oosterhout, Antoon J. M., Postma, Dirkje S., and Ten Hacken, Nick H. T.
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SMOKING ,OBSTRUCTIVE lung diseases ,NEUTROPHILS ,CIGARETTES ,BIOPSY ,INFLAMMATION ,DISEASE susceptibility - Abstract
Background: Cigarette smoking is the most important risk factor for Chronic Obstructive Pulmonary Disease (COPD). Only a subgroup of smokers develops COPD and it is unclear why these individuals are more susceptible to the detrimental effects of cigarette smoking. The risk to develop COPD is known to be higher in individuals with familial aggregation of COPD. This study aimed to investigate if acute systemic and local immune responses to cigarette smoke differentiate between individuals susceptible or non-susceptible to develop COPD, both at young (18-40 years) and old (40-75 years) age. Methods: All participants smoked three cigarettes in one hour. Changes in inflammatory markers in peripheral blood (at 0 and 3 hours) and in bronchial biopsies (at 0 and 24 hours) were investigated. Acute effects of smoking were analyzed within and between susceptible and non-susceptible individuals, and by multiple regression analysis. Results: Young susceptible individuals showed significantly higher increases in the expression of FcγRII (CD32) in its active forms (A17 and A27) on neutrophils after smoking (p = 0.016 and 0.028 respectively), independently of age, smoking status and expression of the respective markers at baseline. Smoking had no significant effect on mediators in blood or inflammatory cell counts in bronchial biopsies. In the old group, acute effects of smoking were comparable between healthy controls and COPD patients. Conclusions: We show for the first time that COPD susceptibility at young age associates with an increased systemic innate immune response to cigarette smoking. This suggests a role of systemic inflammation in the early induction phase of COPD. [ABSTRACT FROM AUTHOR]
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- 2014
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24. Advanced glycation end products in the skin are enhanced in COPD.
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Hoonhorst, Susan J. M., Lo Tam Loi, Adèle T., Hartman, Jorine E., Telenga, Eef D., van den Berge, Maarten, Koenderman, Leo, Lammers, Jan Willem J., Boezen, H. Marike, Postma, Dirkje S., and ten Hacken, Nick H. T.
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OBSTRUCTIVE lung diseases ,SMOKING ,PHYSIOLOGICAL effects of tobacco ,ADVANCED glycation end-products ,ETIOLOGY of diseases ,OXIDATIVE stress - Abstract
Background Cigarette smoking is the main cause of chronic obstructive pulmonary disease (COPD) inducing oxidative stress and local tissue injury, resulting in pulmonary inflammation. Advanced glycation end products (AGEs) are produced by glycation and oxidation processes and their formation is accelerated in inflammatory conditions. In this study we assessed whether AGE accumulation in the skin is elevated in COPD and associates with disease severity. Methods 202 mild-to-very-severe COPD patients and 83 old (40-75 years) and 110 young (18-40 years) healthy smokers and never-smokers were included. AGEs were measured by skin autofluorescence (SAF). Demographic variables, smoking habits, co-morbidities and lung function values were obtained. Results COPD patients (FEV
1 = 55% predicted) had significantly higher SAF values than old and young healthy controls: 2.5 vs. 1.8 and 1.2 (arbitrary units, p < 0.05). No differences in SAF values were found between GOLD stages I-IV (2.4, 2.3, 2.5, 2.5 respectively). Lower function (FEV1 /FVC, MEF50 /FVC, RV/TLC) and higher number of packyears were significantly associated with SAF (p < 0.05). Conclusions SAF is increased in mild-to-very severe COPD patients compared with healthy controls. Interestingly, SAF was not associated with disease severity as values were comparable between different GOLD stages (stage I-IV) of COPD. This may suggest that AGEs play a role in the induction phase of COPD in susceptible smokers. Future studies should further investigate the mechanisms underlying AGEs formation and accumulation in COPD. [ABSTRACT FROM AUTHOR]- Published
- 2014
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25. Untargeted Lipidomic Analysis in Chronic Obstructive Pulmonary Disease.
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Telenga, Eef D., Hoffmann, Roland F., t'Kindt, Ruben, Hoonhorst, Susan J. M., Willemse, Brigitte W. M., van Oosterhout, Antoon J. M., Heijink, Irene H., van den Berge, Maarten, Jorge, Lucie, Sandra, Pat, Postma, Dirkje S., Sandra, Koen, and ten Hacken, Nick H. T.
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- 2014
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26. Co-morbidities are the key nominators of the health related quality of life in mild and moderate COPD.
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Koskela, Jukka, Kilpeläinen, Maritta, Kupiainen, Henna, Mazur, Witold, Sintonen, Harri, Boezen, Marike, Lindqvist, Ari, Postma, Dirkje, and Laitinen, Tarja
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OBSTRUCTIVE lung diseases ,MORTALITY ,QUALITY of life ,HEALTH attitudes ,PSYCHOTHERAPY patients ,ALCOHOLISM ,CARDIOVASCULAR diseases ,DIABETES - Abstract
Background Co-morbidities are common in chronic obstructive pulmonary disease (COPD). We assessed the contribution of common co-morbidities on health related quality of life (HRQoL) among COPD patients. Methods Using both generic (15D) and respiratory-specific (AQ20) instruments, HRQoL was assessed in a hospital based COPD population (N = 739, 64% males, mean age 64 years, SD 7 years) in this observational study with inferential analysis. The prevalence of their co-morbidities was compared with those of 5000 population controls. The patients represented all severity stages of COPD and the patterns of common concomitant disorders differed between patients. Results Co-morbidities such as psychiatric conditions, alcohol abuse, cardiovascular diseases, and diabetes were more common among COPD patients than in age and gender matched controls. Psychiatric conditions and alcohol abuse were the strongest determinants of HRQoL in COPD and could be detected by both 15D (Odds Ratio 4.7 and 2.3 respectively) and AQ20 (OR 2.0 and 3.0) instruments. Compared to respiratory specific AQ20, generic 15D was more sensitive to the effects of comorbidities while AQ20 was slightly more sensitive for the low FEV1. FEV1 was a strong determinant of HRQoL only at more severe stages of disease (FEV1 < 40% of predicted). Poor HRQoL also predicted death during the next five years. Conclusions The results suggest that co-morbidities may impair HRQoL at an early stage of the disease, while bronchial obstruction becomes a significant determinant of HRQoL only in severe COPD. [ABSTRACT FROM AUTHOR]
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- 2014
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27. Glycogen synthase kinase-3 ( GSK-3) regulates TGF-β1-induced differentiation of pulmonary fibroblasts.
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Baarsma, Hoeke A, Engelbertink, Lilian HJM, Hees, Lonneke J, Menzen, Mark H, Meurs, Herman, Timens, Wim, Postma, Dirkje S, Kerstjens, Huib AM, and Gosens, Reinoud
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GLYCOGEN synthase kinase-3 ,TRANSFORMING growth factors-beta ,FIBROBLASTS ,CELL differentiation ,EXTRACELLULAR matrix ,PULMONARY fibrosis ,MYOFIBROBLASTS ,CELLULAR signal transduction - Abstract
Background Chronic lung diseases such as asthma, COPD and pulmonary fibrosis are characterized by abnormal extracellular matrix ( ECM) turnover. TGF-β is a key mediator stimulating ECM production by recruiting and activating lung fibroblasts and initiating their differentiation process into more active myofibroblasts. Glycogen synthase kinase-3 ( GSK-3) regulates various intracellular signalling pathways; its role in TGF-β
1 -induced myofibroblast differentiation is currently largely unknown. Purpose To determine the contribution of GSK-3 signalling in TGF-β1 -induced myofibroblast differentiation. Experimental Approach We used MRC5 human lung fibroblasts and primary pulmonary fibroblasts of individuals with and without COPD. Protein and m RNA expression were determined by immunoblotting and RT-PCR analysis respectively. Results Stimulation of MRC5 and primary human lung fibroblasts with TGF-β1 resulted in time- and dose-dependent increases of α-sm-actin and fibronectin expression, indicative of myofibroblast differentiation. Pharmacological inhibition of GSK-3 by SB216763 dose-dependently attenuated TGF-β1 -induced expression of these myofibroblasts markers. Moreover, silencing of GSK-3 by si RNA or pharmacological inhibition by CT/CHIR99021 fully inhibited the TGF-β1 -induced expression of α-sm-actin and fibronectin. The effect of GSK-3 inhibition on α-sm-actin expression was similar in fibroblasts from individuals with and without COPD. Neither smad, NF-κB nor ERK1/2 were involved in the inhibitory actions of GSK-3 inhibition by SB126763 on myofibroblast differentiation. Rather, SB216763 increased the phosphorylation of CREB, which in its phosphorylated form acts as a functional antagonist of TGF-β/smad signalling. Conclusion and Implication We demonstrate that GSK-3 signalling regulates TGF-β1 -induced myofibroblast differentiation by regulating CREB phosphorylation. GSK-3 may constitute a useful target for treatment of chronic lung diseases. [ABSTRACT FROM AUTHOR]- Published
- 2013
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28. Asthma and Chronic Obstructive Pulmonary Disease.
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Postma, Dirkje S., Kerkhof, Marjan, Boezen, H. Marike, and Koppelman, Gerard H.
- Published
- 2011
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29. A new perspective on optimal care for patients with COPD.
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Postma, Dirkje, Anzueto, Antonio, Calverley, Peter, Jenkins, Christine, Make, Barry J., Sciurba, Frank C., Similowski, Thomas, van der Molen, Thys, and Eriksson, Göran
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OBSTRUCTIVE lung disease treatment ,DISEASE management ,DISEASE risk factors ,PHARMACOLOGY ,HEALTH outcome assessment - Abstract
Worldwide, clinicians face the task of providing millions of patients with the best possible treatment and management of COPD. Currently, management primarily involves short-term 'here-and-now' goals, targeting immediate patient benefit. However, although there is considerable knowledge available to assist clinicians in minimising the current impact of COPD on patients, relatively little is known about which dominant factors predict future risks. These predictors may vary for different outcomes, such as exacerbations, mortality, co-morbidities, and the long-term consequences of COPD. We propose a new paradigm to achieve 'optimal COPD care' based on the concept that here-and-now goals should be integrated with goals to improve long-term outcomes and reduce future risks. Whilst knowledge on risk factors for poorer outcomes in COPD is growing and some data exist on positive effects of pharmacological interventions, information on defining the benefits of all commonly used interventions for reducing the risk of various future disease outcomes is still scarce. Greater insight is needed into the relationships between the two pillars of optimal COPD care: 'best current control' and 'future risk reduction'. This broader approach to disease management should result in improved care for every COPD patient now and into the future. [ABSTRACT FROM AUTHOR]
- Published
- 2011
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30. Increased Systemic Inflammation Is a Risk Factor for COPD Exacerbations.
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Groenewegen, Karin H., Postma, Dirkje S., Hop, Wim C. J., Wielders, Pascal L. M. L., Schlösser, Noel J. J., and Wouters, Emiel F. M.
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- *
MEDICAL research , *OBSTRUCTIVE lung diseases , *INFLAMMATION , *FIBRINOGEN , *BLOOD coagulation factors - Abstract
The article presents a study on the risk factor for chronic obstructive pulmonary disease (COPD) exacerbations. COPD is characterized by episodic increases in respiratory symptoms called exacerbations. It is associated with an increase in local and systemic inflammation. The study demonstrates that besides lung function impairment, systemic inflammation manifested by elevated fibrinogen levels is an independent risk factor for exacerbations of COPD.
- Published
- 2008
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31. Mitochondrial Localization and Function of Heme Oxygenase-1 in Cigarette Smoke--Induced Cell Death.
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Slebos, Dirk-Jan, Ryter, Stefan W., van der Toorn, Marco, Fang Liu, Fengli Guo, Baty, Catherine J., Karlsson, Jenny M., Watkins, Simon C., Hong Pyo Kim, Xue Wang, Lee, Janet S., Postma, Dirkje S., Kauffman, Henk F., and Choi, Augustine M. K.
- Published
- 2007
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32. A pooled analysis of FEV1 decline in COPD patients randomized to inhaled corticosteroids or placebo.
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Soriano, Joan B., Sin, Don D., Xuekui Zhang, Camp, Pat G., Anderson, Julie A., Anthonisen, Nick R., Buist, A. Sonia, Burge, P. Sherwood, Calverley, Peter M., Connett, John E., Peterson, Stefan, Postma, Dirkje S., Szafranski, Wojciech, Vestbo, Jørgen, Zhang, Xuekui, Petersson, Stefan, and Vestbo, Jørgen
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OBSTRUCTIVE lung diseases ,CLINICAL trials ,MEDICAL research ,CORTICOSTEROIDS ,PLACEBOS - Abstract
Background: There is controversy about whether therapy with inhaled corticosteroids (ICSs) modifies the natural history of COPD, characterized by an accelerated decline in FEV(1).Methods: The Inhaled Steroids Effect Evaluation in COPD (ISEEC) study is a pooled study of patient-level data from seven long-term randomized controlled trials of ICS vs placebo lasting >/= 12 months in patients with moderate-to-severe COPD. We have previously reported a survival benefit for ICS therapy in COPD patients using ISEEC data. We aimed to determine whether the regular use of ICSs vs placebo improves FEV(1) decline in COPD patients, and whether this relationship is modified by gender and smoking.Results: There were 3,911 randomized participants (29.2% female) in this analysis. In the first 6 months after randomization, ICS use was associated with a significant mean (+/- SE) relative increase in FEV(1) of 2.42 +/- 0.19% compared with placebo (p < 0.01), which is quantifiable in absolute terms as 42 mL in men and 29 mL in women over 6 months. From 6 to 36 months, there was no significant difference between placebo and ICS therapy in terms of FEV(1) decline (-0.01 +/- 0.09%; p = 0.86). The initial treatment effect was dependent on smoking status and gender. Smokers who continued to smoke had a smaller increase in FEV(1) during the first 6 months than did ex-smokers. Female ex-smokers had a larger increase in FEV(1) with ICS therapy than did male ex-smokers.Conclusions: We conclude that in COPD in the first 6 months of treatment, ICS therapy is more effective in ex-smokers than in current smokers with COPD in improving lung function, and women may have a bigger response to ICSs than men. However, it seems that after 6 months, ICS therapy does not modify the decline in FEV(1) among those who completed these randomized clinical trials. [ABSTRACT FROM AUTHOR]- Published
- 2007
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33. Safety of Sputum Induction During Exacerbations of COPD.
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Bathoorn, Evik, Liesker, Jeroen, Postma, Dirkje, Koëter, Gerard, Van Oosterhout, Antoon J. M., and Kerstjens, Huib A. M.
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SPUTUM ,OBSTRUCTIVE lung diseases ,RESPIRATORY obstructions ,MULTIVARIATE analysis ,PATIENTS - Abstract
The article assess the safety of sputum induction (SI) during the chronic obstructive pulmonary disease (COPD) exacerbations. The research concluded that SI can be safety carried out in patients with mild-to-moderate COPD who experience an exacerbation. The only independent association was with the larger decrease in FEV
1 in the stable phase in a multivariate analysis.- Published
- 2007
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34. Small Airways Dysfunction and Neutrophilic Inflammation in Bronchial Biopsies and BAL in COPD.
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Lapperre, Thérëse S., Willems, Luuk N. A., Timens, Wim, Rabe, Klaus F., Hiemstra, Pieter S., Postma, Dirkje S., and Sterk, Peter J.
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OBSTRUCTIVE lung diseases ,RESPIRATION ,AIRWAY (Anatomy) ,BRONCHOALVEOLAR lavage ,LUNG biopsy ,SPUTUM - Abstract
The article discusses a study which examined whether uneven ventilation and airway closure are associated with specific markers of airway inflammation as obtained by bronchial biopsies, bronchoalveolar lavage (BAL) and induced sputum in chronic obstructive pulmonary disease patients. The results of the single-breath N
2 test are associated with neutrophilic inflammation in bronchial biopsies and BAL.- Published
- 2007
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35. Detrimental Effects of β-Blockers in COPD.
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van der Woude, Hanneke J., Zaagsma, Johan, Postma, Dirkje S., Winter, Trea H., van Hulst, Marinus, and Aalbers, René
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ADRENERGIC beta agonists ,ADRENERGIC beta blockers ,LUNG diseases ,PLACEBOS ,ASTHMA ,FORMOTEROL ,THERAPEUTICS - Abstract
Introduction: β-Blockers are known to worsen FEV1 and airway hyperresponsiveness (AHR) in patients with asthma. Both characteristics determine the outcome of COPD, a disease with frequent cardiac comorbidity requiring β-blocker treatment. Objective: To determine the effects of β-blockers on AHR (provocative concentration of methacholine causing a 20% fall in FEV
1 [PC20 ]), FEV1, and response to formoterol in patients with COPD. Design: A double-blind, placebo-controlled, randomized, cross-over study. Setting: An ambulatory, hospital outpatient clinic of pulmonary diseases. Patients: Patients with mild-to-moderate irreversible COPD and AHR. Intervention: Fifteen patients received propranolol (80 mg), metoprolol (100 mg), celiprolol (200 mg), or placebo for 4 days, followed by a washout period ≥ 3 days. On day 4 of treatment, FEV1 and PC20 were assessed. Immediately hereafter, formoterol (12 μg) was administered and FEV1 was measured for up to 30 min. Results: PC20 was significantly lower (p < 0.01) with propranolol and metoprolol treatment (geometric means, 2.06 mg/mL and 2.02 mg/mL, respectively) than with placebo (3.16 mg/mL) or celiprolol (3.41 mg/mL). FEV1 deteriorated only after propranolol treatment (2.08 ± 0.31 L) [mean ± SD] compared with placebo (2.24 ± 0.37 L). The fast bronchodilating effect of formoterol was hampered by propranolol (mean increase in FEV1 at 3 min, 6.7 ± 8.9%) but was unaffected by the other β-blockers (16.9 ± 9.8%, 22 ± 11.6%, and 16.9 ± 9.0% for placebo, metoprolol, and celiprolol, respectively). Conclusions: Pulmonary effects did not occur by celiprolol. Only propranolol reduced FEV1 and the bronchodilating effect of formoterol. Both metoprolol and propranolol increased AHR. Thus, different classes of β-blockers have different pulmonary effects. The anticipated beneficial cardiovascular effects of a β-blocker must be weighted against the putative detrimental pulmonary effects, ie, effect on FEV1 , AHR, and response to additional β2 -agonists. [ABSTRACT FROM AUTHOR]- Published
- 2005
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36. Rationale for the Dutch Hypothesis*.
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Postma, Dirkje S. and Boezen, H. Marike
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- *
OBSTRUCTIVE lung diseases , *ASTHMA , *RESPIRATORY diseases , *THEORY , *LUNG diseases - Abstract
The Dutch hypothesis, formulated in the 1960s, holds that the various forms of airway obstruction are different expressions of a single disease entity. It suggests that genetic factors (eg, airway hyperresponsiveness [AHR] and atopy), endogenous factors (eg, sex and age), and exogenous factors (eg, allergens, infections, and smoking) all play a role in the pathogenesis of chronic nonspecific lung disease. This review finds evidence that AHR and smoking are common risk factors for asthma and COPD. To prove the Dutch hypothesis definitively, however, genetic studies, preferably longitudinal, must be performed. Such studies must include subjects who have airway obstruction that does not necessarily meet the current strict definitions of asthma or COPD (ie, the extremes of these conditions) that are used in clinical studies. [ABSTRACT FROM AUTHOR]
- Published
- 2004
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37. Opportunities and Challenges in the Genetics of COPD 2010: An International COPD Genetics Conference Report
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Agusti, Alvar, Anderson, Wayne, Bakke, Per S, Barnes, Kathleen C, Barr, R Graham, Bleecker, Eugene R, Boezen, H Marike, Burkart, Kristin M, Cookson, William OC, Croxton, Thomas, Daley, Denise, Gan, Weiniu, Garcia-Aymerich, Judith, Hall, Ian P, Hansel, Nadia N, Kalsheker, Noor, Kiley, James P, Lambrechts, Diether, Lee, Sang-Do, Lomas, David A, London, Stephanie J, Nishimura, Masaharu, Postma, Dirkje S, Puhan, Milo A, Tesfaigzi, Yohannes, Tobin, Martin D, Vogelmeier, Claus, Wouters, Emiel, Ziegler-Heitbrock, Loems, MacNee, William, Crapo, James D, Vestbo, Jørgen, Silverman, Edwin Kepner, Cho, Michael Hyosang, Celli, Bartolome R, Demeo, Dawn Lisa, Hersh, Craig Palmer, Wilk, Jemma B, Nørdestgaard, Borge G., Young, Robert P., O'Donnell, Christopher J., Kim, Woo Jin, and Litonjua, Augusto Ampil
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COPD ,genetics ,association analysis ,consortium - Published
- 2011
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38. High Cessation Rates of Cigarette Smoking in Subjects With and Without COPD.
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Willemse, Brigitte, Lesman-Leegte, Ivonne, Timens, Wim, Postma, Dirkje, and ten Hacken, Nick
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SMOKING cessation ,OBSTRUCTIVE lung diseases ,BEHAVIOR therapy ,LUNG diseases ,BRONCHITIS ,THERAPEUTICS - Abstract
This article evaluates a one-year program on smoking cessation. This program studies the differential effects of smoking cessation in Chronic Obstructive Pulmonary Disease (COPD) and healthy subjects. This program was developed by the Foundation for Community Health and Smoking in the Netherlands. It was based on cognitive behavioral therapy in which aspects such as motivation and self-efficacy play an important role. The results of this study show a high cessation rates of 42 percent both in smokers with COPD or chronic bronchitis.
- Published
- 2005
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39. A chronic obstructive pulmonary disease related signature in squamous cell lung cancer
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Boelens, Mirjam C., Gustafson, Adam M., Postma, Dirkje S., Kok, Klaas, van der Vries, Gerben, van der Vlies, Pieter, Spira, Avrum, Lenburg, Marc E., Geerlings, Marie, Sietsma, Hannie, Timens, Wim, van den Berg, Anke, and Groen, Harry J.M.
- Subjects
- *
OBSTRUCTIVE lung diseases , *SQUAMOUS cell carcinoma , *LUNG cancer , *EPIDEMIOLOGY , *CHROMOSOME abnormalities , *REVERSE transcriptase polymerase chain reaction , *GENE expression , *MITOCHONDRIA - Abstract
Abstract: The epidemiological relationship between squamous cell lung cancer (SCC) and chronic obstructive pulmonary disease (COPD), both smoking-related diseases, suggests that they have also a genetic basis. We compared 35 SCC patients with and without COPD with whole-genome gene expression profiles of laser microdissected tissue. Validation of differential expression was performed for 25 genes using quantitative (q)RT-PCR. Subsequently, we performed array-based CGH on the same tumor samples. We found that 374 probes were differentially expressed in SCC from patients with and without COPD. Forty-four probes were derived from genes with mitochondrial functions and 34 probes were located on 5q. All these probes showed a lower expression level in SCC from non-COPD patients. For a random selection of 25 mitochondrial and 5q genes, we confirmed the differential expression by qRT-PCR. Loss of 3p, 5q and 9p was observed, via array-CGH, to be more frequent in SCC from non-COPD patients as compared to SCC from COPD patients. Combination of chromosomal aberrations and the location of the differentially expressed genes showed significant association for loss of the 5q31.2–31.3 region and reduced expression of the 5q genes. In conclusion, a more frequent loss of 5q and a low expression of genes located on 5q in SCC tumors of non-COPD patients compared to tumors from COPD patients was identified suggesting that different oncogenetic pathways are operational in patients with and without COPD. [Copyright &y& Elsevier]
- Published
- 2011
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40. Asthma and COPD: Smoking, Atopy and Corticosteroid responsiveness
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Fatemeh Fattahi, Timens, Wim, Postma, Dirkje, Hacken ,ten, Nicolaas, and Hylkema, Machteld
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Atopy ,medicine.medical_specialty ,COPD ,business.industry ,medicine.drug_class ,Internal medicine ,Medicine ,Corticosteroid ,business ,medicine.disease ,Asthma ,respiratory tract diseases - Abstract
The aim of this thesis was to describe, investigate and compare the effects of smoking and atopy in asthma and COPD. A part of the research focused on asthmatic patients with ageing and smoking COPD phenotype, resulting in difficulties to discriminate between these two disorders. The following conclusions can be drawn: • Pathologists are able to differentiate between asthma and COPD, on condition they use a number of pathological criteria, and take the clinical setting into account, particularly the use of inhaled corticosteroids (ICS). • Prevalence of atopy is significantly higher in COPD patients who are males, have overweight and lower age. Atopy significantly associates with higher prevalence of respiratory symptoms and higher likelihood to lose cough upon treatment with busedonide.• Absence of atopy and non-ICS use contribute independently to higher numbers of IL-17 expressing cells. IL17-positive cells were found to be predominantly neutrophils. • CCL20 levels are higher in sputum of asthmatics who use ICS, whereas glucocorticoids increase the release of CCL20 by primary bronchial epithelial cells in vitro.• Smoking associates with higher epithelial HDAC-2 expression in airway biopsies from asthmatics, independent of ICS-use. • Increased Eosinophil Peroxidase (EPX) immunopositivity in airway biopsies from asthmatic subjects associates significantly with lower intact epithelium, particularly in uncontrolled asthma.In summary: heterogeneous populations of asthma and COPD patients determine the broad spectrum of obstructive airway diseases. Smoking and atopy may modulate the underlying inflammatory and clinical phenotype, and affect corticosteroid responsiveness. This heterogeneity should be taken into account when designing clinical studies.
- Published
- 2021
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