Article Text

Original article
C reactive protein and chronic obstructive pulmonary disease: a Mendelian randomisation approach
  1. Morten Dahl1,2,3,4,
  2. Jørgen Vestbo3,4,5,6,
  3. Jeppe Zacho1,2,3,4,
  4. Peter Lange3,4,5,
  5. Anne Tybjærg-Hansen2,3,4,7,
  6. Børge G Nordestgaard1,2,3,4
  1. 1Department of Clinical Biochemistry, Herlev Hospital, Copenhagen, Denmark
  2. 2The Copenhagen General Population Study, Herlev Hospital, Copenhagen, Denmark
  3. 3The Copenhagen City Heart Study, Bispebjerg Hospital, Copenhagen, Denmark
  4. 4Faculty of Health Sciences, University of Copenhagen, Copenhagen, Denmark
  5. 5Department of Cardiology and Respiratory Medicine, Hvidovre Hospital, Copenhagen, Denmark
  6. 6Respiratory Medicine Research Group, University of Manchester, Manchester, UK
  7. 7Department of Clinical Biochemistry, Rigshospitalet, Copenhagen, Denmark
  1. Correspondence to Børge G Nordestgaard, Professor, Chief Physician, Department of Clinical Biochemistry, Herlev Hospital, Copenhagen University Hospital, Herlev Ringvej 75, DK-2730 Herlev, Denmark; brno{at}heh.regionh.dk

Abstract

Background It is unclear whether elevated plasma C reactive protein (CRP) is causally related to chronic obstructive pulmonary disease (COPD). The authors tested the hypothesis that genetically elevated plasma CRP causes COPD using a Mendelian randomisation design.

Methods The authors measured high-sensitivity CRP in plasma, genotyped for four single nucleotide polymorphisms in the CRP gene, and screened for spirometry-defined COPD and hospitalisation due to COPD in 7974 individuals from the Copenhagen City Heart Study and in 32 652 individuals from the Copenhagen General Population Study.

Results Elevated plasma CRP >3 mg/l compared with <1 mg/l was associated with risk estimates of 1.8 and 2.8 for spirometry-based COPD and of 1.6 and 1.8 for hospitalisation due to COPD in the Copenhagen City Heart Study and the Copenhagen General Population Study, respectively. Genotype combinations of the four CRP polymorphisms were associated with up to a 62% increase in plasma CRP. However, these genotype combinations did not associate with increased risk of COPD or hospitalisation due to COPD in either cohort or in the two cohorts combined. On instrumental variable analysis, a doubling of plasma CRP versus a doubling of genetically elevated CRP resulted in ORs for COPD of 1.27 (95% CI 1.25 to 1.30) versus 1.01 (0.81 to 1.26) and for COPD hospitalisation of 1.47 (1.43 to 1.51) versus 0.82(0.59 to 1.13).

Conclusion Although elevated CRP is related to both a diagnosis of COPD and subsequent hospital admission, genetically elevated plasma CRP is not associated with an increased risk of clinical COPD. This suggests that the association between CRP levels and COPD is not causal.

  • COPD
  • genetics
  • CRP
  • biomarker
  • Mendelian randomisation
  • clinical epidemiology
  • COPD pathology
  • innate immunity

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Introduction

Chronic obstructive pulmonary disease (COPD) remains the fourth leading cause of death in the World.1 2 The diagnosis of COPD is based on a lung function test showing obstruction of lung airflow, but the disease also comprises airway inflammation, mucociliary dysfunction, structural changes and extrapulmonary effects. New markers that describe these other components of COPD are being explored with the aim to improve the clinical assessment of COPD.3–5

One important inflammatory marker in COPD is elevated plasma C reactive protein (CRP). Small increases in this acute phase reactant are associated with both disease activity and future risk of hospitalisation and death from COPD.6–16 Van Durme et al has found that CRP haplotypes do not associate with increased risk of COPD,16 but whether CRP is causally related to COPD or solely a marker of the disease activity is not totally clear.17 The answer to this question has clinical importance as drugs that specifically lower CRP are being developed.18

One approach to testing for causality between CRP and COPD would be to perform an intervention study with a CRP lowering drug. However, an alternative concept termed ‘Mendelian randomisation’ can also be used. This design can assess gene-related risk factors for causal association with clinical outcomes. This is because individuals inherit gene variants randomly from their parents.19 Thus, genetic variants in the CRP gene that increase plasma concentrations of CRP are an ideal system for testing whether elevated plasma CRP is causally related to COPD.

To test whether genetically elevated plasma CRP is associated with an increased risk of COPD, we have asked the following three questions: (1) is elevated plasma CRP associated with increased risk of COPD, (2) are single nucleotide polymorphisms in the CRP gene associated with increased plasma CRP and (3) is genetically elevated plasma CRP associated with increased risk of COPD. To answer these questions, we measured high-sensitivity CRP in plasma, genotyped for single nucleotide polymorphisms in the CRP gene, screened for COPD using spirometric criteria and obtained information on hospitalisation due to COPD in 7974 individuals from the Copenhagen City Heart Study and 32 652 individuals from the Copenhagen General Population Study.7 20

Methods

We studied two independent cohorts of white individuals of Danish descent. The two groups were defined so that no individual appears twice in any of the groups, thus permitting independent findings in each group. The studies were approved by Herlev Hospital and by Danish ethics committees, and were conducted according to the Declaration of Helsinki. Written informed consent was obtained from all participants.

Study cohorts

The Copenhagen City Heart Study7 21 is a prospective study of a cohort of individuals 20 years and older randomly selected from the population of Copenhagen. Data were available from this study on COPD (FEV1/FVC<0.7 and FEV1<80% of predicted, excluding individuals with self-reported asthma) and on rate of hospitalisation due to COPD (WHO ICD8: 491–492; ICD10: J41–J44) ascertained from 1976 to 2009. From this study, 10 230 participants were included in the present analysis.

The Copenhagen General Population Study20 22 is a cross-sectional study of individuals 20 years and older selected like those in the Copenhagen City Heart Study, from the population of Copenhagen. Data were available from this study on COPD (FEV1/FVC<0.7 and FEV1<80% of predicted, excluding individuals with self-reported asthma) and on prevalence of COPD hospitalisation (WHO ICD8: 491–492; ICD10: J41–J44) ascertained from 1976 to 2009. From this study, 36 036 participants were included in the present analysis. We did not have longitudinal data with repeated examinations for the Copenhagen General Population Study and did not perform time-dependent analyses for this cohort.

Genotyping, biochemical analyses and other covariates

Blood samples were routinely collected for the two source studies. The ABI PRISM® 7900HT Sequence Detection System (Applied Biosystems Inc., Foster City, California, USA) was used to genotype for four single nucleotide polymorphisms in the CRP gene (rs3091244, rs1130864, rs1205, rs3093077).20 23 Genotyping was verified by DNA sequencing in >30 individuals with each genotype. High-sensitivity CRP was measured using nephelometry or turbidimetry. CRP levels were classified as low (<1.0 mg/l), average (1.0–3.0 mg/l), or high (>3.0 mg/l). If subjects with CRP levels >10 mg/l were excluded from the analyses, the results were similar to those presented in this study, except for a significantly decreased OR for COPD hospitalisation among individuals with CRP genotype combination #9 when combining the two cohorts. Physical activity during leisure time was assessed by The Copenhagen City Heart Study Leisure Time Physical Activity Questionnaire.24 Asthma medication was an affirmative answer to the question ‘Do you daily take medication for asthma and/or bronchitis?’.

Statistics

We used Stata for all analyses and NCSS-PASS for power calculations. For trend tests the different groupings of subjects by CRP level, genotype or genotype combination were coded 1, 2, 3, etc, and ranked according to increasing CRP levels. From the four CRP polymorphisms we generated all possible genotype combinations and ranked the nine most common combinations according to increasing plasma CRP levels.

To examine our study hypothesis, we first analysed the relationship between plasma CRP and risk of COPD and hospitalisation due to COPD. Logistic regression estimated ORs for COPD in the Copenhagen City Heart Study and the Copenhagen General Population Study. Cox regression estimated HRs for COPD hospitalisation in the prospective Copenhagen City Heart Study,25 and logistic regression estimated ORs for COPD hospitalisation in the Copenhagen General Population Study. The proportional hazard assumption for Cox regression was tested by visual inspection of ln(–ln[survival]) versus ln(analysis time) for all comparisons; no major violations were observed. The models were adjusted for (1) age, sex and smoking or (2) age, sex, smoking, body mass index, physical activity, asthma medication and ischaemic heart disease (ICD8: 410–414; ICD10: I20–I25); the models for hospitalisation due to COPD were also adjusted for FEV1% predicted. Overall p values are test for trend of risk estimates (ORs or HRs) where CRP groups with increasing level of plasma CRP has been coded 1, 2 and 3.

Second, we analysed the relationship between CRP polymorphisms and polymorphism combinations and plasma CRP in the cross-sectional Copenhagen General Population Study. Analyses were performed using Kruskal–Wallis analysis of variance. p Values are for test of trend of mean CRP levels, where CRP genotype/combination groups ranked according to increasing CRP levels have been coded 1, 2, 3 and so forth.

Third, we analysed the relationship between CRP polymorphisms and risk of COPD outcomes. Logistic regression estimated ORs for COPD in the Copenhagen City Heart Study and the Copenhagen General Population Study. Cox regression estimated HRs for COPD hospitalisation in the prospective Copenhagen City Heart Study,25 and logistic regression estimated ORs for COPD hospitalisation in the Copenhagen General Population Study. The models were adjusted for (1) age, sex and smoking or (2) age, sex, smoking, body mass index, physical activity, asthma medications and ischaemic heart disease; the models for hospitalisation due to COPD were also adjusted for FEV1% predicted. p Values are for test of trend of mean CRP levels, where CRP genotype/combination groups ranked according to increasing CRP levels have been coded 1, 2, 3 and so forth.

Fourth, the increase in HRs for COPD for a 1% increase in CRP levels in the Copenhagen City Heart Study was used to predict theoretical HRs for COPD for the change in CRP levels caused by the combined genotypes. Observed and theoretically predicted HRs as a function of plasma CRP levels were corrected for regression dilution bias.26 27 Logistic regression analysis was used to calculate a combined OR for COPD and hospitalisation due to COPD as a function of genotype for both studies combined.

Finally, the estimated causal OR for COPD in the two cohorts combined was calculated according to Greenland et al28 29 and compared with the observed OR30; for this purpose, we used generalised least-squares regression.

To address possible misclassification of COPD in younger and older adults from the use of the fixed FEV1/FVC threshold, we performed a sensitivity analysis defining COPD based on the fifth percentile lower limit of normal. These analyses using the lower limit of normal definition of COPD yielded similar results to those presented in this study for COPD defined by FEV1/FVC<0.7 and FEV1<80% of predicted.

Results

Table 1 presents the distribution of clinical characteristics among the individuals who were free from COPD, had COPD according to spirometry or were hospitalised due to COPD in the Copenhagen City Heart Study and Copenhagen General Population Study. As would be expected, the individuals who had any COPD outcome were more likely males and smokers, were older, and had lower percentage predicted FEV1. More than half of the patients who had spirometry-defined COPD or were hospitalised due to COPD in the Copenhagen City Heart Study did not fulfil the spirometry-based definition of COPD when they entered the study.

Table 1

Characteristics of participants

Plasma CRP and COPD

Plasma CRP>3 mg/l versus <1 mg/l was associated with an OR of 1.4 (95% CI 1.1 to 1.9) for COPD and HR of 2.4 (1.6 to 3.6) for hospitalisation due to COPD in the Copenhagen City Heart Study (figure 1). After multifactorial adjustment the equivalent values were 1.8 (1.4–2.3) and 1.6 (1.1–2.5), respectively. The p values for trend were <0.001 for all analyses.

Figure 1

Risk of chronic obstructive pulmonary disease (COPD) according to plasma levels of C reactive protein (CRP). High-sensitivity CRP level was measured in 8974 individuals participating in the 1991–1994 examination of the Copenhagen City Heart Study and subsequently correlated with spirometry-defined COPD or followed with respect to hospitalisation due to COPD. High-sensitivity CRP level was also measured in 32 652 individuals participating in the Copenhagen General Population Study and subsequently correlated with COPD and hospitalisation due to COPD. Multiple adjustment was for age, sex, smoking, body mass index, physical activity, asthma medication and ischaemic heart disease; models for hospitalisation due to COPD were also adjusted for FEV1% predicted. Overall p values are test for trend of risk estimates (ORs or HRs), where CRP groups with increasing level of plasma CRP have been coded 1, 2 and 3.

Plasma CRP>3 mg/l versus <1 mg/l was associated with ORs of 1.7 (1.6 to 1.9) and 2.4 (2.1 to 2.9) for COPD and hospitalisation due to COPD in the Copenhagen General Population Study (figure 1). After multifactorial adjustment the equivalent values were 2.8 (2.4 to 3.1) and 1.8 (1.4 to 2.3). The p values for trend were <0.001 for all analyses. The CRP results for COPD hospitalisation in the Copenhagen City Heart Study describe pre-outcome CRP levels, while the Copenhagen General Population Study describes simultaneous or post-outcome levels. The association between CRP levels and risk of COPD, stratified for smoking status, is shown in Supplementary figure 1.

CRP polymorphisms and plasma CRP

In line with our previous results20 the CRP polymorphism rs1205 AA genotype was associated with decreased plasma CRP levels of 24% compared with the GG genotype (figure 2, Trend p<0.001). The rs1130864 TT genotype versus CC genotype was associated with a 25% increase in plasma CRP level, rs3091244 AA genotype versus CC genotype with a 71% increase, and rs3093077 GG genotype versus TT genotype with a 55% increase (all Trend p<0.001). Combining the genotypes resulted in up to 62% increase in plasma CRP levels between the highest and lowest levels among the nine most common genotype combinations (figure 2). Partial r2 values for the different CRP polymorphisms ranged from 0.4% to 1.8%.

Figure 2

Plasma levels of C reactive protein (CRP) according to CRP genotype and genotype combinations in the Copenhagen General Population Study. High-sensitivity CRP levels and CRP genotyping was determined in 36 036 individuals. Partial r2 values were after adjustment for variation in plasma CRP levels due to age, gender, smoking and body mass index. p Values are for Cuzick non-parametric test for trend of mean CRP levels, where CRP genotype/combination groups ranked according to increasing CRP levels have been coded 1, 2, 3 and so forth.

CRP polymorphisms and COPD

The ORs for COPD as a function of genotype in the Copenhagen City Heart Study and the Copenhagen General Population Study did not differ from 1.0 for any of the individual CRP polymorphisms, or for genotype combinations (p for trend 0.24–0.80; figure 3A). Similarly, the HR for COPD hospitalisation in the Copenhagen City Heart Study and the OR for COPD hospitalisation in the Copenhagen General Population Study did not differ consistently from 1.0 for any of the individual CRP polymorphisms, or for genotype combinations (p for trend 0.12–0.78; figure 3B).

Figure 3

(A, B) Risk of chronic obstructive pulmonary disease (COPD) according to C reactive protein (CRP) genotype and genotype combinations. The ORs and HRs were adjusted for age, sex and smoking. After multiple adjustment for age, sex, smoking, body mass index, physical activity, asthma medication, ischaemic heart disease and/or FEV1% predicted, the risk estimates were similar to those presented. Overall p values are test for trend of risk estimates (ORs or HRs), where CRP genotype/combination groups ranked according to increasing CRP levels have been coded 1, 2, 3 and so forth.

When analysing the annual decline in FEV1 among individuals with COPD in the Copenhagen City Heart Study, there was no significant difference for any of the individual CRP polymorphisms, or for genotype combinations (p for trend 0.19 to 0.65; figure 4). Partial r2 values for the different CRP polymorphisms ranged from 0.09% to 0.81%.

Figure 4

Annual FEV1 decline according to C reactive protein (CRP) genotype and genotype combinations among individuals with spirometry-defined chronic obstructive pulmonary disease in the Copenhagen City Heart Study. Annual FEV1 decline and CRP genotyping was determined in 1513 individuals with COPD. Partial r2 values were after adjustment for variation in annual FEV1 decline due to age, gender, smoking and body mass index. p Values are for Cuzick non-parametric test for trend of mean FEV1 decline, where CRP genotype/combination groups ranked according to increasing CRP levels have been coded 1, 2, 3 and so forth.

Predicted versus observed risk of COPD

We assumed that genetically elevated plasma CRP levels confer the same OR for COPD as that observed for plasma CRP levels in the general population. Based on this assumption, increments in plasma CRP levels of up to 62% as a function of CRP genotype combinations theoretically predicted ORs of up to 1.16 (1.09 to 1.23) for COPD and 1.35 (1.28 to 1.42) for hospitalisation due to COPD (figure 5). However, when COPD events and controls from all studies shown in figure 3 were combined to achieve the maximal statistical power, the observed ORs for COPD and hospitalisation due to COPD as a function of genotype combinations did not differ from 1.0 (figure 5). Genotype combinations #7–9 versus #1 resulted in an increase in plasma CRP of 45% and thus theoretically predicted an OR of 1.11 (1.07 to 1.16) for COPD and 1.25 (1.20 to 1.29) for hospitalisation due to COPD (figure 5). However, the observed ORs for COPD and hospitalisation due to COPD for genotype combinations #7–9 versus #1 were 1.05 (0.93 to 1.19) and 0.92 (0.77 to 1.10), respectively. Combining all individuals with COPD or hospitalisation due to COPD from the two studies, the #7–9 versus #1 genotype combinations had 80% power to detect ORs of 1.16 for spirometrically defined COPD and 1.22 for hospitalisation due to COPD (figure 5).

Figure 5

Predicted versus observed risk of chronic obstructive pulmonary disease (COPD) as a function of C reactive protein (CRP) genotype combination. The OR used for calculating the theoretically predicted risk of COPD was adjusted for age, sex, and smoking status. The ORs for the observed risk of COPD were adjusted for age, sex and smoking status. In order to achieve maximal statistical power, we combined all individuals with the nine most common CRP genotype combinations from the Copenhagen City Heart Study and the Copenhagen General Population Study (4613 COPD cases vs 38 667 controls and 2285 individuals hospitalised due to COPD vs 37 824 controls). The right column shows the OR at one-sided p<0.05 that can be detected in these combined studies at 80% statistical power.

On instrumental variable analysis a doubling of plasma CRP resulted in an OR of 1.27 (1.25 to 1.30) for COPD, while a doubling of genetically elevated CRP resulted in an OR of 1.01 (0.81 to 1.26) for COPD (p=0.04 for the comparison between the two ORs). Corresponding ORs for COPD hospitalisation were 1.47 (1.43 to 1.51) and 0.82 (0.59 to 1.13) (p=0.001).

Discussion

To examine whether genetically elevated plasma CRP is causally related to COPD, this study has measured high-sensitivity CRP in plasma, genotyped for variants in the CRP gene, and screened for COPD in 40 626 individuals from two ethnically homogenous Danish populations. Three salient findings are provided by the study: (1) plasma CRP above 3 mg/l is associated with increased risk for clinical COPD, (2) variants in the CRP gene are associated with elevated levels of plasma CRP and (3) analysing this data using a Mendelian randomisation design, we find that genetically elevated plasma CRP is not associated with risk of clinical COPD. This suggests that elevated plasma CRP is not causally related to COPD, but more likely serves as a marker of disease severity in COPD.

Consistent with our results van Durme et al have found that three tagging polymorphisms in the CRP gene (1184, 2042, 2911) are not associated with altered risk of COPD.16 In contrast to this, Sunyer et al found that the rs1205 polymorphism in the CRP gene and two haplotypes tagged by the rs1205 and rs1800947 polymorphisms were associated with better lung function.31 It is uncertain whether the two previous studies had enough genetic CRP range and study size to examine for causality between CRP and features of COPD. On instrumental variable analysis we now find that a doubling of plasma CRP resulted in an elevated risk for COPD outcomes, while a doubling of genetically elevated plasma CRP had no relation to COPD. This strongly suggests that the association between CRP levels and COPD is reverse causal or confounded by a third factor like inflammation in general.

Our results do not preclude clinical use for plasma CRP in the assessment of COPD. Plasma CRP may be a marker of prognosis in COPD as small increases are associated with a poor COPD prognosis in the present study and other studies.7 12 Plasma CRP may also be a marker of the efficacy of COPD therapy. Anti-inflammatory treatments that are beneficial towards COPD are linked with reduction in plasma CRP level in some14 32 33 but not all studies.34 It is possible that elevated plasma CRP in combination with other risk markers of lung disease can be used to categorise individuals with low, medium and high risk of future COPD or be used after further validation to guide the efficacy of therapy in COPD.32 33

The cause for the increased level of plasma CRP in COPD patients is not totally clear. One hypothesis suggests that plasma CRP is raised as a result of IL-6 production from the inflamed lungs in COPD. Cigarette smoking is the most commonly encountered risk factor for COPD and contributes to both lung inflammation and elevated CRP in COPD patients. Asthma, passive smoking, inhalation of outdoor and indoor air pollutants, obesity and physical inactivity could also cause lung inflammation and raise plasma CRP levels, and this could be particularly relevant among non-smoking COPD patients.

The potential limitations of the study also need to be considered. Mendelian randomisation can be used for the study of causation between modifiable exposures and disease, provided the following six criteria are fulfilled.35

  1. The presence of suitable genetic variants for the study of the modifiable exposure of interest: the CRP variant rs3091244 modulates transcription factor binding to the CRP gene and is the single most important polymorphism influencing CRP levels, while the CRP variants rs1130864, rs1205 and rs3093077 can be used as tag single nucleotide polymorphisms together describing most of the variation in plasma CRP levels.20

  2. Reliable genotype-intermediate-phenotype and genotype-disease associations can be established: we showed that the four CRP polymorphisms are associated with elevated plasma CRP levels, but not with risk of COPD in two independent studies analysing data from up to 44 359 individuals.

  3. There is no confounding of these relationships: linkage disequilibrium could not be detected between the four CRP polymorphisms used in our study and other known nearby genes potentially influencing plasma CRP and/or risk of COPD.20

  4. There are no pleiotropic effects of the genetic variants of interest: we are not aware of any known association of the four CRP polymorphisms with a phenotype besides changes in CRP level that could influence the risk of COPD.

  5. There is no compensation by other genes during development (canalisation)35 36: canalisation and compensation by other genes during development are generally difficult to assess; however, we are not aware of any such potential effects.

  6. Population admixture that differs between cases and controls: we studied two large and ethnically homogenous populations of Danish descent, and effectively can exclude admixture.

Hence, classical limitations of the Mendelian randomisation do not appear to be of major importance in the present study.

A large percentage of CRP variability depends on other non-genetic factors, and this could limit the Mendelian randomisation approach. Genetically determined CRP concentrations varied less than plasma CRP levels. It could be that plasma CRP causes COPD or protects from the disease at CRP levels beyond those determined by the CRP genotype data. However, there is a linear relationship between levels of CRP and risk of COPD in this study and there was sufficient statistical power to exclude a causal association between plasma CRP and COPD even within the limited plasma CRP range determined by the genotype data (figures 3 and 5). CRP is an acute phase reactant and was only measured once in our two cohorts. However, the results of the two studies were similar and when analysing only those subjects with CRP<10 mg/l the results were similar to those presented in this study.

We used both cross-sectional and prospective study designs to confirm our data in two independent cohorts and to achieve maximal statistical power for assessing a causal relationship between CRP and COPD. Since an established COPD implies the development of systemic inflammation, a cross-sectional study design does not seem to be the best option to explore causality using conventional epidemiology. On the contrary, the prospective study offers an excellent design to explore the relationship between CRP levels and incident COPD cases and hospitalisations. Therefore, even though the results obtained from both studies are similar, the results from the prospective study are the most important in this manuscript for the association between common CRP levels and COPD; for genetically derived CRP levels, the cross-sectional study is valid indeed, because the effect of the CRP single nucleotide polymorphisms on plasma CRP levels is lifelong. The phenotype of COPD differs by the two definitions used in our study; however, the results for the two definitions were also similar. We studied only Caucasian people and our results may not necessarily apply to other ethnic groups.

In conclusion, we find that lifelong genetically elevated CRP is not associated with risk of having COPD. This suggests that the association between CRP levels and COPD is not causal. The finding is similar to those from studies in cardiovascular disease where elevated CRP is associated with cardiovascular disease, but genetic variants of CRP were not associated with disease risk.20 37 Thus, our finding is not exclusive to COPD. It may be that for all chronic diseases associated with chronic inflammation, it is not the chronic inflammation with CRP elevation that causes disease but that the disease is driving chronic inflammation and CRP elevation.

Acknowledgments

We thank laboratory technicians Hanne Damm, Dorthe Uldall Andersen and Dorthe Kjeldgaard Hansen, Department of Clinical Biochemistry, Herlev Hospital for assisting with the large-scale genotyping.

References

Supplementary materials

  • Web Only Data thx.2009.131193

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Footnotes

  • Funding Danish Heart Foundation and Danish Lung Association.

  • Competing interests None.

  • Ethics approval This study was conducted with the approval of Herlev Hospital and Danish ethics committees.

  • Provenance and peer review Not commissioned; externally peer reviewed.