Low-density lipoprotein cholesterol and risk of COPD: a Mendelian randomization study

Josefine Freyberg Justesen; Benjamin Nilsson Wadström; Sarah Caroline Weisenfeldt Marott; Eskild Morten Landt; Børge Grønne Nordestgaard; Shoaib Afzal; Morten Dahl

doi:10.1038/s41598-026-48823-6

Low-density lipoprotein cholesterol and risk of COPD: a Mendelian randomization study

Josefine Freyberg Justesen, Benjamin Nilsson Wadström, Sarah Caroline Weisenfeldt Marott, Eskild Morten Landt, Børge Grønne Nordestgaard, Shoaib Afzal, Morten Dahl^*

^*Corresponding author af dette arbejde

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

Abstract

Statins have shown effects on exacerbation rates and lung function in individuals with chronic obstructive pulmonary disease (COPD) in randomized controlled trials. This has led to speculation that elevated LDL cholesterol may increase the risk of adverse COPD outcomes. We tested the hypothesis that high LDL cholesterol is causally associated with increased risk of severe COPD exacerbation, COPD-specific mortality, and spirometric COPD through a one-sample Mendelian randomization study design using individual-level data in two cohorts. We examined 108,438 adults from the Copenhagen General Population Study (CGPS). A weighted allele score was calculated using nine biologically relevant genetic variants associated with LDL cholesterol levels, and causal risk estimates for the three outcomes were determined using instrumental variable analysis. Findings were validated using one-sample Mendelian randomization in 389,627 individuals from the UK Biobank (UKB). Causal odds ratios from the CGPS were not statistically significant for severe COPD exacerbation (odds ratio (OR) 1.12 (95% CI: 0.88–1.42), p = 0.34) or COPD-specific mortality (OR 1.08 (0.69–1.69), p = 0.74). Similar findings were seen in the UKB. Causal estimates showed a decreased risk of cross-sectional spirometric COPD with 1 mmol/L (39 mg/dL) higher LDL cholesterol in the CGPS (OR 0.78 (0.66–0.92), p < 0.001); however, causal estimates were not statistically significant in the UKB (OR 1.03 (0.95–1.11), p = 0.50). Sensitivity analyses using MR Egger, inverse-variance weighted, weighted median, and weighted mode methods did not indicate a true causal association for any outcome in either cohort. In conclusion, in the CGPS and UKB, high LDL cholesterol did not causally increase the risk of severe COPD exacerbation and COPD-specific mortality. Further, our findings do not provide consistent evidence to support a causal role of high LDL cholesterol in reducing the risk of developing COPD.

Originalsprog	Engelsk
Tidsskrift	Scientific Reports
ISSN	2045-2322
DOI	https://doi.org/10.1038/s41598-026-48823-6
Status	E-pub ahead of print - 15 apr. 2026

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title = "Low-density lipoprotein cholesterol and risk of COPD: a Mendelian randomization study",

abstract = "Statins have shown effects on exacerbation rates and lung function in individuals with chronic obstructive pulmonary disease (COPD) in randomized controlled trials. This has led to speculation that elevated LDL cholesterol may increase the risk of adverse COPD outcomes. We tested the hypothesis that high LDL cholesterol is causally associated with increased risk of severe COPD exacerbation, COPD-specific mortality, and spirometric COPD through a one-sample Mendelian randomization study design using individual-level data in two cohorts. We examined 108,438 adults from the Copenhagen General Population Study (CGPS). A weighted allele score was calculated using nine biologically relevant genetic variants associated with LDL cholesterol levels, and causal risk estimates for the three outcomes were determined using instrumental variable analysis. Findings were validated using one-sample Mendelian randomization in 389,627 individuals from the UK Biobank (UKB). Causal odds ratios from the CGPS were not statistically significant for severe COPD exacerbation (odds ratio (OR) 1.12 (95% CI: 0.88–1.42), p = 0.34) or COPD-specific mortality (OR 1.08 (0.69–1.69), p = 0.74). Similar findings were seen in the UKB. Causal estimates showed a decreased risk of cross-sectional spirometric COPD with 1 mmol/L (39 mg/dL) higher LDL cholesterol in the CGPS (OR 0.78 (0.66–0.92), p < 0.001); however, causal estimates were not statistically significant in the UKB (OR 1.03 (0.95–1.11), p = 0.50). Sensitivity analyses using MR Egger, inverse-variance weighted, weighted median, and weighted mode methods did not indicate a true causal association for any outcome in either cohort. In conclusion, in the CGPS and UKB, high LDL cholesterol did not causally increase the risk of severe COPD exacerbation and COPD-specific mortality. Further, our findings do not provide consistent evidence to support a causal role of high LDL cholesterol in reducing the risk of developing COPD.",

author = "Justesen, {Josefine Freyberg} and Wadstr{\"o}m, {Benjamin Nilsson} and Marott, {Sarah Caroline Weisenfeldt} and Landt, {Eskild Morten} and Nordestgaard, {B{\o}rge Gr{\o}nne} and Shoaib Afzal and Morten Dahl",

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doi = "10.1038/s41598-026-48823-6",

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TY - JOUR

T1 - Low-density lipoprotein cholesterol and risk of COPD

T2 - a Mendelian randomization study

AU - Justesen, Josefine Freyberg

AU - Wadström, Benjamin Nilsson

AU - Marott, Sarah Caroline Weisenfeldt

AU - Landt, Eskild Morten

AU - Nordestgaard, Børge Grønne

AU - Afzal, Shoaib

AU - Dahl, Morten

PY - 2026/4/15

Y1 - 2026/4/15

N2 - Statins have shown effects on exacerbation rates and lung function in individuals with chronic obstructive pulmonary disease (COPD) in randomized controlled trials. This has led to speculation that elevated LDL cholesterol may increase the risk of adverse COPD outcomes. We tested the hypothesis that high LDL cholesterol is causally associated with increased risk of severe COPD exacerbation, COPD-specific mortality, and spirometric COPD through a one-sample Mendelian randomization study design using individual-level data in two cohorts. We examined 108,438 adults from the Copenhagen General Population Study (CGPS). A weighted allele score was calculated using nine biologically relevant genetic variants associated with LDL cholesterol levels, and causal risk estimates for the three outcomes were determined using instrumental variable analysis. Findings were validated using one-sample Mendelian randomization in 389,627 individuals from the UK Biobank (UKB). Causal odds ratios from the CGPS were not statistically significant for severe COPD exacerbation (odds ratio (OR) 1.12 (95% CI: 0.88–1.42), p = 0.34) or COPD-specific mortality (OR 1.08 (0.69–1.69), p = 0.74). Similar findings were seen in the UKB. Causal estimates showed a decreased risk of cross-sectional spirometric COPD with 1 mmol/L (39 mg/dL) higher LDL cholesterol in the CGPS (OR 0.78 (0.66–0.92), p < 0.001); however, causal estimates were not statistically significant in the UKB (OR 1.03 (0.95–1.11), p = 0.50). Sensitivity analyses using MR Egger, inverse-variance weighted, weighted median, and weighted mode methods did not indicate a true causal association for any outcome in either cohort. In conclusion, in the CGPS and UKB, high LDL cholesterol did not causally increase the risk of severe COPD exacerbation and COPD-specific mortality. Further, our findings do not provide consistent evidence to support a causal role of high LDL cholesterol in reducing the risk of developing COPD.

AB - Statins have shown effects on exacerbation rates and lung function in individuals with chronic obstructive pulmonary disease (COPD) in randomized controlled trials. This has led to speculation that elevated LDL cholesterol may increase the risk of adverse COPD outcomes. We tested the hypothesis that high LDL cholesterol is causally associated with increased risk of severe COPD exacerbation, COPD-specific mortality, and spirometric COPD through a one-sample Mendelian randomization study design using individual-level data in two cohorts. We examined 108,438 adults from the Copenhagen General Population Study (CGPS). A weighted allele score was calculated using nine biologically relevant genetic variants associated with LDL cholesterol levels, and causal risk estimates for the three outcomes were determined using instrumental variable analysis. Findings were validated using one-sample Mendelian randomization in 389,627 individuals from the UK Biobank (UKB). Causal odds ratios from the CGPS were not statistically significant for severe COPD exacerbation (odds ratio (OR) 1.12 (95% CI: 0.88–1.42), p = 0.34) or COPD-specific mortality (OR 1.08 (0.69–1.69), p = 0.74). Similar findings were seen in the UKB. Causal estimates showed a decreased risk of cross-sectional spirometric COPD with 1 mmol/L (39 mg/dL) higher LDL cholesterol in the CGPS (OR 0.78 (0.66–0.92), p < 0.001); however, causal estimates were not statistically significant in the UKB (OR 1.03 (0.95–1.11), p = 0.50). Sensitivity analyses using MR Egger, inverse-variance weighted, weighted median, and weighted mode methods did not indicate a true causal association for any outcome in either cohort. In conclusion, in the CGPS and UKB, high LDL cholesterol did not causally increase the risk of severe COPD exacerbation and COPD-specific mortality. Further, our findings do not provide consistent evidence to support a causal role of high LDL cholesterol in reducing the risk of developing COPD.

U2 - 10.1038/s41598-026-48823-6

DO - 10.1038/s41598-026-48823-6

M3 - Journal article

C2 - 41986588

SN - 2045-2322

JO - Scientific Reports

JF - Scientific Reports

ER -