Genome-wide association study of post COVID-19 syndrome in a population-based cohort in Germany

被引:0
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作者
Anne-Kathrin Ruß [1 ]
Stefan Schreiber [2 ]
Wolfgang Lieb [3 ]
J. Janne Vehreschild [2 ]
Peter U. Heuschmann [4 ]
Thomas Illig [5 ]
Katharina S. Appel [6 ]
Maria J. G. T. Vehreschild [7 ]
Dagmar Krefting [8 ]
Lennart Reinke [9 ]
Alin Viebke [10 ]
Susanne Poick [4 ]
Stefan Störk [11 ]
Jens-Peter Reese [12 ]
Thomas Zoller [13 ]
Lilian Krist [3 ]
David Ellinghaus [3 ]
Bärbel U. Foesel [2 ]
Christian Gieger [3 ]
Bettina Lorenz-Depiereux [14 ]
Martin Witzenrath [15 ]
Gabriele Anton [6 ]
Michael Krawczak [7 ]
Jan Heyckendorf [16 ]
Thomas Bahmer [17 ]
机构
[1] Kiel University,Institute of Medical Informatics and Statistics, University Medical Center Schleswig
[2] Kiel University,Holstein
[3] University Medical Center Schleswig-Holstein,Institute of Epidemiology, University Medical Center Schleswig
[4] Goethe University Frankfurt,Holstein
[5] University Hospital CologneUniversity of Cologne,Department of Internal Medicine I
[6] University of Würzburg,Institute of Digital Medicine and Clinical Data Science, Faculty of Medicine
[7] University Hospital Würzburg,Department I of Internal Medicine, Faculty of Medicine
[8] University Hospital Würzburg,Institute of Clinical Epidemiology and Biometry
[9] Hannover Unified Biobank,Institute of Medical Data Science
[10] Hannover Medical School,Clinical Trial Center
[11] German Center for Lung Research,Biomedical Research in Endstage and Obstructive Lung Disease Hannover
[12] Goethe University Frankfurt,Medical Department 2, Center for Internal Medicine, University Hospital Frankfurt
[13] University Medical Center Göttingen,Department of Medical Informatics
[14] Campus Institute Data Sciences,Department of Clinical Research and Epidemiology, Comprehensive Heart Failure Center
[15] University Hospital Würzburg,Department of Internal Medicine I
[16] University Hospital Würzburg,Faculty of Health Sciences
[17] THM University of Applied Sciences,Department of Infectious Diseases, Respiratory and Critical Care Medicine
[18] Charité - Universitätsmedizin Berlin,Institute of Social Medicine, Epidemiology and Health Economics
[19] Freie Universität Berlin,Institute of Clinical Molecular Biology
[20] Humboldt-Universität zu Berlin,Institute of Epidemiology, Research Unit of Molecular Epidemiology
[21] Charité - Universitätsmedizin Berlin,Department of Infectious Diseases and Critical Care Medicine
[22] Freie Universität Berlin,Medical School OWL
[23] Humboldt-Universität zu Berlin,Airway Research Center North (ARCN)
[24] University Medical Center Schleswig-Holstein,undefined
[25] Kiel University,undefined
[26] Helmholtz Munich - German Research Center for Environmental Health,undefined
[27] Charité - Universitätsmedizin Berlin,undefined
[28] Freie Universität Berlin,undefined
[29] Humboldt-Universität zu Berlin,undefined
[30] CAPNETZ Stiftung,undefined
[31] Bielefeld University,undefined
[32] German Center for Lung Research (DZL),undefined
[33] Leibniz Lung Clinic,undefined
关键词
SARS-CoV-2; Long-COVID; Genotype-phenotype association; Linkage disequilibrium; Single nucleotide polymorphism; Olfactory receptor; Virus repression; Macrophage activation;
D O I
10.1038/s41598-025-00945-z
中图分类号
学科分类号
摘要
If health impairments due to coronavirus disease 2019 (COVID-19) persist for 12 weeks or longer, patients are diagnosed with Post-COVID Syndrome (PCS), or Long-COVID. Although the COVID-19 pandemic has largely subsided in 2024, PCS is still a major health burden worldwide, and identifying potential genetic modifiers of PCS remains of great clinical and scientific interest. We therefore performed a case-control type genome-wide association study (GWAS) of three recently developed PCS (severity) scores in 2,247 participants of COVIDOM, a prospective, multi-centre, population-based cohort study of SARS-CoV-2-infected individuals in Germany. Each PCS score originally represented the weighted sum of the binary indicators of all, or a subset, of 12 PCS symptom complexes, assessed six months or later after the PCR test-confirmed SARS-CoV-2 infection of a participant. For various methodical reasons, however, the PCS scores were dichotomized along their respective median values in the present study, prior to the GWAS. Of the 6,383,167 single nucleotide polymorphisms included, various variants were found to be associated with at least one of the PCS scores, although not at the stringent genome-wide statistical significance level of 5 × 10− 8. With p = 6.6 × 10− 8, however, the genotype-phenotype association of SNP rs9792535 at position chr9:127,166,653 narrowly missed this threshold. The SNP is located in a region including the NEK6, PSMB7 and ADGRD2 genes which, however, does not immediately suggest an etiological connection to PCS. As regards functional plausibility, variants of a possible effect mapped to the olfactory receptor gene region (lead SNP rs10893121 at position chr11:123,854,744; p = 2.5 × 10− 6). Impairment of smell and taste is a pathognomonic feature of both, acute COVID-19 and PCS, and our results suggest that this connection may have a genetic basis. Three other genotype-phenotype associations pointed towards a possible etiological role in PCS of cellular virus repression (CHD6 gene region), activation of macrophages (SLC7A2) and the release of virus particles from infected cells (ARHGAP44). All other gene regions highlighted by our GWAS did not relate to pathophysiological processes currently discussed for PCS. Therefore, and because the genotype-phenotype associations observed in our GWAS were generally not very strong, the complexity of the genetic background of PCS appears to be as high as that of most other multifactorial traits in humans.
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