Glycoprotein Acetyls: A Novel Inflammatory Biomarker of Early Cardiovascular Risk in the Young-Reference-Cited by-同舟云学术

Glycoprotein Acetyls: A Novel Inflammatory Biomarker of Early Cardiovascular Risk in the Young

Published:2022-02-15 Issue:4 Volume:11 Page:
ISSN:2047-9980
Container-title:Journal of the American Heart Association
language:en
Short-container-title:JAHA

Author:

Chiesa Scott T.¹^ORCID,Charakida Marietta²,Georgiopoulos Georgios²,Roberts Justin D.³,Stafford Simon J.⁴,Park Chloe⁵,Mykkänen Juha⁶⁷,Kähönen Mika⁸⁹,Lehtimäki Terho⁹¹⁰,Ala‐Korpela Mika¹¹¹²¹³,Raitakari Olli⁶⁷¹⁴,Pietiäinen Milla¹⁵,Pussinen Pirkko¹⁵^ORCID,Muthurangu Vivek¹⁶,Hughes Alun D.⁵¹⁷^ORCID,Sattar Naveed¹⁸^ORCID,Timpson Nicholas J.¹⁹²⁰,Deanfield John E.¹

Affiliation:

1. Institute of Cardiovascular Science University College London UK

2. Department of Imaging Science and Biomedical Engineering King’s College London UK

3. Cambridge Centre for Sport and Exercise Sciences Anglia Ruskin University Cambridge UK

4. Molecular Diagnostics Unit Medical Technology Research Centre Faculty of Health, Education, Medicine & Social Care Anglia Ruskin University Chelmsford UK

5. Cardiometabolic Phenotyping Group Institute of Cardiovascular Science University College London UK

6. Research Centre of Applied and Preventive Cardiovascular Medicine University of Turku Finland

7. Centre for Population Health Research University of Turku and Turku University Hospital Finland

8. Department of Clinical Physiology Tampere University Hospital Tampere Finland

9. Finnish Cardiovascular Research Center Tampere Faculty of Medicine and Health Technology Tampere University Tampere Finland

10. Department of Clinical Chemistry Fimlab Laboratories Tampere Finland

11. Computational Medicine Faculty of Medicine University of Oulu and Biocenter Oulu Finland

12. Center for Life Course Health Research University of Oulu Finland

13. NMR Metabolomics Laboratory School of Pharmacy University of Eastern Finland Kuopio Finland

14. Department of Clinical Physiology and Nuclear Medicine Turku University Hospital Turku Finland

15. Oral and Maxillofacial Diseases University of Helsinki and Helsinki University Hospital Helsinki Finland

16. Centre for Cardiovascular Imaging UCL Institute of Cardiovascular Science London United Kingdom

17. MRC Unit for Lifelong Health and AgeingUniversity College London UK

18. Institute of Cardiovascular and Medical Sciences British Heart Foundation (BHF) Glasgow Cardiovascular Research CentreUniversity of Glasgow UK

19. Population Health Sciences Bristol Medical School Faculty of Health Sciences University of Bristol UK

20. Medical Research Council Integrative Epidemiology Unit University of Bristol UK

Abstract

Background Low‐grade inflammation in the young may contribute to the early development of cardiovascular disease. We assessed whether circulating levels of glycoprotein acetyls (GlycA) were better able to predict the development of adverse cardiovascular disease risk profiles compared with the more commonly used biomarker high‐sensitivity CRP (C‐reactive protein). Methods and Results A total of 3306 adolescents and young adults from the Avon Longitudinal Study of Parents and Children (mean age, 15.4±0.3; n=1750) and Cardiovascular Risk in Young Finns Study (mean age, 32.1±5.0; n=1556) were included. Baseline associations between inflammatory biomarkers, body composition, cardiovascular risk factors, and subclinical measures of vascular dysfunction were assessed cross‐sectionally in both cohorts. Prospective risk of developing hypertension and metabolic syndrome during 9‐to‐10‐year follow‐up were also assessed as surrogate markers for future cardiovascular risk. GlycA showed greater within‐subject correlation over 9‐to‐10‐year follow‐up in both cohorts compared with CRP, particularly in the younger adolescent group (r=0.36 versus 0.07). In multivariable analyses, GlycA was found to associate with multiple lifestyle‐related cardiovascular disease risk factors, cardiometabolic risk factor burden, and vascular dysfunction (eg, mean difference in flow‐mediated dilation=−1.2 [−1.8, −0.7]% per z‐score increase). In contrast, CRP levels appeared predominantly driven by body mass index and showed little relationship to any measured cardiovascular risk factors or phenotypes. In both cohorts, only GlycA predicted future risk of both hypertension (risk ratio [RR], ≈1.1 per z‐score increase for both cohorts) and metabolic syndrome (RR, ≈1.2–1.3 per z‐score increase for both cohorts) in 9‐to‐10‐year follow‐up. Conclusions Low‐grade inflammation captured by the novel biomarker GlycA is associated with adverse cardiovascular risk profiles from as early as adolescence and predicts future risk of hypertension and metabolic syndrome in up to 10‐year follow‐up. GlycA is a stable inflammatory biomarker which may capture distinct sources of inflammation in the young and may provide a more sensitive measure than CRP for detecting early cardiovascular risk.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

Reference47 articles.

1. C-reactive protein and its role in metabolic syndrome: mendelian randomisation study

2. C-Reactive Protein, the Metabolic Syndrome, and Risk of Incident Cardiovascular Events

3. C-Reactive Protein, the Metabolic Syndrome, and Prediction of Cardiovascular Events in the Framingham Offspring Study

4. Life-Course Implications of Pediatric Risk Factors for Cardiovascular Disease

5. C-Reactive Protein and Features of the Metabolic Syndrome in a Population-Based Sample of Children and Adolescents

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