Eicosanoid Inflammatory Mediators Are Robustly Associated With Blood Pressure in the General Population

Author:

Palmu Joonatan12ORCID,Watrous Jeramie D.3,Mercader Kysha3ORCID,Havulinna Aki S.24ORCID,Lagerborg Kim A.3ORCID,Salosensaari Aaro15ORCID,Inouye Mike67,Larson Martin G.78,Rong Jian7,Vasan Ramachandran S.79ORCID,Lahti Leo5ORCID,Andres Allen3ORCID,Cheng Susan71011ORCID,Jousilahti Pekka2ORCID,Salomaa Veikko2ORCID,Jain Mohit3,Niiranen Teemu J.1212ORCID

Affiliation:

1. Department of Internal Medicine University of Turku Finland

2. Department of Public Health Solutions Finnish Institute for Health and Welfare Turku and Helsinki Finland

3. Departments of Medicine and Pharmacology University of California, San Diego CA

4. Institute for Molecular Medicine Finland and Helsinki Institute of Life Science Helsinki Finland

5. Department of Future Technologies University of Turku Finland

6. Department of Public Health and Primary Care University of Cambridge United Kingdom

7. National Heart, Lung and Blood Institute's and Boston University's Framingham Heart Study Framingham MA

8. Department of Biostatistics Boston University School of Public Health Boston MA

9. Sections of Preventive Medicine and Epidemiology, and Cardiovascular Medicine Department of Medicine Department of Epidemiology Boston University Schools of Medicine and Public Health Boston MA

10. Division of Cardiology Brigham and Women's Hospital Boston MA

11. Smidt Heart InstituteCedars‐Sinai Medical Center Los Angeles CA

12. Division of Medicine Turku University Hospital Turku Finland

Abstract

Background Epidemiological and animal studies have associated systemic inflammation with blood pressure (BP). However, the mechanistic factors linking inflammation and BP remain unknown. Fatty acid–derived eicosanoids serve as mediators of inflammation and have been suggested to regulate renal vascular tone, peripheral resistance, renin‐angiotensin system, and endothelial function. We hypothesize that specific proinflammatory and anti‐inflammatory eicosanoids are linked with BP. Methods and Results We studied a population sample of 8099 FINRISK 2002 participants randomly drawn from the Finnish population register (53% women; mean age, 48±13 years) and, for external validation, a sample of 2859 FHS (Framingham Heart Study) Offspring study participants (55% women; mean age, 66±9 years). Using nontargeted liquid chromatography–mass spectrometry, we profiled 545 distinct high‐quality eicosanoids and related oxylipin mediators in plasma. Adjusting for conventional hypertension risk factors, we observed 187 (34%) metabolites that were significantly associated with systolic BP ( P <Bonferroni‐corrected threshold of 0.05/545). We used forward selection linear regression modeling in FINRISK to define a general formula for individual eicosanoid risk score. Individuals of the top risk score quartile in FINRISK had a 9.0 (95% CI, 8.0–10.1) mm Hg higher systolic BP compared with individuals in the lowest quartile in fully adjusted models. Observed metabolite associations were consistent across FINRISK and FHS. Conclusions Plasma eicosanoids demonstrate strong associations with BP in the general population. As eicosanoid compounds affect numerous physiological processes that are central to BP regulation, they may offer new insights about the pathogenesis of hypertension, as well as serve as potential targets for therapeutic intervention.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

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