Epigenetic Regulation of F2RL3 Associates With Myocardial Infarction and Platelet Function

Laura J Corbin; Stephen J White; Amy E Taylor; Christopher M Williams; Kurt Taylor; Marion T van den Bosch; Jack E Teasdale; Matthew Jones; Mark Bond; Matthew T Harper; Louise Falk; Alix Groom; Georgina G J Hazell; Lavinia Paternoster; Marcus R Munafò; Børge G Nordestgaard; Anne Tybjærg-Hansen; Stig E Bojesen; Caroline Relton; Josine L Min; George Davey Smith; Andrew D Mumford; Alastair W Poole; Nicholas J Timpson

doi:10.1161/CIRCRESAHA.121.318836

Epigenetic Regulation of F2RL3 Associates With Myocardial Infarction and Platelet Function

Circ Res. 2022 Feb 4;130(3):384-400. doi: 10.1161/CIRCRESAHA.121.318836. Epub 2022 Jan 11.

Authors

Laura J Corbin^{1

2}, Stephen J White³, Amy E Taylor^{2

4}, Christopher M Williams^{2

5}, Kurt Taylor², Marion T van den Bosch⁵, Jack E Teasdale⁶, Matthew Jones⁶, Mark Bond⁶, Matthew T Harper⁷, Louise Falk^{1

2}, Alix Groom^{1

2}, Georgina G J Hazell⁷, Lavinia Paternoster^{1

2}, Marcus R Munafò^{1

8}, Børge G Nordestgaard^{9

10

11}, Anne Tybjærg-Hansen^{10

12

11}, Stig E Bojesen^{9

10

11}, Caroline Relton^{1

2}, Josine L Min^{1

2}, George Davey Smith^{1

2}, Andrew D Mumford¹³, Alastair W Poole⁵, Nicholas J Timpson^{1

2}

Affiliations

¹ MRC Integrative Epidemiology Unit at University of Bristol, United Kingdom (L.J.C., L.F., A.G., L.P., M.R.M., C.R., J.L.M., G.D.S., N.J.T.).
² Population Health Sciences, Bristol Medical School (L.J.C., A.E.T., K.T., L.F., A.G., L.P., C.R., J.L.M., G.D.S., N.J.T.), University of Bristol, United Kingdom.
³ Department of Life Sciences, Manchester Metropolitan University, United Kingdom (S.J.W.).
⁴ NIHR Biomedical Research Centre at the University Hospitals Bristol NHS Foundation Trust and the University of Bristol, United Kingdom (A.E.T.).
⁵ School of Physiology, Pharmacology and Neuroscience (C.M.W., M.T.v.d.B., A.W.P.), University of Bristol, United Kingdom.
⁶ Translational Health Sciences, Bristol Medical School (J.E.T., M.J., M.B.), University of Bristol, United Kingdom.
⁷ Department of Pharmacology, University of Cambridge, Tennis Court Road (M.T.H., G.G.J.H.).
⁸ UK Centre for Tobacco and Alcohol Studies and School of Experimental Psychology (M.R.M.), University of Bristol, United Kingdom.
⁹ Department of Clinical Biochemistry, Herlev and Gentofte Hospital (B.G.N., S.E.B.), Copenhagen University Hospital, Denmark.
¹⁰ The Copenhagen City Heart Study, Frederiksberg Hospital (B.G.N., A.T.-H., S.E.B.), Copenhagen University Hospital, Denmark.
¹¹ Faculty of Health and Medical Sciences, University of Copenhagen, Denmark (B.G.N., A.T.-H., S.E.B.).
¹² Department of Clinical Biochemistry, Rigshospitalet (A.T.-H.), Copenhagen University Hospital, Denmark.
¹³ School of Cellular and Molecular Medicine (A.D.M.), University of Bristol, United Kingdom.

Abstract

Background: DNA hypomethylation at the F2RL3 (F2R like thrombin or trypsin receptor 3) locus has been associated with both smoking and atherosclerotic cardiovascular disease; whether these smoking-related associations form a pathway to disease is unknown. F2RL3 encodes protease-activated receptor 4, a potent thrombin receptor expressed on platelets. Given the role of thrombin in platelet activation and the role of thrombus formation in myocardial infarction, alterations to this biological pathway could be important for ischemic cardiovascular disease.

Methods: We conducted multiple independent experiments to assess whether DNA hypomethylation at F2RL3 in response to smoking is associated with risk of myocardial infarction via changes to platelet reactivity. Using cohort data (N=3205), we explored the relationship between smoking, DNA hypomethylation at F2RL3, and myocardial infarction. We compared platelet reactivity in individuals with low versus high DNA methylation at F2RL3 (N=41). We used an in vitro model to explore the biological response of F2RL3 to cigarette smoke extract. Finally, a series of reporter constructs were used to investigate how differential methylation could impact F2RL3 gene expression.

Results: Observationally, DNA methylation at F2RL3 mediated an estimated 34% of the smoking effect on increased risk of myocardial infarction. An association between methylation group (low/high) and platelet reactivity was observed in response to PAR4 (protease-activated receptor 4) stimulation. In cells, cigarette smoke extract exposure was associated with a 4.9% to 9.3% reduction in DNA methylation at F2RL3 and a corresponding 1.7-(95% CI, 1.2-2.4, P=0.04) fold increase in F2RL3 mRNA. Results from reporter assays suggest the exon 2 region of F2RL3 may help control gene expression.

Conclusions: Smoking-induced epigenetic DNA hypomethylation at F2RL3 appears to increase PAR4 expression with potential downstream consequences for platelet reactivity. Combined evidence here not only identifies F2RL3 DNA methylation as a possible contributory pathway from smoking to cardiovascular disease risk but from any feature potentially influencing F2RL3 regulation in a similar manner.

Keywords: DNA methylation; blood platelets; epigenomics; myocardial infarction; smoking; thrombin; tobacco.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Aged
Blood Platelets / metabolism*
DNA Methylation
Epigenesis, Genetic*
Female
Humans
Male
Middle Aged
Myocardial Infarction / blood
Myocardial Infarction / epidemiology
Myocardial Infarction / genetics*
Receptors, Thrombin / genetics*
Receptors, Thrombin / metabolism
Smoking / epidemiology

Substances

Receptors, Thrombin
protease-activated receptor 4

Abstract

Publication types

MeSH terms

Substances

Grants and funding