Subtle renal dysfunction and bleeding risk in atrial fibrillation: symmetric dimethylarginine predicts HAS-BLED score

Nathan Ek Procter; Jocasta Ball; Tamila Heresztyn; Vivek B Nooney; Saifei Liu; Cher-Rin Chong; Doan Tm Ngo; Jeffrey S Isenberg; Yuliy Y Chirkov; Simon Stewart; John D Horowitz

Subtle renal dysfunction and bleeding risk in atrial fibrillation: symmetric dimethylarginine predicts HAS-BLED score

Am J Cardiovasc Dis. 2015 Aug 1;5(2):101-9. eCollection 2015.

Authors

Affiliations

¹ Basil Hetzel Institute, The Queen Elizabeth Hospital, University of Adelaide Australia.
² Centre for The Heart and Mind, Mary MacKillop Institute for Health Research, Australian Catholic University Melbourne, Australia.
³ Basil Hetzel Institute, The Queen Elizabeth Hospital, University of South Australia Australia.
⁴ Heart, Lung, Blood and Vascular Medicine Institute, Division of Pulmonary, Allergy and Critical Care Medicine, Department of Medicine, University of Pittsburgh Pittsburgh, Pennsylvania, U.S.
⁵ National Health and Medical Research Council (NHMRC) Centre of Excellence to Reduce Inequality in Heart Disease, Mary MacKillop Institute for Health Research, Australian Catholic University Melbourne, Australia ; Baker IDI Heart and Diabetes Institute Melbourne, Australia.

PMID: 26309773
PMCID: PMC4539096

Abstract

Background: Risk of substantial haemorrhage represents a critically important limitation to effective anti-thrombotic treatment in patients with atrial fibrillation (AF). While it is known that this risk is increased in anticoagulated patients either in the presence of anti-aggregatory drugs or concomitant renal insufficiency, there are currently few data on the potential interactions between endogenous platelet aggregability and bleeding risk.

Objective: We therefore evaluated in a cohort of AF patients: (1), the putative relationship between platelet aggregability and HAS-BLED score; (2), the potential biochemical bases for such a relationship.

Methods: Patients were included as part of SAFETY, a randomised controlled trial evaluating outpatient management of AF patients. Platelet response to ADP was evaluated via whole blood impedance aggregometry; clinical and biochemical correlates of platelet aggregation were sought via univariate and multivariate analysis.

Results: Platelet aggregation correlated inversely (r=-0.220, p<0.05) with HAS-BLED score. Univariate biochemical correlates of decreased platelet aggregation were plasma concentrations of symmetric dimethylarginine (SDMA) and asymmetric dimethylarginine (ADMA). On multivariate analyses, plasma SDMA concentration (β=-0.318, p<0.01), platelet content of thioredoxin-interacting protein (Txnip, β=0.261, p<0.05) and plasma thrombospondin-1 (TSP-1, β=0.249, p<0.05) concentration were predictive of platelet ADP response. Consistent with previous reports, plasma SDMA concentrations were strongly and inversely correlated with estimated glomerular filtration rate (eGFR, r=-0.780, p<0.001).

Conclusions: These data therefore suggest that (1), physiologically impaired, like pharmacologically impaired, platelet aggregability may increase bleeding risk in anticoagulated AF patients; (2), the biochemical basis for this may include impaired effects of nitric oxide (via Txnip, TSP-1) but also concomitant renal dysfunction.

Keywords: Atrial fibrillation; platelet aggregation; symmetric dimethylarginine; thioredoxin-interacting protein; thrombospondin-1.

Abstract

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