TY - JOUR T1 - Characterisation of clot microstructure properties in stable coronary artery disease JF - Open Heart JO - Open Heart DO - 10.1136/openhrt-2016-000562 VL - 4 IS - 2 SP - e000562 AU - Ahmed Sabra AU - Matthew James Lawrence AU - Robert Aubrey AU - Daniel Obaid AU - Alexander Chase AU - Dave Smith AU - Phillip Thomas AU - Sharon Storton AU - Gareth R Davies AU - Karl Hawkins AU - Phylip Rhodri Williams AU - Keith Morris AU - Phillip Adrian Evans Y1 - 2017/06/01 UR - http://openheart.bmj.com/content/4/2/e000562.abstract N2 - Background Coronary artery disease (CAD) is associated with an increased prothrombotic tendency and is also linked to unfavourably altered clot microstructure. We have previously described a biomarker of clot microstructure (df) that is unfavourably altered in acute myocardial infarction. The df biomarker assesses whether the blood will form denser or looser microstructures when it clots. In this study we assessed in patients with stable chest pain whether df can differentiate between obstructed and unobstructed CAD.Methods A blood sample prior to angiography was obtained from 251 consecutive patients undergoing diagnostic coronary angiography. Patients were categorised based on angiographic findings as presence or absence of obstructive CAD (stenosis ≥50%). The blood sample was assessed using the df biomarker, standard laboratory markers and platelet aggregometry (Multiplate).Results A significant difference (p=0.028) in df was observed between obstructive CAD (1.748±0.057, n=83) and unobstructive CAD (1.732±0.052, n=168), where patients with significant CAD produce denser, more tightly packed clots. df was also raised in men with obstructive CAD compared with women (1.745±0.055 vs 1.723±0.052, p=0.007). Additionally df significantly correlated with the platelets response to arachidonic acid as measured by the ASPItest area under the curve readings from platelet aggregometry (correlation coefficient=0.166, p=0.008), a low value of the ASPItest indicating effective aspirin use was associated with looser, less dense clots.Conclusions For the first time, we characterise clot microstructure, as measured by df, in patients with stable CAD. df can potentially be used to risk-stratify patients with stable CAD and assess the efficacy of therapeutic interventions by measuring changes in clot microstructure. ER -