Potency of Antiplatelet Drugs in MAFLD

Rationale: The aetiology of approximately 40% of all patients with cirrhosis is metabolic dysfunction associated fatty liver disease (MAFLD) – a percentage that is expected to only increase in the next decades. In addition to liver-related morbidity and mortality, there is a close relationship between MAFLD and risk of cardiovascular disease. Primary or secondary prevention of cardiovascular events generally consist of lifestyle advice, optimisation of blood glucose levels and blood pressure, use of statins and use of antiplatelet drugs. However, both platelet levels and platelet function appear to be altered in patients with chronic liver disease, which raises the question whether current strategies as used in the general population might be sufficient for this specific patient group.
Objective: To investigate the in vitro effect of clinically used antiplatelet drugs on platelet adhesion, activation and aggregation in patients with MAFLD.
Study design: A prospective cross-sectional, mono-center study.
Study population: One hundred and twenty patients with various stages of MAFLD, who have given informed consent will be included in this study. In addition, forty healthy controls will be recruited to establish reference values for the various tests employed.
Intervention (if applicable): The grade of liver steatosis and fibrosis will be determined by transient elastography (FibroScan). Blood samples (27 mL) will be drawn by venepuncture at the same time of routine blood tests.
Main study parameters/endpoints: The extent by which platelet reactivity decreases after in vitro addition of various active metabolites of antiplatelet drugs. Platelet reactivity will be assessed prior to and after addition of antiplatelet drugs by flow-based platelet adhesion assays, whole blood platelet aggregation tests, and flow cytometry-based approaches.

Platelet activity of patients with MAFLD after addition of antiplatelet drugs in vitro is similar to that of patients without MAFLD.

After verbal consent, the participant will be approached during their regular outpatient clinic appointment where the Informed Consent form can be signed and the participant can be included. Each participant will undergo an interview, blood sampling and FibroScan once, either right before or after their regular outpatient clinic appointment. For the participant, the study ends after these procedures have been completed.

The grade of liver steatosis and fibrosis will be determined by transient elastography (FibroScan). Blood samples (27 mL) will be drawn by venepuncture at the same time of routine blood tests.