[No authors listed]
Molecular imaging of inflammatory mediators in atria may contribute to thrombotic risk assessment of atrial fibrillation (AF). We investigated the feasibility of ultrasound molecular imaging (UMI) targeted to P-selectin to assess thrombotic risk in AF. Rat AF models were established with rapid atrial pacing. Microbubbles targeted to P-selectin were injected into the rats, followed by left atrial (LA) UMI examination. Furthermore, P-selectin, platelets (PLTs), fibrin and tissue factor (TF) of LA were detected by histopathology and scanning electron microscopy. Plasma levels of P-selectin, thrombin-antithrombin complex (TAT) and prothrombin fragment 1â+â2 (F1â+â2) were measured by enzyme-linked immunosorbent assay. The data showed that P-selectin in LA was correlated with PLT, fibrin and TF (râ=â0.735, pâ<â0.05; râ=â0.827, pâ<â0.05; râ=â0.785, pâ<â0.05, respectively). The plasma level of P-selectin was correlated with the expression of TAT and F1â+â2 (râ=â0.866, pâ<â0.05; râ=â0.916, pâ<â0.05, respectively). The contrast video intensity of adhered microbubbles targeted to P-selectin was correlated with the levels of P-selectin, PLT and fibrin in LA (râ=â0.768, pâ<â0.05; râ=â0.798, pâ<â0.05; râ=â0.745, pâ<â0.05, respectively). In conclusion, P-selectin may serve as a biomarker for thrombotic risk in AF and can be quantified by UMI to assess thrombotic risk.
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