Rivaroxaban reduced recurrent stroke by 74% in patients with atrial diameter >46 mm compared to aspirin, emphasizing the need for tailored anticoagulation strategies in ESUS.
Do individualized diagnostic markers and targeted anticoagulation strategies reduce recurrent stroke and improve atrial fibrillation detection in patients with Embolic Stroke of Undetermined Source?
Patients with Embolic Stroke of Undetermined Source (ESUS) from 7 pivotal trials (NAVIGATE ESUS, RESPECT ESUS, CRYSTAL AF, ARCADIA, COMPASS, ESCAPE NA, and AF ESUS)
Individualized diagnostic markers (Cardiac MRI, PTFV1, NT-proBNP, LA diameter, extended ECG monitoring) and targeted anticoagulation strategies (rivaroxaban, dabigatran)
Standard secondary prevention (antiplatelets/aspirin)
Recurrent stroke and atrial fibrillation incidencehard clinical
Moving beyond a uniform antiplatelet approach to individualized risk assessment using biomarkers, imaging, and targeted anticoagulation may optimize secondary stroke prevention in ESUS.
Method: We conducted a targeted synthesis of seven pivotal trials, NAVIGATE ESUS, RESPECT ESUS, CRYSTAL AF, ARCADIA, COMPASS, ESCAPE NA, and AF ESUS, to explore diagnostic markers and therapeutic implications for optimizing individualized ESUS management. Results: Key ESUS sources with diagnostic and therapeutic implications may inform individualized care 1. Moderate LV dysfunction (LVEF 40 percent) and regional wall motion abnormalities are common in ESUS and may increase embolic risk. An exploratory NAVIGATE ESUS analysis showed rivaroxaban reduced recurrent stroke vs.aspirin in this group. Risk stratification using Cardiac MRI, with higher LV thrombus sensitivity, alongside ECHO, may help identify patient population for anticoagulation (AC). 2. Atrial cardiopathy markers, PTFV1, NT-proBNP >250 pg mL and LA diameter >3 cm msquare are prospectively linked to stroke risk, despite ARCADIA’s neutral findings. PTFV1 reflects LA pathophysiology, with evidence connecting elevated PTFV1 and LA enlargement to cryptogenic stroke. NAVIGATE ESUS showed a 74% stroke reduction with rivaroxaban in patients with LA diameter >46 mm, underscoring the need to refine AC selection markers. 3. RE-SPECT ESUS linked NT-proBNP >505 pg/mL and older age to higher AFib incidence, with age >75 benefiting from low-dose dabigatran. CRYSTAL AF associated older age and prolonged PR interval with AFib. Extended cardiac/ECG monitoring is warranted in patients with elevated NT-proBNP, age >75, HAVOC scores ≥3 to identify covert AFib and guide anticoagulation. 4. NAVIGATE ESUS, ESCAPE NA, and RE-SPECT ESUS identified carotid plaques ≥3 mm and 30–50% stenosis as key ipsilateral stroke markers. AF-ESUS showed lower Afib detection in ESUS patients with such plaques. In younger cryptogenic stroke patients, a negative plaque–PFO association was observed, supporting non-stenosing atherosclerosis as a stroke source. COMPASS trial secondary analyses suggest rivaroxaban plus aspirin may reduce recurrence by up to 70% in stable and possibly non-stenotic atherosclerosis. Similar trends emerged- AREST ESUS pilot. This approach necessitates individualized risk assessment. Conclusion: Despite antiplatelets remaining the standard for secondary prevention, ESUS carries a 5% annual recurrence. This review underscores a need to move beyond a uniform approach—highlighting how emerging biomarkers, imaging modalities, and targeted anticoagulation strategies could help individualize stroke prevention in specific ESUS population.
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SAGARIKA GOPALKRISHNAN
Saad Hasan
Prachi Raichur
Stroke
University of Louisville
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GOPALKRISHNAN et al. (Thu,) reported a other. Rivaroxaban reduced recurrent stroke by 74% in patients with atrial diameter >46 mm compared to aspirin, emphasizing the need for tailored anticoagulation strategies in ESUS.
www.synapsesocial.com/papers/6980fd18c1c9540dea80ece8 — DOI: https://doi.org/10.1161/str.57.suppl_1.tp022
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