Catheter ablation has become a common treatment for atrial fibrillation (AF), and many patients undergo the procedure in hopes of stopping anticoagulation. However, the risks and benefits of discontinuing anticoagulation after successful ablation have not been clearly defined. Current guidelines recommend continuing anticoagulation indefinitely after ablation based on stroke risk factors rather than ablation success, but these recommendations are based on limited evidence from small, nonrandomized studies. Since catheter ablation is not 100% curative and AF can recur without symptoms, stopping anticoagulation after the procedure may increase stroke risk. Conversely, continuing anticoagulation increases bleeding risk. Two recent randomized trials have examined this question.

In the ALONE-AF trial, an open-label, multicenter, randomized clinical trial, 840 patients (mean age 64 years, mean CHA₂DS₂-VASc score 2.1) with AF who had undergone catheter ablation and had no documented AF recurrence for at least one year were randomized to discontinuing oral anticoagulant therapy (n=417) or continuing it with direct oral anticoagulants (n=423). After two years, the primary outcome, a composite of stroke, systemic embolism, and major bleeding, occurred in 0.3% of the discontinue group versus 2.2% of the continue group (absolute difference, -1.9 percentage points [95% CI, -3.5 to -0.3]; P=0.02). Ischemic stroke occurred in 0.3% and 0.8%, respectively, and major bleeding in 0% and 1.4% (P=0.03). Antiplatelet therapy was used in 8.6% of patients in the discontinue group versus 5.0% in the continue group. In the OCEAN trial, an open-label, randomized, blinded-outcome-assessment trial, 1,284 patients (mean age 66 years, mean CHA₂DS₂-VASc score 2.2) who had undergone successful catheter ablation for AF at least one year earlier were randomized to rivaroxaban 15 mg daily (n=641) or aspirin 70 to 120 mg daily (n=643) and followed for three years. The primary outcome, a composite of stroke, systemic embolism, or new covert embolic stroke detected by MRI, occurred in 0.8% of the rivaroxaban group versus 1.4% of the aspirin group (relative risk, 0.56; 95% CI, 0.19 to 1.65; P=0.28). Stroke occurred in 0.8% and 1.1%, respectively. Fatal or major bleeding occurred in 1.6% of the rivaroxaban group versus 0.6% of the aspirin group (hazard ratio, 2.51; 95% CI, 0.79 to 7.95).

Both trials demonstrate that stroke rates are very low after successful ablation, with annualized stroke rates of approximately 0.3% to 0.4% in patients without documented AF recurrence. The ALONE-AF trial found that discontinuing anticoagulation was superior to continuing it, primarily due to reduced bleeding events without an increase in stroke risk. The OCEAN trial found no significant difference between rivaroxaban and aspirin for stroke prevention, but rivaroxaban was associated with more bleeding. These findings suggest that for patients with successful ablation and no documented AF recurrence, the stroke risk may be low enough that anticoagulation discontinuation or aspirin therapy may be reasonable alternatives to continued anticoagulation, particularly for patients concerned about bleeding risk. However, both trials emphasize the importance of regular rhythm monitoring to detect AF recurrence, as asymptomatic recurrences can occur. The criteria used in these studies for documenting successful ablation serve as a starting point for selecting patients who may be candidates for anticoagulation discontinuation or de-escalation.

• ALONE-AF trial definition of successful ablation: No documented atrial arrhythmia recurrence for at least one year after ablation. Atrial arrhythmia recurrence was defined as any documented episode lasting 30 seconds or longer for AF, atrial flutter, or atrial tachycardia, assessed using at least two sessions of 24- to 72-hour Holter monitoring and ECG monitoring, with at least one session performed within two months prior to enrollment.
• OCEAN trial definition of successful ablation: No clinical evidence of any atrial arrhythmia and no atrial arrhythmia lasting longer than 30 seconds on at least one 24-hour Holter monitor study between 2 and 6 months after the ablation procedure and on at least one 24-hour Holter monitor study at any time after 6 months after the ablation procedure. Additional 48-hour Holter monitoring was performed during the 2 months before enrollment.

• ALONE-AF trial [PubMed abstract]
• OCEAN trial [PubMed abstract]
• Atrial fibrillation review
• Article on webpage

For decades, clinicians have debated the optimal management of asymptomatic high-grade carotid stenosis. While revascularization (stenting or endarterectomy) is often performed to prevent future strokes, previous trials comparing these interventions to medical therapy are outdated, predating the era of high-intensity statins and aggressive blood pressure control. To determine if revascularization provides a benefit over modern pharmacotherapy, researchers conducted CREST-2, a pair of parallel, multicenter, randomized trials involving 2,485 patients with severe asymptomatic carotid stenosis (≥70%).

In the study, all participants received intensive medical management (IMM) involving lifestyle coaching and pharmacotherapy targeting a systolic blood pressure <130 mm Hg and an LDL cholesterol <70 mg/dL. Patients were then randomized into two distinct trials based on their suitability for revascularization type: one comparing carotid artery stenting (CAS) plus IMM versus IMM alone (n=1,245), and another comparing carotid endarterectomy (CEA) plus IMM versus IMM alone (n=1,240). The primary outcome was a composite of perioperative stroke or death (within 44 days) or ipsilateral ischemic stroke up to 4 years. The results were as follows:

• CAS Trial Primary Outcome: CAS group - 2.8% vs. IMM group - 6.0% (P=0.02)
• CEA Trial Primary Outcome: CEA group - 3.7% vs. IMM group - 5.3% (P=0.24)
• Periprocedural Safety (Stroke/Death): CAS - 1.3%, CEA - 1.5%, Medical Management - 0%

The CREST-2 study suggests that the benefit of revascularization for asymptomatic carotid stenosis depends heavily on the modality used. Carotid stenting combined with intensive medical management significantly reduced the risk of stroke or death compared to medical management alone. Conversely, carotid endarterectomy did not demonstrate a statistically significant benefit over medical therapy.

Perhaps the most clinically relevant finding from CREST-2 is the low rate of stroke in the medically managed groups (approximately 1.3% to 1.7% annualized rate). These rates are markedly lower than those seen in historical trials, confirming that modern, aggressive management of blood pressure and lipids is highly effective at stabilizing plaque and preventing events. This poses a challenge to the "fix it" reflex; while stenting offered a relative risk reduction, the absolute risk difference was modest. Furthermore, any procedural intervention carries an upfront risk of periprocedural stroke or death (1.3% to 1.5% in this study).

These findings support a nuanced approach to patient care. For patients with asymptomatic disease who are good candidates for stenting and have a reasonable life expectancy, CAS offers a durable advantage. However, for patients who are surgical candidates or those preferring a conservative approach, intensive medical management alone is a safe and robust strategy, provided that strict targets for blood pressure and lipids are achieved.

• CREST-2 Study [PubMed abstract]
• Carotid stenosis review
• Article on webpage

• 0.25 mg and 0.5 mg: $199/month for new patients, otherwise $349/month
• 1.0 mg, 1.7 mg, and 2.4 mg: $349/month

• 1.5 mg: $149/month
• 4 mg: $149/month for new patients, otherwise $199/month
• 9 mg and 25 mg: $299/month

• Wegovy review
• Article on webpage

• Beta-blockers in CAD Without Heart Failure
• Article on webpage

• Increasing the Potassium Level in Patients at High Risk for Ventricular Arrhythmias, NEJM (2025)
• Article on webpage