VT Ablation in Ischemic Cardiomyopathy

Definition

Catheter ablation for ventricular tachycardia (VT) in patients with prior myocardial infarction involves electroanatomic substrate mapping of post-infarct scar and radiofrequency delivery to render VT noninducible. It is now supported as a first-line strategy in patients with clinically significant VT and ischemic cardiomyopathy who have not previously failed antiarrhythmic drugs.

Key Concepts

Mechanistic Basis

• Post-MI scar creates fixed anatomical barriers and slow conduction zones that support scar-based re-entrant VT (sustained monomorphic VT is the predominant form)
• Electroanatomic mapping defines the arrhythmic substrate; ablation targets sites of earliest activation (entrainment mapping), abnormal potentials (late potentials), and channels within scars
• Radiofrequency energy renders the substrate noninducible by eliminating slow conduction channels

Antiarrhythmic Drugs — Comparators and Limitations

• Sotalol (Class III + non-selective beta-blocker): preferred when LVEF ≥20%, eGFR ≥30 ml/min/1.73m², NYHA I/II, no torsades de pointes, no QT prolongation, and qualifying arrhythmia is not VT storm; dose 120 mg BD
• Amiodarone (Class III): preferred for severe ventricular dysfunction or electrical storm; dose 400 mg BD ×2w → 400 mg daily ×4w → 200 mg maintenance; more effective but higher noncardiac toxicity (pulmonary, thyroid, hepatic, neurological)
• Drug adverse events leading to discontinuation or dose reduction are common in long-term follow-up: 21.6% nonfatal in VANISH2 over 4.3 years (sources/vt-ablation-vanish2-nejm-2025, rating: very high)

VANISH2 Trial — First-Line Ablation vs AAD (2025)

• 416 patients, prior MI, clinically significant VT, all ICD recipients, no prior antiarrhythmic drug exposure for VT; 22 centres in Canada, USA, France; median follow-up 4.3 years (sources/vt-ablation-vanish2-nejm-2025, rating: very high)
• Primary endpoint (composite: death/VT storm/ICD shock/treated sustained VT >14 days): Ablation 50.7% vs drugs 60.6%; HR 0.75 (95% CI 0.58–0.97; P=0.03)
• Mortality alone: HR 0.84 (NS) — no mortality difference
• VT storm: HR 0.95 (NS) — no significant difference
• Appropriate ICD shock: HR 0.75 (NS trend)
• Treated sustained VT below ICD detection limit: HR 0.26 (95% CI 0.13–0.55) — the largest and most significant effect, driving primary endpoint difference
• Drug-related adverse events: 21.6% (nonfatal, leading to drug discontinuation/reduction) vs 3.4% in ablation arm; 1 death from pulmonary toxicity; 7 pulmonary infiltrates/fibrosis in drug arm
• Ablation procedural complications (30 days): Death 1.0%, stroke 1.0%, cardiac perforation 0.5%, vascular injury 2.5%
• Conclusion: First large RCT supporting catheter ablation as first-line therapy over AADs in ischemic VT; challenges conventional "drugs first, ablation after failure" paradigm

VANISH Trial — Ablation vs Escalated AAD (2016)

• Among patients with VT on baseline antiarrhythmic therapy, ablation + continuation of baseline drugs was superior to escalation of antiarrhythmic drug therapy for a composite of death, ICD shock, or VT storm (sources/VA-SCD-ESC-2022, rating: very high)
• Together, VANISH and VANISH2 support ablation over drug escalation at multiple stages: whether naive to drugs or already on them

Substrate Approach and Procedural Standards

• Ablation performed within 14 days of randomization in VANISH2
• Standardized approach: VT induction → electroanatomic mapping of the ventricular substrate → radiofrequency delivery to render VT noninducible
• 319 total ablation procedures were performed in VANISH2 (including 79 among drug-therapy patients who crossed over): underlines the complexity and repeated-procedure nature of VT management
• ICD programming was standardized to published guidelines in VANISH2

Residual Disease Burden Despite Treatment

• Even with the superior ablation strategy: 22.2% died, 21.7% had VT storm, 29.6% had ICD shock, 4.4% had treated sub-threshold VT over 4.3 years
• High residual burden demonstrates that VT in ischemic cardiomyopathy remains a severe condition with no curative option

Guideline Context

• Current AHA/ACC/HRS (2017) and ESC (2022) guidelines recommend antiarrhythmic drugs first with ablation for drug-refractory cases (Class I)
• VANISH2 directly challenges this sequence — first-line ablation now supported by the largest and longest RCT in this space
• Emergency catheter ablation for incessant VT/ES refractory to AADs: Class I in ESC 2022 (unchanged)

Contradictions / Open Questions

• Mortality benefit not established: VANISH2 was not powered to detect a mortality difference; both VANISH and VANISH2 show a trend toward lower mortality with ablation (HR ~0.84) but neither reached significance. A meta-analysis of ablation vs AAD trials might clarify this. (sources/vt-ablation-vanish2-nejm-2025)
• VT storm not reduced by ablation: Counter-intuitively, VANISH2 showed no significant reduction in VT storm with ablation (HR 0.95). This may reflect the acute re-entrant nature of storm in the immediate post-ablation period versus chronic suppression of sub-threshold VT. (sources/vt-ablation-vanish2-nejm-2025)
• Guideline lag: Current guidelines list catheter ablation only after drug failure; VANISH2 data are not yet incorporated into revised guidelines. The "drugs first" standard may change in next guideline iteration.
• Generalizability to non-ischemic VT: VANISH2 restricted to post-MI patients. Non-ischemic cardiomyopathy (DCM, ACM) has different substrate characteristics and ablation outcomes; this evidence cannot be directly extrapolated.
• Operator variability: Ablation outcomes depend heavily on operator/centre experience. VANISH2 was conducted at high-volume centres; real-world ablation outcomes at lower-volume centres may differ.
• Long-term amiodarone toxicity underestimated: Median 4.3-year follow-up may understate cumulative amiodarone toxicity risk (pulmonary, thyroid, neurologic); longer follow-up would likely further widen the safety gap. (sources/vt-ablation-vanish2-nejm-2025, sources/amiodarone-pulmonary-clin-chest-2004)

Connections

• Related to concepts/Electrical-Storm — ablation is Class I for SMVT-related ES; VANISH2 supports use before drug failure
• Related to concepts/Amiodarone-Pulmonary-Toxicity — VANISH2 quantifies real-world pulmonary toxicity (1 death, 7 pulmonary infiltrates/fibrosis in AAD arm over 4.3 years)
• Related to concepts/Catheter-Ablation-AF — ablation technology and technique parallels
• Related to concepts/Late-Gadolinium-Enhancement — LGE-CMR delineates scar substrate targeted by VT ablation
• Related to concepts/Myocardial-Viability — ischemic cardiomyopathy substrate context
• Related to entities/Amiodarone — comparator drug; toxicity profile motivates ablation-first
• Related to entities/Sotalol — comparator drug for lower-risk patients in VANISH2

Sources

• sources/vt-ablation-vanish2-nejm-2025
• sources/VA-SCD-ESC-2022