What question did this study set out to answer?

This research aims to determine the effectiveness of ET-1 antagonists in reducing stroke incidence in populations at risk of cerebral small vessel disease.

May 8, 2026Open Access

Abstract Number: Esoc2026a1169 Decreased Risk of Stroke in Randomised Controlled Trials Of et-1 Antagonists: A Systematic Review and Meta-Analysis

Key Points

This research aims to determine the effectiveness of ET-1 antagonists in reducing stroke incidence in populations at risk of cerebral small vessel disease.
Conducted a systematic review and meta-analysis of randomized controlled trials comparing ET-1 antagonists to placebo or standard care.
Searched MEDLINE, EMBASE, and CENTRAL for trials reporting stroke incidence, with a minimum follow-up of 12 weeks.
Analyzed data using inverse-variance weighted random effects meta-analysis.
6 out of 7 eligible trials (N=4,177) showed a lower incidence of stroke with ET-1 antagonists (pooled IRR=0.35, 95% CI:0.19-0.66, p=0.00113).
The effect remained consistent in trials with 52 weeks of follow-up (pooled IRR=0.301, 95% CI:0.143-0.634, p=0.0016).
The large SONAR trial demonstrated a significant benefit of atrasentan in chronic kidney disease (IRR=0.296, p=0.0024), despite similar trends being non-significant when included.

Abstract

Abstract Background and aims Cerebral small vessel disease (cSVD) is responsible for 30% of all-cause stroke. Endothelin-1 (ET-1) is the most potent cerebral endothelial vasoconstrictor. ET-1 is elevated during acute stroke and predicts cognitive outcomes. However, its potential in stroke prevention remains undetermined. We therefore performed a meta-analysis of stroke incidence in randomised controlled trials (RCTs) of ET-1 antagonists. Methods MEDLINE, EMBASE and CENTRAL were searched from inception until October 2025, including RCTs of ET-1 antagonists versus placebo/standard care (≥12 weeks) which reported stroke incidence. We excluded trials requiring large vessel cerebrovascular pathologies (subarachnoid haemorrhage, Moya-moya etc). Results were combined by inverse-variance weighted random effects meta-analysis. Results 6/7 eligible RCTs (N=4,177) reported lower incidence of stroke during ET-1 inhibition versus controls (pooled incidence rate ratio (IRR)=0.35, 95% CI:0.19-0.66, p=0.00113; I2=0, p-heterogeneity=0.979), although event rates were low in most trials. Effects were consistent in trials with ≥52 weeks of follow-up (pooled IRR=0.301, 95% CI:0.143-0.634, p=0.0016; I2=0, p-heterogeneity=0.99). Although no longer significant (pooled IRR=0.48, p=0.177), the effect was similar when excluding the large SONAR trial in chronic kidney disease (CKD) which independently demonstrated a significant benefit using atrasentan (IRR= 0.296, p=0.0024; 8 vs 27 events in 2,648 participants). Conclusions ET-1 antagonism was associated with reduced incidence of stroke in RCTs of populations at risk of cSVD, consistent with a significant effect in the large SONAR trial in CKD which dominated results. Endothelin-1 antagonism warrants testing as a novel target to reduce risk of cSVD-related stroke. Conflict of interest Caoimhe Byrne: PhD funded by the Alzheimer's Society Doctoral Training Centre for Vascular and Immune Contributors to Dementia (VIDA). Prof Webb: Nothing to disclose. Figure 1 - belongs to Results

Abstract Number: Esoc2026a1169 Decreased Risk of Stroke in Randomised Controlled Trials Of et-1 Antagonists: A Systematic Review and Meta-Analysis

Key Points

Abstract

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