https://doi.org/10.55788/597a584c
Results from PACIFIC-AMI
Prof. John Alexander (Duke University, NC, USA) presented the results from the phase 2 PACIFIC-AMI trial (NCT04304534), which were simultaneously published in Circulation [1,2]. By means of explaining the rationale of the study, Prof. Alexander said: “Following an acute MI, patients remain at increased risk for recurrent events despite the excellent therapies we have today. Antiplatelet therapy with aspirin and P2Y12 inhibitors is a benefit and considered standard-of-care but is limited because of the risk of bleeding. Oral anticoagulation, that is, vitamin K antagonists and the factor X inhibitor rivaroxaban, have also been shown to be beneficial post-MI, but their use is also limited by bleeding and are, thus, rarely used.”
PACIFIC-AMI aimed to test the efficacy and safety of 3 different doses of asundexian after acute MI, when added to standard of care DAPT. Participants (n=1,600, 51% had an ST-segment elevation MI) were randomised to 10 mg, 20 mg, 50 mg asundexian, or placebo once daily for 6–12 months.
The primary efficacy endpoint was a composite of cardiovascular death, MI, stroke, or stent thrombosis. The primary safety endpoints were Bleeding Academic Research Consortium (BARC) type 2, 3, or 5 bleeding and any bleeding in the 2 weeks after study drug discontinuation.
As evidence of on-target activity, participants exhibited >70%, 80%, and 90% reduction in factor XIa activity when given asundexian 10 mg, 20 mg, and 50 mg once daily, compared with placebo (see Figure). With a median follow-up of 368 days, there were no trends for reductions in the composite primary outcome among patients assigned to any dose of asundexian compared with placebo. Notably, Prof. Alexander pointed out, there were only few total events, and therefore the conclusion is still uncertain. The primary safety endpoint, however, was met: there was no increase in bleeding among patients assigned to asundexian compared with placebo.
Figure: Factor XIa inhibition at 4 weeks in PACIFIC-AMI [1]
Vertical bars indicate the % residual Factor XIa activity compared with baseline
Prof. Alexander concluded: “These results, together with existing genetic and preclinical evidence, support the further study of the factor XIa inhibitor asundexian, in adequately sized phase 3 trials as a potentially safer anticoagulant for patients following an acute MI.”
Results from PACIFIC-Stroke
Associate Prof. Ashkan Shoamanesh (McMaster University, Canada) presented the results of the PACIFIC-Stroke trial (NCT04304508), which assessed the same doses of asundexian compared with placebo [3]. PACIFIC-Stroke randomised patients (n=1,808, mean age 67 years, 34% women) within 48 hours of non-cardioembolic stroke symptom onset (mean interval 36 hours), with a primary efficacy endpoint of ischaemic stroke or brain infarct at 6 months.
With a median follow-up of 10.6 months, recurrent symptomatic ischaemic stroke or transient ischaemic attack (TIA) occurred in 8.3% of the placebo arm compared with 7.7% of the asundexian 10 mg arm, 6.2% in the 20 mg arm, and 5.4% in the 50 mg arm. Although there were numeric differences, statistical significance was not reached in the risk of events in patients given asundexian compared with placebo (P=0.8). However, after a post-hoc exploratory analysis that replaced the initial primary endpoint component of covert brain infarct with TIA, researchers observed a lower risk with 50 mg asundexian compared with placebo (5.4% vs 8.3%; HR 0.64; 95% CI 0.41–0.98), especially in the subgroup of patients with atherosclerotic plaques (3.1% vs 8.1%; HR 0.39; 95% CI 0.18–0.85).
At 12 months follow-up, the rates of bleeding were not significantly different between asundexian and placebo (3.9% vs 2.4%; HR 1.57; 90% CI 0.91–2.71).
“Asundexian did not reduce the composite endpoint of intracranial infarction or ischaemic stroke in a dose-dependent manner,” explained Associate Prof. Shoamanesh. “However, treatment with asundexian 50 mg daily did reduce recurrent symptomatic ischaemic strokes and TIAs in this population with acute non-cardioembolic ischaemic stroke, particularly among those with atherosclerosis, without a statistically significant increase in major bleeding.” He concluded: “The promising results from this phase 2 trial require validation in an adequately powered phase 3 randomised trial”.
- Alexander J, et al. PACIFIC-AMI - Efficacy and safety of factor XIa inhibitor asundexian on top of dual antiplatelet therapy after acute myocardial infarction. Hot Line Session 5, ESC Congress 2022, Barcelona, Spain, 26–29 August.
- Rao SV, et al. Circulation. 2022 Aug 27. doi: 10.1161/CIRCULATIONAHA.122.061612. Epub ahead of print.
- Shoamanesh A, et al. PACIFIC-STROKE - Phase 2 Program of AntiCoagulation via Inhibition of FXIa by the oral Compound BAY 2433334 – non-cardioembolic STROKE study. Hot Line Session 5, ESC Congress 2022, Barcelona, Spain, 26–29 August.
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Table of Contents: ESC 2022
Featured articles
ESC Clinical Practice Guidelines
Prevention of VT and sudden cardiac death: the new recommendations
New and first ESC cardio-oncology guideline
The 2022 ESC/ERS guidelines for the diagnosis and treatment of pulmonary hypertension
Cardiovascular assessment and management of patients undergoing non-cardiac surgery
Heart Failure
Old dogs, new tricks: Acetazolamide plus loop diuretics improves decongestion
No effect of neprilysin inhibition on cognition
Dapagliflozin DELIVERs for HFmrEF/HFpEF
Meta-analysis of DELIVER and EMPEROR-Preserved
Anticoagulation
Rheumatic heart disease-associated AF: standard-of-care holds ground
New anticoagulant safe and maybe effective: PACIFIC-AMI and PACIFIC-Stroke outcomes
AXIOMATIC-SSP: Reducing risk of ischaemic stroke with factor XIa inhibition?
Evolving evidence for P2Y12 inhibition in chronic coronary syndromes: PANTHER
Prevention
Danish study suggests starting CVD screening before age 70
Polypill SECUREs win in secondary prevention in elderly
Long-term therapy with evolocumab associated with lower CV mortality
ARBs + beta-blockers may delay Marfan syndrome aortic root replacement
ENTRIGUE: Subcutaneous pegozafermin in severe hypertriglyceridaemia
Artificial Intelligence & Digital Health – What Is New
First RCT evidence for use of AI in daily practice
AI-enhanced echography supports aortic stenosis patients
Ischaemia
Medical therapy versus PCI for ischaemic cardiomyopathy
Allopurinol disappoints in ALL-HEART
Conservative or invasive management for high-risk kidney disease patients with ischaemia?
Genotype-guided antiplatelet therapy in patients receiving PCI
Other HOTLINE Sessions
BOXing out oxygen and blood pressure targets
Coronary CT angiography diagnostics compared head-to-head
High-dose influenza vaccine: mortality benefit?
FFR-guided decision-making in patients with AMI and multivessel disease
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