Onyx One Clinical Evidence
The only DES with 1-month DAPT evidence in complex high bleeding risk (HBR) patients.
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Complex HBR Patient Population in the Onyx ONE Month DAPT Program1
Onyx One Global Trial
First prospective, randomized,
1-month DAPT trial comparing a DES to a DES in ~2,000 HBR patients.
Primary Endpoint
Resolute Onyx™ DES met the primary endpoint for cardiac death, myocardial infarction, and stent thrombosis, showing non-inferiority vs. BioFreedom™* DCS at 12 months (17.1% vs. 16.9%).2
Acute Performance
- Superior device success†
- Significantly higher crossover from BioFreedom DCS to Resolute Onyx DES‡
- Significantly higher acute gain‡
Landmark Analysis
1–12 Months
after DAPT
Discontinuation§2
Low event rates for Resolute Onyx DES in a highly complex HBR patient population, including significantly lower MI vs. BioFreedom DCS||
Onyx One Global Trial Resources
Onyx ONE Global Trial Results
Published by The New England Journal of Medicine
Onyx ONE Clear Study
The first study in the United States and Japan evaluating 1-month DAPT duration in HBR patients with a current DES.
Onyx ONE Clear Analysis
- 752 HBR patients from the United States and Japan in a prospective, multicenter, single-arm trial
- Pooled with similar “clear” Resolute Onyx DES patients from the Onyx ONE Global Trial
- ~1,500 total patients included in primary endpoint analysis
“Clear” patients are defined as being event-free¶ and DAPT-adherent for the first 30 days post-procedure.
Primary Endpoint Results
The Onyx ONE Clear analysis showed 7.0% cardiac death or myocardial infarction at one year, beating the performance goal of 9.7%.3
Performance goal derived from contemporary 1-month DAPT trials.#
Onyx ONE Clear Study Resources
Resolute Onyx DES Is safe and effective in real-world HBR patients on 1-month DAPT
Based on results from the Onyx ONE Clear Analysis, evaluating over 1,500 complex HBR patients.
DAPT duration decisions are best made on an individual basis. Premature discontinuation or interruption of prescribed antiplatelet medication could result in a higher risk of ST, MI, or death.
*
Third-party brands are trademarks of their respective owners.
†
Device success was not a powered endpoint or adjusted for multiplicity.
‡
Crossover and acute gain were not prespecified, powered, or adjusted for multiplicity.
§
From one month to one year.
||
Post-hoc analyses were not powered.
¶
Patients must be free of spontaneous MI, repeat revascularization, stroke, stent thrombosis, and death through one month.
#
ZEUS, LEADERS FREE, and SENIOR trials.
**
Some products, indications, therapy areas may not be licensed in accordance with Canadian Law. Please contact your local representative for further information.
References
1
Kedhi E, Latib A, Abizaid A, et al. Rationale and design of the Onyx ONE global randomised trial: A randomised controlled trial of high-bleeding risk patients after stent placement with 1 month of dual antiplatelet therapy. Am Heart J. August 2019;214:134-141.
2
Windecker S, Latib A, Kedhi E, et al. Polymer-based or Polymer-free Stents in Patients at High Bleeding Risk. N Engl J Med. March 26, 2020;382(13):1208-1218.
3
Kandzari DE, Kirtane AJ, Windecker S, et al. One-Month Dual Antiplatelet Therapy Following Percutaneous Coronary Intervention With Zotarolimus-Eluting Stents in High-Bleeding-Risk Patients. Circ Cardiovasc Interv. November 2020;13(11):e009565.
- Onyx Frontier™ DES, Licensed as RESOLUTE ONYX ZOTAROLIMUS-ELUTING CORONARY STENT SYSTEM