Risk of Bleeding Among Cangrelor-Treated Patients Administered Upstream P2Y(12) Inhibitor Therapy: The CAMEO Registry

Authors

Jennifer Rymer
Brooke Alhanti
Steven Kemp
Deepak L. Bhatt
Ajar Kochar
Dominick J. Angiolillo
Miguel Diaz
Kirk N. Garratt
Neil J. Wimmer
Ron Waksman
Ajay J. Kirtane
Lawrence Ang
Richard Bach
Colin Barker
Ronald Jenkins
Mir B. Basir, Henry Ford HealthFollow
Alex Sullivan
Hijrah El-Sabae
Leo Brothers
E. Magnus Ohman
W. Schuyler Jones
Jeffrey B. Washam
Tracy Y. Wang

Recommended Citation

Rymer J, Alhanti B, Kemp S, Bhatt DL, Kochar A, Angiolillo DJ, Diaz M, Garratt KN, Wimmer NJ, Waksman R, Kirtane AJ, Ang L, Bach R, Barker C, Jenkins R, Basir MB, Sullivan A, El-Sabae H, Brothers L, Ohman EM, Jones WS, Washam JB, and Wang TY. Risk of Bleeding Among Cangrelor-Treated Patients Administered Upstream P2Y(12) Inhibitor Therapy: The CAMEO Registry. J Soc Cardiovasc Angiogr Interv 2024; 3(2):101202.

Document Type

Article

Publication Date

2-1-2024

Publication Title

J Soc Cardiovasc Angiogr Interv

Abstract

BACKGROUND: Little is known about the bleeding risk associated with cangrelor use in patients with myocardial infarction (MI) who are exposed to an oral P2Y(12) inhibitor before coronary angiography.

METHODS: Cangrelor in Acute MI: Effectiveness and Outcomes (CAMEO) is an observational registry studying platelet inhibition for patients with MI. Upstream oral P2Y(12) inhibition was defined as receipt of an oral P2Y(12) inhibitor within 24 hours before hospitalization or in-hospital before angiography. Among cangrelor-treated patients, we compared bleeding after cangrelor use through 7 days postdischarge between patients with and without upstream oral P2Y(12) inhibitor exposure.

RESULTS: Among 1802 cangrelor-treated patients with MI, 385 (21.4%) received upstream oral P2Y(12) inhibitor treatment. Of these, 101 patients (33.8%) started cangrelor within 1 hour, 103 (34.4%) between 1 and 3 hours, and 95 (31.8%), >3 hours after in-hospital oral P2Y(12) inhibitor administration; the remaining received an oral P2Y(12) inhibitor before hospitalization. There was no statistically significant difference in rates of bleeding among cangrelor-treated patients with and without upstream oral P2Y(12) inhibitor exposure (6.5% vs 8.8%; adjusted odds ratio [OR], 0.62; 95% CI, 0.38-1.01). Bleeding was observed in 5.0%, 10.7%, and 3.2% of patients treated with cangrelor <1, 1 to 3, and >3 hours after the last oral PY(12) inhibitor dose, respectively; bleeding rates were not statistically different between groups (1-3 hours vs <1 hour: adjusted OR, 2.70; 95% CI, 0.87-8.32; >3 hours vs <1 hour: adjusted OR, 0.65; 95% CI, 0.15-2.85).

CONCLUSIONS: Bleeding risk was not observed to be significantly higher after cangrelor treatment in patients with and without upstream oral P2Y12 inhibitor exposure.

PubMed ID

39132213

Volume

3

Issue

2

First Page

101202

Last Page

101202