Aspirin versus anticoagulation in cervical artery dissection (TREAT-CAD): an open-label, randomised, non-inferiority trial.
Acenocoumarol
/ therapeutic use
Adult
Anticoagulants
/ therapeutic use
Aspirin
/ therapeutic use
Carotid Artery, Internal, Dissection
/ complications
Denmark
Female
Germany
Humans
Male
Middle Aged
Phenprocoumon
/ therapeutic use
Platelet Aggregation Inhibitors
/ therapeutic use
Stroke
/ diagnostic imaging
Switzerland
Vertebral Artery Dissection
/ complications
Warfarin
/ therapeutic use
Journal
The Lancet. Neurology
ISSN: 1474-4465
Titre abrégé: Lancet Neurol
Pays: England
ID NLM: 101139309
Informations de publication
Date de publication:
05 2021
05 2021
Historique:
received:
07
10
2020
revised:
22
01
2021
accepted:
02
02
2021
pubmed:
26
3
2021
medline:
12
5
2021
entrez:
25
3
2021
Statut:
ppublish
Résumé
Cervical artery dissection is a major cause of stroke in young people (aged <50 years). Historically, clinicians have preferred using oral anticoagulation with vitamin K antagonists for patients with cervical artery dissection, although some current guidelines-based on available evidence from mostly observational studies-suggest using aspirin. If proven to be non-inferior to vitamin K antagonists, aspirin might be preferable, due to its ease of use and lower cost. We aimed to test the non-inferiority of aspirin to vitamin K antagonists in patients with cervical artery dissection. We did a multicentre, randomised, open-label, non-inferiority trial in ten stroke centres across Switzerland, Germany, and Denmark. We randomly assigned (1:1) patients aged older than 18 years who had symptomatic, MRI-verified, cervical artery dissection within 2 weeks before enrolment, to receive either aspirin 300 mg once daily or a vitamin K antagonist (phenprocoumon, acenocoumarol, or warfarin; target international normalised ratio [INR] 2·0-3·0) for 90 days. Randomisation was computer-generated using an interactive web response system, with stratification according to participating site. Independent imaging core laboratory adjudicators were masked to treatment allocation, but investigators, patients, and clinical event adjudicators were aware of treatment allocation. The primary endpoint was a composite of clinical outcomes (stroke, major haemorrhage, or death) and MRI outcomes (new ischaemic or haemorrhagic brain lesions) in the per-protocol population, assessed at 14 days (clinical and MRI outcomes) and 90 days (clinical outcomes only) after commencing treatment. Non-inferiority of aspirin would be shown if the upper limit of the two-sided 95% CI of the absolute risk difference between groups was less than 12% (non-inferiority margin). This trial is registered with ClinicalTrials.gov, NCT02046460. Between Sept 11, 2013, and Dec 21, 2018, we enrolled 194 patients; 100 (52%) were assigned to the aspirin group and 94 (48%) were assigned to the vitamin K antagonist group. The per-protocol population included 173 patients; 91 (53%) in the aspirin group and 82 (47%) in the vitamin K antagonist group. The primary endpoint occurred in 21 (23%) of 91 patients in the aspirin group and in 12 (15%) of 82 patients in the vitamin K antagonist group (absolute difference 8% [95% CI -4 to 21], non-inferiority p=0·55). Thus, non-inferiority of aspirin was not shown. Seven patients (8%) in the aspirin group and none in the vitamin K antagonist group had ischaemic strokes. One patient (1%) in the vitamin K antagonist group and none in the aspirin group had major extracranial haemorrhage. There were no deaths. Subclinical MRI outcomes were recorded in 14 patients (15%) in the aspirin group and in 11 patients (13%) in the vitamin K antagonist group. There were 19 adverse events in the aspirin group, and 26 in the vitamin K antagonist group. Our findings did not show that aspirin was non-inferior to vitamin K antagonists in the treatment of cervical artery dissection. Swiss National Science Foundation, Swiss Heart Foundation, Stroke Funds Basel, University Hospital Basel, University of Basel, Academic Society Basel.
Sections du résumé
BACKGROUND
Cervical artery dissection is a major cause of stroke in young people (aged <50 years). Historically, clinicians have preferred using oral anticoagulation with vitamin K antagonists for patients with cervical artery dissection, although some current guidelines-based on available evidence from mostly observational studies-suggest using aspirin. If proven to be non-inferior to vitamin K antagonists, aspirin might be preferable, due to its ease of use and lower cost. We aimed to test the non-inferiority of aspirin to vitamin K antagonists in patients with cervical artery dissection.
METHODS
We did a multicentre, randomised, open-label, non-inferiority trial in ten stroke centres across Switzerland, Germany, and Denmark. We randomly assigned (1:1) patients aged older than 18 years who had symptomatic, MRI-verified, cervical artery dissection within 2 weeks before enrolment, to receive either aspirin 300 mg once daily or a vitamin K antagonist (phenprocoumon, acenocoumarol, or warfarin; target international normalised ratio [INR] 2·0-3·0) for 90 days. Randomisation was computer-generated using an interactive web response system, with stratification according to participating site. Independent imaging core laboratory adjudicators were masked to treatment allocation, but investigators, patients, and clinical event adjudicators were aware of treatment allocation. The primary endpoint was a composite of clinical outcomes (stroke, major haemorrhage, or death) and MRI outcomes (new ischaemic or haemorrhagic brain lesions) in the per-protocol population, assessed at 14 days (clinical and MRI outcomes) and 90 days (clinical outcomes only) after commencing treatment. Non-inferiority of aspirin would be shown if the upper limit of the two-sided 95% CI of the absolute risk difference between groups was less than 12% (non-inferiority margin). This trial is registered with ClinicalTrials.gov, NCT02046460.
FINDINGS
Between Sept 11, 2013, and Dec 21, 2018, we enrolled 194 patients; 100 (52%) were assigned to the aspirin group and 94 (48%) were assigned to the vitamin K antagonist group. The per-protocol population included 173 patients; 91 (53%) in the aspirin group and 82 (47%) in the vitamin K antagonist group. The primary endpoint occurred in 21 (23%) of 91 patients in the aspirin group and in 12 (15%) of 82 patients in the vitamin K antagonist group (absolute difference 8% [95% CI -4 to 21], non-inferiority p=0·55). Thus, non-inferiority of aspirin was not shown. Seven patients (8%) in the aspirin group and none in the vitamin K antagonist group had ischaemic strokes. One patient (1%) in the vitamin K antagonist group and none in the aspirin group had major extracranial haemorrhage. There were no deaths. Subclinical MRI outcomes were recorded in 14 patients (15%) in the aspirin group and in 11 patients (13%) in the vitamin K antagonist group. There were 19 adverse events in the aspirin group, and 26 in the vitamin K antagonist group.
INTERPRETATION
Our findings did not show that aspirin was non-inferior to vitamin K antagonists in the treatment of cervical artery dissection.
FUNDING
Swiss National Science Foundation, Swiss Heart Foundation, Stroke Funds Basel, University Hospital Basel, University of Basel, Academic Society Basel.
Identifiants
pubmed: 33765420
pii: S1474-4422(21)00044-2
doi: 10.1016/S1474-4422(21)00044-2
pii:
doi:
Substances chimiques
Anticoagulants
0
Platelet Aggregation Inhibitors
0
Warfarin
5Q7ZVV76EI
Acenocoumarol
I6WP63U32H
Phenprocoumon
Q08SIO485D
Aspirin
R16CO5Y76E
Banques de données
ClinicalTrials.gov
['NCT02046460']
Types de publication
Comparative Study
Equivalence Trial
Journal Article
Multicenter Study
Randomized Controlled Trial
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
341-350Investigateurs
Timo Kahles
(T)
Krassen Nedeltchev
(K)
Valerian Altersberger
(V)
Leo H Bonati
(LH)
Alex Brehm
(A)
Nicole Bruni
(N)
Gian Marco De Marchis
(GM)
Stefan T Engelter
(ST)
Thomas Fabbro
(T)
Urs Fisch
(U)
Joachim Fladt
(J)
Henrik Gensicke
(H)
Lisa Hert
(L)
Philippe A Lyrer
(PA)
Marina Maurer
(M)
Nils Peters
(N)
Alexandros Polymeris
(A)
Marios-Nikos Psychogios
(MN)
Sabine Schaedelin
(S)
Christoph Stippich
(C)
Sebastian Thilemann
(S)
Christopher Traenka
(C)
Benjamin Wagner
(B)
Marcel Arnold
(M)
Urs Fischer
(U)
Barbara Goeggel Simonetti
(B)
Jan Gralla
(J)
Mirjam Heldner
(M)
Simon Jung
(S)
Stephen L Leib
(SL)
David J Seiffge
(DJ)
Hubertus Mueller
(H)
Lukas Sveikata
(L)
Roman Sztajzel
(R)
Hubertus Mueller
(H)
Pamela Correia
(P)
Ashraf Eskandari
(A)
Ivo Meyer
(I)
Patrik Michel
(P)
Stefania Nannoni
(S)
Suzette Remillard
(S)
Gaia Sirimarco
(G)
Alexandros Zachariadis
(A)
Georg Kaegi
(G)
Anna Mueller
(A)
Jochen Vehoff
(J)
Janne Hamann
(J)
Andreas R Luft
(AR)
Levke Steiner
(L)
Susanne Wegener
(S)
Hebun J Erdur
(HJ)
Christian H Nolte
(CH)
Regina von Rennenberg
(R)
Jan F Scheitz
(JF)
Katharina Feil
(K)
Lars Kellert
(L)
Hanne Christensen
(H)
Sverre Rosenbaum
(S)
Commentaires et corrections
Type : CommentIn
Informations de copyright
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