Atrial Fibrillation Clinical Trial
Official title:
Prospective Registry of Non-vitamin K Antagonist Oral Anticoagulants for ThromboEmbolic Prevention in Adult Patients With Atrial Tachyarrhythmias and Congenital Heart Disease (NOTE)
Rationale: Adult patients with congenital heart disease (CHD) with atrial tachyarrhythmias
need to be anticoagulated. It is not known whether non-vitamin K antagonist oral
anticoagulants (NOAC) in this patient group are efficient and safe.
Aim: The purpose of the NOTE registry is to evaluate the efficacy and safety of NOACs for
thromboembolic prevention in atrial tachyarrhythmias in adult patients with congenital heart
disease (CHD).
Methods: In this multicenter prospective registry adult CHD patients with atrial
tachyarrhythmias on NOACs (switch from VKA or new on anticoagulants) will be followed for a
minimum of two years.
Primary efficacy endpoints are defined as thromboembolism, i.e. the composite of ischemic
stroke, systemic and pulmonary embolism and intracardiac thrombosis, and as the composite of
stroke and systemic embolism. Primary safety endpoint is defined as major bleeding according
to the ISTH criteria. Secondary endpoints include each thromboembolic or bleeding event
analysed separately, all-cause mortality, therapy adherence, quality of life, risk
assessment of stroke and evaluation of natural history of atrial tachyarrhythmia in adult
CHD patients.
Primary endpoint assessment will be performed with a per protocol analysis, and demonstrated
as Kaplan Meyer estimates of event free survival and event rates per year.
Rationale: Adult patients with congenital heart disease (CHD) with atrial tachyarrhythmias
need to be anticoagulated. It is not known whether non-vitamin K antagonist oral
anticoagulants (NOAC) in this patient group are efficient and safe.
Aim: The purpose of the NOTE registry is to evaluate the efficacy and safety of NOACs for
thromboembolic prevention in atrial tachyarrhythmia's in adult patients with CHD.
Methods: In this multicenter prospective registry adult CHD patients with atrial
tachyarrhythmia's on NOACs will be followed for a period of two years.
Patient population: Registry population consists of CHD patients with tachyarrhythmia's,
defined as atrial fibrillation (AF) or atrial tachycardia's (AT), including atrial flutter,
on NOACs. Patients with new-onset atrial tachyarrhythmia's who are eligible for NOACs, will
be started directly on a NOAC. Patients on vitamin K antagonists (VKA) can be switched
actively to NOACs during outpatient clinic visits, in case of agreement of both patient and
physician. The switch can be initiated for various reasons, including bleeding complications
on VKA, unstable INR measurements, and user friendliness. Eligibility for NOAC use is
defined conform clinical practice, i.e. a patient with nonvalvular atrial tachyarrhythmia's,
but without a mechanical heart valve, significantly elevated risk of bleeding, impaired
renal function, or pregnancy.
Registration process: Patients will be included in the registry at start of NOAC treatment.
Exclusion criteria are an expected survival of less than two years and an additional
indication for anticoagulation besides atrial tachyarrhythmia's. At baseline general patient
characteristics will be registered. Standard echocardiography and laboratory assessments for
follow-up in adult CHD patients will be recorded during the registration period. Quality of
life and therapy adherence will be assessed with questionnaires. Registry follow-up will be
warranted by telephone contact or during outpatient clinic visits. At each follow-up point
the occurrence of pre-defined events will be recorded. A detailed description of each
variable used by the registry is provided in the protocol. Anonymized data will be collected
at each investigational site and entered in a central database at the main investigational
site (Academic Medical Center, Amsterdam, The Netherlands).
Quality assurance: At all investigational sites the investigators are trained to the
registry protocol, case report forms and registry procedures prior to enrolling subjects.
The assigned monitoring investigator at the main site, will assure regular site monitoring
and auditing at all investigational sites. Source data will be verified by comparing the
data to medical records and case report forms in the form of a random sample. To avoid or
minimize bias, an independent clinical events committee at the main investigational site,
consisting of independent physicians, assesses all primary endpoint clinical events.
Intermediate evaluation will take place one year after enrollment of the last patient and
consists of a verification of recorded data, assessment of accuracy of patient follow-up and
primary endpoint analysis.
Drop-outs: Patients who quite NOACs or are lost to follow-up are considered drop-outs. Those
who (temporarily) quite NOACs will be followed until the total follow-up of 2 years will be
completed. The events that occur in the period off-NOAC will not be included in the
analyses. A clear description of the reason of NOAC arrest or interruption and possible
alternative anticoagulant therapy is assessed.
Endpoints: Primary efficacy endpoints are defined as thromboembolism, i.e. the composite of
ischemic stroke, systemic and pulmonary embolism and intracardiac thrombosis, and as the
composite of stroke and systemic embolism. Primary safety endpoint is defined as major
bleeding according to the ISTH criteria. Secondary endpoints include each thromboembolic or
bleeding event analyzed separately, all-cause mortality, therapy adherence, quality of life,
risk assessment of stroke and evaluation of natural history of atrial tachyarrhythmia in
adult CHD patients.
Sample size: By using estimates of event rates in the described patient population
(thromboembolism event rate of 1.4% per year, mainly on VKA; unpublished data) and a
relative risk reduction of 0.81 for stroke or systemic embolism on NOACs compared to VKA
[Ruff et al, Lancet 2013], a sample size of 300 patients followed for two years is necessary
to demonstrate the safety of NOACs for thromboembolic prevention with a safety margin of
2.7% thromboembolic events per year.
Statistical analysis: Endpoint assessment will be performed with a per protocol analysis,
and demonstrated as Kaplan Meyer (KM) estimates of event free survival and event rates per
year. The results will be compared with KM estimates and event rates from a historical
similar cohort on VKA in a non-inferiority assay. Drop-outs (see below) will be censored at
time of drop-out in time-to-event analyses, and included for event-rate analyses up to time
of drop-out. No adjustment or imputation of missing data will be performed and all available
data will be presented.
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Observational Model: Cohort, Time Perspective: Prospective
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