Thromboembolic Events Clinical Trial
Official title:
Association of Genetic Variants With Risk of Stroke in Patients With Atrial Fibrillation Off-anticoagulation
Life-long therapy with oral anticoagulants (OAC) is strongly recommended in AF patients receiving left atrial appendage isolation (LAAI) to prevent thromboembolic (TE) events. However, some patients are observed to remain stroke-free while off OACs for years whereas others experience TE events if OAC is discontinued even for a short period of time. Therefore, we aim to evaluate the association of genetic variants (single nucleotide polymorphisms - SNPs) with off-anticoagulation stroke-risk in AF patients.
1. BACKGROUND Atrial fibrillation (AF) is known to be a leading cause of thrombo-embolic
(TE) events (1).The left atrial appendage (LAA), an embryological remnant of the
primitive left atrium, has been reported to be the source of thrombus formation in more
than 90% of patients with non-valvular AF (2). More specifically, the loss of
contractile function in the LAA following electrical isolation of the appendage (LAAI)
leads to stasis and thrombus formation, which may then embolize into the systemic
circulation. For this reason, life-long oral anticoagulation (OAC) is strongly
recommended in post-LAAI cases to reduce the stroke-risk. However, intolerance to OAC,
non-compliance, increase in the risk of bleeding in patients with bleeding disorders or
in elderly with high fall-risk and difficulty in maintaining the therapeutic level for
certain novel oral anticoagulants in patients with renal dysfunction are several
limitations of the OAC therapy (3). Furthermore, patients occasionally need to
discontinue OACs as advised by their treating physicians while undergoing other medical
procedures. Patient-preference and non-compliance are other important reasons for OAC
discontinuation.
Whatever may be the cause, the consequence in terms of TE events, is observed to be
highly variable. Some patients experience a TE event after withdrawal of OAC for a very
short period while others remain stroke-free even after years while off OAC therapy.
This intriguing observation triggers a vital question; does genetics play a role in
increasing predisposition to stroke or providing protection from TE events? The current
pilot study aims to address that question as understanding the underlying molecular
mechanism would be highly useful in risk-prediction, counselling and optimal management
of post-LAAI patients.
Prior studies have reported an association between several single-nucleotide
polymorphisms (SNPs) with stroke in patients with or without AF (4-19). Most were
documented to be linked with elevated stroke-risk whereas few were found to have a
protective impact. However, SNPs associated with stroke in the post-LAAI cases have not
been elucidated yet. More importantly, it is not known why discontinuation of OAC has a
differential impact on this high-risk population. Therefore, in this pilot study, we aim
to test a number of SNPS (a list is provided at the end of the protocol) in post-LAAI
cases to determine their association with stroke after discontinuation of OAC.
1.1 Safety This study poses minimal risk to the subject. More specifically, the risks
are those that are associated with venipuncture (pain, bleeding, bruising, infection,
and inflammation at the site), during the single blood specimen collection.
2. STUDY RATIONALE We hypothesize that there will be significant differences in the allele
frequencies of SNPs among patients with and without TE events.
3. STUDY OBJECTIVES 3.1 Primary Objective To compare the SNP profile of post-LAAI patients
that have or have not experienced any TE events after discontinuation of OAC.
4. STUDY DESIGN 4.1 Study Overview This is a single center, observational clinical trial.
Subjects who meet all inclusion criteria and none of the exclusion criteria will be
screened and consecutive consenting patients will be enrolled in the study. We will
screen all patients that have stopped OAC after LAAI and enroll the consenting patients
that have or have not experienced stroke during discontinuation of OAC.
The total duration of subject participation will be 1 day. The total duration of the study is
expected to be 1 year.
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