Atrial Fibrillation Clinical Trial
Official title:
The Effect of Losartan on Atrial Fibrillation and Pacemaker Dependence in Sick Sinus Syndrome (SSS) Patients Receiving Physiological Pacemaker - A Prospective, Randomized, Multicenter Study in Taiwan
This is a an investigator-initial, multicenter, open-label, randomized, parallel-group comparative study to evaluate the effect on the incidence of AF and pacemaker dependence in SSS patients receiving physiological atrial-based pacing alone or adding losartan 100mg to physiological atrial-based pacing treatment. The duration of the study will be approximately 13 months, comprising 4-week pre-study period, and 12-month treatment period.
Sick sinus syndrome is a common indication for permanent cardiac pacing in the community. It
results from disordered impulse generation within the sinus node or impaired conduction of
the impulse to the surrounding atrial tissue, thus leading to the clinical manifestation of
bradycardia. In patients with SSS, AF frequently develops after pacemaker implantation,and
progresses to persistent AF over long term follow up.
The occurrence of AF have been shown to be an independent predictor for major cardiovascular
events in SSS patients receiving physiologic pacing. Recent prospective clinical trials have
demonstrated that physiologic pacing mode reduces the risk of AF compared to single chamber
ventricular pacing in patients with SSS. However, the effectiveness of physiologic pacing in
reducing the incidence of AF in patients with sinus node dysfunction is still incomplete.
One recent clinical study had reported that 68% of SSS patients with a DDDR pacemaker have
atrial tachyarrhythmias detected by the pacemaker devices at median 718 days follow-up.
Modern pacemakers have diagnostic features that permit the detection and storage of
information about the date, time of onset, and duration of multiple, sequential episodes of
atrial tachyarrhythmias. Since a high percentage of AF episodes may be asymptomatic, AF
"burden" have been used as surrogate end points. Prolonged P wave, shortened refractoriness,
or remarkably abnormal conduction disturbances in the presence of prolonged refractoriness
limit the effectiveness of standard physiologic pacing in AF prevention. This could explain,
at least in part, the tendency of SSS to develop AF as a part of its natural history.
Clinical electrophysiology has focused the attention on the electrophysiological and
structural properties of the atrial muscle in patients with SSS: shortened and inhomogeneous
refractoriness and local and regional conduction slowing, as well as prolonged intra- and
inter-atrial conduction disturbances, are well described as increased interstitial fibrosis
associated with the genesis of AF.
A growing body of evidences has shown that inhibition of the renin-angiotensin system can
prevent the promotion of AF by suppressing the development of atrial fibrosis and structural
remodeling. At present, the influence of a treatment target aiming on altered fibrosis and
structural substrate in patients with SSS is not yet known. One striking result of the
losartan intervention for endpoint reduction in hypertension (LIFE) study was that new-onset
AF and associated stroke were significantly reduced by losartan- compared to atenolol-based
antihypertensive treatment with similar blood pressure reduction.
The relative risk of new-onset AF in losartan group is 0.67 compared to atenolol group
(i.e.; 33% risk reduction) Therefore, there is every reason to believe that blocking the
renin-angiotensin pathway with angiotensin II type 1 receptor blockade would have positive
influence on AF burden in this clinical setting. Recently, enalapril has been reported to
prevent rapid atrial pacing (4 weeks)-induced interstitial fibrosis and fatty degeneration
of the sinus node and to improve sinus node function in canine model, supporting the
important role of structural changes of sinus node in the regulation of sinus node function.
This possibility supporting therapeutic interventions using RAS inhibitors forms an
attractive theoretical basis for interventions to reverse SND in such patients.
In support of these hypotheses, the present study was undertaken to determine whether
selective angiotensin II type 1 receptor blockade with high dose losartan was effective in
reducing AF burden, pacemaker dependence, shortening of sinus node recovery time, hsCRP, and
NT-pro BNP, and associated cardiovascular events in SSS patients receiving physiologic
pacing.
In this study, all pacemakers are standard rate-adaptive dual chamber pacemakers:
Medtronic Kappa 900 or Versa. At implantation, all patients were programmed to DDI mode at
50 ppm to minimize the ventricular pacing. All patients had the atrial tachyarrhythmia
detection feature programmed "on" after pacemaker implantation. This feature provides
information on the date, time of onset, and duration of the first 15 consecutive episodes of
an atrial tachyarrhythmia. This information can be retrieved during follow-up visits using
the pacemaker programmer.Patients were evaluated every 3 months after pacemaker
implantation. At each visit, the atrial tachyarrhythmia diagnostic data were retrieved. Each
episode classified as an atrial tachyarrhythmia was reviewed by one of the investigators.
False-positive detections of AF due to oversensing were excluded using specific rules
developed in the course of previous clinical trials. On review of the beat-to-beat intervals
stored in the diagnostic counters during an episode classified as AF, far-field oversensing
was defined if
1. Long intervals between successive detected atrial events were paced and short intervals
were sensed; or
2. The difference between the first, third, fifth, and seventh atrial intervals and the
second, fourth, sixth, and eighth intervals was > 150 beats/min; or
3. The sum of the long and short interatrial intervals was equal to the interatrial
intervals recorded before or after termination of the episode.
The atrial tachycardia detection feature in the Medtronic Kappa 900 or Versa was used for AF
detection in this study. This feature has been reported to have a high sensitivity and
specificity for the detection of atrial tachyarrhythmias. All atrial leads were bipolar. The
atrial sensitivity was programmed to 0.5 mV, which is the standard clinic protocol. The
programming parameters for AF detection included a post-ventricular atrial blanking period
of 150 msec, a tachycardia detection rate of 180 beats/min, the number of beats for atrial
tachycardia detection of 200, the number of beats for tachycardia termination of 10, and the
diagnostic arrhythmia counter was frozen in order to collect information on the first 15
tachycardia episodes. These parameters were selected to optimize the detection of AF and to
reduce the likelihood that nonsustained AF would fill the diagnostic counters. AF episodes <
1 minute in duration were not detected as an episode of AF. To maximize collection of
sequential episodes of AF, the atrial electrogram storage feature was not used. In the Kappa
900 or Versa, an electrogram can be retrieved for the first episode of AF detected (if the
episode occurs within a programmable time) and, in these cases, the electrogram was reviewed
to ensure appropriate classification of AF.
Sustained AF was defined as an atrial tachyarrhythmia with an atrial rate > 250 beats/min
and duration > 1 minute. The atrial rate was determined based on review of the interatrial
intervals stored in the device diagnostics during each episode.
AF burden was defined as the quantity of AF documented during the follow-up period and
expressed as a portion of the follow-up period (hours/day). When the event counters were
filled, AF burden was calculated as the total duration of AF during the time required to
fill the counters.
Permanent AF was defined as AF present at two consecutive visits and an AF burden of 24
hours/day between those visits.
CSNRT at pacemaker implant and each visit :
The corrected sinus node recovery time (CSNRT) was assessed at CLs of 600, 500 and 400 ms
after a 30-second pacing train from the atrial lead. The measurement of CSNRT was repeated 3
times, and averaged. Atrial-based pacemaker dependence Pacemaker dependency was defined as
the absence of escape or intrinsic rhythm for at least 30 seconds after gradual slowing of
the pacing rate to 30 beats/min. Pacemaker dependency was examined every 3 months.
Measurement of Intrinsic Heart Rate Pacing system follow-ups, including measurements of
pacing/sensing characteristics, lead impedance, and surveillance of battery status were
performed every 3 months in each patient. Endocardial atrial and ventricular electrograms
were recorded via a programmer with the pacing mode temporarily set to AAI at a lower rate
of 30 beats/min. A temporary programmable function that allows markers to appear on the
programmer's electrocardiographic recording, corresponding to spontaneous events sensed by
the pulse generator, was used to measure the rate of intrinsic or escape rhythms.
Pacing rate was manually step-downed to 30 beats/min in every 10 beats/min from the lower
pacing rate, and intrinsic or escape rhythms were checked at each pacing rate. A fixed
pacing rate of 30 beats/min following the gradual decrease was maintained for at least 30
seconds to allow the emergence of intrinsic or escape rhythms.
Approximately 220 male and female patients, aged 20 to 80 years, with SSS will be enrolled
and randomly assigned to the losartan add on physiological atrial-based pacing or
physiological atrial-based pacing alone treatment arm. The sample size was calculated to
provide the study with 80% power for a two-sided alpha level of 0.05. Assuming a 33%
reduction of AF incidence rate in the losartan group compared with physiological pacing only
group after 1 year after randomization. Based on these assumptions, the total sample size
required was estimated to be 100 patients in each arm. Thus we need to enroll 220 eligible
cases.
Study medication (losartan) will be in tablet form. Patients randomized to the losartan arm
will receive 50 mg once a day for 2 weeks, patients will then be up-titrated to 50 mg of
losartan twice a day following the first 2-week therapy. Each patient will be assessed
following 4 weeks of losartan therapy at this dose. If the patient is well tolerated for
this dose they will be maintained on it for the remaining time of the study. If they are
unable to tolerate this target dose they will be permitted to down-titrate and continue on
the highest tolerated dose. Only those patients able to tolerate at least the lowest dose of
losartan will be permitted to continue on study until the end of study period.
Normotensive patients who weigh less than 50 kg, or who are aged over 70 years will receive
25 mg/day for the first 2 weeks, then increase to 50 mg/day, with the aim of reaching 100
mg/day for the rest of the study.
;
Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Single Blind (Subject), Primary Purpose: Treatment
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