Ischemic Heart Disease Clinical Trial
Official title:
Italian Multicenter PROject on Echo Assessment of Left VEntricular (IMPROVE) Dyssynchrony Study
Background. Clinical benefits of cardiac resynchronization therapy (CRT) have been clearly
demonstrated in heart failure (HF) patients with severe left ventricular (LV) dysfunction
and wide QRS at surface electrocardiogram. However, there is a growing evidence that QRS
duration poorly predicts responses to CRT, and that ~30% of patients do not experience any
benefit from CRT when pre-implant dyssynchrony is defined according to electrocardiographic
criteria. A number of echocardiographic criteria have been proposed to assess mechanical LV
dyssynchrony, but at present there is no consensus on their use to predict response to CRT.
Study Design. The Italian Multicenter PROject on echo assessment of left VEntricular
(IMPROVE) dyssynchrony study is a prospective, multicenter, observational study aimed to
assess feasibility and predictive power of mechanical dyssynchrony assessed by
echocardiography in consecutive consenting patients candidate to CRT by clinical and
electrocardiographic criteria. IMPROVE will enroll 120 healthy subjects and 216 HF patients
in 6 sites in Italy. CRT response criteria will be based on improvement in NYHA class and LV
reverse remodeling evaluated by 3D-echocardiography. Enrollment is expected to conclude
early 2009.
Implications. CRT is today part of the therapeutic armamentarium for symptomatic HF patients
refractory to medical therapy, with wide QRS complex and severe LV systolic dysfunction. The
IMPROVE study has been designed to evaluate reference values of indexes of ultrasound
mechanical dyssynchrony that have been proposed in the literature and compare their ability
to predict response to CRT in HF patients.
The IMPROVE study has 3 main purposes:
1. definition of reference values of echocardiographic mechanical dyssynchrony (DYS)
indexes in a population of healthy subjects;
2. definition of the feasibility and reproducibility of such indexes in healthy subjects
and in HF patients undergoing implantation of a biventricular pacemaker;
3. definition of the accuracy of such indexes for predicting response to CRT.
STUDY DESIGN. Multicenter, prospective, observational study that will be carried out in
6 Italian sites of acknowledged expertise in LV DYS evaluation and biventricular
pacemaker implantation. At least 120 healthy subjects (about 20 per site) and 216 HF
patients candidates to CRT (about 36 per site) will be enrolled. With this sample
volume it is possible to test statistically significative differences of about 7%, with
an alfa=0.05 and beta=0.50. Definition of healthy subject includes absence of history
and symptoms of any cardiovascular disease, normal physical examination and ECG. The
same commercial ultrasound equipment will be used for image acquisition in each
investigating center and echo studies will be sent to a core-lab for analysis.
Both ischemic and non ischemic etiology of HF will be considered. Patients with
permanent or persistent atrial fibrillation or flutter will be excluded, as these
patients cannot benefit from the atrial-ventricular component of resynchronization.
The following evaluations:
- clinical examination, including NYHA class estimate;
- 12-lead standard ECG;
- echocardiographic examination. will be performed within 7 days before CRT and
repeated after 3 months of CRT. Patients will receive all appropriate treatments
for HF, which include a diuretic, an ACE- inhibitor, or an angiotensin receptor
blocker and usually digitalis and a beta-blocker. Doses of these background
medications will be kept maximized during the follow-up period.
Response to CRT will be assessed after 3 months of CRT as follows:
- CRT response: combined end-point defined as NYHA class improvement by at least one
grade and echocardiographic LV end-systolic volume decrease by at least 10% with
respect to baseline (variations are considered as relative values);
- CRT non-response: death for cardiac causes or failure to reach the above
pre-specified NYHA class and echocardiographic changes.
Patients who will die for non-cardiac causes will not be considered as non-responders
but will exit the study.
ECHOCARDIOGRAPHY
- Image acquisition. Conventional M-mode and B-mode two-dimensional (2D)
echocardiography, conventional pulsed (PW), continuous (CW) wave and color Doppler,
tissue Doppler imaging (TDI), triplane tissue synchronization imaging (TSI) and RT3DE
techniques will be used for data acquisition in each site using a GE-Vingmed Vivid 7
Dimension echo scanner (GE Healthcare, Horten, Norway), equipped with a broad-band M3s
probe (2.5 MHz) and a matrix-array 3V probe (2.5 MHz), and the EchoPAC software v. BT05
or more.
Ultrasound scanning will be performed after 10 min rest with the patient in left
lateral decubitus position (unless differently specified). Standard parasternal, apical
and subcostal views will be acquired in conventional 2D modality. From the parasternal
approach the 3 standard short-axis views (basal, mid-ventricle and apical) will be
collected. The mid-LV short-axis view will be selected with the papillary muscle as a
consistent internal anatomic landmark, and great care will be taken to orient the image
to the most circular geometry possible. Oblique views with elliptical geometry will not
be recorded. From the apical approach, the 3 standard apical views (4-chamber,
2-chamber, long-axis) will be acquired also in triplane mode. Using this technique,
once the apical 4-chamber view is optimized similar to the one obtained with the
traditional 2D transducer, secondary image planes (i.e., apical 2-chamber and long-axis
views) are automatically displayed in a quad screen view. The relative angles between
the 3 image planes will be adjusted to acquire the 3 standard apical views according to
anatomical landmarks. All apical images (2D and triplane) will be collected in
gray-scale, color TDI and TSI modality. Gain settings will be adjusted for routine
clinical gray-scale 2D imaging to optimize endocardial definition; frame rates will be
kept between 55 and 70 fps to allow subsequent speckle tracking analysis (see below).
Sector angle, depth, and Doppler pulse repetition frequency will be optimized to obtain
the highest possible frame rate (>100 fps) avoiding loss of spatial data and aliasing
in the TDI modality. RT3DE datasets will be obtained from the apical approach
immediately after acquisition of 2D apical views, with the patient in the same
position. In order to include the entire LV into the 3D dataset, a full-volume
acquisition mode will be used. Using this approach it is possible to "stitch" together
4 sub-volumes obtained in real-time over consecutive cardiac cycles according to a
previously described technique and protocol. This will create an on-line rendered image
of the scanning sector with a time resolution of around 40-50 ms equivalent to a volume
rate of 20-25 volumes per second. Measurements of RT3DE volumes will be performed
off-line (4D analysis, TomTec Gmbh, Ubterschlessheim, Germany).
For the study of MR, the standard color Doppler examination will be performed in the
apical 4- and 2-chamber views to visualize the regurgitant jet; the flow convergence
area will be recorded in the apical 4-chamber view in zoom mode, with color bar
baseline set between 30 and 40 cm/s; finally, the CW Doppler tracing of the regurgitant
jet will be acquired in the 4-chamber view.
The PW Doppler examination will be performed positioning the sample volume at the level
of the valve tips in the apical 4-chamber view for assessment of mitral inflow and at
the level of the aortic anulus for assessment of aortic outflow.
All conventional and TDI images will be acquired in a cineloop format during hold
end-expiration (unless differently specified). Each cineloop and Doppler tracing will
contain 3 cardiac cycles. All images and tracings will be stored on a CD-ROM for
subsequent analysis. At the time of the echo examination blood pressure will be also
measured.
- Measurements. LV size will be evaluated measuring the end-diastolic and end-systolic
diameters (EDD, ESD, cm) on 2D parasternal short-axis view images and calculating the
end-diastolic and end-systolic volumes (EDV, ESV, ml) using RT3DE. The EDD and EDV will
be indexed for body surface area. LV systolic function will be evaluated using both the
ejection fraction (EF, %) calculated from volumes and the Doppler dP/dt (mmHg/ms)
calculated from the CW MR tracing, when available. MR severity will be evaluated by:
(1) the maximal regurgitant jet area visualized by color Doppler in the apical 4- and
2-chamber views (the average value of the two views will be calculated); (2) the PISA
method; (3) the duration of the CW Doppler tracing of the regurgitant flow. Systolic
pulmonary artery pressure (sPAP) will be calculated from the CW tricuspid regurgitation
tracing.
Several indexes of LV DYS have been selected based on published validation studies in
which LV reverse remodeling has been considered as an end-point (single or combined)
and at least 3 months of follow-up after CRT have been used. Dyssynchrony indexes will
be calculated as previously reported in the literature (the respective cut-off value to
predict positive response to CRT is shown in parentheses).
M-mode indexes
- Septal-to-posterior wall motion delay (cut-off value= 130 ms): measurement will be
obtained from the M-mode tracing of the LV as the time interval between the
maximal inward motion of the septum and the left posterior wall.
- Lateral wall postsystolic displacement: difference of intervals from QRS onset to
maximal systolic displacement of the basal LV lateral wall (assessed by M-mode in
apical 4-chamber view) and from QRS onset to the beginning of the E wave (assessed
by PW Doppler of mitral inflow); a positive value identifies a pathologic
post-systolic contraction.
TDI time intervals and indexes
- Time to peak systolic velocity: the interval from onset of the QRS to the maximum
positive velocity during the ejection period. The velocities in the isovolumic
contraction and relaxation periods will not be used in this measurement. The region of
interest (ROI) (6 x 6-mm circular shape) will be positioned in the middle of each
segment. Time to peak velocity (Tv) will be measured on each curve from the beginning
of the Q (or R)-wave on the ECG to the peak positive systolic velocity during the
ejection phase, previously defined by the aortic valve opening and closure times. If a
positive velocity will not be observed, the segment will be excluded from the
calculation. If there will be multiple peaks in ejection period with the same velocity,
the earliest peak will be chosen.
- Time to peak velocity, including the postejection period: the interval from onset
of the QRS to the maximum positive velocity, including the period after aortic
valve closure. Everything else as above.
- Time to peak strain: the interval from onset of the QRS to peak negative strain
throughout the cardiac cycle, including postsystolic shortening. The region of
interest (ROI) (6 x 12-mm oval shape) will be positioned in the middle of each
segment. If negative strain will not be identified, the segment will be excluded
from the calculation.
- Time to peak strain exceeding aortic valve closure (ExcT: exceeding time): the
interval between the marker of aortic closure and the nadir of the strain tracing.
ExcT will be considered 0 when the nadir of strain curve will not exceed aortic
valve closure. Everything else as above.
In addition to the time intervals described above, the triplane TSI display of LV
electro-mechanical delays will be evaluated visually (VT-TSI) during the systolic
ejection phase to identify a severe lateral wall delay, marked by the presence of red
color on the lateral wall (alone or in association with other severely delayed
segments).
Using the above described time intervals, the following DY indexes reported in the
literature will be measured:
- Septal-lateral delay (cut-off value= 65 ms): maximum time delay between peak
systolic velocities among four basal segments in 4 chamber and 2 chamber view.
- Anteroseptal-posterior delay (cut-off value= 65 ms): absolute time difference in
time to peak systolic velocity, including the postejection period, between the
basal inferolateral and basal anteroseptal segments.
- Standard deviation in time to peak systolic velocity in the 12 basal and mid
segments using both the two-dimensional tissue Doppler (cut-off value= 33.6 ms)
and the novel triplane TSI modality (Tv-SD index).
- Standard deviation in time to peak strain (cut-off value= 60 ms) among 12 basal
and mid segments as a strain-derived dyssynchrony index (11).
- Overall time of strain exceeding aortic valve closure (cut-off value= 760 ms) as
the sum of 12 basal and mid segments ExcTs (10).
Also, the combined approach based on the Tv-SD index (cut-off value= 34.4 ms) and
VT-TSI severe lateral wall delay will be tested as described by Yu et al.
RT3DE For each of the 16 LV segment, the time taken to reach the minimum regional
volume will be measured and expressed as a percentage of the cardiac cycle. Then, the
systolic dyssynchrony index (cut-off value= 8.3%) will be calculated as the standard
deviation in time to minimum regional volume.
Speckle-tracking analysis For each of the 6 segments of the mid-ventricle short-axis
view, the time to peak radial strain will be measured. Then, the radial strain DYS
(cut-off value= 130 ms) index will be calculated as the difference between earliest and
latest time to peak strain.
Echo core and peripheral laboratory. All investigators must obtain the approval of the
core laboratory before participating in the study by sending a test CD-ROM of adequate
quality to the core laboratory. The core laboratory will be located in Udine (L.P.
Badano). A number of ultrasound images and tracings will be read in 2 peripheral
laboratories to test the interlaboratory reproducibility for evaluation of dyssynchrony
indexes.
Optimization of atrio-ventricular delay will be performed at pre-discharge using
Doppler echocardiography of transmitral flow to provide the maximum LV filling time
without compromising cardiac resynchronization.
Statistical analysis plan.
- Descriptive statistics. Continuous variables will be described as mean and
standard deviation and categorical variables as counts and percentages.
- Statistical analysis: generality. The analysis for the continuous variables will
be conducted by standard methods, unless there is evidence of important deviation
from assumptions of normality, in which case non-parametric "bootstrap" methods
will be used to generate confidence intervals. A two-sided p-value<0.05 will be
considered statistically significant.
1) Evaluation of feasibility and reproducibility of DYS indexes
- Feasibility. Feasibility is defined for each DYS index by the number of patients
in whom the index was actually measured or calculated relative to the number of
patients in whom the measure or calculation was attempted. Feasibility will be
evaluated separately in normals and in patients.
- Measurements of DYS indexes will be repeated in 15 baseline normal studies and 15
baseline patient studies by the same and a second observer at least one week after
the first assessment in the core laboratory to test intra and interobserver
variability. The same normal and patient studies will be read in two peripheral
laboratories to test the interlaboratory variability. All observers will be
unaware of the patients' characteristics, including ECG data. The Lin correlation
coefficient and the Bland-Altman limits of agreement (LOA) will be used to
evaluate intraobserver, interobserver and interlaboratory variabilities.
- To evaluate the strength of the association between dyssynchrony indexes values at
baseline both in normals and in patients, the Pearson R and its 95% confidence
interval (95% C.I.) will be computed.
2) Evaluation of the effects of CRT
- Variations over time. A paired Student t test or an exact symmetry homogeneity
test will be used to compare baseline and 3-month continuous and categorical
values, respectively.
3) Evaluation of the predictive value of the dyssynchrony indexes
- Association with CRT response and power analysis. The association between baseline
dyssynchrony indexes, considered as continuous variables, and CRT response after 3
months will be assessed by means of a logistic model. With the available sample
size and an alpha of 5%, the power for detecting the observed association of the
dyssynchrony indexes with CRT response is computed to 80% for each parameter.
- Association with CRT response based on DYS cut-off values. DYS parameters will
also be dichotomized according to the pre-specified cut-off values derived from
previous reports (see above). Model performances will be empirically compared
through the c statistics for the discriminating ability (corresponding to the
model based area under the ROC curve: the closer to 1, the better the model).
Sensitivity and specificity of the dichotomized dyssynchrony parameters with
respect to response will be computed.
- Association with echocardiographic changes. The association of baseline
dyssynchrony indexes on a continuous scale with the relative changes in
echocardiographic EF and ESV after 3 months of CRT will be assessed by means of
Pearson R.
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