For Publishers
DiscoveryMetadataPeer reviewHostingPublishing
For Researchers
JoinPublishReviewCollect
Register
Blog
About
Search
Advanced search
My ScienceOpen
Search
For Publishers
For Researchers
Blog
About
606
views
20
references
 Top references
cited by
0
    
0 reviews
 Review
0
comments
 Comment
0
recommends
+1 Recommend
1 collections
    6
    shares
      219
      similar
       All similar

      CVIA now indexed by SCOPUS from February 2024. CVIA received its first Journal Impact Factor (0.5) in the 2023 Journal Citation Reports Release. 

      Interested in becoming a CVIA published author?

      • Platinum Open Access with no APCs. 
      • Fast peer review/Fast publication online after article acceptance.

      Submissions should be made electronically at: https://mc04.manuscriptcentral.com/cvia-journal.

      Please refer to the Author Guidelines at https://cvia-journal.org/instructions-to-authors/ before submission.

       

      scite_

      Cardiovascular Innovations and Applications

      Volume 3, Issue 1
       
      • Record: found
      • Abstract: found
      • Article: found
      Is Open Access

      Evaluation of Left Ventricular Systolic Function after Pulmonary Valve Replacement Using Cardiovascular Magnetic Resonance Imaging

      review-article
      Bookmark

            Abstract

            Following reparative surgery for tetralogy of Fallot or critical pulmonary stenosis (PS), patients frequently present with severe right ventricular (RV) volume overload due to pulmonary regurgitation, resulting in decreased RV function. Surgical pulmonary valve replacement (PVR) is known to improve RV function, but changes in left ventricular (LV) function after PVR have rarely been described. We sought to determine the midterm results regarding LV systolic function after PVR using cardiac MRI in 40 consecutive patients with repaired TOF (31 patients) or PS (9 patients) with an age of 29±9 years who underwent PVR from 2006 to 2011 at a single center. Cardiac MRI RV and LV volumes before and after PVR were analyzed. Demographics, clinical variables, cardiopulmonary bypass duration, and medications were reviewed. LV ejection fraction (LVEF) increased from (54±8) to (57±6)% (P=0.02). Before PVR, 26 patients had depressed LVEF of (49±5)% (range 36–54%). In this group, LVEF increased by (7±7)% (P<0.0001) after PVR. Low LVEF before PVR was correlated with increased LVEF after PVR (regression coefficient −0.7, R2=0.59, P<0.0001). Demographics, medications, prior pregnancies, and cardiopulmonary bypass duration had no effect on LVEF after PVR. The increase in LVEF was most significant in patients with low pre-PVR LVEF.

            Main article text

            Abbreviations

            ACE-I

            Angiotensin-converting enzyme inhibitor

            CAD

            Coronary artery disease

            CMR

            Cardiovascular magnetic resonance

            LV

            Left ventricular

            LVEDVI

            Left ventricular end-diastolic volume index

            LVEF

            Left ventricular ejection fraction

            LVESVI

            Left ventricular end-systolic volume index

            PR

            Pulmonary regurgitation

            PS

            Pulmonary stenosis

            PVR

            Pulmonary valve replacement

            rTOF

            Repaired tetralogy of Fallot

            RV

            Right ventricular

            RVEF

            Right ventricular ejection fraction

            TOF

            Tetralogy of Fallot

            Background

            Tetralogy of Fallot (TOF) accounts for approximately 10% of all cases of congenital heart disease, and is one of the most common cyanotic congenital heart defects [1]. It has been more than five decades since the first total TOF repair was performed in 1955 [2]. Reparative surgery permits more than 85% of children born with TOF to survive into adulthood [3]. With advances in surgical techniques, perioperative support, and imaging modalities, long-term outcomes have also substantially improved in the last 20 years, but resultant abnormalities such as severe pulmonary regurgitation (PR), significant right ventricular (RV) enlargement, dyskinetic interventricular septal motion, and reduced RV systolic function are still present in more than half of these patients [4, 5]. It is now commonly accepted that pulmonary valve replacement (PVR) in patients with severe PR and concomitant RV volume overload can result in preservation or recovery of RV function. As such, much of the current literature on congenital heart disease focuses on preservation and recovery of RV function in patients with repaired TOF (rTOF).

            In the last two decades, the presence of left ventricular (LV) systolic dysfunction in adults with rTOF has been increasingly recognized, and was reported in multiple recent studies [69]. Although the left ventricle is not directly involved in the surgical repair of patients with TOF, patients who have undergone total repair appear to be prone to developing LV dysfunction that is out of proportion to the severity of any residual left-to-right shunting or residual PR [10]. The cause of LV dysfunction in such patients remains unclear. Fibrosis, hypertrophy of the interventricular septum, or the presence of a prosthetic patch could prevent the LV chamber from appropriately changing shape or accommodating an increased preload during diastolic filling. Conceivably, such interventricular septal changes could adversely affect LV systolic function, although this remains to be unequivocally proven [11]. Studies have also shown that LV dysfunction is independently predictive of adverse clinical events in patients with rTOF [12]. Khairy et al. [13] showed that the most important variable associated with the risk of appropriate implantable cardioverter-defibrillator shocks in a multivariate analysis of various predictors in patients with rTOF was an elevated LV end-diastolic pressure rather than PR severity, RV function, or the degree of RV volume loading. Broberg et al. [6] in a multicenter study showed that 21% of 511 patients with rTOF had at least mild LV dysfunction, with 6% of their population having an LV ejection fraction (LVEF) of less than 45%. In their study, predictors of LV dysfunction were RV systolic dysfunction, longer palliative shunt duration before complete repair, and arrhythmia history.

            Two recent small cross-sectional studies showed a statistically significant, but modest, increase in LVEF after PVR for volume-overloaded right ventricles. In both studies the degree of improvement in LV systolic function was greater in patients who had depressed LV systolic function before PVR than in those patients who had normal LV systolic function [14]. Echocardiographic parameters, including ventricular strain and strain rate, speckle tracking, and vector velocity imaging have also been used to document abnormalities in LV function or to evaluate interventricular dyssynchrony in patients with rTOF [1517].

            Our primary aim was to determine if surgical PVR would correlate with an increase in LVEF measured by cardiovascular magnetic resonance (CMR) analysis in patients with volume-loaded right ventricles secondary to PR. The secondary aims were to determine the prevalence of LV systolic dysfunction in patients with rTOF or critical pulmonary stenosis (PS), a population with similar issues of PR and RV volume loading following surgical intervention, and to evaluate if demographic and clinical variables, including cardiopulmonary bypass duration, heart failure medication use, coexisting hypertension, and concomitant coronary artery disease (CAD) or diabetes, related to LV systolic dysfunction in this cohort.

            Methods

            Study Population

            Following institutional review board approval, a single-center retrospective review of all patients who underwent surgical PVR from January 2006 to September 2011 was performed. Patients aged 16 years or older at the time of surgery with an initial diagnosis of TOF or critical PS were included if they had undergone CMR imaging before and after PVR. All CMR studies were performed 2 years or less before PVR and at least 6 months after PVR.

            Patient Data

            Relevant medical and surgical history, including date of birth, sex, anatomic diagnosis, surgical history, date of PVR, and date of CMR study, were extracted from medical record review. A history of hypertension, diabetes, or hyperlipidemia and previous or current tobacco use was recorded. Height, weight, and blood pressure at the time of the visit were recorded, if available. New York Heart Association functional class and QRS duration measured from an electrocardiogram (ECG) at the time of CMR imaging were reviewed before and after PVR.

            Cardiac Magnetic Resonance Imaging

            Studies were performed with a commercially available 1.5 T scanner (Magnetom Avanto, Siemens, Erlangen, Germany). Torso or cardiac phased array coils were chosen according to body size. Ventricular dimensions and function were assessed with an ECG-gated steady-state free precession pulse sequence with the following parameters: echo time 1.27 ms, repetition time 41 ms, flip angle 90o, maximum field of view tailored to the patient’s body size to avoid wrap, matrix size 256×100, slice thickness 8 mm, interslice gap 20%, and 12–18 views per segment (depending on heart rate). Steady-state free precession cine imaging sequences were acquired in the following planes during breath holds: two-chamber plane, four-chamber plane, and short-axis plane with 12–15 slices fully covering the ventricular mass. Flow measurements were performed in the proximal main pulmonary artery with a prospectively gated velocity-encoded cine MRI pulse sequence with the following parameters: echo time 1.97 ms, repetition time 48.25 ms, maximum field of view based on the patient’s size to avoid wrap of the vessel, matrix size 192×99, slice thickness 6 mm, and velocity encoding of 150–400 cm/s during free breathing. End-diastolic volumes, end-systolic volumes, stroke volumes, and ventricular ejection fraction were measured with a commercially available software package (Leonardo, Siemens, Erlangen, Germany). All volumes were indexed to body surface area. An ejection fraction between 45 to 55% was considered mildly depressed; an ejection fraction between 35 and 45% was considered moderately depressed; an ejection fraction of 35% or less was considered severely depressed. The last ECG before PVR and the ECG performed at the time of the post-PVR CMR imaging were measured off-line by a single investigator (WAK).

            Statistical Analysis

            All continuous variables are presented as the mean±standard deviation when normally distributed. Paired t tests or the Wilcoxon signed-ranked test were used to compare pre-PVR and post-PVR ventricular volumes and ejection fraction, and a unpaired t test or a Mann-Whitney test was used to compare continuous variables between groups of patients. Statistical significance was inferred when P was less than 0.05.

            Results

            During the study period, 40 patients met the inclusion criteria: 31 had rTOF and 9 had critical PS. The age at the time of PVR was 29±9 years (range 16–53 years). Baseline demographic information is shown in Table 1. Before PVR, LVEF ranged from 35 to 70% as shown in Figure 1. The low-LVEF group consisted of 26 patients (65%) with baseline LVEF of less than 55%; (49±5)%, range 36–54%. Of these, the age at the time of PVR was 31±9 years, with 1.6±0.9 prior open heart surgical procedures. Twenty-one of these patients (81%) had rTOF, and 5 patients had PS. There was no history of CAD in any patient in this group; one patient had diabetes, and four patients used tobacco products. After PVR, in 19% of the patients in the low-LVEF group, angiotensin-converting enzyme inhibitor (ACE-I) therapy was started, and in 31% of the patients, β-blocker therapy was started. In this low-LVEF group, the use of heart failure medications (either ACE-I or β-blocker) did not correlate with significant postoperative increase in LVEF (P=0.75). The normal-LVEF group consisted of 14 patients with LVEF of 55% or more before PVR, age of 25±7 years at the time of PVR, and 1.4±0.5 open heart surgical procedures before PVR. Ten patients (71%) in the normal-LVEF group had rTOF, and four patients had PS. No patients in the normal-LVEF group had diabetes or CAD; two patients had a history of tobacco abuse. After PVR, in 29% of patients ACE-I therapy was started, and in 14% of patients β-blocker therapy was stared. In the normal-LVEF group, the use of heart failure medications (either ACE-I or β-blocker) was not associated with a statistically significant difference in postoperative LVEF increase (P=0.96). Demographics, clinical variables, β-blocker or ACE-I use, prior pregnancies, and cardiopulmonary bypass duration had no effect on post-PVR LVEF (Table 2).

            Figure 1

            Range of Left Ventricular Ejection Fraction before Pulmonary Valve Replacement in all Patients.

            Table 1

            Baseline Demographic Data in Patients before Pulmonary Valve Replacement (PVR).

            VariableEntire cohort (n=40)LVEF <55% before PVR (n=26)LVEF ≥55% before PVR (n=14)P-value
            Age at PVR (years)28.6±8.931±925±70.06
            Male sex17 (43%)12 (46%)5 (36%)0.74
            Body mass index (kg/m2)25.8±5.526.5±5.824.7±5.00.18
            NYHA class1.9±0.62.0±0.61.8±0.60.32
            Diagnosis of TOF31 (78%)21 (81%)10 (71%)0.69
            TOF: transannular patch repair23/31 (74%)14/21 (67%)9/10 (90%)0.22
            TOF: prior shunt8/31 (26%)3/21 (14%)5/10 (50%)0.07
            Diagnosis of PS9 (22%)5 (19%)4 (29%)0.69
            Known CAD000
            Diabetes mellitus1 (2%)1 (4%)0 (0%)1.00
            Tobacco abuse6 (15%)4 (15%)2 (14%)1.00
            Previous pregnancy12/23 women (52%)7/14 women (50%)5/9 women (56%)1.00
            ACE inhibitor use after PVR9 (23%)5 (19%)4 (29%)0.69
            β-blocker use after PVR (%)2531140.44
            Number of surgical procedures before PVR1.5±0.81.6±0.91.4±0.50.45

            ACE, angiotensin-converting enzyme; CAD, coronary artery disease; LVEF, left ventricular ejection fraction; NYHA, New York Heart Association; PS, pulmonary stenosis; TOF, tetralogy of Fallot.

            Table 2

            Demographic Data in Patients After Pulmonary Valve Replacement (PVR).

            VariableLVEF <55% after PVR (n=15)LVEF ≥55% after PVR (n=25)P-value
            Age at PVR (years)31.8±8.426.6±8.80.07
            Male sex8 (53%)9 (36%)0.34
            Body mass index (kg/m2)27.3±6.225.0±5.00.19
            NYHA class before PVR2.1±0.51.9±0.60.32
            Diagnosis of TOF9 (60%)22 (88%)0.06
            TOF: transannular patch repair6/9 (67%)17/22 (77%)0.66
            TOF: prior shunt1/9 (11%)7/22 (32%)0.38
            Known CAD00
            Diabetes mellitus1 (7%)00.38
            Tobacco abuse3 (20%)3 (12%)0.65
            ACE inhibitor use after PVR4 (27%)5 (20%)0.71
            β-blocker use after PVR5 (33%)6 (24%)1.00
            Cardiopulmonary bypass duration during PVR (min)116±46124±710.68

            ACE, angiotensin-converting enzyme; CAD, coronary artery disease; LVEF, left ventricular ejection fraction; NYHA, New York Heart Association; TOF, tetralogy of Fallot.

            Twelve women had successful pregnancies; seven of these had baseline LVEF of less than 55%. Two women had one pregnancy, six women had two pregnancies, three women had three pregnancies, and one woman had four pregnancies. There were no differences in pre-PVR or post-PVR LVEF or volumetric indices when CMR data for women with and without pregnancies were compared (Table 1). There were no patients with known CAD; one patient had diabetes mellitus, one patient had a history of hypertension, and six patients (15%) were known smokers. There was no statistically significant correlation between these risk factors for CAD and reduced LVEF before or after PVR. There were also no differences in any of the CMR variables (PR, ejection fraction, or volumetric indices) between patients with a pre-PVR BMI of less than 25 kg/m2 and those with a pre-PVR BMI of 25 kg/m2 or more (P=0.32) (Table 1).

            All patients with moderately reduced LVEF (LVEF 35–45%) also had moderately to severely reduced RV ejection fraction (RVEF) before PVR (Figure 2). There was no significant correlation between LVEF and RVEF before PVR. There was no statistically significant difference in RVEF before PVR between the rTOF group and the PS group; (40±9)% and (36±13)%, respectively (P=0.21) (Table 3). The pre-PVR and post-PVR RV end-diastolic volume indices were comparable in both groups. There was also no statistically significant difference in pulmonary regurgitant fraction between the rTOF group and the PS group (P=0.195) (Table 3).

            Figure 2

            Correlation of Right Ventricular Ejection Fraction (RVEF) and Left Ventricular Ejection Fraction (LVEF) before Pulmonary Valve Replacement (PVR).

            All patients with moderately reduced LVEF before PVR also had moderately to severely reduced RVEF.

            Table 3

            Comparison of Cardiac Magnetic Resonance Parameters between the Tetralogy of Fallot (TOF) Group and the Pulmonary Stenosis (PS) Group.

            VariableTOF groupPS groupP-value
            Number of patients319
            Male sex14 (45%)3 (33%)0.707
            Age at time of PVR (years)27.5±8.632.1±9.30.181
            LVEF before PVR (%)53±854±90.736
            LVEF after PVR (%)58±655±60.153
            RVEF before PVR (%)40±936±130.210
            RVEF after PVR (%)44±943±110.894
            RVEDVI before PVR (mL/m2)128±36122±160.645
            RVEDVI after PVR (mL/m2)90±2387±380.730
            RVEDV/LVEDV ratio before PVR2.0±0.52.4±1.00.154
            RVEDV/LVEDV ratio after PVR1.3±0.31.4±0.90.394
            LVEDVI before PVR (mL/m2)67±1761±290.446
            LVEDVI after PVR (mL/m2)73±1966±220.396
            Pre-PVR PR regurgitant fraction (%)47±1141±160.195
            QRS duration before PVR (ms)150±26129±330.048
            QRS duration after PVR (ms)148±25127±310.041
            Cardiopulmonary bypass duration during PVR (min)119±47129±1030.687
            Total number of cardiac surgical procedures2.5±0.72.6±1.00.892
            ACE inhibitor or β-blocker use after PVR12 (39%)3 (33%)1.000

            ACE, angiotensin-converting enzyme; LVEDV, left ventricular end-diastolic volume; LVEDVI, left ventricular end-diastolic volume index; LVEF, left ventricular ejection fraction; PR, pulmonary regurgitation; PVR, pulmonary valve replacement; RVEDV, right ventricular end-diastolic volume; RVEDVI, right ventricular end-diastolic volume index; RVEF, right ventricular ejection fraction.

            Pre-PVR CMR studies were done at 173±103 days (range 33–459 days) before surgery, and the post-PVR CMR studies were done at 412±196 days (range 188–730 days, median 375 days) after surgery. In the entire cohort, LVEF increased from (54±8) to (57±6)% (P=0.023). Before PVR, there were 26 patients with depressed LVEF: (49±5)%, range 36–54%. In this group, LVEF increased by (7±7)% after PVR (P<0.0001). By multivariate analysis to assess CMR predictors for increased LVEF after PVR, the only independent variable that was significantly associated with a postoperative increase in ejection fraction was a low LVEF before PVR, as seen in Figures 3 and 4 (regression coefficient −0.7, R2=0.59, P<0.0001). In the entire cohort (n=40), the LV end-diastolic volume index (LVEDVI) after PVR increased from 66±20 mL/m2 to 71±19 mL/m2 (P=0.03), with no significant change in LV end-systolic volume index (LVESVI): 31±12 mL/m2 before PVR and 34±14 mL/m2 after PVR (P=0.15) (Table 4). LVEF increased to (56.3±5.8)% after PVR in patients with a baseline low pre-PVR LVEF and increased to (58.7±5.7)% in patients who had a preserved LVEF of 55% or greater (P=0.22) (Table 4).

            Figure 3

            Change in Left Ventricular Ejection Fraction (LVEF) after Pulmonary Valve Replacement (PVR).

            Red lines depict patients with initial LVEF of less than 55%. Blue lines depict patients with initial LVEF of 55% or more. The mean LVEF of the low-LVEF group (red lines) increased from 49 to 56% (P<0.0001). The change in LVEF of the normal-LVEF group (blue lines) was not statistically significant (P=0.138).

            Figure 4

            Change in Left Ventricular Ejection Fraction (LVEF) as a Function of LVEF before Pulmonary Valve Replacement (PVR).

            The only statistically significant variable to correlate with an increase in LVEF after PVR was the pre-PVR LVEF. Lower pre-PVR LVEF correlates with a statistically significant increase in LVEF after PVR (P<0.0001).

            Table 4

            Comparison of Cardiac Magnetic Resonance Parameters in Patients with Baseline Low Left Ventricular Ejection Fraction (LVEF) (≤55%) and Normal LVEF (≥55%) before Pulmonary Valve Replacement (PVR).

            VariableEntire cohort (n=40)Baseline LVEF <55% (n=26)Baseline LVEF ≥55% (n=14)P-value
            LVEF before PVR (%)57.1±5.856.3±5.858.7±5.70.22
            RVEF before PVR (%)39.2±9.839.2±9.839.3±10.10.99
            RVEF after PVR (%)43.5±9.244.9±9.440.8±8.50.18
            Pre-PVR QRS duration (ms)145±29144±32146±220.84
            RVEDVI before PVR (mL/m2)127±32125±32131±350.55
            RVEDVI after PVR (mL/m2)89±2789±2990±220.85
            LVEDVI before PVR (mL/m2)66±2065±2366±130.86
            LVEDVI after PVR (mL/m2)71±1973±2168±170.39
            LVESVI before PVR (mL/m2)31±1233±1326±70.04
            LVESVI after PVR (mL/m2)34±1432±1027±60.15
            RVEDV/LVEDV ratio before PVR2.06±0.692.10±0.792.00±0.500.69
            RVEDV/LVEDV ratio after PVR1.30±0.501.22±0.271.45±0.770.17
            PR regurgitant fraction (%)46±1248±1442±80.13

            LVEDV, left ventricular end-diastolic volume; LVEDVI, left ventricular end-diastolic volume index; LVESVI, left ventricular end-systolic volume index; PR, pulmonary regurgitation; RVEDV, right ventricular end-diastolic volume; RVEDVI, right ventricular end-diastolic volume index; RVEF, right ventricular ejection fraction.

            The CMR volumetric and functional (LVEF) parameters were also compared in patients after PVR, with the patients divided into two main groups: patients with normal LVEF and those with low LVEF (<55%) after PVR. For patients with low LVEF after PVR, there was no significant change in LVEF in this subgroup: pre-PVR LVEF of (52.8±8)% and post-PVR LVEF of (51.2±2.6)% (P=0.46) (Table 5). However, in patients with low LVEF after PVR, RVEF significantly increased from (36.0±7.1) to (42.5±9.2)% (P=0.01) after PVR (Table 5). There were no statistically significant changes in the diastolic or systolic LV volumetric indices before or after PVR in patients who had either a low LVEF or preserved LVEF after PVR. The degree of PR before PVR did not correlate with either RV or LV diastolic/systolic indices or RVEF or LVEF in either group after PVR (Table 5).

            Table 5

            Comparison of Cardiac Magnetic Resonance Parameters in Patients with Low Left Ventricular Fraction (LVEF) and Normal LVEF After Pulmonary Valve Replacement (PVR).

            VariableEntire cohort (n=40)Post-PVR LVEF <55% (n=15)Post-PVR LVEF ≥55% (n=25)P-value
            LVEF before PVR (%)53.7±8.152.8±8.0%54.2±8.2%0.61
            LVEF after PVR (%)57.1±5.851.2±2.6%60.7±3.9%
            RVEF before PVR (%)39.2±9.836.0±7.1%41.2±10.8%0.11
            RVEF after PVR (%)43.5±9.242.5±9.2%44.1±9.3%0.60
            Pre-PVR QRS duration (ms)145±29133±34153±230.03
            RVEDVI before PVR (mL/m2)127±32118±18132±380.20
            RVEDVI after PVR (mL/m2)89±2781±2694±260.15
            LVEDVI before PVR (mL/m2)66±2062±2168±190.34
            LVEDVI after PVR (mL/m2)71±1966±2274±170.20
            LVESVI before PVR (mL/m2)31±1229±1231±110.58
            LVESVI after PVR (mL/m2)34±1432±1129±80.34
            RVEDV/LVEDV ratio before PVR2.06±0.692.13±0.852.02±0.600.65
            RVEDV/LVEDV ratio after PVR1.30±0.501.35±0.761.28±0.670.68
            PR regurgitant fraction (%)46±1241±1248±120.136

            LVEDV, left ventricular end-diastolic volume; LVEDVI, left ventricular end-diastolic volume index; LVESVI, left ventricular end-systolic volume index; PR, pulmonary regurgitation; RVEDV, right ventricular end-diastolic volume; RVEDVI, right ventricular end-diastolic volume index; RVEF, right ventricular ejection fraction.

            Discussion

            Although the right ventricle has been the primary focus of attention in patients with rTOF, LV dysfunction is not an uncommon finding in these patients, and may play a role in determining long-term morbidity and mortality. The presence of LV systolic dysfunction in adults with rTOF has been increasingly recognized, and was reported in multiple recent studies [69]. It has been suggested that the reduced volume load on the right ventricle after PVR results in the rapid improvement of RV systolic function and in a more gradual recovery of RV diastolic function [17]. Although the right ventricle and left ventricle are separate chambers, their interdependence has been described in the past. The ventricular chambers are anatomically linked in several ways, including by spiral muscle fibers that ensure synchronous contraction, with evidence for hemodynamic impact of the right ventricle on the left ventricle, and vice versa. This has been demonstrated in several studies in both the normal heart and the diseased heart [18, 19]. Since the right ventricle is more compliant than the left ventricle, a significant degree of RV volume overload is required to adversely affect LV compliance and geometry with consequent LV dysfunction. Such ventricular changes are often seen in patients with rTOF secondary to long-standing severe PR. It therefore stands to reason that LV function may improve following restoration of pulmonary valve competence. This functional recovery can differ depending on the preoperative status of LV function [19].

            Although LV systolic dysfunction has been reported in rTOF, there are only sparse data regarding its prevalence, associated factors, and etiological cause [9]. Factors playing a role in decreased LV function can include abnormalities of the ventricular septum due to surgical patch material and septal or myocardial fibrosis from prior surgical repair, all of which would be difficult to reverse with PVR [14]. Our findings of an LVEF increase for all patients and a significantly larger LVEF increase for patients with more depressed LVEF at the baseline (before PVR) are similar to those of recent studies by Tobler et al. [19] using CMR imaging and Kane et al. [14] using echocardiography. The findings of Tobler et al. [19] imply that there was an increase in LV contractility, rather than an increase in LV end-diastolic volumes, driving the increase in LVEF after PVR in patients with an abnormal LVEF at the baseline. An alternative hypothesis to explain LVEF increase after PVR is that restored pulmonary valve competence results in increased forward flow through the pulmonary vasculature and thus increased pulmonary venous return to the left atrium and left ventricle, thereby increasing LVEDVI without changing contractility.

            Studies in young adults have demonstrated a significant increase in LVEDVI with a significant improvement in CMR or echocardiographic indices of LV systolic function following PVR [14, 20]. We found a statistically significant, but only mild, increase in LVEDVI of 5 mL/m2 in the entire cohort (P=0.03). There was a statistically significant increase in LVEDVI in the low-LVEF group, but this trend was not demonstrated in patients with preserved LVEF before PVR. There was no significant change in LVESVI in either the low-LVEF group or the preserved-LVEF group. Our study did not show any relationship between the severity of PR and LV dysfunction (P=0.136).

            Since all rTOF patients had a ventricular septal defect patch as part of their complete intracardiac repair, the mechanics of the interventricular septum are likely very different in rTOF patients compared with PS patients given that a ventricular septal defect patch has no contractility. However, both disease processes (rTOF and PS) are associated with hemodynamically significant PR and resultant RV dilation and dysfunction, which are thought to affect LV function adversely.

            Limitations

            We are limited by the retrospective nature of this study. Because this was a retrospective study, data were limited to those available from medical record review. Referral bias is expected because patients were selected from a single established tertiary care adult congenital heart disease center. This was a single-center study with a small number of patients and, thus, limited statistical power.

            Conclusions

            Although LV volume and systolic function can be abnormal in adults late after TOF repair, PVR may have a beneficial effect on LV systolic function. We found that the only independent CMR predictor of postoperative improvement in LV systolic function is preoperative LV systolic dysfunction. This may be secondary to normalization of interventricular interactions after PVR, but the exact mechanisms responsible are as yet unknown. Larger studies are needed to further analyze our findings and determine accurate predictors associated with increased LVEF following PVR.

            Author Contributions

            Both authors designed the study, contributed to data acquisition, analysis, and interpretation, and read and approved the final manuscript.

            Conflict of Interest

            The authors declare no conflict of interest.

            References

            1. HoffmanJI. Incidence of congenital heart disease: I. Postnatal incidence. Pediatr Cardiol 1995;16:10313.

            2. TherrienJ, SiuSC, McLaughlinPR, LiuPP, WilliamsWG, WebbGD. Pulmonary valve replacement in adults late after repair of tetralogy of Fallot: are we operating too late? J Am Coll Cardiol 2000;36:16705.

            3. MurphyJG, GershBJ, MairDD, FusterV, McGoonMD, IlstrupDM, et al. Long-term outcome in patients undergoing surgical repair of tetralogy of Fallot. N Engl J Med 1993;329:5939.

            4. WaldRM, LyseggenE, OechslinEN, WebbGD, SilversidesCK. Variability in surgical referral patterns for pulmonary valve replacement in adults with repaired tetralogy of Fallot. Congenit Heart Dis 2009;4:2318.

            5. EyskensB, BrownSC, ClausP, DymarkowskiS, GewilligM, BogaertJ, et al. The influence of pulmonary regurgitation on regional right ventricular function in children after surgical repair of tetralogy of Fallot. Eur J Echocardiogr 2010;11:3415.

            6. BrobergCS, AboulhosnJ, MongeonFP, KayJ, ValenteAM, KhairyP, et al. Prevalence of left ventricular systolic dysfunction in adults with repaired tetralogy of Fallot. Am J Cardiol 2011;107:121520.

            7. GevaT, SandweissBM, GauvreauK, LockJE, PowellAJ. Factors associated with impaired clinical status in long-term survivors of tetralogy of Fallot repair evaluated by magnetic resonance imaging. J Am Coll Cardiol 2004;43:106874.

            8. Babu-NarayanSV, KilnerPJ, LiW, MoonJC, GoktekinO, DavlourosPA, et al. Ventricular fibrosis suggested by cardiovascular magnetic resonance in adults with repaired tetralogy of Fallot and its relationship to adverse markers of clinical outcome. Circulation 2006;113:40513.

            9. GhaiA, SilversidesC, HarrisL, WebbGD, SiuSC, TherrienJ. Left ventricular dysfunction is a risk factor for sudden cardiac death in adults late after repair of tetralogy of Fallot. J Am Coll Cardiol 2002;40:167580.

            10. RocchiniAP, KeaneJF, FreedMD, CastanedaAR, NadasAS. Left ventricular function following attempted surgical repair of tetralogy of Fallot. Circulation 1978;57:798802.

            11. BorowKM, GreenLH, CastanedaAR, KeaneJF. Left ventricular function after repair of tetralogy of Fallot and its relationship to age at surgery. Circulation 1980;61:11508.

            12. KnauthAL, GauvreauK, PowellAJ, LandzbergMJ, WalshEP, LockJE, et al. Ventricular size and function assessed by cardiac MRI predict major adverse clinical outcomes late after tetralogy of Fallot repair. Heart 2008;94:2116.

            13. KhairyP, HarrisL, LandzbergMJ, ViswanathanS, BarlowA, GatzoulisMA, et al. Implantable cardioverter-defibrillators in tetralogy of Fallot. Circulation 2008;117:36370.

            14. KaneC, KogonB, PernetzM, McConnellM, KirshbomP, RodbyK, et al. Left ventricular function improves after pulmonary valve replacement in patients with previous right ventricular outflow tract reconstruction and biventricular dysfunction. Tex Heart Inst J 2011;38:2347.

            15. CheungEW, LiangXC, LamWW, CheungYF. Impact of right ventricular dilation on left ventricular myocardial deformation in patients after surgical repair of tetralogy of Fallot. Am J Cardiol 2009;104:126470.

            16. van der HulstAE, DelgadoV, HolmanER, KroftLJ, de RoosA, HazekampMG, et al. Relation of left ventricular twist and global strain with right ventricular dysfunction in patients after operative “correction” of tetralogy of Fallot. Am J Cardiol 2010;106:7239.

            17. MuellerM, RentzschA, HoetzerK, Raedle-HurstT, BoettlerP, StillerB, et al. Assessment of interventricular and right-intraventricular dyssynchrony in patients with surgically repaired tetralogy of Fallot by two-dimensional speckle tracking. Eur J Echocardiogr 2010;11:78692.

            18. SpadaroJ, BingOH, GaaschWH, WeintraubRM. Pericardial modulation of right and left ventricular diastolic interaction. Circ Res 1981;48:2338.

            19. ToblerD, CreanAM, RedingtonAN, Van ArsdellGS, CaldaroneCA, NanthakumarK, et al. The left heart after pulmonary valve replacement in adults late after tetralogy of Fallot repair. Int J Cardiol 2012;160:16570.

            20. FrigiolaA, RedingtonAN, CullenS, VogelM. Pulmonary regurgitation is an important determinant of right ventricular contractile dysfunction in patients with surgically repaired tetralogy of Fallot. Circulation 2004;110(11 Suppl 1):II-1537.

            Author and article information

            Journal
            Journal ID (publisher-id): CVIA
            Title: Cardiovascular Innovations and Applications
            Abbreviated Title: CVIA
            Publisher: Compuscript (Ireland )
            ISSN (Electronic): 2009-8782
            ISSN (Print): 2009-8618
            Publication date (Print): May 2018
            Publication date (Electronic): May 2018
            Volume: 3
            Issue: 1
            Pages: 21-30
            Affiliations
            [1] 1Columbus Ohio Adult Congenital Heart Disease Program, The Heart Center, Nationwide Children’s Hospital and Division of Cardiovascular Medicine, Wexner Medical Center, The Ohio State University, Columbus, OH, USA
            [2] 2Division of Pediatric Cardiology, The Heart Center, Nationwide Children’s Hospital, The Ohio State University, Columbus, OH, USA
            [a] aNow at: Adult Congenital Heart Disease Program, Indiana University/Indiana University Health, Riley Children’s Hospital, 1801 N Senate Blvd, Suite 2000 Indianapolis, IN 46202, USA.
            [b] bNow at: Montefiore Einstein Center for Heart & Vascular Care, The Children’s Hospital at Montefiore, The Albert Einstein College of Medicine 111 East 210th Street, NY 10467, USA.
            Author notes
            Correspondence: Ali N. Zaidi, MD, Director – Montefiore Adult Congenital Heart Disease Program (MAtCH), Associate Professor Internal Medicine and Pediatrics, Montefiore Einstein Center for Heart and Vascular Care, The Children’s Hospital of Montefiore, The University Hospital for Albert Einstein College of Medicine, 111 East 210th Street, New York, NY 10467, USA, Tel.: +1-718-9205882, E-mail: azaidi@ 123456montefiore.org
            Article
            Publisher ID: cvia20170050
            DOI: 10.15212/CVIA.2017.0050
            SO-VID: 8034e69e-4ffa-4a24-aa87-d853b56850d7
            Copyright © Copyright © 2018 Cardiovascular Innovations and Applications
            License:

            This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 Unported License (CC BY-NC 4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. See https://creativecommons.org/licenses/by-nc/4.0/.

            History
            Date received : 17 November 2017
            Date revision received : 12 February 2018
            Date accepted : 13 March 2018
            Categories
            Subject: Reviews

            ScienceOpen disciplines: General medicine,Medicine,Geriatric medicine,Transplantation,Cardiovascular Medicine,Anesthesiology & Pain management
            Keywords: pulmonary valve replacement,tetralogy of Fallot

            Comments

            Comment on this article