Abstract
Objective. Pulmonary arterial hypertension (PAH) is a life-threatening complication of connective tissue diseases (CTD). Our aim was to compare the diagnostic utility of noninvasive imaging modalities, i.e., magnetic resonance imaging (MRI), computed tomography (CT), and echocardiography, in evaluation of these patients.
Methods. In total, 81 consecutive patients with CTD and suspected PH underwent cardiac MRI, CT, and right heart catheterization (RHC) within 48 hours. Functional cardiac MRI variables [ventricle areas and ratios, delayed myocardial enhancement, position of the interventricular septum, right ventricular mass, ventricular mass index (VMI), and pulmonary artery distensibility] were all evaluated. The pulmonary artery size, pulmonary artery/aortic ratio (PA/Ao), left and right ventricular (RV) diameter ratio, RV wall thickness, and grade of tricuspid regurgitation were measured on CT. Tricuspid gradient (TG) and size of the RV were assessed using echocardiography.
Results. In our study of 81 patients with CTD, 55 had PAH, 22 had no PH, and 4 had PH owing to left heart disease. There was good correlation between mean pulmonary artery pressure (mPAP) and pulmonary vascular resistance (PVR) measured by RHC and VMI derived from MRI (mPAP, r = 0.69, p < 0.001; PVR, r = 0.78, p < 0.001) and systolic area ratio (mPAP, r = 0.69, p < 0.001; PVR, r = 0.68, p < 0.001) and TG derived from echocardiography (mPAP, r = 0.84, p < 0.001; PVR, r = 0.76, p < 0.001). In contrast, CT measures showed only moderate correlation. MRI and echocardiography each performed better as a diagnostic test for PAH than CT-derived measures: VMI ≥ 0.45 had a sensitivity of 85% and specificity 82%; and TG ≥ 40 mm Hg had a sensitivity of 86% and specificity 82%. Univariate Cox regression analysis showed the MRI measurements were better at predicting mortality. Patients with RV end diastolic volume < 135 ml had a better prognosis than those with a value > 135 ml, with a 1-year survival of 95% versus 66%, respectively.
Conclusion. In patients with CTD and suspected PAH, cardiac MRI and echocardiography have greater diagnostic utility than CT in the assessment of patients with suspected PAH, and MRI has prognostic value.
- PULMONARY ARTERIAL HYPERTENSION
- SYSTEMIC SCLEROSIS
- CONNECTIVE TISSUE DISEASE
- MAGNETIC RESONANCE IMAGING
- COMPUTED TOMOGRAPHY
- SURVIVAL
Pulmonary arterial hypertension (PAH) is a serious complication of connective tissue disease (CTD) and is one of the leading causes of mortality1. The prevalence of CTD-associated PAH (CTD-PAH) is estimated to be as high as 13% based on right heart catheterization (RHC)2. This is most commonly seen in the setting of systemic sclerosis (SSc), whereas in patients with systemic lupus erythematosus the estimated prevalence is < 1%3. Patients with CTD-PAH generally have a poor outcome compared to those with idiopathic PAH3,4,5. Within this group, patients with PAH associated with SSc have the poorest prognosis.
Diagnostic tools capable of identifying the presence of PAH with a high degree of accuracy and identifying patients at increased risk of early mortality are essential in this patient population. Echocardiography is recommended as a screening test, with annual echocardiography recommended in patients with SSc and in other forms of CTD when patients have symptoms of breathlessness. However, estimates of pulmonary artery pressure (PAP) cannot always be made and echocardiography can both underestimate and overestimate PAP. RHC remains the “gold standard” to confirm a diagnosis of PH but this is an invasive investigation. In addition it gives only limited information on the cause of PH and gives no detail of the morphology of the cardiac chambers or the pulmonary vascular bed. A noninvasive test that may aid the clinician in risk stratification of patients with CTD who have a poor-quality echocardiogram or in whom the results are equivocal would be of value in diagnosing the presence of PH and aiding classification.
Patients with suspected CTD-PAH routinely undergo high-resolution chest computed tomography (HRCT) to diagnose the presence of interstitial lung disease (ILD) and often CT pulmonary angiography to exclude thromboembolic disease. Cardiac MRI is currently the standard method for morphological and quantitative assessment of cardiac function, and there is increasing interest in its use as a diagnostic tool in patients with suspected PH6. Studies have evaluated cardiac MRI and CT for prediction of the severity of PH associated with various etiologies7,8,9,10, but very little has been reported on the role of cardiac MRI in patients with CTD and suspected PAH. Our aim was to compare the diagnostic usefulness of various MRI, CT, and echocardiographic measures with RHC in patients with CTD and suspected PH, and to evaluate the ability of these imaging modalities to assess severity of PAH and predict mortality.
MATERIALS AND METHODS
Study group
This was a retrospective study of 81 consecutive patients suspected of having CTD-PH and identified from a large cohort of patients referred to our center with suspected PH. The study was carried out in a nationally designated referral center for PH with a referral population of 15 million. Patients were referred to our center for further evaluation of clinical features suggesting PH or after implementation of a screening protocol using the combination of echocardiography, lung function testing, and assessment of symptoms of breathlessness. We recommend that screening be performed in patients with SSc on an annual basis in rheumatology centers referring to our center. From the screening program, patients underwent cardiac catheterization (1) if tricuspid gradient (TG) was ≥ 40 mm Hg; (2) if the TG was ≥ 30 mm Hg but < 40 mm Hg with DLCO < 50%; or (3) in the presence of symptoms of unexplained progressive breathlessness regardless of the results of the echocardiogram11. The diagnosis of CTD was made according to standard criteria and in most cases this was by the referring physician12,13,14. Patients in the study were required to have had CT, MRI, and RHC performed within 48 hours. For comparison with echocardiography this had to be performed at our center within 3 months of RHC. Local research ethics committee approval was obtained for retrospective analysis of imaging techniques. All the CT and MRI scans were reviewed by 2 chest radiologists (SR, AS) blinded to RHC hemodynamics.
The study included patients from January 2008 to March 2010 with a median followup of 24 months. The census date for mortality was March 31, 2011. Patients were treated according to UK national guidelines and prescription of therapies was in accord with the UK national commissioning policy.
Echocardiography protocol
Echocardiography was performed using a Powervision 8000 instrument (Toshiba, Tokyo, Japan). Right ventricle size and TG were measured using the maximum velocity of tricuspid regurgitation and the simplified Bernoulli equation. The median time interval between echocardiogram and RHC was 34 days (interquartile range 3 to 59 days). In 9 patients the echocardiogram data were not available.
CT protocol
CT pulmonary angiography was performed on a 64-slice multidetector CT scanner (Light-Speed, General Electric Medical Systems, Milwaukee, WI, USA). The following measures were used: automated dose reduction 100 mA, 120 kV, 1 pitch, rotation time 0.5 s, 0.625-mm collimation, field of view (FOV) 400 × 400 mm; 100 ml intravenous contrast agent (Ultravist 300; Bayer Schering, Berlin, Germany) was administered at a rate of 5 ml/s. From the contrast-enhanced acquisition, HRCT images were reconstructed for every 10 mm using a high spatial resolution filter.
CT image analysis
The following CT variables were measured: widest short axis diameter of the main pulmonary artery (PA) and the corresponding transverse diameter of the ascending aorta. The right and left PA diameter were also noted15. The maximum short axis distance of the right and left ventricle and right ventricle wall thickness were measured in an axial plane as described16. The severity of reflux of contrast into the inferior vena cava (IVC) or hepatic veins was graded as 0 = no reflux into IVC; 1 = trace of reflux into IVC only; 2 = reflux into IVC but not hepatic veins; 3 = reflux into IVC and proximal hepatic veins; 4 = reflux into IVC and distal hepatic veins17. The presence or absence of pericardial effusion was also assessed on CT. HRCT images were graded for presence or absence of ILD using a scoring system described by Bezante, et al18.
MRI protocol
MRI was performed on a 1.5-T whole-body scanner, the GE HDx (GE Healthcare). The following measures were used for 4-chamber and short-axis cine images: cardiac gated multislice balanced steady-state free-precession sequence, 20 frames per cardiac cycle, slice thickness 5 mm, FOV 48 × 43.2, matrix 256 × 256, BW 125 KHz/pixel, TR 3.7 ms, and TE 1.6 ms. For delayed myocardial enhancement (DME), a short-axis inversion recovery sequence was performed at a single timepoint 10–12 min after intravenous injection of 0.05 ml/kg Gadovist (Bayer, Berlin, Germany). The phase-contrast sequence was performed orthogonal to the pulmonary artery trunk using an electrocardiogram-gated sequence with TR 5.6 ms, TE 2.7 ms, slice thickness 10 mm, FOV 48 × 28.8, and matrix 256 × 128.
MRI analysis
The contours of the right ventricle (RV) and left ventricle (LV) were delineated manually by a blinded observer in the short-axis stack images and processed using GE software. The RV end diastolic volume (RVEDV), RV end systolic volume (RVESV), RV ejection fraction, stroke volume, and cardiac output were then calculated. The systolic and diastolic areas of the RV and LV chambers were measured on the mid-4-chamber view and a ratio was derived. The RV end diastolic mass (RVEDM), left ventricular end diastolic mass (LVEDM) and the ventricular mass index as the ratio of RVEDM/LVEDM (VMI) were calculated from the end diastolic short-axis stack of images19. The RV longitudinal and transverse motion was quantified on the mid-4-chamber cardiac view by means of the tricuspid annular systolic excursion (TAPSE) and septum-to-free wall distance, respectively, according to the method described by Kind, et al20 (Figures 1 and 2). From the mid-4-chamber image the RV relative area change (RV area in end diastole – RV area in end systole/RV area in end diastole × 100) and systolic and diastolic RV/LV area ratios were measured (Figure 3). Phase-contrast MRI were processed using specialized software. The contours of the main PA were traced simultaneously on magnitude and velocity-map images and peak velocity, PA blood flow, and PA distensibility were calculated21. The motion of the interventricular septum was visually analyzed on short-axis and 4-chamber views for presence or absence of paradoxical septal movement. The presence or absence of myocardial delayed enhancement at the interventricular septum insertion points was also noted (Figure 4).
Right heart catheterization
RHC was performed through the internal jugular vein using a 7 French Swan-Ganz catheter by one of 3 PH consultants (DGK, CAE, RC). The form of PH was classified according to standard criteria22 and required at RHC a mean pulmonary artery pressure (mPAP) ≥ 25 mm Hg to establish a diagnosis of PH. Patients with PAH were required to have mPAP ≥ 25 mm Hg and pulmonary wedge pressure ≤ 15 mm Hg.
Statistical analysis
The statistical analysis was performed with SPSS version 16.0 (SPSS, Chicago, IL, USA). To compare CT and MRI measurements between patients with PH and no-PH subjects, independent t tests and chi-square tests were used as appropriate. Pearson’s test was used to determine correlations between imaging and RHC measures. Diagnostic strength, for identification of patients with PAH, was assessed using receiver-operated characteristic (ROC) curve analysis. Survival curves were derived using the Kaplan-Meier method and were compared using a log-rank test. Median values were used to separate continuous variables into 2 groups. Univariate Cox regression analysis was used to calculate the hazard ratio and CI for the following predictors: age, mean right atrial pressure, mixed venous oxygen saturation, cardiac index, mPAP, pulmonary vascular resistance (PVR), RVEDM, RVEDV, pulmonary artery to aortic ratio (PA/Ao), and RV wall thickness. A p value of < 0.05 was considered statistically significant for all analysis.
RESULTS
Demographic data
In total, 81 patients with CTD were identified, of whom 55 had PAH and 4 had PH owing to left heart disease. Twenty-two patients with CTD had “no PH.” Phase-contrast MRI was performed in 51 patients and the ventricular mass was available for 62 patients. The study profile is outlined in Figure 5 and patients’ demographic details are summarized in Table 1.
Correlation of MRI, CT, and echocardiography findings with hemodynamic data
Table 2 summarizes the correlations between MRI measurements and mPAP and PVR derived from RHC. Good correlation was found between mPAP and PVR and VMI, RVEDM, and systolic and diastolic RV/LV area ratio; and a moderate correlation was found with TAPSE, PA distensibility, and right ventricle relative area change. The PA average blood flow measured from phase-contrast MRI showed a moderate correlation with cardiac output derived from RHC (r = 0.59, p < 0.001) but not with mPAP or PVR. For variables measured from CT scans, PA size, PA/Ao ratio, RV wall thickness, RV/LV ratio, and graded hepatic vein reflux showed only moderate correlation with the mPAP and PVR. The results of the CT and TG findings are summarized in Table 3. TG from echocardiography correlated strongly with mPAP and PVR measured at RHC (mPAP, r = 0.84, p < 0.001; and PVR, r = 0.76, p < 0.001).
Diagnostic value of MRI, CT, and echocardiography to identify PAH in the at-risk population
The performance of the MRI and CT scans and different thresholds of TG are outlined in Tables 4, 5, and 6. VMI was the best performing MRI measure, with a cutoff value ≥ 0.45 determined by ROC analysis [area under the curve (AUC) = 0.87], having a sensitivity of 85%, specificity of 82%, and likelihood ratio of 4.5. PA distensibility with the cutoff point ≤ 15 (AUC = 0.85) had a sensitivity of 80%, specificity of 78%, and likelihood ratio of 3.6. Of the CT measures evaluated, presence of PA/Ao ratio ≥ 1 (AUC = 0.71) had a low sensitivity of 59%, specificity of 73%, and likelihood ratio of 2.2. RV wall thickness ≥ 3.5 mm as determined by ROC analysis (AUC = 0.73) showed a sensitivity of 65%, specificity of 67%, and likelihood ratio of 1.9. Although the presence of pericardial effusion had 100% specificity, the sensitivity was poor (23%), as this was present in only 12 patients. TG performed strongly as a diagnostic test for the group (AUC = 0.87). The strongest TG threshold for diagnosing PH was 40 mm Hg and at this cutoff point the sensitivity was 86%, specificity was 82%, and likelihood ratio was 4.6 for diagnosing PH.
Survival analysis
The mean followup period was 24 months and there were 10 deaths during the study period. Univariate Cox regression analysis demonstrated that mean right arterial pressure, mixed venous oxygen saturation, RVEDV, RVESV, VMI, and RVEDM predicted mortality in PAH (Table 7). Kaplan-Meier survival curves showed patients with RVEDV < 135 ml had significantly better survival than those with RVEDV > 135 ml (log-rank test, p = 0.024). The Kaplan-Meier survival curve for RVEDV is shown in Figure 6. In our group of patients, the Kaplan-Meier survival curve for VMI using a median value of 0.75 also predicted mortality with a p value of 0.04 (Figure 7). A multivariable analysis was not performed because of the low number of deaths.
DISCUSSION
We compared the diagnostic utility of MRI with that of CT and selected echocardiographic measures, for the first time, in a large unselected group of patients with CTD and suspected PAH. We have demonstrated that both MRI and echocardiographic indices have a good correlation with mPAP and PVR at the time of RHC and performed well in predicting the presence of PAH in a high-risk population. In addition, measures of volume and mass derived from MRI predicted outcome. In contrast, CT indices correlated only moderately with invasive measures of pulmonary hemodynamics and had poorer diagnostic utility for PAH.
Several studies have investigated the role of echocardiography in the assessment of PH and have shown strong correlation with mPAP and PVR at RHC, and our results are in agreement with previous reports23,24,25,26. Echocardiography is established in routine clinical practice for screening for PAH in SSc. The TG calculated from the peak tricuspid velocity is the most commonly used measure, with a TG ≥ 40 mm Hg having a good positive predictive value for the identification of PAH, which we have confirmed. However, there is no threshold that can confidently exclude the presence of PAH in symptomatic patients and this has resulted in interest in other diagnostic tests. Although cost-effective and readily available, echocardiography is operator-dependent and in 1 study, adequate estimation of the TG was not possible in roughly one-third of SSc patients with suspected PAH27. MRI is noninvasive and does not involve ionizing radiation, and importantly it allows detailed analysis of both structural and functional evidence, and in contrast to the TG measured by echocardiography these can be accurately quantified in the vast majority of patients. The utility of cardiac MRI in patients with suspected CTD-PAH is underreported and has been limited to patients with SSc and PAH18,26,28. To our knowledge, our study is the first to analyze several quantitative MRI measures in a subgroup of patients with CTD and suspected PAH in comparison to gold standard RHC.
In PAH, a proliferative vasculopathy results in an increase in mPAP and PVR, leading to remodeling and compensatory hypertrophy of the RV. As the afterload continues to increase, RV dilatation and failure ensue29. Consequently, there has been interest in measures that are likely to reveal the remodeling process, such as RV mass and fluid overload as indicated by change in chamber volume. In our cohort, RV mass showed the best correlation with mPAP (RVEDM, r = 0.70; VMI, r = 0.68); this is not surprising because RV mass partially reflects the effect of RV afterload29. We and others have previously shown that VMI can predict disease severity in patients with PAH19,30; however, acquisition and post-processing for RV mass assessment is a time-consuming process. In our study we also demonstrated that simpler and quicker measurements such as RV/LV systolic area ratio also show good correlation with the catheter hemodynamics (mPAP, r = 0.68; PVR, r = 0.69). Indeed, as a diagnostic tool, PA distensibility measured from phase-contrast MRI was equally reliable in diagnosing PAH as VMI when the estimated value was ≤ 15, and this measurement can be performed rapidly. A simple approach to quantify systolic RV function has been to measure RV wall motion. Tricuspid annular plane systolic excursion (TAPSE) quantifies the longitudinal systolic function of the RV. Septum-to-free wall distance (SFD) is a measure of the transverse movement of the RV free wall and takes into consideration the position of the interventricular septum. Both these measures have previously been applied in MRI in patients with idiopathic PAH20,31, and our results showed a better relationship of TAPSE with mPAP compared to SFD. Primary myocardial involvement has been reported in SSc and established myocardial involvement characteristically results in myocardial fibrosis32. On contrast-enhanced delayed MRI, scarring or fibrosis appears as an area of high signal intensity and characteristically occurs at the insertion points of the interventricular septum in patients with PAH33. Tzelepis, et al analyzed 36 patients with SSc and found 66% had DME34. The DME was characteristically mid-wall of the left ventricle; however, a small number of patients also had DME at the interventricular septum insertion points in the absence of PH as assessed on echocardiography. Our study examined the prevalence of DME in patients with suspected PAH; interestingly, 4 patients with SSc had DME in the absence of PAH based on RHC. The process of “primary” myocardial involvement in SSc may account for this finding in our patients without PAH35.
The development of PAH in patients with CTD is known to have a major effect on survival, and patients in this group have poorer prognosis compared to other forms of PAH3,4,36. VMI was noted to predict outcome in a selected group of patients with SSc-associated PAH19. In patients with PAH, Gan, et al found that PA distensibility, which is thought to reflect the stiffness of the pulmonary artery, was a strong predictor of mortality when measured noninvasively37. Van Wolferen, et al found that low stroke volume, RV end diastolic volume index, and impaired left ventricular filling independently predicted mortality in patients with PAH29. We have shown that these findings are broadly applicable in patients with CTD-PAH and have demonstrated the ability of MRI measurements of RV volume and VMI to identify patients with better outcome.
The widespread availability of CT has resulted in interest in using this in addition to echocardiography to improve diagnostic accuracy23. Chest CT is an important and established modality to investigate breathless patients with CTD and can provide useful morphological information. HRCT in particular can identify even subtle parenchymal lung involvement. In a recent study, we demonstrated moderate correlation between RV/LV ratio measured by CT and reflux of contrast into hepatic veins and pulmonary hemodynamics23. However, as individual measurements, the role of morphological CT data appears to be limited as a prognostic and diagnostic tool. PA measurement, one of the features routinely assessed on CT in suspected PH, is an unreliable predictor of the presence of PH in patients with ILD38. The extent of contrast reflux into the IVC and hepatic veins mirrors the regurgitant volume39, and significant correlations between hepatic vein reflux and mPAP and PVR have been observed23; similar results were seen in our study. This sign, however, may not be very specific because a Valsalva maneuver during breath-hold will elevate right atrial pressure and can theoretically lead to contrast reflux. RV hypertrophy is common in the patients with PH. Revel, et al reported good agreement between RV wall thickness and mPAP in a cardiac-gated CT study in patients with PH40. We have reproduced a similar correlation in a subgroup of patients with CTD using noncardiac-gated CT. Our study, however, does establish that MRI has greater diagnostic accuracy than CT, which is not surprising given the gated origin of the acquired images and the functional information that can be gleaned from MRI.
There are limitations to our study. The study was carried out in a quaternary referral center for PH, where patients were referred with suspected PH either from screening programs or due to the presence of symptoms. This group is at particularly high risk of having PAH; therefore it would be most appropriate to consider further noninvasive assessment in these patients. The CT pulmonary angiography used for evaluation of cardiac measurements was not cardiac-gated. However, CT performed for suspected PH is not routinely cardiac-gated and our study reflects the utility of CT that is typically performed in a routine clinical setting. In a recent report, Meune, et al proposed a score to stratify risk of PAH based on clinical tests in patients with SSc41. Selecting patients using such a risk stratification tool might be an option, especially in the low-risk population. However, our results show the value of MRI in a high-risk group.
Our results show that cardiac MRI had diagnostic accuracy similar to that of TG measurement, when this could be assessed using echocardiography; and it is superior to CT in assessing the severity of disease and diagnosing PAH in patients with CTD who are at high risk of having PAH. MRI can identify with a high degree of certainty patients likely to have PAH and may be of particular value in patients with suspected PAH who have poor-quality echocardiograms or in patients reluctant to have invasive investigation in establishing a positive diagnosis of PAH. In addition, cardiac MRI also offers the added advantage of predicting mortality in this subgroup of patients with CTD-PAH, and may be valuable in identifying patients for more aggressive therapy. Neither imaging test can confidently exclude PAH and right heart catheterization remains the definitive investigation to do this in patients with ongoing symptoms despite reassuring noninvasive investigations.
Footnotes
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S. Rajaram and D. Capener are supported by unrestricted research grants from Pfizer and Bayer, respectively. A.J. Swift, R. Condliffe, C. Davies, J.M. Wild, and D.G. Kiely receive funding from the National Institute for Health Research through the Biomedical Research Units funding scheme. J.M. Wild is also funded by the Engineering and Physical Sciences Research Council.
- Accepted for publication March 2, 2012.