JACC: CARDIOVASCULAR IMAGING
VOL.
-, NO. -, 2020
ª 2020 BY THE AMERICAN COLLEGE OF CARDIOLOGY FOUNDATION PUBLISHED BY ELSEVIER
ORIGINAL RESEARCH
Prognostic Value of Stress Dynamic Computed Tomography Perfusion With Computed Tomography Delayed Enhancement Satoshi Nakamura, MD,a Kakuya Kitagawa, MD,b Yoshitaka Goto, MD,a Masafumi Takafuji, MD,a Shiro Nakamori, MD,c Tairo Kurita, MD,c Kaoru Dohi, MD,c Hajime Sakuma, MDa
ABSTRACT OBJECTIVES This study sought to evaluate the prognostic value of stress dynamic computed tomography (CT) perfusion (CTP) with CT delayed enhancement (CTDE) in patients with suspected or known coronary artery disease (CAD) and in subgroups of patients with stent, heavy calcification, or stenosis. BACKGROUND The prognostic value of stress dynamic CTP with CTDE is unknown. METHODS Participants were 540 patients with suspected or known CAD. Major adverse cardiac events (MACEs) consisted of cardiac death, nonfatal myocardial infarction, unstable angina, or hospitalization for congestive heart failure. Ischemic score was calculated by scoring the reduction of normalized myocardial blood flow in 16 segments excluding areas of myocardial scarring. Ischemic perfusion defect (IPD) was defined as Ischemic score $4. Scar score was also calculated by scoring the transmural extent of scarring in each segment on CTDE. RESULTS During a median follow-up of 2.9 years, 43 MACEs occurred. By adding IPD to obstructive CAD ($50% stenosis) on coronary CT angiography, the concordance index for predicting MACEs increased from 0.73 to 0.82 in patients with suspected CAD (p ¼ 0.028) and from 0.61 to 0.73 in patients with known CAD (p ¼ 0.004). IPD and scar score of $4 were independent predictors when adjusted for each other in patients with suspected (adjusted hazard ratios: 7.5 [p < 0.001] and 3.0 [p ¼ 0.034], respectively) or known CAD (adjusted hazard ratios: 4.4 [p ¼ 0.001] and 3.2 [p ¼ 0.024], respectively). Patients with IPD had a higher annualized event rate than those without IPD in subgroups of those with stent (11.5% vs. 2.6%; p < 0.001), heavy calcification (13.3% vs. 3.1%; p < 0.001), 50% to 69% stenosis (8.8% vs. 1.0%; p < 0.001), or $70% stenosis (12.4% vs. 3.6%; p < 0.001). CONCLUSIONS Stress dynamic CTP with CTDE had incremental prognostic value over CT angiography in each group with suspected or known CAD and was prognostically useful in subgroups of patients with stent, heavy calcification, or obstructive CAD. IPD and myocardial scarring may play complementary roles in prognostic stratification. (J Am Coll Cardiol Img 2020;-:-–-) © 2020 by the American College of Cardiology Foundation.
From the aDepartment of Radiology, Mie University Graduate School of Medicine, Tsu, Mie, Japan; bDepartment of Advanced Diagnostic Imaging, Mie University Graduate School of Medicine, Tsu, Japan; and the
c
Department of Cardiology and
Nephrology, Mie University Graduate School of Medicine, Tsu, Mie, Japan. This study was partly supported by research grants from Siemens Japan. Dr. Dohi has received financial support from Otsuka and Takeda. Dr. Sakuma has received research grants from Daiichi Sankyo, Fuji Pharma, Fujifilm RI Pharma, and Eisai. All other authors have reported that they have no relationships relevant to the contents of this paper to disclose. Manuscript received July 3, 2019; revised manuscript received December 12, 2019, accepted December 20, 2019.
ISSN 1936-878X/$36.00
https://doi.org/10.1016/j.jcmg.2019.12.017
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Prognostic Value of Stress Dynamic CTP With CTDE
ABBREVIATIONS AND ACRONYMS ATP = adenosine triphosphate CABG = coronary artery bypass grafting
CAD = coronary artery disease CCS = coronary calcium score CI = confidence interval CMR = cardiac magnetic resonance
CT = computed tomography CT-FFR = computed tomography–derived fractional
C
oronary computed tomography (CT)
motion or breathing (n ¼ 15). Thus, 55 patients who
angiography (CTA) is an established
met the criteria were excluded, and we enrolled 563
imaging technique for the diagnosis
patients, who had follow-up after the cardiac CT was
and exclusion of coronary artery disease
performed.
(CAD) (1). However, CTA provides poor pre-
follow-up; therefore, the final study population CAD. Known CAD was defined as having a history of myocardial infarction (MI), percutaneous coronary
myocardial perfusion, could complement
intervention or coronary artery bypass grafting
the limited capability of CTA to assess the he-
(CABG).
modynamic significance of coronary stenosis (3,4).
Nonetheless,
abnormal
perfusion
detected by CTP can be induced not only by enhancement (CTDE) is a feasible and reliable imaging technique for detecting myocar-
CTDE = computed tomography
dial scarring. CTDE has been reported to offer
delayed enhancement
high diagnostic performance for detecting
CTP = computed tomography
infarcted areas determined by cardiac magnetic resonance (CMR) (5–7). Therefore, combined CTP and CTDE has the potential to
FFR = fractional flow reserve
differentiate
HR = hazard ratio
infarction. Previous studies showed that
IPD = ischemic perfusion defect
myocardial ischemia detected with perfusion
LAD = left anterior descending
imaging and delayed enhancement imaging
artery
by MRI was a strong predictor of cardiac
MACE = major adverse cardiac
events (8,9). Similarly, the detection of
myocardial
ischemia
from
myocardial ischemia by CTP with CTDE might improve risk stratification.
MI = myocardial infarction
We sought to evaluate the prognostic
ROC = receiver-operating
value of stress dynamic CTP with CTDE in
characteristic curve
to
imaging method with CT for evaluating
angiography
MBF = myocardial blood flow
lost
comprised 540 patients with suspected or known
ischemia but also by infarction. CT delayed
event
were
diction of hemodynamically significant ste-
flow reserve
ECG = electrocardiogram
patients
nosis (2). CT perfusion (CTP) imaging, an
CTA = computed tomography
perfusion
Twenty-three
patients with suspected or known CAD and in subgroups of patients with stent, heavy calcification, or stenosis.
IMAGE ACQUISITION. All CT data were acquired with
a second-generation (SOMATOM Definition Flash, Siemens Healthineers, Forchheim, Germany) or thirdgeneration dual-source CT scanner (SOMATOM Force; Siemens Healthineers). Patients were asked to avoid drinks containing caffeine for at least 24 h before undergoing stress testing. Unenhanced images for Agatston calcium scoring were acquired with electrocardiogram
(ECG)-triggered
high-pitch
spiral
scanning with 120-kV tube voltage before stress dynamic CTP (10). During the administration of 20 mg of adenosine triphosphate (ATP) at 160 m g/kg/min for >3 min (11), scan acquisition of dynamic CTP was initiated by injecting 40 ml of contrast medium with an iodine concentration of 370 mg/ml at a flow rate of 5 ml/s. Dynamic datasets were acquired for 30 s via ECGtriggered axial scan mode repeated at 2 alternating table positions to obtain a z-axis coverage of 73 mm or 105 mm for the second- or third-generation scanner, respectively. Tube voltage was set at 80 kV or 70 kV for the second- or third-generation scanner, respectively, and tube current was determined by using an automatic exposure control system with the quality
METHODS
reference of 350 mA/rotation at 120 kV (12). After completing data acquisition, ATP administration was
STUDY POPULATION. This study was designed as a
stopped. ECG images, blood pressure, and arterial
single-center, retrospective study. Medical records
oxygen saturation were monitored and recorded
were reviewed for 618 consecutive patients who
throughout the procedure.
completed a comprehensive cardiac CT examination
After dynamic stress CTP, standard prospective CTA
for evaluation of ischemic heart disease at our hos-
was performed at rest with the following scan param-
pital
2017
eters: 2 100-kV tube voltage or 80-kV and 0.28-s
(Figure 1). The cardiac CT examinations included
gantry rotation time, with injection of 0.84 ml/kg of
calcium scoring, CTA, stress dynamic CTP, and CTDE.
contrast medium with an iodine concentration of
The acquisition and analysis of the cardiac CT images
370 mg/ml over 12 s. Tube current was determined
were approved by the institutional review board, and
with the angular modulation technique.
between
March
2012
and
February
written informed consent was obtained from all pa-
CTDE images were acquired 7 min after CTA
tients at the time of cardiac CT. Exclusion criteria for
without additional contrast administration and were
this study were as follows: 1) age of <45 or >85 years
reconstructed by using targeted special frequency
(n ¼ 25); 2) no written informed consent for follow-
filtration and half-scan reconstruction (3). Tube
up, which was approved by the institutional review
voltage was 80 kV and tube current was 370 mA for a
board (n ¼ 15); and 3) severe artifacts on CTP due to
second-generation scanner and were automatically
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determined by the automatic exposure-control system with the quality reference of 580 mA/rotation at 80 kV for a third-generation scanner. IMAGE ANALYSIS. Analysis of dynamic CTP images
Prognostic Value of Stress Dynamic CTP With CTDE
F I G U R E 1 Flow Chart of Patient Selection
Patients who completed the cardiac CT n = 618
was performed with commercially available perfusion Exclusion criteria for the study, n = 55 - Age <45 or >85, n = 25 - No written informed consent for follow up, n = 15 - Severe artifacts, n = 15
software (Syngo Volume Perfusion CT Body, Siemens Healthineers). Myocardial blood flow (MBF) was estimated by using a dedicated parametric deconvolution technique, based on a 2-compartment model of the intravascular and extravascular spaces. The
Enrolled patients n = 563
maximum slope of time-attenuation curves fitted for every voxel was used to generate an MBF map of 3-
Follow-up loss n = 23
mm thickness and 1-mm increments. Polygonal regions of interest measuring 1 to 2 cm 2
Final study population n = 540
were placed within each of the 16 American Heart Association myocardial segments (excluding an apical segment) in the short-axis view on the MBF map, at a minimum distance of 1 mm from the endocardial and
A flow chart of the patient selection in this study. Medical records were reviewed for 618 consecutive patients who completed a comprehensive
epicardial borders to avoid contamination. When any
cardiac CT examination. Of them, 55 patients who met the exclusion criteria
myocardial scarring was identified on CTDE, we did
were excluded, and we therefore enrolled 563 patients in the study.
not include areas matching the myocardial scarring
Twenty-three patients were lost to follow-up; therefore, the final study
within regions of interest on the MBF map. A normalized MBF value was calculated as an MBF
population comprised 540 patients with suspected or known coronary artery disease. CT ¼ computed tomography.
value in each segment divided by the highest MBF value within the 16 segments on the MBF map. Ischemic score was calculated by adding the scores of
scale: 0: 0%; 1: 1% to 49%; 2: 50% to 69%; 3: 70% to
all segments using a 5-point scale based on normal-
99%; and 4: 100%.
ized MBF values: 0 ¼ normal (>0.75), 1 ¼ mildly
CTDE images were visually evaluated to determine
abnormal (#0.75, >0.675), 2 ¼ moderately abnormal
the presence or absence of hyperenhancement sug-
(#0.675, >0.60), 3 ¼ severely abnormal (#0.6), and
gestive of myocardial scarring within each of the 16
4 ¼ absent (11). Ischemic perfusion defect (IPD) was
segments by the consensus decision of 2 observers.
defined as ischemic score $4. When myocardial
Examples of perfusion defect and myocardial scarring
scarring covered an entire segment, the score for that
are shown in Figure 2. The transmural extent of
segment was counted as 0.
scarring was scored in each segment on CTDE images
Calcium score images were analyzed with a
using a 5-point scale: 0: 0%; 1: 1% to 24%; 2: 25% to
commercially available software package (Ziosta-
49%; 3: 50% to 74%; and 4: 75% to 100%. Scar score
tion2, Ziosoft Inc., Tokyo, Japan) using the Agatston
was calculated by summing up the scores in all
score with a cutoff of 130 Hounsfield units. The
segments.
analysis for calcium score was performed only for
FOLLOW-UP. Follow-up information was collected
patients with suspected CAD, because most of the
through a review of hospital records or telephone
patients with known CAD had stents or bypass grafts
interviews blinded to CT results. Patients who un-
(13). CTA images were visually evaluated in a joint
derwent early (#60 days after CT) revascularization
reading by 2 observers, including a radiologist with 10
were censored from follow-up thereafter. Major
years of experience in CTA. Coronary segments with a
adverse cardiac events consisted of cardiac death,
reference diameter of $1.5 mm were assessed for the
nonfatal MI, unstable angina, and hospitalization for
detection of stenosis. Obstructive CAD, severe ste-
congestive heart failure. Hard events included cardiac
nosis, multivessel disease, and proximal left anterior
death and nonfatal MI. Cardiac death was defined as
descending artery (LAD) stenosis on CTA was defined
death caused by acute MI, ventricular arrhythmias, or
as $50% stenosis in $1 vessel, $70% stenosis in $1
congestive heart failure. Nonfatal MI was defined as
vessel, $50% stenosis in $2 vessels, and $50% ste-
prolonged angina accompanied by new ECG abnor-
nosis in the left main or proximal LAD, respectively.
malities and increased cardiac biomarkers. Unstable
Stenosis score was calculated by summing up points
angina was defined as new-onset, worsening, or rest
for stenosis in each vessel according to a 5-point
angina requiring hospital admission. Congestive
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Prognostic Value of Stress Dynamic CTP With CTDE
F I G U R E 2 Examples of Perfusion Defect and Myocardial Scarring
A
B
C
D
Representative myocardial blood flow map (left) and CT delayed enhancement (right) showing (A) perfusion defect larger than myocardial scarring, (B) perfusion defect with matching myocardial scarring, (C) perfusion defect without myocardial scarring, and (D) no perfusion defect or myocardial scarring. White and black arrows represent perfusion defect and myocardial scarring, respectively.
heart failure was defined as the development of
predictor was evaluated by calculating the global chi-
appropriate symptoms, such as cough, shortness of
square test and receiver-operating characteristic
breath, dyspnea on exertion, paroxysmal nocturnal
(ROC) curves analysis. ROC curves were built based
dyspnea, and reduced exercise tolerance, associated
on a logistic regression model, and the Delong test
with either new radiologic findings consistent with
was used to compare the concordance index. Kaplan-
congestive heart failure or new physical signs
Meier curves were used to estimate cumulative event
including pulmonary rales, S 3 gallop sound, and
rates of MACEs. Differences between time-to-event
weight gain.
curves were compared by using the log-rank test.
STATISTICAL ANALYSIS. Continuous variables are
Annualized event rates were calculated by dividing 3-
presented as the mean SD and were evaluated with
year Kaplan-Meier event rates by 3. A 2-sided p
the Mann-Whitney U test. Categorical variables are
value <0.05 was considered statistically significant.
expressed
were
All analyses were performed by using the SPSS sta-
compared by using the Fisher exact test. The influ-
tistical package, version 23.0 (IBM, Armonk, New
ence of predictors on MACEs was determined by us-
York) and the R statistical package, version 3.4.4 (R
ing Cox proportional hazards regression analysis, and
Foundation
the results are reported as hazard ratios (HRs) with
Austria).
as
frequency
(proportion)
and
for
Statistical
Computing,
Vienna,
95% confidence intervals (CIs). Univariate Cox proportional hazards regression analysis was performed
RESULTS
to identify potential predictors of MACEs. Multivariate Cox proportional hazards regression analysis was
PATIENT
performed by using stepwise forward selection for
AND
CHARACTERISTICS,
variables with p < 0.05 in the univariate analysis to
STRESS. Table 1 shows baseline patient characteris-
determine independent predictors of MACEs. The
tics in all patients and those with suspected or
incremental value of a predictor over another
known CAD.
HEMODYNAMIC
RADIATION
RESPONSE
DURING
DOSE, ATP
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Prognostic Value of Stress Dynamic CTP With CTDE
T A B L E 1 Baseline Patient Characteristics
T A B L E 2 Imaging Results
All Patients (N ¼ 540)
Suspected CAD (n ¼ 332)
Male
350 (65)
221 (67)
129 (62)
Age, yrs
68 9.1
67 10
69 8.9
Body mass index, kg/m2
Known CAD (n ¼ 208)
24.0 3.7 24.0 3.7 23.9 3.6
Coronary risk factors
All Patients (N ¼ 540)
Suspected CAD (n ¼ 332)
Known CAD (n ¼ 208)
Coronary calcium score 0
—
92 (28)
—
1–99
—
88 (27)
—
100–399
—
68 (20)
—
$400
—
84 (25)
—
Hypertension
374 (69)
225 (68)
149 (72)
Dyslipidemia
334 (62)
162 (49)
172 (83)
Diabetes
179 (33)
98 (30)
81 (39)
Obstructive CAD
244 (45)
118 (36)
126 (61)
Current smoker
80 (15)
48 (14)
32 (15)
Severe stenosis
142 (26)
68 (20)
74 (36)
Family history of CAD
101 (19)
52 (16)
49 (24)
Multivessel disease
144 (27)
70 (21)
74 (36)
Body mass index >25 kg/m2
177 (33)
112 (34)
65 (31)
Proximal LAD stenosis
117 (22)
44 (13)
73 (35)
Stenosis score $6
155 (29)
55 (17)
100 (48)
169 (31)
88 (26)
81 (39)
38 (11)
41 (20) 154 (74)
Echocardiography
Coronary CT angiography
LVEF <50%
64 (12)
20 (6)
44 (21)
Dynamic CT perfusion
Wall motion abnormality
168 (31)
50 (15)
118 (57)
Ischemic score $4* Ischemic score $8
Symptom Typical
62 (11)
34 (10)
Atypical
28 (13)
79 (14)
CT delayed enhancement
107 (20)
76 (23)
31 (15)
Myocardial scar
196 (36)
42 (13)
Nonanginal
81 (15)
57 (17)
24 (12)
$2 segments with scarring
150 (28)
26 (8)
124 (60)
Dyspnea
62 (11)
37 (11)
25 (12)
Scar score $4
126 (23)
20 (6)
106 (51)
Scar score $8
73 (14)
8 (2)
65 (31)
148 (27)
0 (0)
148 (71)
Stent
137 (25)
0 (0)
137 (66)
Values are n (%). *Ischemic perfusion defect was defined as ischemic score $4.
Stent without CABG
124 (23)
0 (0)
124 (60)
CAD ¼ coronary artery disease; CT ¼ computed tomography; LAD ¼ left anterior descending artery.
42 (8)
0 (0)
42 (20)
108 (20)
0 (0)
108 (52)
History of CAD PCI
CABG Old myocardial infarction Values are n (%) or mean SD.
CABG ¼ coronary artery bypass grafting; CAD ¼ coronary artery disease; LVEF ¼ left ventricular ejection fraction; PCI ¼ percutaneous coronary intervention.
n ¼ 24) experienced a MACE: cardiac death: n ¼ 3, nonfatal MI: n ¼ 7, unstable angina: n ¼ 23, and hospitalizations for congestive heart failure: n ¼ 10. Noncardiac death was observed in 16 patients. Fortyfive patients who underwent early revascularization (percutaneous coronary intervention: n ¼ 44, CABG:
The dose-length products for CTA, CTP, and CTDE were 191 117, 315 109, and 117 35 mGy$cm, respectively, and the effective doses for each imaging modality were 2.67 1.64, 4.42 1.53, and 1.64 0.48 mSv, respectively, using a conversion coefficient of 0.014. The effective dose for calcium scoring was <0.5 mSv for all patients. Heart rate increased significantly from 64 11 beats/min at baseline to 76 12 beats/min under stress (p < 0.001). Systolic blood pressure decreased significantly from 131 20 mm Hg at baseline to 116 20 mm Hg during stress (p < 0.001), whereas diastolic blood pressure declined significantly from 67 10 mm Hg to 57 10 mm Hg (p < 0.001). In our population, no patients had any major complications related to stress agent. At CTA acquisition, the mean heart rate was 67 10 beats/min.
n ¼ 1) were censored at the time of revascularization. UNIVARIATE
COX
PROPORTIONAL
HAZARDS
REGRESSION ANALYSIS. Univariate predictors for
MACEs are listed in Table 3. Sex, age, and clinical predictors were not statistically significant. Ischemic score $4 was the strongest predictor in all patients (HR: 7.5; 95% CI: 3.9 to 14.6; p < 0.001) and those with suspected CAD (HR: 9.9; 95% CI: 3.6 to 27.6; p < 0.001), and ischemic score $8 was the strongest predictor in patients with known CAD (HR: 6.8; 95% CI: 3.0 to 15.6; p < 0.001). All predictors of CTA (obstructive CAD, severe stenosis, multivessel disease, proximal LAD stenosis, and stenosis score $6) were significant predictors for all patients and those with suspected or known CAD. Univariate predictors for hard events are listed in Supplemental Table 1. Significant predictors of hard
IMAGING RESULTS. Results for coronary calcium
events in all patients were current smoker, wall motion
score (CCS), CTA, CTP, and CTDE are presented in
abnormality, CTA findings (obstructive CAD, severe
Table 2.
stenosis, multivessel disease, and proximal LAD ste-
OUTCOMES. During a median follow-up of 2.9 years,
nosis), ischemic score of $4 and $8, and CTDE findings
43 patients (suspected CAD, n ¼ 19; known CAD,
($2 segments with scarring and scar score $ 4).
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Prognostic Value of Stress Dynamic CTP With CTDE
T A B L E 3 Univariate Predictors of MACEs
All Patients
Suspected CAD
Known CAD
HR (95% CI)
p Value
HR (95% CI)
p Value
HR (95% CI)
Male
0.9 (0.5–1.7)
0.727
0.6 (0.3–1.5)
0.310
0.9 (0.4–2.4)
p Value
0.897
Age >70 yrs
1.5 (0.8–2.7)
0.195
2.0 (0.8–5.1)
0.123
1.1 (0.5–2.5)
0.826
Hypertension
1.1 (0.6–2.1)
0.796
1.3 (0.5–3.5)
0.654
0.9 (0.4–2.1)
0.748
Dyslipidemia
1.5 (0.8–2.8)
0.235
0.9 (0.4–2.2)
0.840
1.7 (0.5–5.7)
0.386
Diabetes
1.8 (0.9–3.3)
0.057
1.9 (0.8–4.8)
0.158
1.4 (0.6–3.2)
0.376
Current smoker
0.9 (0.4–2.1)
0.747
1.1 (0.3–3.9)
0.826
0.6 (0.2–2.2)
0.482
Coronary risk factors
Family history of CAD
1.3 (0.6–2.6)
0.510
0.3 (0.0–2.0)
0.207
2.2 (0.9–4.9)
0.069
Body mass index >25 kg/m2
0.9 (0.5–1.7)
0.659
0.3 (0.1–1.2)
0.086
1.8 (0.8–3.9)
0.176
2.0 (0.9–4.5)
0.093
3.6 (1.0–12.4)
0.044
1.2 (0.4–3.5)
0.754
2.1 (1.1–3.8)
0.019
1.6 (0.5–5.0)
0.379
1.6 (0.7–3.8)
0.272
Echocardiography LVEF <50% Wall motion abnormality Coronary calcium score $100
—
—
3.7 (1.3–10.3)
0.012
—
—
$400
—
—
6.5 (2.6–16.8)
<0.001
—
—
Coronary CT angiography Obstructive CAD
5.1 (2.5–10.3)
<0.001
6.6 (2.4–18.3)
<0.001
2.9 (1.1–7.8)
0.033
Severe stenosis
5.6 (3.1–10.4)
<0.001
8.0 (3.2–19.9)
<0.001
3.2 (1.3–7.4)
0.005
Multivessel disease
4.3 (2.4–7.9)
<0.001
5.6 (2.3–13.8)
<0.001
3.3 (1.4–7.4)
0.005
Proximal LAD stenosis
6.2 (3.4–11.3)
<0.001
11.0 (4.4–27.3)
<0.001
3.1 (1.4–7.1)
0.006
Stenosis score $6
4.8 (2.6–8.8)
<0.001
6.8 (2.8–16.9)
<0.001
3.0 (1.3–7.2)
0.012
Dynamic CT perfusion Ischemic score $4*
7.5 (3.9–14.6)
<0.001
9.9 (3.6–27.6)
<0.001
5.3 (2.2–12.9)
<0.001
Ischemic score $8
6.9 (3.7–12.5)
<0.001
7.5 (3.0–18.6)
<0.001
6.8 (3.0–15.6)
<0.001 0.064
CT delayed enhancement Myocardial scarring
3.7 (2.0–6.8)
<0.001
4.0 (1.5–10.4)
0.005
3.1 (0.9–10.5)
$2 segments with scarring
3.2 (1.7–5.8)
<0.001
5.0 (1.8–13.8)
0.002
1.8 (0.7–4.3)
0.197
Scar score $4
5.3 (2.9–9.7)
<0.001
7.7 (2.9–20.4)
<0.001
4.1 (1.5–11.0)
0.005
*Ischemic perfusion defect was defined as ischemic score $4. CI ¼ confidence interval; HR ¼ hazard ratio; MACE ¼ major adverse cardiac event; other abbreviations as in Tables 1 and 2.
Ischemic score $4 was the strongest predictor of hard
predictor when adjusted for obstructive CAD, severe
events (HR: 25.8; 95% CI: 3.3 to 204; p ¼ 0.002).
stenosis, proximal LAD stenosis, multivessel disease,
MULTIVARIATE
and scar score $4. In these models, multivessel dis-
COX
PROPORTIONAL
HAZARDS
for multivariate
ease and scar score $4 were independent predictors
analysis were created to evaluate whether IPD
against IPD, whereas obstructive CAD, severe steno-
(ischemic score $4) was an independent predictor
sis, and proximal LAD stenosis were not.
REGRESSION
ANALYSIS. Models
when adjusted for each of the predictors (Table 4). In
Multivariate analysis of predictors for hard events
all patients, IPD was an independent predictor when
are listed in Supplemental Table 2. IPD remained an
adjusted for obstructive CAD, severe stenosis, prox-
independent predictor of hard events in all patients
imal LAD stenosis, scar score $4, and wall motion
when adjusted for current smoker, wall motion ab-
abnormality. In these models, obstructive CAD, se-
normality, severe stenosis, and scar score $4. In
vere stenosis, proximal LAD stenosis, and myocardial
these analysis, current smoker was an independent
scarring were also independent predictors against
predictor against IPD, whereas wall motion abnor-
IPD, but wall motion abnormality was not. In patients
mality, severe stenosis, and scar score $4 were not.
with suspected CAD, IPD remained an independent
RISK STRATIFICATION BY IPD IN ALL PATIENTS AND
predictor when adjusted for obstructive CAD, severe
THOSE
stenosis, proximal LAD stenosis, scar score $4, and
Kaplan-Meier curves by IPD (Figure 3) showed that
WITH
SUSPECTED
OR
KNOWN
CAD.
CCS $400. In these models, obstructive CAD, severe
annualized event rates for MACEs were significantly
stenosis, proximal LAD stenosis, scar score $4, and
different between patients with and without IPD
CCS $400 were independent predictors against IPD.
among all patients (8.4% vs. 1.1%; p < 0.001) (Figure 3A)
In patients with known CAD, IPD was an independent
and those with suspected (7.8% vs. 0.8%; p < 0.001)
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calculated (Figure 4). Figure 4A shows that, by adding
T A B L E 4 Multivariate Analysis
IPD to obstructive CAD, global chi-square scores
Predictors
HR (95% CI)
p Value
IPD
5.5 (2.8–10.9)
<0.001
Versus obstructive CAD
3.2 (1.5–6.7)
IPD
5.0 (2.4–10.2)
All patients 0.002 <0.001 0.001
increased significantly from 25.1 to 59.5 in all patients (p < 0.001), from 17.5 to 37.9 in patients with suspected CAD (p < 0.001), and from 5.0 to 18.6 in patients with known CAD (p ¼ 0.001). ROC curve analysis for prediction of MACEs
Versus severe stenosis
3.1 (1.6–6.0)
IPD
5.1 (2.6–10.3)
<0.001
Versus proximal LAD stenosis
3.7 (2.0–7.1)
<0.001
adding IPD to obstructive CAD was significantly
IPD
5.4 (2.7–10.8)
<0.001
higher than that in obstructive CAD alone in all pa-
(Figure 4B) showed that the concordance index after
Versus scar score $4
3.2 (1.7–6.0)
<0.001
tients and in those with suspected and known CAD.
IPD
6.7 (3.4–13.3)
<0.001
By adding IPD to obstructive CAD, the concordance
Versus wall motion abnormality
1.5 (0.8–2.7)
0.256
index increased from 0.68 to 0.78 in all patients
Patients with suspected CAD IPD
6.8 (2.4–19.5)
<0.001
(p < 0.001), from 0.73 to 0.82 in patients with suspected CAD (p ¼ 0.028), and from 0.61 to 0.73 in pa-
Versus obstructive CAD
3.9 (1.4–11.3)
0.012
IPD
6.0 (2.0–18.2)
0.001
Versus severe stenosis
3.6 (1.4–9.8)
0.007
Supplemental Figure 2 shows the incremental
IPD
6.0 (2.0–17.5)
0.001
prognostic value of IPD over subcategories of CTA-
tients with known CAD (p ¼ 0.004).
Versus proximal LAD stenosis
6.1 (2.3–15.9)
<0.001
detected stenosis (severe stenosis, multivessel dis-
IPD
7.5 (2.5–22.2)
<0.001
Versus scar score $ 4
ease, and proximal LAD stenosis) in all patients and in
3.0 (1.1–8.5)
IPD
7.0 (2.4–20.1)
<0.001
Versus coronary calcium score $400
4.0 (1.5–10.6)
0.004
IPD
4.5 (1.8–11.2)
0.001
Versus obstructive CAD
1.9 (0.7–5.3)
0.204
those with suspected and known CAD (p < 0.05 for each
IPD
3.8 (1.5–9.7)
0.002
group) (Supplemental Figure 3). The best cutoffs of
Versus severe stenosis
2.1 (0.9–4.9)
0.100
stenosis score and ischemic score for prediction of
IPD
4.4 (1.8–10.9)
0.001
MACEs in all patients were 6 and 4, respectively.
Versus multivessel disease
2.3 (1.0–5.5)
0.049
IPD
4.3 (1.7–10.8)
0.002
Versus proximal LAD stenosis
2.1 (0.9–4.9)
0.091
IPD
4.4 (1.8–10.8)
0.001
difference in annualized event rates for MACEs be-
Versus scar score $4
3.2 (1.2–8.7)
0.023
tween patients without obstructive CAD and without
0.034
Patients with known CAD
those with suspected and known CAD by global chisquare tests (p < 0.05 for each test). Furthermore, we performed ROC curve analysis for stenosis score versus stenosis score plus ischemic score in all patients and in
We compared Kaplan-Meier curves by CTA and CTP (Supplemental Figure 4). There was no significant
IPD (p ¼ 0.959) and between patients with obstructive IPD ¼ ischemic perfusion defect; other abbreviations as in Tables 1 and 2.
CAD and with IPD (p ¼ 0.139). RISK STRATIFICATION BY IPD IN THE SETTING OF
(Figure 3C) or known (9.2% vs. 1.9%; p < 0.001)
STENT OR HEAVY CALCIFICATION. Figure 5A shows
(Figure 3E) CAD. For prediction of hard events, patients
that, among patients with stents who had no CABG, a
with IPD displayed higher event rates than those
significant difference in annualized event rates was
without IPD among all patients (2.6% vs. 0.2%;
apparent between patients with and without IPD
p < 0.001) (Figure 3B) and among those with suspected
(11.5% vs. 2.6%; p < 0.001).
(3.1% vs. 0%; p < 0.001) (Figure 3D) or known (2.1% vs.
In patients with heavy calcification, among those with suspected CAD, IPD had a significant association
0.6%; p ¼ 0.021) (Figure 3F) CAD. Annualized event rates for MACEs in patients with
with poor prognosis. Annualized event rates for
ischemic scores of #3, 4 to 7, and $8 were 1.1%, 6.3%
MACEs were significantly higher in patients with IPD
and 11.3% respectively, in all patients (p < 0.001);
than in those without among patients with a calcium
0.8%, 5.8%, and 11.1% in patients with suspected CAD
score 400 (13.3% vs. 3.1%; p < 0.001) (Figure 5B).
respectively, (p < 0.001); and 1.9%, 6.7%, and 11.0%
RISK
in patients with known CAD, respectively (p < 0.001)
STRATIFICATION
BY
IPD ACCORDING
TO
DEGREE OF STENOSIS. Kaplan-Meier curves by IPD
(Supplemental Figure 1).
according to CTA results (Figure 6) showed that pa-
INCREMENTAL PROGNOSTIC VALUE OF IPD OVER
tients with IPD had a worse prognosis than those
OBSTRUCTIVE CAD. To evaluate the incremental
without IPD among those with moderate (50% to
prognostic value of IPD over obstructive CAD, global
69%) stenosis but no severe ($70%) stenosis (annu-
chi-square
alized event rate: 8.8% vs. 1.0%; p < 0.001)
scores
and
concordance
index
were
7
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F I G U R E 3 Kaplan-Meier Curves by IPD in All Patients and Those With Suspected or Known CAD
All Patients
A
B
Prediction of MACEs 1.0
Prediction of Hard Events 1.0
IPD (-)
IPD (-)
0.8
Event-Free Survival
Event-Free Survival
IPD (+) IPD (+) 0.6 0.4 0.2 log-rank, p < 0.001
0.0 0
1
2
3
0.8 0.6 0.4 0.2 log-rank, p < 0.001
0.0 0
4
Follow-Up Time (Years)
1
2
3
4
Follow-Up Time (Years)
Patients at risk
Patients at risk
IPD (-)
371
326
259
170
102
IPD (-)
371
326
259
170
102
IPD (+)
169
117
90
54
29
IPD (+)
169
117
90
54
29
Patients with Suspected CAD
C
D
Prediction of MACEs
Prediction of Hard Events
IPD (-)
0.8 IPD (+) 0.6 0.4 0.2 log-rank, p < 0.001
0.0 0
1
2
3
IPD (-) IPD (+)
1.0 Event-Free Survival
Event-Free Survival
1.0
0.8 0.6 0.4 0.2 log-rank, p < 0.001
0.0 0
4
Follow-Up Time (Years)
1
2
3
4
Follow-Up Time (Years) Patients at risk
Patients at risk IPD (-)
244
217
179
118
75
IPD (-)
244
217
179
118
75
IPD (+)
88
60
46
29
18
IPD (+)
88
60
46
29
18
Patients with Known CAD
E
F
Prediction of MACEs
Prediction of Hard Events 1.0
1.0
IPD (-)
0.8 IPD (+)
0.6 0.4 0.2 log-rank, p < 0.001
0.0 0
1
2
3
Event-Free Survival
IPD (-) Event-Free Survival
8
IPD (+)
0.8 0.6 0.4 0.2 log-rank, p = 0.021
0.0 0
4
Follow-Up Time (Years)
1
2
3
4
Follow-Up Time (Years)
Patients at risk
Patients at risk
IPD (-)
127
109
80
52
27
IPD (-)
127
109
80
52
27
IPD (+)
81
57
44
25
11
IPD (+)
81
57
44
25
11
Kaplan-Meier curves by IPD for prediction of MACEs in (A) all patients, (C) those with suspected CAD, and (E) those with known CAD and Kaplan-Meier curves by IPD for prediction of hard events in (B) all patients, (D) those with suspected CAD, and (F) those with known CAD. CAD ¼ coronary artery disease; IPD ¼ ischemic perfusion defect; MACE ¼ major adverse cardiac event.
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F I G U R E 4 Incremental Prognostic Value of IPD Over Obstructive CAD
A
B
Global Chi-Square Test All Patients
Suspected CAD
ROC Curve Analysis All Patients
Known CAD
Suspected CAD
p < 0.001
p = 0.001
p < 0.001
Known CAD
p = 0.028
p < 0.001
p = 0.004
1
59.5
0.82
0.78
0.73
0.68 0.61
C-Index
Global Chi-Square
0.73
37.9
25.1 18.6
17.5
5.0
0 Obstructive Obstructive CAD CAD + IPD
Obstructive Obstructive CAD CAD + IPD
Obstructive Obstructive CAD CAD + IPD
Obstructive Obstructive CAD CAD + IPD
Obstructive Obstructive CAD CAD + IPD
Obstructive Obstructive CAD CAD + IPD
(A) Global chi-square tests and (B) receiver-operating characteristic (ROC) curve analysis to evaluate the incremental prognostic value of IPD over obstructive CAD. C-index ¼ concordance index; other abbreviations as in Figure 3.
(Figure 6A), with severe ($70%) stenosis (12.4% vs.
RISK STRATIFICATION BY COMBINATION OF IPD
3.6%; p < 0.001) (Figure 6B), with 1-vessel ($50%
AND SCAR SCORE. Kaplan-Meier curves by combi-
stenosis in 1 vessel) disease (7.4% vs. 0.6%; p ¼ 0.001)
nation of CTP and CTDE (Figure 7A) showed that,
(Figure 6C), and with multivessel ($50% stenosis
among patient groups stratified by the presence or
in $2 vessels) disease (13.3% vs. 3.8%; p ¼ 0.002)
absence of IPD and scar score $4, annualized event
(Figure 6D).
rates for MACEs were 12.1%, 5.7%, 2.5%, and 0.9%
F I G U R E 5 Kaplan-Meier Curves by IPD in the Setting of Stent or Heavy Calcification
A
B
Stent
Calcium Score ≥400 1.0
1.0
IPD (-)
IPD (-) 0.8
0.6
Event-Free Survival
Event-Free Survival
0.8
IPD (+)
0.4
IPD (+)
0.6 0.4 0.2
0.2 log-rank, p < 0.001
0.0 0
1
2
3
log-rank, p < 0.001
0.0 0
4
Follow-Up Time (Years)
1
2
3
4
Follow-Up Time (Years)
Patients at risk
Patients at risk
IPD (-)
87
77
58
38
20
IPD (-)
45
34
29
19
12
IPD (+)
37
26
20
12
8
IPD (+)
39
24
15
11
5
Kaplan-Meier curves by IPD for the prediction of MACEs in patients with (A) stent or (B) coronary calcium score of $400. For patients with stent, those who had undergone bypass grafting were excluded. Abbreviations as in Figure 3.
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F I G U R E 6 Kaplan-Meier Curves by IPD According to Degree of Stenosis
A
B
50-69% Stenosis
≥70% Stenosis
1.0
1.0
IPD (-)
IPD (-) IPD (+)
Event-Free Survival
Event-Free Survival
0.8 0.6 0.4 0.2
0.8 0.6
IPD (+)
0.4 0.2
log-rank, p < 0.001
0.0 0
1
2
3
log-rank, p < 0.001
0.0 0
4
Follow-Up Time (Years)
1
2
3
4
Follow-Up Time (Years)
Patients at risk
Patients at risk
IPD (-)
69
62
49
31
16
IPD (-)
56
41
31
24
15
IPD (+)
33
27
17
6
2
IPD (+)
86
52
39
24
12
C
D
One-Vessel Disease 1.0
Multi-Vessel Disease
IPD (-)
1.0
Event-Free Survival
0.8 Event-Free Survival
10
IPD (+) 0.6 0.4 0.2 log-rank, p = 0.001
0.0 0
1
2
3
IPD (-)
0.8 0.6
IPD (+)
0.4 0.2 log-rank, p = 0.002
0.0 0
4
Follow-Up Time (Years)
1
2
3
4
Follow-Up Time (Years)
Patients at risk
Patients at risk
IPD (-)
59
52
41
32
20
IPD (-)
66
51
39
24
11
IPD (+)
42
29
23
13
7
IPD (+)
78
51
34
18
8
Kaplan-Meier curves by IPD for prediction of MACEs in patients (A) with moderate (50% to 69%) stenosis, (B) severe ($70%) stenosis, (C) 1-vessel ($50% stenosis in 1 vessel) disease, and (D) multivessel ($50% stenosis in $2 vessels) disease on CTA. Abbreviations as in Figure 3.
in patients with IPD (þ) and scar score $4, with IPD (þ)
and
scar
score
<4,
with
IPD(–)
and
scar
score $4, and with IPD(–) and scar score <4, respectively (p < 0.001). In Figure 7B, global chi-
Supplemental Figure 5 shows annualized event rates for MACEs in patients with and without scar score of $4 or IPD. Kaplan-Meier
curves
in
patients
with
sub-
square tests showed that IPD and scar score $4
endocardial (having segments with scar score 1 to 2
had incremental prognostic value over each other
and not having segments with scar score $3) or
(p < 0.001).
transmural (having segments with scar score $3)
Figure 8 and the Central Illustration showed annu-
scarring are shown in Supplemental Figure 6. Annu-
alized event rates for MACEs by combination of
alized event rates were 3.6% and 9.5% in patients
obstructive CAD, scar score $ 4, and IPD in all pa-
with subendocardial or transmural scar, respectively
tients and those with suspected or known CAD.
(p ¼ 0.002).
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F I G U R E 7 Complementary Prognostic Value of IPD and Scar Score
B
Kaplan-Meier Curves by Combination of IPD and Scar
Event-Free Survival
1.0 0.8
IPD (-) + Scar Score <4 IPD (-) + Scar Score ≥4 IPD (+) + Scar Score <4
0.6
IPD (+) + Scar Score ≥4
0.4
Global Chi-Square Test p < 0.001
p < 0.001
67.3
Global Chi-Square
A
67.3
48.6 36.0
0.2 log-rank, p < 0.001
0.0 0
1
2
3
IPD
4
Follow-Up Time (Years)
IPD +Scar Score ≥4
Scar Score ≥4 Scar Score ≥4 +IPD
Patients at risk IPD (-) + Scar Score <4 311
279
222
147
IPD (-) + Scar Score ≥4 60
47
37
23
89 13
IPD (+) + Scar Score <4 103
67
52
32
21
IPD (+) + Scar Score ≥4 66
50
38
22
8
(A) Kaplan-Meier curves by combination of IPD and scar score in all patients. (B) Global chi-square test shows incremental prognostic value of IPD and scar score of $4 over each other. IPD ¼ ischemic perfusion defect.
Details of events in patients with IPD or scarring
emission CT among 379 patients with suspected or
are given in Supplemental Table 3. There was no
known CAD. However, in that study, no analysis for
significant difference in the number of each event
each patient group with suspected or known CAD was
between IPD and scar score $4.
performed. The present study demonstrates the
DISCUSSION The main findings of the present study were that: 1)
F I G U R E 8 Annualized Event Rates for Maces by Combination of Stenosis, Scar, or IPD
stress dynamic CTP with CTDE had incremental 15.6
prognostic value over CTA in each patient group with unfavorable prognosis in subgroups of patients with stent, heavy calcification, or obstructive CAD; and 3) IPD and myocardial scarring were independent predictors when adjusted for each other, with incremental prognostic value over each other. Compared with the prior study (11), we emphasized use of CTDE, distinction between ischemia and scarring, analysis in patients with known CAD, and role of IPD in the subcategories of patients with stent, heavy calcification, or moderate stenosis. RISK STRATIFICATION WITH CTP IN PATIENTS WITH
11.8
12.9
11.3 10.2
9.1
8.7
6.3 6.1 6.5
1.1 0.8
1.9
Obstructive CAD (-)
Obstructive CAD (+)
SUSPECTED OR KNOWN CAD. Several studies have
evaluated the prognostic value of CTP in patients
13.5
13
Annualized Event Rate (%)
suspected or known CAD; 2) IPD was associated with
All Patients
Obstructive Obstructive Obstructive CAD (+) CAD (+) CAD (+) + Scar Score ≥4 + IPD (+) + Scar Score ≥4 + IPD (+) Suspected CAD
Known CAD
with suspected or known CAD (14–16). Chen et al. (14) reported that the combination of CTA and static CTP
Annualized event rates for MACEs by combination of obstructive CAD, scar score, and
yielded a prediction of 2-year event-free survival
IPD. Abbreviations as in Figure 3.
similar to that obtained by ICA and single-photon
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C E NT R AL IL L U STR AT IO N Prognostic Value of Stress Dynamic Computed Tomography Perfusion With Computed Tomography Delayed Enhancement
A
B
Ischemic Perfusion Defect (IPD)
15.6
CT Delayed Enhancement Annualized Event Rate (%)
Stress Dynamic CT Perfusion
Risk Stratification by Stenosis, Scar, and IPD
8.7
6.3 6.1 6.5
1.9
Obstructive CAD (-)
Obstructive CAD (+)
All Patients
Obstructive Obstructive Obstructive CAD (+) CAD (+) CAD (+) + Scar Score ≥4 + IPD (+) + Scar Score ≥4 + IPD (+) Suspected CAD
Known CAD
Risk Stratification by IPD According to Coronary Status Heavy Calcification
Stents Event-Free Survival
12.9
11.3 10.2
9.1
1.1 0.8
C
13.5
13 11.8
Obstructive CAD
1.0
1.0
1.0
1.0
0.8
0.8
0.8
0.8
0.6
0.6
0.6
0.6
0.4
0.4
0.4
0.2
0.2 p < 0.001
0.0 0
1
2
3
4
0.4
0.2 p < 0.001
0.0 0
(Year)
1
2
3
50%-69% stenosis
0.2
p < 0.001
0.0
0.0
4
1
0
2
3
4
≥70% stenosis p < 0.001 0
1
(Year)
(Year) IPD (+)
2
3
4
(Year)
IPD (–)
Nakamura, S. et al. J Am Coll Cardiol Img. 2020;-(-):-–-.
(A) Images derived from dynamic CT perfusion with CT delayed enhancement for a patient with IPD. (B) Annualized event rates for MACEs by combination of stenosis, IPD, and scar score in all patients and those with suspected or known CAD. (C) Kaplan-Meier curves in patients stratified by the presence or absence of IPD according to coronary status (stent, heavy calcification, moderate stenosis, and severe stenosis). CT ¼ computed tomography; CTA ¼ computed tomography angiography; CAD ¼ coronary artery disease; IPD ¼ ischemic perfusion defect; MACE ¼ major adverse cardiac event.
prognostic value of CTP in each patient group with or
invasive angiography. The present study shows that,
without a history of CAD.
in the setting of moderate stenosis on CTA, the
RISK STRATIFICATION BY IPD IN PATIENTS WITH
presence of IPD was associated with adverse out-
OBSTRUCTIVE CAD ON CTA. One study showed that
comes, whereas patients without IPD had good
CTP improved risk stratification among patients
prognosis, implying the utility of IPD for the selective
with $50% stenosis with $70% stenosis on CTA (11).
use of invasive angiography in patients with moder-
However, evaluating the prognostic value of CTP in
ate stenosis.
patients with moderate (50% to 69%) stenosis and no
COMPARISON OF CTP WITH CT-DERIVED FRACTIONAL
severe stenosis on CTA is of interest because this is
FLOW
the population in which functional assessment may
computation from coronary CTA datasets (CT-FFR)
be important for the selection of patients undergoing
has emerged as a promising noninvasive tool for
RESERVE. Fractional
flow
reserve
(FFR)
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assessing the hemodynamic severity of epicardial
the present study used IPD from CTP and CTDE,
coronary stenosis. A recent study showed that dy-
whereas
namic CTP and CT-FFR both identify functionally
perfusion by CTP alone. Fifth, in our study, there
significant CAD with comparable accuracy, and by
were many comparisons using the alpha criterion of
combining the 2 techniques, diagnostic performance
0.05; the results might include type 1 errors. Finally,
can be improved (3). However, CT-FFR may not be
we performed not vessel territory–based but patient-
suitable for patients with known CAD after stenting or
based analysis to show the prognostic importance of
heavy calcification (17). A prior study showed the
IPD and scarring in a patient level. Further studies are
clinical potential of CTP to improve the diagnostic
needed to evaluate the prognostic value of IPD and
accuracy of CTA for detecting in-stent stenosis (18). In
scarring involving sites with stents or calcification.
the present study, CTP was useful for risk stratification of patients with stent or heavy calcification, implying that CTP may be a preferred method for predicting prognosis in such patients. In this study, ischemic score was obtained by scoring the reduction of normalized MBF values in each myocardial segment, thereby enabling dynamic CTP to quantify the severity of the ischemic burden. The poorer prognosis associated with larger ischemic burden demonstrated in our study suggests the importance of assessment of the severity of myocardial
perfusion
defect
for
risk
stratification.
In
contrast, CT-FFR provides information only on lesions in epicardial coronary arteries and cannot provide direct measurement of microvascular disease or diffuse atherosclerotic burden in the left ventricular myocardium level. STUDY LIMITATIONS. First, this study was a single-
center, retrospective study. A prospective, multicenter study should be performed to confirm the results of this study. Second, although the total radiation dose in this study was relatively small (mean effective dose: 8.7 mSv), adding CTP and CTDE to CTA increased the radiation dose compared with CTA alone. Third, all images in this study were obtained using dual-source CT. Further investigation is needed to clarify whether the same results as in our study could be obtained by using other types of CT scanners. Fourth, although the population in this
the
previous
study
adopted
abnormal
CONCLUSIONS Stress dynamic CTP with CTDE had incremental prognostic value over CTA in each group with suspected or known CAD and was prognostically useful in subgroups of patients with stent, heavy calcification, or obstructive CAD. IPD and myocardial scarring may
play
complementary
roles
in
prognostic
stratification. ADDRESS
FOR
CORRESPONDENCE:
Dr.
Kakuya
Kitagawa, Department of Radiology, Mie University Graduate School of Medicine, 2-174 Edobashi, Tsu, Mie 514-8507, Japan. E-mail:
[email protected]. mie-u.ac.jp. PERSPECTIVES COMPETENCY IN MEDICAL KNOWLEDGE: Stress dynamic CTP with CTDE provided incremental prognostic value over CTA not only in patients with suspected CAD but also in those with known CAD and may be recommended for prediction of prognosis in patients with stent, heavy calcification, or obstructive CAD. IPD and myocardial scarring may play complementary roles in prognostic stratification. TRANSLATIONAL OUTLOOK: Additional studies are needed to validate these findings in a prospective, multicenter setting.
study included patients from our previous study (11),
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KEY WORDS CT delayed enhancement, dynamic CT perfusion, prognostic value
A PPE NDI X For supplemental figures and tables, please see the online version of this paper.