Numerical Approach to the TH model with Flexible Distance Steps Along the Capillary (NTH_f)

Fig 1 presents a schematic diagram of the TH-based exchange model. The abbreviations used in this section are summarized in Table 1. From the observed blood tracer concentration of an upstream AIF, C_AIF(t), we estimate an arterial plasma input delivered to the tissue, C_a(t), through a convolution by an arterial transfer function, h_a(t,τ), to account for delay and prolongation of the tracer bolus between the point of observation and the tissue (e.g., characterized by a bolus arrival time, τ), including correction for the large vessel hematocrit (Hct) for plasma concentration: (1) Since there is only limited experimental data to draw on, h_a(t,τ) is estimated by using a model of lagged normal density curves, resulting from the convolution of a Gaussian with a decaying exponential, scaled by a delay parameter, τ.[14] Note that we primarily consider plasma transport here, as the tracer is assumed to be dissolved only in the plasma space of the blood.

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Fig 1. Schematics of the TH-based exchange model.

C_AIF, blood concentration of AIF; h_a, arterial transfer function; C_a, concentration of the arterial plasma input to the tissue; F_p, plasma flow per unit tissue volume; C_p, concentration in the tissue capillary plasma space; C_e, concentration in the extravascular space; v_p, plasma volume in the tissue; v_e, extravascular interstitial volume; PS, product of the permeability and the surface area between the compartments; x_i, a position along the capillary.

https://doi.org/10.1371/journal.pone.0162067.g001

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Table 1. Definitions of perfusion parameters.

https://doi.org/10.1371/journal.pone.0162067.t001

Given a position along the capillary (as shown in Fig 1), x = x_i, and time, t = t_j, we define J(x_i,t_j) as the passive diffusive flux of tracer between the tissue capillary plasma space and the extravascular space, i.e., J(x_i,t_j) = PS ∙ (C_p(x_i,t_j) − C_e(t_j)), where PS is the product of the permeability and the effective surface area of the membrane between the compartments, C_p(x_i,t_j) is the concentration in the tissue capillary plasma space, and C_e(t_j) is the concentration in the extravascular space. Following the TH model, we assume that C_e(t_j) does not depend on position. A conventional TH model considers the exchange of tracer between the flowing plasma and the extravascular space from a spatially fixed, “Eulerian” frame of reference, balancing the tracer fluxes across discrete segments of the capillary from advection along the capillary and diffusion across the wall of the capillary; this can lead to numerical problems at high flow rates. Instead, we consider the exchange from a “Lagrangian” frame of reference traveling with the plasma. That is, we estimate the exchange over a flexible discrete fractional distance traveled along the capillary by a plasma element and assume: 1) the extravascular concentration is uniform and effectively constant during a time step, Δt, and 2) the capillary plasma concentration within the plasma element is effectively constant during Δt at a given location, while the mean transit time (MTT) (the average time taken by the tracer to travel through the tissue) is estimated iteratively. Then, C_p(x_i,t_j) and C_e(t_j) are calculated numerically from C_a(t) and a given set of values of the model parameters, given the boundary condition C_p(0,t) = C_a(t): (2) (3) where v_p is the fractional plasma volume in the tissue, v_e is the fractional extravascular interstitial volume, δ_x = Δt/MTT is the fractional distance traveled along the capillary by a plasma element during Δt and MTT = v_p/F_p, F_p is the plasma flow per unit tissue volume, and N is the number of discretization intervals of x. We approximate the extravascular concentration as being effectively constant during Δt. The net concentration of tracer in the capillary-tissue unit, C_t(t), is calculated by summing over the capillary elements, together with the extravascular space: (4) A nonlinear least-squares solver is used to find optimal parameter values (F_p, v_p, v_e, PS and τ) to minimize the mean squared difference between the predicted C_t(t) and the observed tissue concentrations, given the observed AIF. Maximum number of iterations is set to 400 and the termination tolerance is set to 10⁻⁶. In order to convert the plasma concentrations and flow to equivalent blood concentrations and blood flow, the value of Hct can be measured by sampling blood from a large vessel. However, the capillary hematocrit (Hct_c) would generally be lower than the large vessel value, due to the fact that red cells transit more rapidly than plasma through the microcirculation [15]. Unfortunately, Hct_c is not readily measured, so we instead rely on estimates derived from the literature [16] to scale the large vessel hematocrit values to estimated equivalent capillary values (Hct_c = 0.7 × Hct). Thus, for application of the analysis to myocardial perfusion calculation, the myocardial blood flow through the tissue per unit mass of tissue (MBF) (ml/g/min), was calculated by , where ρ is the assumed tissue density of 1.05 (g/cc) (for F_p in units of ml/cc/sec). Myocardial perfusion reserve index (MPRI) was calculated by dividing results of myocardial perfusion at stress by results at rest, with an associated independence from many common constant factors.

Study Population

This study was approved by our Institutional Review Board at the NYU School of Medicine, and all subjects provided written informed consent before the procedure. We prospectively studied 8 patients (6 male; age, 62 ± 13 years old; body mass index, 29.4 ± 4.3 kg/m²) with suspected coronary artery disease (CAD), who underwent first-pass perfusion rest and stress CMR imaging (described below), followed by a clinical diagnostic invasive coronary angiography examination on the same day. Exclusion criteria included unstable angina, irregular heart rate, valvular heart disease, and contraindications for MRI examinations (e.g., pacemakers or ferromagnetic vascular clips), contrast agent injection (e.g., contrast allergies), or pharmacologic stress agents (e.g., significant asthma when undergoing regadenoson stress).

CMR Imaging

All subjects were instructed to refrain from foods and beverages containing caffeine for 12 hours prior to the procedure. Imaging was performed on a 3T whole-body MR scanner (Tim Trio; Siemens Medical Solutions, Erlangen, Germany), using a standard phased-array coil that was applied to the anterior chest of the patient in the supine position. Blood pressure, heart rate, and electrocardiogram were monitored during the CMR examination. Rapidly repeated T₁-weighted (T₁w) CMR images were acquired during a contrast agent bolus passage at four slice locations in each heart beat: aortic root, for measuring the AIF, and short-axis slices at three levels of the left ventricle, for measuring the wall response. A first perfusion scan was performed at rest, followed by a second scan, after a delay of 10 minutes to allow for the initial clearance of the first contrast agent injection, during maximal vasodilatation. Maximal vasodilatation was obtained about 90 seconds after infusion of 0.4 mg regadenoson (Lexiscan 0.4 mg IV bolus, Astellas Pharma, USA) over 10 seconds. Each set of perfusion images was acquired during breath-holding for 10 heartbeats before a contrast injection, to acquire baseline T1w images, and for 40 heartbeats during the first-pass transit of a bolus of 0.05 mmol gadolinium-diethylenetriamine pentaacetic acid (Gd-DTPA)/kg body weight (0.5M Berlex Magnevist, Schering AG, Germany), injected at an injection rate of 5 mL/s, followed by a 20 mL bolus of normal saline flush. If breath-holding could not be sustained for the full duration of the data acquisition, subjects were allowed shallow breathing during the remainder of the imaging (respiratory motion was manually compensated for during image analysis; see below).

A cardiac-triggered saturation-recovery (SR) ultrafast gradient echo (i.e., TurboFLASH) pulse sequence was used to sequentially acquire T₁w images at multiple slices with sequential TDs after a single non-selective robust saturation pulse.[13, 17, 18] Imaging parameters included: FOV = 340–400 mm × 289–340 mm, slice thickness = 8 mm, in-plane resolution = 1.06–1.25 mm × 1.06–1.25 mm, TE/TR = 1.2/2.4 ms, flip angle = 10°, temporal resolution = 114–189 ms, generalized autocalibrating partially parallel acquisitions (GRAPPA) [19] with an effective acceleration factor ~ 1.65, centric k-space trajectory, and receiver bandwidth = 1008 Hz/pix. In order to correct for the spatially varying receive coil sensitivities and the unknown equilibrium magnetization, a proton density-weighted (PDw) image (flip angle = 5°) was acquired without the saturation pulse in the first heartbeat, which was used to normalize the subsequent images.[20] The resulting data were analyzed as previously described [13] to calculate the corresponding time course of contrast agent concentration in the blood and the myocardium, assuming rapid relaxation exchange between tissue water and the contrast agent and a known relaxivity of the contrast agent.

Data and Statistical Analyses

Data analysis was performed using custom software developed in MATLAB R2015a (The Mathworks, Inc., Natick, MA) on a 3.47 GHz Intel Core i7 personal computer with 24 Gb of RAM. As shown in Fig 2, a 16-segment model of the left ventricle (LV) based on the standard “17-segment” model (without the apical “cap”) was used, dividing the LV into 6 basal, 6 mid, and 4 apical segments.[21] These segments were also each further divided into epicardial (epi) and endocardial (endo) regions (total 32 segments). Tracking of the segments to compensate for respiratory motion was performed manually; the respiratory motion was assumed to be primarily in-plane. Individual myocardial segments were assigned to the territories of the three major coronary arteries (LAD, left anterior descending; RCA, right coronary artery; LCX, left circumflex) as per standard recommendations (Fig 2).[21] The severity of coronary artery stenosis was determined from the invasive coronary angiography examination by a cardiologist after the procedure and was expressed as a percent reduction in vessel diameter. The lesions were assigned to one of three categories of severity: 1) < 40% narrowing (insignificant), 2) 40% to 80% (mild to moderate), and 3) ≥ 80% (severe). Data are presented as mean ± standard deviation. Student’s t-test was used to compare the results. P values less than 0.05 were considered significant.

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Fig 2. Display of the 16 cardiac short-axis segments divided into epicardial and endocardial regions (total 32 segments).

Colors indicate the three coronary artery territories of the left anterior descending (LAD), right coronary artery (RCA), and the left circumflex coronary artery (LCX).

https://doi.org/10.1371/journal.pone.0162067.g002

Comparison of NTH_f and AATH Perfusion Estimates

For comparison, we used a conventional AATH model to estimate the following perfusion parameters: tissue blood flow, F, transit time through capillary, T_c, capillary permeability-surface area product, PS, and rate constant for the clearance of the tracer, k_adb.[11] C_a(t) calculated from the results of the NTH_f analysis was used as an input function. The Spearman's correlation coefficient was used to evaluate the correlations between the MBFs found from the NTH_f and AATH models. The residual sum-of-squares (RSS) was calculated for each segment, as a measure of the goodness-of-fit, by using the following equation: RSS = ∑_time(observed data − estimated fit)².

Noise Stability Estimation

For noise stability estimation of the NTH_f, myocardial perfusion signals were simulated with a low MBF (= 0.8102 ml/g/min) and a high MBF (= 2.2006 ml/g/min). White Gaussian noise (WGN) sets were generated with a range of the signal-to-noise ratio (SNR) = 1 to 60 (dB) (2 dB steps), using a function (awgn) in MATLAB R2015a, and were added to the simulated [Gd-DTPA] signals. The simulated noisy signals were then used to calculate the estimated MBF. For each SNR value, a computation was repeated 30 times. Percent error (%) was calculated by |estimatedMBF-trueMBF|/trueMBF×100.

NTH_f

The mean MBF of all patient regions at rest supplied by coronary arteries with insignificant stenosis was 0.80 ± 0.33 ml/g/min, which increased to 1.25 ± 0.45 ml/g/min at vasodilator stress, resulting in an average myocardial perfusion reserve index (MPRI) of 1.68 ± 0.54. In regions supplied by vessels with mild to moderate stenosis, the mean MBF at rest (0.74 ± 0.21 ml/g/min) was similar to that in the insignificant stenosis regions, but was lower during vasodilator stress (1.09 ± 0.28 ml/g/min; p < 0.05), resulting in a slightly lower average MPRI of 1.54 ± 0.46 (p < 0.05). In regions supplied by vessels with severe stenosis, the mean MBF at rest (0.79 ± 0.28 ml/g/min) was again similar to that of the regions supplied by vessels with insignificant or the mild to moderate stenosis, but it was even lower during vasodilator stress (0.63 ± 0.34 ml/g/min; p < 0.05). The resulting MPRI (0.85 ± 0.48) was significantly lower than in regions supplied by vessels with mild to moderate stenosis (p < 0.001). The results of the NTH_f and AATH models are summarized in Table 2.

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Table 2. NTH_f and AATH results: MBF and MPRI corresponding to percent diameter stenosis of coronary lesion.

https://doi.org/10.1371/journal.pone.0162067.t002

The perfusion results for a representative patient (83-year-old female) with angiographically normal coronary arteries (Fig 3A) are shown in Fig 3. First-pass CMR perfusion imaging demonstrated a qualitatively uniform delivery of contrast agent to the heart wall (Fig 3B). The mean MBFs at rest were 0.98 ± 0.24 ml/g/min in LAD territory, 1.02 ± 0.15 ml/g/min in RCA territory, and 0.91 ± 0.16 ml/g/min in LCX territory (Fig 3C). The mean MBFs at stress were 1.63 ± 0.39 ml/g/min in LAD territory, 1.67 ± 0.37 ml/g/min in RCA territory, and 1.27 ± 0.31 ml/g/min in LCX territory (Fig 3D). The mean MPRIs were 1.69 ± 0.26 in LAD territory, 1.64 ± 0.22 in RCA territory, and 1.40 ± 0.26 in LCX territory (Fig 3E). On the other hand, Fig 4 shows the results for a representative patient (66-year-old male) with a history of hypertension, hyperlipidemia, diabetes mellitus and known coronary artery disease with prior stents, on maximal medical therapy. Coronary angiography demonstrated severe triple-vessel disease (Fig 4A). First-pass CMR perfusion imaging demonstrated a qualitatively delayed and decreased delivery of contrast agent to the inferior segments, consistent with ischemia or scar. There was also a suggestion of qualitatively milder delayed delivery to the anterior segments at stress (Fig 4B). The mean MBFs at rest were 0.60 ± 0.12 ml/g/min in LAD territory, 0.54 ± 0.08 ml/g/min in RCA territory, and 0.60 ± 0.07 ml/g/min in LCX territory (Fig 4C). The mean MBFs at stress were 0.85 ± 0.15 ml/g/min in LAD territory, 0.52 ± 0.30 ml/g/min in RCA territory, and 0.81 ± 0.18 ml/g/min in LCX territory (Fig 4D). The MPRIs were 1.45 ± 0.35 in LAD territory, 0.97 ± 0.55 in RCA territory, and 1.36 ± 0.18 in LCX territory (Fig 4E). Fig 5 shows another representative patient (65-year-old male) with angiographically severe triple-vessel disease (Fig 5A). First-pass CMR perfusion imaging showed relatively decreased flow to the anterior and anteroseptal wall (Fig 5B). The mean MBFs at rest were 1.00 ± 0.20 ml/g/min in LAD territory, 0.91 ± 0.11 ml/g/min in RCA territory, and 1.02 ± 0.24 ml/g/min in LCX territory (Fig 5C). The mean MBFs at stress were 0.73 ± 0.36 ml/g/min in LAD territory, 0.95 ± 0.38 ml/g/min in RCA territory, and 1.25 ± 0.29 ml/g/min in LCX territory (Fig 5D). The MPRIs were 0.75 ± 0.41 in LAD territory, 1.06 ± 0.44 in RCA territory, and 1.30 ± 0.52 in LCX territory (Fig 5E).

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Fig 3.

(a) Selective coronary angiography in a representative patient (83-year-old female) with angiographically normal coronary arteries. (b) First-pass perfusion mid-level MR image at stress. Bullseye plots of MBF (ml/g/min) (c) at rest and (d) at stress, and (e) MPRI calculated from the NTH_f method.

https://doi.org/10.1371/journal.pone.0162067.g003

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Fig 4.

(a) Selective coronary angiography in a representative patient (66-year-old male) with severe triple-vessel disease (arrows). (b) First-pass enhancement mid-level MR image at stress showing a qualitatively delayed and decreased delivery of contrast agent to the inferior segments and milder delayed delivery to the anterior segments. Bullseye plots of MBF (ml/g/min) (c) at rest and (d) at stress, and (e) MPRI calculated from the NTH_f method.

https://doi.org/10.1371/journal.pone.0162067.g004

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Fig 5.

(a) Selective coronary angiography in a representative patient (65-year-old male) with severe triple-vessel disease (arrows). (b) First-pass perfusion mid-level MR image at stress showing relatively decreased flow to the anterior and anteroseptal wall. Bullseye plots of MBF (ml/g/min) (c) at rest and (d) at stress, and (e) MPRI calculated from the NTH_f method, showing more extensive perfusion abnormality.

https://doi.org/10.1371/journal.pone.0162067.g005

Comparison of NTH_f and AATH Perfusion Estimates

Fig 6 shows representative Gd-DTPA concentration ([Gd-DTPA]) first-pass perfusion time-curves in representative normal and perfusion-defect segments (Fig 6A) of the patient shown in Fig 5. The estimated MBFs at rest using the NTH_f and AATH models were 0.81 and 0.97 in the normal segment, and 0.99 and 0.93 in the perfusion-defect segment, respectively (Fig 6B). The estimated MBFs at stress using the NTH_f and AATH were 1.56 and 1.30 in the normal segment, and 0.49 and 0.57 in the perfusion defect segment, respectively (Fig 6C). Note that the solid and dashed lines in Fig 6B and 6C indicate the predicted plots from the best-fit NTH_f and AATH models, respectively.

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Fig 6.

(a) Bullseye plot indicating representative segments of normal perfusion (blue) and perfusion defect (gray) in the patient with severe triple-vessel disease in Fig 5. Gd-DTPA concentration ([Gd-DTPA]) first-pass perfusion time-curves at (b) rest and (c) stress in the normal (blue circle) and defect (gray triangle) myocardium segments shown in (a) with best fit estimated plots from the NTH_f (solid line) and AATH (dashed line) models. Estimated MBFs (ml/g/min) using the NTH_f model at rest (stress) were 0.81 (1.56) in a normal segment and 0.99 (0.49) in a perfusion defect segment, and estimated MBFs using the AATH model at rest (stress) were 0.97 (1.30) in a normal segment and 0.93 (0.57) in a perfusion defect segment.

https://doi.org/10.1371/journal.pone.0162067.g006

We found strong correlation between the results of the NTH_f and AATH models. The correlation coefficients of MBFs calculated with the NTH_f and AATH models were r = 0.97 at rest (Fig 7A), r = 0.93 at stress (Fig 7B), and r = 0.91 (MPRI; Fig 7C). p < 0.001 for all. In particular, the MBFs estimated from the NTH_f model were higher than those from the AATH model at the higher flows (e.g., MBF > 1). The results of representative Bland-Altman plots are shown in Fig 7D–7F. The mean RSS values for 32 myocardial segments were smaller in the NTH_f (0.0068 ± 0.008 at rest and 0.0071 ± 0.0065 at stress) than the AATH (0.0119 ± 0.0136 at rest and 0.0116 ± 0.0079 at stress), showing a high goodness of fit in the NTH_f.

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Fig 7.

The correlation plots of MBFs from the NTH_f and AATH at (a) rest and (b) stress. (c) The correlation plot of MPRIs from the NTH_f and AATH. p < 0.001 for all. Bland-Altman plots of MBFs from the NTH_f and AATH at (a) rest and (b) stress. (c) Bland-Altman plot of MPRIs from the NTH_f and AATH.

https://doi.org/10.1371/journal.pone.0162067.g007

Noise Stability Estimation

Fig 8A shows representative simulated plots at SNR = 10, 20 and 30, and corresponding fitting plots from the NTH_f model. Over all, the percent errors at MBF = 0.81 and 2.20 are up to 16.6 ± 14.5% and 21.5 ± 20.3% (mean ± 2 SD) for a range of SNR = 0–60, respectively (Fig 8B).

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Fig 8.

Plots simulated with (top) MBF = 0.81 and (bottom) MBF = 2.2. (a) Simulated (or original; solid line), White Gaussian noise added (circle), and estimated from NTH_f (dashed line) plots are shown at SNR = 10, 20, 30. (b) Percent errors for a range of SNR = 0–60 showing average and two standard deviation error bars (each SNR was repeated 30 times).

https://doi.org/10.1371/journal.pone.0162067.g008

Compliance with Ethical Standards

This study was approved by our Institutional Review Board at the NYU School of Medicine, and all subjects provided written informed consent before the procedure.