Feasibility of biventricular volume and function assessment using first-pass gated ¹⁵O-water PET

Nineteen patients aged 47–75 years (median 66 years, 14 men and 5 women) were prospectively recruited from the outpatients of the Nuclear Medicine Department at Caen University Hospital from December 2015 to November 2016 in the frame of the WATERDAY study (ClinicalTrials.​gov unique identifier NCT02278497) aiming to compare myocardial perfusion and flow reserve using dynamic myocardial SPECT to ¹⁵O-water PET and endovascular fractional flow reserve measurement [26]. Inclusion criteria were the presence of at least one significant (≥ 50%), non-occlusive, coronary stenosis on percutaneous coronary angiography, and no history of myocardial infarction. All patients underwent both myocardial SPECT and ¹⁵O-water PET within 3–17 days (median 10 days), without any relevant cardiovascular event or change in cardiotropic medication between the two examinations. The study was approved by the Regional Ethics Committee (CPP Nord-Ouest III, France), and all patients gave written informed consent. The clinical characteristics of the study population are summarized in Table 1.

All SPECT acquisitions were carried out using a dedicated CZT cardiac SPECT camera (D-SPECT; Spectrum-Dynamics, Biosensors, Caesarea, Israel) with the patient in supine position. Rest and stress acquisitions were performed in the same session. Rest images were acquired during 5 min, 6-7 min after injection of 2.5 MBq/kg of ^99mTc-sestamibi. For stress imaging, 7 MBq/kg of ^99mTc-sestamibi was injected at peak hyperaemia following IV injection of 400 μg of regadenoson, and data were acquired 6–7 min later over 2 min. Gated SPECT images were reconstructed using the manufacturer’s dedicated software and post-processed using commercially available software (Corridor4DM, INVIA, Ann Arbor, MI) [27] to obtain LV end-diastolic volume, end-systolic volume, stroke volume, and ejection fraction. The R-R interval was divided into 16 intervals. Myocardial wall segmentation was fully automated, and additional slight manual adjustment of LV basal limit was performed whenever necessary.

All PET acquisitions were achieved using a GE Discovery VCT RX scanner (GE Healthcare, Buc, France) and started with a low-dose transmission CT scan for attenuation correction. Two intravenous injections of ¹⁵O-water (1.5 to 3 MBq/kg) were performed, each one being simultaneously performed with the start of a dynamic gated 4′30″ emission scan. The second emission scan was performed at peak vasodilator stress following IV injection of 400 μg regadenoson. After correction for random coincidences, scatter, and dead time, the acquired list-mode data was reconstructed twice. First, a dynamic 24-frame sequence (14 × 5″, 3 × 10″, 3 × 20″, and 4 × 30″) was obtained using Fourier rebinning and 2D filtered back-projection. It allowed to extract a time-activity curve (TAC) in a region of interest (ROI) centred on the cardiac area. TACs were characterized by a sharp early peak corresponding to tracer first-pass through the right then left cardiac cavities followed by a sustained decreasing plateau corresponding to myocardial uptake then wash out. End of tracer first-pass was detected by visual inspection as the TAC transition point between the peak and the plateau. A second image reconstruction was then performed over the first-pass time range using 3D OSEM (nine subsets, two iterations) with eight-interval gating. Reconstructed images were re-oriented into cardiac canonical axes using CardIQ software on a dedicated workstation (Advantage Windows 4.4, GE Healthcare, Buc, France). Final image matrices were sampled on a 64 × 64 × 47 grid with 3.27 mm cubic voxels.

First-pass gated blood-pool images were post-processed using in-house software (TomPool, freely available for download at http://​scinti.​edu.​umontpellier.​fr) that was originally designed for equilibrium radionuclide angiography and adapted for first-pass data processing. Initial operator intervention was required to set the position of the septal plane (on horizontal long axis images), the valve plane (on vertical long axis images), and the infundibular plane as the upper limit of the RV (on short-axis images). A four-dimensional (4D) immersion algorithm was then run that produced a partition of the gated images into 4D regions centred on local intensity maxima. Each region was then assigned either to LV, RV, or extra-ventricular activity depending on the relative position of its barycentre with respect to the reference planes. Manual correction for misassigned regions was possible as well as semi-automated segmentation refinement. LV segmentation mask was obtained using a thresholding method at a fixed percentage of the 4D maximal intensity value inside the regions belonging to LV. Thresholds ranging from 20 to 40% were tested in order to determine the optimal threshold value. LV volumes were computed using a count-based method in which the volume of each voxel was normalized by the ratio of its intensity to the LV maximal intensity. RV segmentation mask was obtained by applying an adjustable threshold with respect to the 4D maximal intensity value inside the regions belonging to RV, and RV volumes were computed using a geometric method in which each voxel accounted for a constant volume regardless of its intensity. The RV threshold was chosen by the operator based on visual inspection and so as to fit as much as possible RV and LV stroke volumes (which was legitimate since no patient had documented valvular disease). Ventricular ejection curves were fitted to the eight time samples ({t_n, v_n}, n = 1…8) using a deformable curve model v_n = η[R(t_n + τ(t_n))] where R(t) is the reference curve derived from a series of normal patients sampled over 512 time points, η a second-order polynomial, and τ a weighted sum of cosine functions with variable phase shift and frequency.

Continuous variables are expressed as mean ± standard deviation (min-max range). Concordance and correlation between rest and stress functional parameters obtained using first-pass PET were assessed using Pearson’s correlation coefficient (R), Lin’s concordance correlation coefficient (ccc), and Bland-Altman analysis. Comparison between LV volume and function given by first-pass PET and those given by myocardial SPECT was achieved using the same metrics. Difference between homologous variables was characterized using a paired Student’s t test after checking data sample normalcy using the Kolmogorov-Smirnov test. All statistical computations were carried out using Excel (Microsoft, Redmond, WA).