Low-dose ¹⁸F-FDG TOF-PET/MR for accurate quantification of brown adipose tissue in healthy volunteers

In this retrospective study, a total of 20 ¹⁸F-FDG TOF PET/MR datasets from 13 healthy male Caucasian volunteers (median age, 23 years; range, 19–28 years; median body mass index, 22.9 kg/m²; range, 18.6–25.4 kg/m²) were obtained from a prospective clinical study [21]. In that study, each subject received two PET/MR scans, separated by 14 days. However, only 20 datasets were available for retrospective reconstructions. In short, 4 h before the PET/MR scan, all participants received 200 mg mirabegron per os, a selective β₃-adrenoreceptor agonist, to stimulate BAT activity. Two and a half hours before the scan, the volunteers were exposed to a standardized mild cooling protocol by applying two cooling sleeves around the subjects’ abdomen and chest, connected to a medical cooling device (Hilotherm Clinic®, Hilotherm GmbH, Germany). Next, the volunteers were scanned using a simultaneous TOF PET/MR system (SIGNA PET/MR, GE Healthcare, Waukesha, WI, USA), having a PET axial field-of-view (FoV) of 25 cm and a TOF timing resolution of 400 ps [22, 23]. After performing a partial body MR localizer scan, a 30-min dynamic three-dimensional (3D) PET acquisition of the neck area (one bed station) was started and 75 MBq of ¹⁸F-FDG was injected over an intravenous line. The dynamic PET scan was followed by a static 3D PET emission partial body scan. It consisted of three bed stations, each with a duration of 4 min, covering an area from the head to the upper abdomen. During PET scanning, a default 3D dual-echo, spoiled gradient recalled echo MR sequence was performed for PET attenuation correction (MR-AC). Fat and water images were automatically reconstructed from the obtained in-phase and out-of-phase images. The PET attenuation correction algorithm uses an atlas for the head region and a continuous fat-water-based attenuation correction method for the other body parts [24, 25]. Besides the MR-AC sequence, T₁-, T₂-, and T₂*-weighted MR imaging was performed as well as diffusion weighted MR imaging (DWI).

In this study only, the last 10 min of the 30-min PET frames were used for the simulated dose reductions. The minimal dose was expected to be below 40% of the original dose, as the 10-min scan is 2.5 times longer than the standard 4-min static scans used in this and other studies [21, 26]. Therefore, every 10-min dataset was reconstructed using seven dose reduction steps, having approximately 35%, 30%, 25%, 20%, 15%, 10%, and 5% of the original counts.

To do so, first, an artificial trigger signal was inserted every second in the PET list-mode datasets using an in-house developed Matlab script (MATLAB R2018a, MathWorks, Natick, MA, USA). Next, the scanner’s gating options were enabled which allowed us to select only those counts for PET reconstruction that were detected during the above-indicated percentage of time between each trigger signal. This way, the counts are reduced on a second by second basis, thereby simulating a corresponding lower injected dose. It also means that normal effects like decay, biodistribution, and possibly volunteer motion remain included. This unlisting process was repeated seven times for each PET list-mode dataset to generate the seven TOF PET sinograms with approximately the previously indicated counts, simulating a lower activity due to a reduced injected dose.

The 4-min reference datasets applied in this research were created using the same 30-min PET frame datasets that were used for the 10-min reduced activity datasets. During PET reconstruction, the start time was set to 20 min to match the start time of the reduced activity datasets, and the duration was set to 4 min. This means that the “uptake” times of the reference and reduced activity reconstructions are the same.

PET reconstructions were performed using the scanner’s three-dimensional ordered subset expectation maximization (3D-OSEM) based reconstruction algorithm for TOF PET data (VUE Point FX, GE Healthcare, Waukesha, WI, USA). PET reconstructions included all standard corrections like decay, scatter, random, dead time, attenuation, normalization, and the detector response. The number of subsets was 28 and the number of iterations was 2, the reconstruction diameter was 60 cm, and the image grid was 256 × 256 with 2.34 × 2.34 × 2.78 mm³ voxels. All OSEM reconstructions were post-filtered in image space using an in-plane Gaussian convolution kernel with a full-width-at-half-maximum of 5.0 mm, followed by a standard axial filter with a three-slice kernel using relative weights of 1:4:1.

All images were analyzed on a dedicated workstation (Advantage Workstation 4.6, GE Healthcare), which allowed images to be viewed side-by-side as well as in fused mode. PET images were visually examined and scored in consensus by an experienced nuclear medicine physician and a dual trained experienced nuclear medicine physician and radiologist. The image quality was scored using a 5-point Likert scale (1, non-diagnostic image quality to 5, excellent image quality) and image artifacts were scored using a 3-point scale (0, no artifacts; 1, insignificant artifacts; 2, significant artifacts).

For the quantitative analysis, the standardized uptake values (SUL) were normalized using the lean body mass (LBM) [17, 27]. Cubic 16.6cm³ volumes of interest (VOIs) were drawn bilateral in a homogeneous part of the infraspinatus muscle and propagated to all other reconstructions with different activities of the same scan (Additional file 1: Figure S1). Maximum SUL (SUL_max), mean SUL (SUL_mean), and the standard deviation (SUL_std) were obtained from each VOI. To assess the image background noise, the coefficient of variation (SUL_cov = SUL_std/SUL_mean) was calculated.

VOIs were also drawn around artifacts using the workstation autocontour tool. Only artifacts having a minimal SUL of 2.0 g/ml on the 5% activity reconstructions were included as these are expected to affect the reporting of BAT. The 5% activity reconstructions were chosen as those have the highest noise.

The effect of dose reduction on BAT metabolic activity, BAT metabolic volume (BMV), and total BAT glycolysis (TBG; counterpart to the normally used PET-metric “total lesion glycolysis TLG”) was also investigated [8]. For this, VOIs were drawn bilateral around supraclavicular BAT and SUL_max and SUL_mean were obtained. BMV was defined as the sum of all voxel volumes within the suspected BAT region where SUL > 1.2 g/ml. The TBG was defined as the product of the BMV and its corresponding SUL_mea n[17].

Percentage difference (%diff) parameters (X) were calculated using the 4-min datasets as reference: %diff = (X_y% − X_ref%)/X_ref% × 100, where y is any of the reconstructions in the range 5–35%.

The visual assessment showed that the reference and the 35%, 30%, and 25% activity reconstructions have good image quality (Fig. 2a) and no artifacts (Fig. 2b). Although the 20% activity reconstructions have a statistically significant reduction (p = 0.02) in image quality compared to the reference, the image quality was still acceptable with no artifacts. The 15%, 10%, and 5% activity reconstructions have a significantly lower (p < 0.01) image quality. Moreover, the 10% and 5% activity reconstructions also suffer from a significant increase (both p < 0.01) in artifacts and are therefore not recommended.

The SUL_max, SUL_std, and SUL_cov, obtained from VOIs in the homogeneous part of the infraspinatus muscle, increase with decreasing activity (Fig. 3 and Additional file 1: Table S1). There was no significant difference in background SUL_max between the reference and the 35%, 30%, and 25% activity reconstructions. The 20% and lower activity reconstructions started to be significantly different from the reference (all p < 0.01). The background SUL_mean was significantly higher (p = 0.02 for 35% and 30%, p < 0.01 for 25–5%) in all reduced activity reconstructions, compared to the reference. There was no significant difference in background SUL_std between the reference and the 35% and 30% reconstructions. The 25% and lower reconstructions were all significantly different to the reference (all p < 0.01). The background noise (SUL_cov) was previously defined as the ration between SUL_std and SUL_mean. As the SUL_mean is approximately stable over the reduced activity range, the SUL_cov has similar results as the SUL_std. This means that from a quantitative perspective, the noise started to increase at the 25% and lower activity reconstructions (all p < 0.01).

There was no significant difference in artifact SUL_max or SUL_mean between the reference and the 35% and 30% reconstructions (Additional file 1: Table S2). Artifact SUL_max or SUL_mean started to increase at the 25% and lower activity reconstructions (all p < 0.01)

For supraclavicular BAT SUL_max, only the 5% activity reconstructions have a significantly higher value compared to the reference (p < 0.01) (Fig. 4 and Additional file 1: Table S3). There was no significant difference in supraclavicular BAT SUL_mean between the reference and the reduced activity reconstructions. There is no significant difference in supraclavicular BAT BMV and TBG between the reference and the 35%, 30%, 25%, and 20% activity reconstructions. The 15%, 10%, and 5% activity reconstructions have increasing differences compared to the reference (p = 0.02, p < 0.01, p < 0.01, respectively, for both BMV and TBG).

Combining the information from the visual assessment, the quantitative assessment of the background noise and artifacts, and the quantitative assessment of supraclavicular BAT, we can see that the lowest possible dose would be 25% of the original dose. Although the artifacts and the background noise of the 25% activity reconstruction were significantly higher in the quantitative analysis, it was visually still evaluated as having good image quality.