Incremental diagnostic value of [¹⁸F]tetrafluoroborate PET-CT compared to [¹³¹I]iodine scintigraphy in recurrent differentiated thyroid cancer

A consecutive number of 25 [¹⁸F]TFB-PET acquisitions combined with either CT or MRI of patients suffering from DTC (9 males and 16 females, median age 57) were included in this retrospective study (inclusion period: July 2018 to June 2019). Patients were referred to [¹⁸F]TFB-PET due to newly discovered increasing levels of thyroglobulin (TG), autoantibodies against thyroglobulin (antiTG), suspicious cervical lymph nodes, or combinations of the latter. Decision for [¹⁸F]TFB-PET examination was done on a case-by-case basis due to aforementioned clinical indication. Detailed patient characteristics are given by Table 1. The median time from thyroidectomy to [¹⁸F]TFB-PET was 5.1 [6.3] years. The median cumulated therapeutic dosage of [¹³¹I]iodine that was employed in the cohort until [¹⁸F]TFB-PET was 10 [10.4] GBq. All patients were treated with Levothyroxine to suppress thyroid-stimulating hormone (TSH) levels [2].

[¹⁸F]TFB was prepared according to a literature procedure described previously by isotopic exchange of BF₄⁻ with [¹⁸F]fluoride in hot hydrochloric acid and purified using an alumina column [16]. The product activity ranged between 6 and 8 GBq/batch. Radiochemical purities were determined by TLC and HPLC. The HPLC system was composed of a S1122 pump (Sykam, Fürstenfeldbruck, Germany); a S-2500 UV detector (KNAUER, Berlin, Germany); a GabiStar γ-detector (Elysia-Raytest GmbH, Straubenhardt, Germany); an Exsil ODS column, 5 μm, 250 × 4.0 mm (SGE Europe Ltd., Bucks, UK) with a mobile phase of 1-mM tetrabutylammonium hydroxide and 1.3 mM potassium hydrogen phthalate in water (pH 7.5) flowing at 1.0 ml/min, detection at λ = 254 nm; and the GINA Star software (Elysia-Raytest GmbH, Straubenhardt, Germany) ([¹⁸F]fluoride, t_R = 4.7 min; [¹⁸F]TFB, t_R = 11.2 min). Thin-layer chromatography (TLC) was performed on alumina TLC strips (Polygram Alox N/UV₂₅₄, 40 × 80 mm, Machery-Nagel, Düren, Germany) with methanol as mobile phase. Strips were scanned using a radio TLC scanner (Elysia-Raytest GmbH, Straubenhardt, Germany). R_f([¹⁸F]fluoride) = 0.0; R_f([¹⁸F]TFB) = 0.8.

Thyrotropin alfa was administered 48 and 24 h before the administration of [¹⁸F]TFB and [¹³¹I]iodine. A median activity of 317.0 [63.0] MBq [¹⁸F]TFB was administered intravenously. The PET acquisition was initiated 40 min after tracer injection (Biograph mCT flow or Biograph mMR, Siemens Healthineers, Erlangen, Germany; acquisition speed: 2 min/bed position or 1.1 mm/s). Low-dose CT or MRI was acquired for attenuation correction of PET data. A median activity of 315.0 [516.8] MBq [¹³¹I]iodine was administered immediately after completion of the PET acquisition (a month delayed in one patient; only patient #12 received a therapeutic dosage of 3 GBq [¹³¹I]iodine). WBS and SPECT-CT acquisitions were done in accordance with guidelines (Discovery NM/CT 670 Pro, GE Healthcare, Chalfont St Giles, GB or Symbia T2, Siemens Healthineers, Erlangen, Germany) [17].

Blood levels of TSH, free triiodothyronine (fT3), free thyroxine (fT4), TG, and antiTG were measured on the day of the first thyrotropin alfa administration (TG/TSH, Elecsys assays and cobas e 801, Roche Diagnostics, Rotkreuz, CH; TG, assay and KRYPTOR hTg sensitive, BRAHMS GmbH/Thermo Fisher Scientific, Hennigsdorf, Germany). Stimulated TG levels were measured before [¹³¹I]iodine WBS acquisition.

SPSS statistics 24 (IBM, NY, USA) was used for descriptive metrics and statistical testing. The McNemar and Wilcoxon method were used to test for statistically significant differences with the “exact” option of SPSS. H₀ was rejected if p < 0.05. Values are presented as median with standard deviation (SD) in squared brackets.

The detection rate of [¹⁸F]TFB-PET-CT was 52.0% (n = 13). Details are given in Fig. 1. A total number of 27 lesions were detected by [¹⁸F]TFB-PET-CT. All lesions were delineated due to increased [¹⁸F]TFB-PET accumulation. Metastases or local recurrence were discovered in 10 additional patients compared to [¹³¹I]iodine dxWBS/SPECT-CT (Fig. 3). The detection rate of [¹⁸F]TFB-PET-CT was significantly higher compared to [¹³¹I]iodine dxWBS/SPECT-CT (recurrence detected in 13 vs. 3 patients; p = 0.002). A detailed list of findings is given in Table 2 (see also Figs. 4 and 5). Reference standard for [¹⁸F]TFB-PET-CT-positive patients (n = 13) was surgery together with histological examination (in 4 patients), a corresponding [¹³¹I]iodine accumulation (in 3 patients), [¹⁸F]FDG accumulation (in 5 patients), or morphological finding on CT (in 1 patient; lung metastasis). Therefore, the sensitivity of [¹⁸F]TFB-PET-CT was 52% (accuracy: 52%). The median [¹⁸F]TFB uptake of delineated lesions was 4.2 SUV_max [8.4].

Looking at patients who underwent both [¹⁸F]TFB-PET-CT and [¹⁸F]FDG-PET-CT, the detection rate of [¹⁸F]TFB-PET-CT was higher (51.9%) compared to [¹⁸F]FDG-PET-CT (47.6%), yet this difference was not statistically significant. In three patients, [¹⁸F]FDG-PET-CT discovered metabolically active metastases (median SUV_max: 11.9) with no increased [¹⁸F]TFB accumulation. In contrast, [¹⁸F]TFB-PET-CT discovered lesions in six patients (local recurrence, lymph node or lung metastases), with no [¹⁸F]FDG accumulation. Combining [¹⁸F]FDG-PET-CT and [¹⁸F]TFB-PET-CT for staging of suspected recurrent DTC resulted in the highest sensitivity (64%; positive predictive value, 100%; accuracy, 64%).

In 6 patients, cervical lymph node metastases were suspected due to moderately increased [¹⁸F]FDG uptake (median SUV_max: 4.5). Likewise, [¹⁸F]TFB-PET-CT revealed suspicious uptake of theses lymph nodes (median SUV_max: 4.2). [¹⁸F]TFB-PET-CT-guided surgery together with histological analysis was performed in two patients. In both cases, lymph node metastases could be confirmed.

In three patients, [¹³¹I]iodine accumulating metastases were discovered by dxWBS and SPECT-CT (12.0%, one patient received a WBS with therapeutic dosage). In total, 11 lesions were detected by [¹³¹I]iodine imaging, which were significantly fewer compared to [¹⁸F]TFB-PET-CT (p = 0.001). All lesions were also detected by [¹⁸F]TFB-PET-CT, which additionally provided superior image quality (Fig. 2). Given histological CT or FDG-PET findings as reference standard, the sensitivity of iodine imaging was 12% (positive predictive value, 100%; accuracy, 12%). [¹⁸F]FDG accumulating local recurrence or metastases were delineated in 10 patients. The median uptake of these lesions was 5.2 SUV_max. Morphological findings without [¹⁸F]TFB, [¹⁸F]FDG, or [¹³¹I]iodine uptake were present in patients with lung metastases only (n = 3, 12%).

Median TSH suppressed TG and antiTG levels for patients with [¹⁸F]TFB-positive findings were 2.46 [1566.9] ng/ml and 98.7 [144.7] IU/ml, respectively. For comparison, [¹⁸F]TFB-negative patients had median TG levels of 1.87 [4.4] ng/ml. Only one [¹⁸F]TFB-negative patient had elevated antiTG (3267 IU/ml). In six patients, no morphological or molecular findings were detected. Median TG level of these patients was 0.83 [1.2] ng/ml (no patient with elevated antiTG levels).