Introduction
Differentiated thyroid carcinoma (DTC) is the most common (> 90%) type of thyroid carcinoma [
1]. Treatment with surgery, radioactive iodine (RAI), and TSH suppression is effective in most patients, resulting in 10-year survival rates of over 90%. Less than 10% of patients develop distant metastases, and 5–15% of patients become RAI refractory [
2,
3]. These patients do not take up RAI in (a part of) the lesions on diagnostic
131I scan or after
131I therapy or show progression of metastases despite substantial RAI uptake or cumulative
131I activity of > 22.2 GBq [
4]. For these patients, the prognosis is poor as 10-year survival rates decrease to 10%, from the time metastases are detected [
2].
Patients with RAI-refractory disease need alternative therapy, but treatment options are limited. Currently, for patients with asymptomatic, stable, or minimally progressive disease, monitoring while on TSH suppression is advised by the 2015 American Thyroid Association management guidelines [
1]. Interventions should only be used to prevent morbidity or palliate symptoms. In case of threatening or symptomatic lesions, directed therapy such as surgery, radiation, or peptide receptor radionuclide therapy (PRRT) is an option. Systemic therapy such as with tyrosine kinase inhibitors is another alternative (TKIs). However, due to severe side-effects, TKIs can decrease quality of life and should be considered carefully [
1]. Hence, there is a demand for new treatment modalities for patients who suffer from RAI-refractory DTC.
Prostate-specific membrane antigen (PSMA) is a type II transmembrane glycoprotein receptor, expressed in normal prostate tissue and to a greater extent in prostate carcinoma, making it a useful target for radionuclide imaging and therapy for prostate cancer [
5‐
7]. PSMA is also expressed in the neovasculature of other tumors including carcinomas of the lung, breast, colorectum, and thyroid [
8‐
12]. Compared to normal thyroid tissue, PSMA is significantly overexpressed in the neovasculature of DTC, especially in the RAI-refractory type [
13]. Altogether, PSMA is a potential target for theranostics in RAI-refractory DTC. Lütje et al
. and Verma et al
. found results suggesting that the use of
68Ga-PSMA PET/CT in DTC is suitable for determining whether a RAI-refractory patient is eligible for PSMA-targeted therapies, such as treatment with
177Lu-PSMA-617 [
14,
15].
To investigate the value of the theranostic PSMA, we performed a single-center retrospective analysis on patients with RAI-refractory DTC, referred for 68Ga-PSMA PET/CT to investigate suitability for peptide radioligand therapy with 177Lu-PSMA-617.
Methods
Patient selection
The multidisciplinary tumor board, consisting of at least one surgeon, endocrinologist, pathologist, radiologist, and nuclear medicine physician, decided whether patients with RAI-refractory DTC should undergo a 68Ga-PSMA PET/CT to determine their eligibility for therapy with 177Lu-PSMA-617. The 68Ga-PSMA PET/CTs made between 2016 and 2019 were retrospectively analyzed. Written informed consent was obtained from all living patients.
Patient characteristics
Patient characteristics including gender, age, treatment history, presence of locoregional recurrence/metastases or distant metastases, Tg antibodies, Tg levels, and TSH levels were retrieved from the medical files. An immunoradiometric assay (IRMA) (Brahms, Hennigsdorf, Germany) was used for measuring Tg antibodies and Tg until July 2017 and October 2017, respectively. Ever since, a chemiluminescence assay was used on a Liaison analyzer (DiaSorin, Saluggia, Italy). The functional sensitivity was 0.2 μg/L for both Tg assays. Patient characteristics are provided as median and range.
Preparation of radiopharmaceuticals
68Ga-PSMA-11 and 177Lu-PSMA-617 were prepared according to Good Manufacturing Practice using a fully automated system for routine production of radiopharmaceuticals and accompanying reagent kits and cassettes per manufacturer’s recommendations (Modular Lab Easy, Eckert & Ziegler, Berlin, Germany). Eppendorf tubes with 40 μg PSMA-11 or PSMA-617 were defrosted from − 20 °C storage and used for batch preparations (ABX, Radeberg, Germany). A 68Ge-68Ga-generator (GalliaPharm, Eckert & Ziegler, Berlin, Germany) and 177LuCl3 (EndolucinBeta, ITG, Garching, Germany) were used for radiolabeling.
Small aliquots (20–50 μL) were withdrawn from end products for quality controls. Thin-layer chromatography (TLC), high-performance liquid chromatography (HPLC), and pH, endotoxin, and sterility determinations were used for radiochemical purity as described previously [
16,
17].
Image acquisition and analysis
68Ga-PSMA-11 was administered intravenously in a dose of 1.5–2 MBq/kg. Combined PET and CT images were performed approximately 60 min after injection, from the skull vertex to the thighs using a TruePoint Biograph mCT40 scanner (Siemens, Erlangen, Germany). A low-dose CT scan was performed using Care Dose 4D and Care kV, with the following reference parameters: 40 mAs and 120 kV. PET was acquired according to the European Association of Nuclear Medicine recommendations with the following parameters: PET with time-of-flight and point spread function (TrueX) reconstruction, four iterations, 21 subsets, with a filter of 7.5 mm full width at half maximum [
18]. For standardized uptake values (SUV) measurements, the lean body mass corrected values were used.
68Ga-PSMA PET/CT scans were collected and reviewed by a dedicated board-certified head and neck nuclear medicine physician (BdK) experienced in 68Ga-PSMA PET/CT. On each scan, pathological focal tracer uptake was assessed and SUV measurements were performed on representative metastases. This included both the region of the (former) primary tumor, as well as regional or distant metastasis. Maximum SUV (SUVmax) were measured using a freehand isocontour volume of interest in these areas, using Syngo.via (Siemens, Erlangen, Germany). Also, all 18FDG PET/CTs performed within 3 months before or after 68Ga-PSMA PET/CT were reexamined for comparison. Outcome measurements are provided as median and range.
Eligibility for 177Lu-PSMA-617
The multidisciplinary tumor board decided whether patients were eligible for treatment with 177Lu-PSMA-617. Patients were deemed eligible if metastases were predominantly PSMA positive on 68Ga-PSMA PET, PET scans were assessed visually, and no pre-defined SUV cut-off values were used to decide whether or not to treat patients.
Discussion
This study describes our first experience with
68Ga-PSMA PET/CT imaging and subsequent therapy of metastatic RAI-refractory DTC using
177Lu-PSMA-617.
68Ga-PSMA PET/CT detected various types of lesions including lymph node, pulmonary, and bone metastases. This is in concordance with Taywade et al
., Verma et al
., and Lütje et al
., who also detected these and various other lesions [
14,
15,
19]. Furthermore, our results show uptake in liver metastases, which was also shown in RAI-sensitive patients by Verma et al
. [
15]. In addition, we found PSMA uptake in leptomeningeal metastases. Our results, although based on only five patients, indicate the potential clinical usefulness of
68Ga-PSMA PET/CT; not only because it is able to depict tumor lesions in various locations, but also because it may detect lesions which are not picked up by
18FDG PET/CT. Furthermore,
68Ga-PSMA PET/CT can be used for patient selection for therapy with
177Lu-PSMA-617.
Treatment with
177Lu-PSMA-617 has been proven to be safe and effective in patients with prostate carcinoma. Hofman et al
. showed a PSA decline of 50% or more in 57% of patients and an objective response in 82% of patients with measurable disease, after administering up to 4 cycles with a mean radioactivity of 7.5 GBq with relatively mild side-effects [
20]. Because of PSMA uptake in DTC metastases, treatment with
177Lu-PSMA-617 in RAI-refractory DTC was initiated. Patients with intermediate to intense PSMA uptake in all known lesions are most eligible for treatment with
177Lu-PSMA-617 [
14]. In our study, two patients underwent this therapy. Patient 2 showed slight, temporary response on imaging, while Tg values decreased from 17 to 9 μg/L. However, Tg antibodies increased simultaneously. In patient 5, the lesions increased on imaging and Tg levels rose after
177Lu-PSMA-617 therapy. Although in patient 2 the
177Lu-PSMA-617 therapy shows some potential, data of more patients is needed to draw conclusions on the effectiveness of this therapy.
In prostate carcinoma, PSMA expression is found mostly in the cytoplasm and membrane of the epithelium. This is in contrast to most other solid tumors, where PSMA is expressed predominantly in the endothelium of the neovasculature [
21]. Immunohistochemical expression of PSMA has previously been investigated in various forms of thyroid cancer. Lodewijk et al
. found PSMA positivity in neovasculature in more than 92% of medullary thyroid carcinoma, while the tumor cells were PSMA negative [
22]. Heitkötter et al
. studied PSMA on IHC in PTC and follicular thyroid carcinoma and found positivity in tumor-associated neovasculature in 18 out of 31 and 4 out of 10 patients, respectively [
23]. Moore et al
. investigated 37 patients and found PSMA significantly overexpressed in the neovasculature of DTC, particularly in RAI-refractory patients and in distant metastases. No PSMA expression was seen on the tumor cells [
13]. Recently, in a study including 59 DTC patients, Sollini et al. found PSMA positivity in microvessels in 80%. Of these cases, 53% was moderately positive and 47% highly positive [
24]. In conclusion, the localization of PSMA expression in the neovasculature of thyroid carcinoma instead of in tumor cells as in prostate carcinoma might explain why
177Lu-PSMA treatment is less effective in DTC than in prostate carcinoma.
Interestingly, PSMA uptake was heterogeneous in our patients. Since PSMA expression in thyroid carcinoma is a relatively new finding, biological behavior needs to be further investigated. We hypothesize that the amount of proliferation may vary in different lesions, which influences the amount of vascularization. As PSMA expression is seen in neovasculature, this might explain the heterogeneous uptake.
Conclusion
For patients with RAI-refractory DTC, 68Ga-PSMA PET/CT can be valuable for staging, as it is able to detect various types of lesions and may detect lesions which are not picked up by 18FDG PET/CT. Furthermore, 68Ga-PSMA PET/CT might be used to identify patients for treatment with 177Lu-PSMA-617. One of the two patients who underwent 177Lu-PSMA-617 therapy showed slight, temporary response. To draw conclusions on the effectiveness of this therapy, evaluation of more patients is needed.
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