Abstract
Introduction
3,4-Dihydroxy-6-[18F]-fluoro-l-phenylalanine (FDOPA) positron emission tomography (PET) is sensitive for identifying primary brain tumors. However, increased FDOPA uptake has been reported in pseudotumoral brain lesions. Our aim was to analyse FDOPA-PET in patients with pseudotumoral brain lesions and to compare them with patients with brain tumors.
Methods
We retrospectively analysed consecutively recruited patients with suspected primary brain tumor (based on clinical and magnetic resonance imaging findings) referred for FDOPA-PET in our centre between November 2013 and June 2019 (n = 74). FDOPA-PET parameters (maximum and mean lesion standardised uptake values [SUV] and ratios comparing lesion with different background uptake SUV) and thresholds were evaluated to determine which offered optimal discrimination between pseudotumoral and tumoral lesions.
Results
Overlapping PET values were observed between pseudotumoral (n = 26) and tumoral (n = 48) lesion, particularly for low-grade tumors. Based on receiver operating characteristic (ROC) analyses, the optimal PET parameters to discriminate pseudotumoral from tumoral lesions were SUVmax lesion/basal ganglia, SUVmax lesion/grey matter, SUVmean lesion/grey matter, and SUVmax lesion/mirror area in contralateral hemisphere (all ratios showing area under the curve [AUC] 0.85, 95% CI). The narrowest 95% sensitivity–95% specificity window was observed for SUVmax lesion/basal ganglia ratio, with ratio values of 0.79 and 1.35 corresponding to 95% sensitivity and 95% specificity, respectively.
Conclusion
FDOPA-PET uptake should be interpreted with caution in patients with suspected primary brain tumor, especially in patients showing low or intermediate SUV values and ratios.
Clinical Trial Registration-URL
https://www.clinicaltrials.gov. Unique identifier: NCT04306484
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Introduction
Amino acid tracers present several advantages over 18F-2-fluoro-2-deoxy-d-glucose for positron emission tomography (PET) imaging of brain tumors (especially in low-grade tumors due to the lower background uptake of amino acid tracers compared with18F-2-fluoro-2-deoxy-d-glucose). They are now considered as the tracers of choice for initial and progression diagnosis and for evaluation of treatment response [1]. Amino acid PET tracers include 11C-methyl-l-methionine (MET), O-(2-[18F]fluoroethyl)-l-tyrosine (FET), and 3,4-dihydroxy-6-[18F]-fluoro-l-phenylalanine (FDOPA). The uptake of radiolabelled amino acids is based on the expression of the Na+-independent large neutral amino acid transporters (LAT1 and LAT2) on the cell surface of tumor cells, which are relatively independent from blood–brain barrier permeability allowing these tracers to depict non contrast-enhancing brain tumor regions [2]. MET and FDOPA uptake is thought to be largely due to LAT1, while FET is transported by both LAT1 and LAT2. No relevant differences have been shown between available radiolabelled amino acids in terms of tumor to brain contrast, although differences exist concerning tracer biodistribution in the brain and the time-activity curves of tracer uptake [3,4,5]. In general, higher uptake is observed in patients with a high-grade tumor compared with those with a low-grade tumor, with the exception of oligodendroglioma which sometimes show higher uptake than high-grade astrocytomas, likely due to their increased cellular and vascular density in this glioma subtype [6,7,8,9,10,11,12]. FDOPA is a substrate for the enzyme aromatic amino acid decarboxylase in dopaminergic neurons, explaining the prominent physiological uptake by the basal ganglia (BG). Although amino acid PET shows high accuracy for the detection of brain tumors, increased uptake has been reported in numerous pseudotumoral brain lesions (including inflammatory, infectious, vascular, seizure-related, and brain developmental lesions).[8, 9, 13,14,15,16,17,18,19,20,21,22].
The largest amino acid PET study analysing pseudotumoral lesions used FET tracer. In that retrospective study of a large unselected patient population (n = 393), one-third of the 87 patients with a pseudotumoral lesion showed increased uptake reflecting the low specificity of 68% (but relatively high sensitivity of 87%) for brain tumor diagnosis, with uptake values in pseudotumoral lesions in the same range as low-grade brain tumors [9].
For FDOPA-PET, only case reports and small series of pseudotumoral lesions showing increased uptake have been reported [14,15,16, 19,20,21,22].
In studies reporting on amino acid PET in pseudotumoral and tumoral lesions, different PET parameters and standardised uptake value (SUV) cut-offs were used to determine the presence of increased uptake and so-called PET positivity. A minority of studies assessed optimal discriminating SUV thresholds (i.e. optimal combined sensitivity and specificity, or analyses favouring higher sensitivity or specificity).
Our aims were to compare FDOPA-PET performed in patients with pseudotumoral and (low- and high-grade) tumoral brain lesions, and to determine optimal PET parameters and thresholds to discriminate both lesion types.
Methods
Patient population
We retrospectively analysed consecutive patients referred for FDOPA-PET in our centre (Nîmes University Hospital, France) between November 2013 and June 2019 for suspected primary brain tumor based on clinical and magnetic resonance imaging (MRI) findings. Inclusion criteria were presence of defined tumor (histologically confirmed) or pseudotumor (diagnosed by histological or other analyses) diagnosis, clinical and MRI follow-up of > 24 months, and FDOPA-PET scan < 2 months before surgery or stereotactic biopsy (if performed).
We screened 184 FDOPA-PET scans performed in 166 different patients with suspected primary brain tumor. In patients with several FDOPA-PET scans performed, only the initial scan was taken into account. We excluded 75 tumor patients in whom FDOPA-PET was performed after initial surgery or biopsy. In addition, 17 patients were excluded who did not conform to the inclusion criteria (i.e. no definite tumor or pseudotumor diagnosis could be made or follow-up was < 24 months), resulting in 74 patients for analysis including 26 pseudotumor and 48 tumor patients. Flowchart of patient selection is shown in Fig. 1.
Patients with a tumoral lesion were classified according to the WHO 2016 grading system into low-grade (i.e. grade I and II glioma) or high-grade (i.e. grade III and IV glioma, or other high-grade non-glioma). Genetic analyses in search for isocitrate dehydrogenase mutation and 1p/19q co-deletion were performed in grade II and III gliomas and integrated in the WHO 2016 grading system used in our study. For patients with a pseudotumoral lesion, final diagnosis was based on histology, MRI, additional blood/cerebrospinal fluid, or follow-up analyses.
FDOPA-PET imaging and data analysis
PET-CT was performed on a GE Discovery 710 Elite system (GE Healthcare). Patients were asked to fast for at least 4 h before image acquisition. The patients were placed in supine position on the examination table, infused with a catheter, with head immobilized in a headrest. The imaging sequence started 6 min after intravenous administration of FDOPA (2 MBq/kg), with a scout view (90° angle of view, 120 kV, 30 mAs). CT scan was performed for attenuation correction (120 kV, 5mAs, pitch 0.531, slice thickness 3.75 mm, slice increment 3.27 mm, QAC filter, DFOV 25). Finally, the PET was acquired in static 3D mode for 20 min, 8 min after FDOPA injection (axial field of view 25, matrix 256 × 256). After ordered subset expectation maximization (OSEM) reconstruction using 6 iterations and 24 subsets, with attenuation, scattering and point-spread-function (PSF) correction, and 4 mm full width at half maximum (FWHM) of Gaussian filter, 47 joined axial sections of 3.26 mm were obtained.
FDOPA-PET/CT images were co-registered with MRI images, based on fluid-attenuated inversion recovery and gadolinium-enhanced T1 sequences using "Integrated Registration" software (GE Healthcare's). Using the PET-MRI fusion images, a volume of interest (VOI) was placed directly on the lesion in case of increased FDOPA uptake by checking for congruence with the signal abnormality on the MRI corresponding to the lesion. In absence of obvious FDOPA uptake, the VOI was positioned over the MRI signal abnormality and transposed to the FDOPA-PET. For lesion F-DOPA uptake, a threshold of 42% of the maximum was used. Background reference FDOPA uptake was assessed using VOIs positioned on the contralateral basal ganglia (BG), the contralateral hemispheric grey matter (i.e. a non-spherical VOI involving the cortical area showing the most intense F-DOPA uptake on axial slices), the contralateral hemispheric white matter (i.e. a spherical VOI placed in the centrum semiovale), and the homologous mirror brain area in the contralateral hemisphere. These FDOPA-PET analyses resulted in ten quantitative parameters used in our study: SUVmax and SUVmean of the lesion and eight lesion-to-background ratios (i.e. SUVmax lesion/SUVmax BG, SUVmax lesion/SUVmax grey matter, SUVmax lesion/SUVmax white matter, SUVmax lesion/SUVmax mirror area in contralateral hemisphere, SUVmean lesion/SUVmean BG, SUVmean lesion/SUVmean grey matter, SUVmean lesion/SUVmean white matter, SUVmean lesion/SUVmean mirror area in contralateral hemisphere).
Lesion size (maximum diameter; volume) of tumoral and pseudotumoral lesions were calculated based on the MRI, using both gadolinium-enhancement T1-weighted imaging and FLAIR sequence (especially for lesions or part of lesions lacking gadolinium-enhancement) and by excluding signal changes corresponding to perilesional oedema, performed preceding the PET scan.
Statistical analysis
The patients’ characteristics and SUV parameters were described according to the presence of tumoral or pseudotumoral brain lesion using frequency for categorical variables and median and interquartile range (IQR) for continuous variables. The performance of the different FDOPA-PET parameters for discriminating pseudotumoral from tumoral lesions, was analysed using receiver operating curve (ROC) analysis [23]. The area under the curve (AUC) value of each SUV parameter was compared to the AUC of the other SUV parameters using the nonparametric method described by DeLong et al. [24]. We applied three cut-offs for the SUV parameters with the best AUC: (1) the cut-off that maximized the Youden's J-index (sensitivity + specificity-1), (2) the best cut-off that maximized specificity (specificity > 95%), and the best cut-off that maximized sensitivity (sensitivity > 95%). Analyses were performed with a bilateral alpha level of 0.05 using SAS software, version 9.4 (SAS Institute, Cary, NC, USA).
Ethics approval was obtained according to local regulations.
Results
A total of 74 FDOPA-PET scans from 74 patients were analysed: 26 patients with pseudotumoral and 48 patients with tumoral brain lesion. Patient characteristics and FDOPA-PET data of the different groups are shown in Table 1. Age did not differ significantly between both tumoral and pseudotumoral patients (median 58.5 vs. 50.5 years, p = 0.16).
The 48 tumor patients included 8 low-grade (grade II glioma, n = 7; grade II ependymoma, n = 1), and 40 high-grade (grade III glioma, n = 12; grade IV glioma, n = 25, primary cerebral lymphoma, n = 1; medulloblastoma, n = 1, and metastatic cerebral breast cancer, n = 1) tumors. Histology was available for all tumor patients.
The pseudotumor group included patients with an inflammatory lesion (n = 11), lobar primary intracerebral haemorrhage (n = 3), cortical dysplasia (n = 3), infectious lesion (n = 2, both toxoplasmosis), cerebral cavernomatous malformation (n = 1), seronegative autoimmune limbic encephalitis (n = 1), deep venous sinus thrombosis-related oedema (n = 1), brain infarction (n = 1), chronic posttraumatic brain lesion (n = 1), radionecrosis after radiation therapy for arteriovenous malformation (n = 1), and mixed inflammatory/infectious lesion (n = 1). The 11 patients with an inflammatory lesion included patients with multiple sclerosis (n = 6), isolated inflammatory lesion (n = 3), solitary sclerosis (n = 1), and chronic lymphocytic inflammation with pontine perivascular enhancement responsive to steroids (CLIPPERS) (n = 1). Six pseudotumor patients had histological analysis (multiple sclerosis, n = 2; isolated inflammatory lesion, n = 2; and infectious lesion, n = 2). Demographic, diagnostic, histological, MRI and FDOPA-PET data of pseudotumoral patients are shown in Table 2.
Lesion diameter differed significantly between tumoral and pseudotumoral lesions (mean 39.3 mm vs. 27.1 mm, p = 0.0032), whereas lesion volume did not differed significantly (mean 27.8 cm3 vs. 17.9 cm3, p = 0.18). Tumoral and pseudotumoral patients included no and one patient with lesion diameter < 10 mm, and two and three patients with lesion diameter < 12 mm, respectively.
Using ROC analyses, SUVmax lesion/BG, SUVmax lesion/grey matter, SUVmean lesion/grey matter, and SUVmax lesion/mirror area in contralateral hemisphere ratios showed the highest AUC values (all AUC 0.85, 95% CI) for discriminating pseudotumoral from tumoral lesions (Fig. 2). Thresholds for optimal combined sensitivity/specificity, 95% sensitivity, and 95% specificity for SUVmax lesion/BG, SUVmax lesion/grey matter, SUVmean lesion/grey matter, and SUVmax lesion/mirror area in contralateral hemisphere ratios are shown in Table 3.
SUVmax lesion/basal ganglia ratio showed thresholds with the narrowest 95% sensitivity (SUVmax lesion/basal ganglia ratio value of 0.79) and 95% specificity (SUVmax lesion/basal ganglia ratio value of 1.35) window. Box-and-whisker diagrams for the SUVmax lesion/basal ganglia ratio values comparing the different groups and subgroups are shown in Fig. 3. Box-and-whisker diagrams for the three other parameters are shown in Supplemental Fig. 1. This SUVmax lesion/basal ganglia 0.79–1.35 window included 16 (33%) tumor patients and 13 (50%) pseudotumor patients. Two tumor patients showed a value of < 0.79 value (i.e. 0.67 in a grade IV astrocytoma, and 0.76 in a grade II glioma) and one pseudotumor patient showed a value of > 1.35 (i.e. 2.02 in a patient with radionecrosis after radiation therapy for arteriovenous malformation). The pseudotumor patients with a SUVmax lesion/basal ganglia ratio value between 1.00 (corresponding to the cut-off value often used in the literature to consider uptake as increased) and 1.35 (corresponding to the cut-off value associated with 95% specificity in our study) were: one patient with an infectious lesion (value of 1.01), three patients with an inflammatory lesion (two multiple sclerosis patients with values of 1.02 and 1.06, and one patient with an isolated inflammatory lesion with a value of 1.16), one patient with a mixed inflammatory/infectious lesion (value of 1.22), and one patient with a lobar cerebral amyloid angiopathy-related intracerebral haemorrhage (value of 1.34).
There was no statistical difference in lesion FDOPA-PET activity between pseudotumor patients with or without biopsy (p = 0.4 for SUVmax lesion/BG).
Discussion
SUVmax lesion/BG, SUVmax lesion/grey matter, SUVmean lesion/grey matter, and SUVmax lesion/mirror area in contralateral hemisphere ratios were the optimal parameters to best discriminate pseudotumoral from tumoral lesions with relatively high overlap in SUV values between both groups. Optimal discriminating thresholds depended on whether sensitivity or specificity was privileged. SUVmax lesion/basal ganglia showed the narrowest 95% sensitivity–95% specificity window, with one low-grade and one high-grade tumor showing SUVmax lesion/basal ganglia ratio values below the value corresponding to the 95% sensitivity cut-off and one patient with radionecrosis after radiation therapy for arteriovenous malformation above the value corresponding the 95% specificity cut off.
The patient with radionecrosis (with symptom onset related to intracranial hypertension four years after radiation therapy, and FDOPA-PET performed 2 years later) showed very high FDOPA uptake (SUVmax lesion/BG ratio value of 2.02). Earlier reports analysing FDOPA-PET use for differentiating progressive brain tumor from radionecrosis (after radiation therapy for brain tumor) showed relative high sensitivity (i.e. 81% and 90%) and specificity (i.e. 84% and 92%) [19, 20, 25]. In our patient, however, radiation therapy was given for arteriovenous malformation, in the absence of brain tumor.
In earlier reports, different amino acid PET tracers showed high sensitivity for detecting tumoral lesions and tumor recurrence, in contrast with only moderate specificity [9, 10]. Several of these studies reporting on sensitivity and specificity of amino acid PET tracers used a threshold SUV lesion/background ratio value of 1, probably favouring sensitivity due to the relative high proportion of slightly elevated uptake in pseudotumor patients [9, 19]. The non-specific increased uptake of pseudotumoral lesions is an important issue since aggressive diagnostic and therapeutic procedures (i.e. stereotactic biopsy or surgery) may be proposed in these pseudotumoral patients based on PET data only.
Amino acid PET uptake in tumoral lesions probably reflects both tumor and vascular cells of biologically active tumor tissue together with passive tracer influx due to enhanced blood–brain barrier permeability (since tracer accumulation is associated with contrast enhancement on MRI) [8]. Therefore, enhanced blood–brain barrier permeability may play a role in the increased tracer uptake sometimes observed in active contrast-enhancing pseudotumoral lesions. Amino acid tracer uptake has also been observed in brain areas showing reactive astrogliosis near gliomas, hematomas, infarction, inflammatory and infectious lesions [26,27,28,29,30,31]. In some of these reported lesions, increased LAT1/2 expression has been observed, probably explaining increased amino acid tracer uptake [29]. Increased LAT1/2 expression related to reactive astrogliosis may therefore also explain the increased uptake in some of these pseudotumoral, sometimes non-contrast-enhancing lesions.
In our study, all tumor patients had histology (required for inclusion), whereas less than one third of pseudotumor patients had histology, possibly creating a verification bias (i.e. PET results may have influenced the decision to biopsy or surgery) and study limitation.
Recently, reconstructed PET images using PSF correction has been shown to be non-quantitative for small lesions (< 10–12 mm), since recovery coefficients are non-monotonic as a function of lesion size, less reproducible, and more slowly converging [32]. This non-linearity may lead to a disproportionate increase of activity of small lesions [32]. Therefore, PSF correction was not recommended by the joint EANM/EANO/RANO practice guidelines/SNMMI procedure standards (published online at the end of 2018) for PET imaging of gliomas [33]. PET scans in our patients were performed between 2013 and 2019, with PSF correction in the vast majority of patients. This may have affected both tumor and reference region activity (and calculated cut-off levels) in our study patients. Therefore, cut-off levels may not be directly comparable to the values in the literature of studies using PET imaging without PSF correction. The effect of PET analysis with PSF correction in our study probably had only a minimal impact on the results since only a very small minority of patients presented with small lesions.
For FDOPA-PET, the BG is the background reference area most frequently used in the literature (and therefore also used in our study). However, since BG uptake is age dependent, uptake ratios (and the corresponding calculated cut-off values) using BG may have been impacted by the age of the included patients [34]. The age-dependant BG uptake was probably not a major study limitation since the age did not differed significantly between tumoral and pseudotumoral patients, and since similar PET results were observed when using other (i.e. than BG) reference areas in our study (although age-related uptake differences might not be excluded in those other areas neither).
Conclusion
FDOPA-PET uptake should be interpreted with caution in patients with suspected brain tumor based on clinical and brain imaging findings, especially in patients showing low or intermediate SUV values and ratios. FDOPA-PET lesion uptake must be interpreted taking into account all clinical, radiological, and biological data to decide if other complementary analyses are needed to determine the underlying pseudotumoral cause or if aggressive diagnostic and therapeutic procedures are required in case of brain tumor. FDOPA has to be compared with other amino acid tracers to identify the PET tracer yielding optimal discriminating properties for tumoral and pseudotumoral lesions.
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Acknowledgements
We would like to thank Dr. Sarah Kabani (Service de Biostatistique, Epidémiologie Clinique, Santé Publique et Innovation en Méthodologie (BESPIM), CHU de Nîmes, 4 Rue du Professeur Debré, 30029 Nîmes Cedex 09) for proofreading our manuscript.
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415_2020_10269_MOESM1_ESM.jpg
Supplementary Figure 1 Box-and-whisker diagrams presented as medians and interquartile ranges of lesion/GM max, lesion/GM mean, and lesion/mirror area max by comparing pseudotumor vs. tumor, pseudotumor vs. low-grade tumor vs. high-grade tumor, and pseudotumor vs. grade II glioma vs. grade III glioma vs. grade IV glioma vs. other high-grade tumor (JPG 3667 kb)
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Renard, D., Collombier, L., Laurent-Chabalier, S. et al. 18F-FDOPA-PET in pseudotumoral brain lesions. J Neurol 268, 1266–1275 (2021). https://doi.org/10.1007/s00415-020-10269-9
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DOI: https://doi.org/10.1007/s00415-020-10269-9