Abstract
Biliary-tract-carcinomas (BTC), pancreatic-ductal-adenocarcinomas (PDAC) and adenoidcystic-carcinomas (AC) have in common that they are traditionally treated with large clinical-target-volumes (CTV). The aim of this study is to examine the impact of pretreatment-[68Ga]FAPI-PET/CT on target-volume-definition and posttreatment-[68Ga]FAPI-PET/CT-response-assessment for BTC-, PDAC- and AC-patients referred to radiation-therapy. All consecutive BTC-, PDAC-, and AC-patients who received pretreatment-[68Ga]FAPI-PET/CT±[18F]FDG-PET/CT were included from 01.01.2020 to 01.03.2022. MTV and SUVmax were separately generated based on [68Ga]FAPI- and [18F]FDG-PET/CT-images. A [68Ga]FAPI- and [18F]FDG-based-CTV was defined. Treatment-plans were compared. Treatment-response was reassessed by a second [68Ga]FAPI-PET/CT and [18F]FDG-PET/CT after treatment-completion. Intermodality comparison of lesion-to-background-ratios [SUVmax_lesion/SUVmean_background] for individual timepoints t1 and t2 revealed significant higher values for [68Ga]FAPI compared to [18F]FDG (t1, p = 0.008; t2, p = 0.005). Intermodality comparison of radiation-therapy-plans showed that [68Ga]FAPI-based planning resulted in D100% = 97.2% and V95% = 98.8% for the [18F]FDG-MTV. [18F]FDG-based-planning resulted in D100% = 35.9% and V95% = 78.1% for [68Ga]FAPI-MTV. [18F]FDG-based-planning resulted only in 2 patients in V95% > 95% for [68Ga]FAPI-MTV, and in 1 patient in D100% > 97% for [68Ga]FAPI-MTV. GTV-coverage in terms of V95% was 76.4% by [18F]FDG-based-planning and 99.5% by [68Ga]FAPI-based-planning. Pretreatment [68Ga]FAPI-PET/CT enhances radiation-treatment-planning in this particular group of patients. While perilesional and tumoral follow-up [18F]FDG-uptake behaved uniformly, perilesional and tumoral reaction may differ in follow-up [68Ga]FAPI-imaging. Complementary [68Ga]FAPI- and [18F]FDG-imaging enhance treatment-response-assessment.
Similar content being viewed by others
Introduction
For curative-intent radiotherapy high-end multimodal imaging is crucial for precision therapy. High-end imaging allows delivering highly conformal doses to the tumor by, at the same time, minimizing radiation dose to healthy tissue. Nowadays, target volume delineation based on PET/CT-images has become reference standard in radiotherapy planning for many tumor entities, entering into national and international guidelines from brain, thoracic to pelvic malignancies. In a prospective multicentre trial, 2-deoxy-2-[18F]fluoro-d-glucose ([18F]FDG) [18F]FDG-PET/CT altered treatment management in ~ 72% of patients with lung cancer, in 85% of patients with pancreatic ductal adenocarcinomas and 78% of patients with cancer of unknown origin1. The mean adaptation rate of radiotherapy treatment plans based on [18F]FDG-PET was 55.4% (range 44.0–69.2%), with major treatment plan modifications made in 43.3–68.2% of cases1. Typically the gross tumor volume (GTV) comprises PET-positive lesions that will be expanded to the clinical target volume (CTV) by 5–8 mm margins with respect of anatomic boundaries2,3. Complementary functional and morphological changes allow an accurate non-invasive assessment of disease spread and activity. Multimodality staging by EBUS-TBNA and PET-imaging allowed the identification of frequent patterns of lymphogenic metastatic spread in non-small lung cancer4. Furthermore, early phase-II-trials were conducted to examine the value of interim [18F]FDG-PET/CT-imaging for delineation of residual metabolic target volumes in patients with locally advanced non-small cell lung cancer5,6. These randomized trials were promising, allowing for improved local tumor control by focused radiation dose escalation targeted to the residual [18F]FDG-avid tumor5,6. However, the corresponding subsequent randomized trial yielded no confirmatory results7.
Metabolic shrinkage may be greater than plain anatomic changes5. Thus, it can represent a valid prognostic parameter of interim [18F]FDG-PET/CT-imaging as supported by a large retrospective study examining post-induction chemotherapy, interim PET-parameters8. Interim [18F]FDG-PET/CT-imaging is reported to have a significant progonstic impact and to represent a valuable tool for guiding individualized treatment intensification8.
For a long time [18F]FDG-PET/CT was the most widely used application of molecular imaging for initial tumor staging and restaging. However, now, more and more studies predict the end of the hegemony of [18F]FDG-PET/CT9. Randomized prospective, phase-III trials have been designed to determine, whether PSMA-PET/CT-imaging can improve outcomes in patients with prostate cancer10, combined [18F]FDG- and [68Ga]DOTATATE PET/CT for noninvasive assessment of tumor heterogeneity in G2 and G3 NETs11, MET-PET reported a useful modality for the diagnosis of radiation-induced changes in brain metastases with SUVmax12 or MET-PET and random-forest based analysis for outcome prediction of patients with brain tumors and for differentiating recurrent brain tumor from radiation necrosis13 are only a few of a whole series of studies building the architecture of diagnostic prospects.
Recent developments bring the fibroblast activation protein (FAP) inhibitor (FAPI) as PET tracer in oncology forward. [68Ga]FAPI represents a novel radiopharmacon that may be used as diagnostic or therapeutic target. The FAP-specific enzyme inhibitor (FAPI) binds to FAP by blocking its chemical reaction. FAP represents a transmembrane glycoprotein expressed on cancer-associated fibroblasts (CAFs) of several tumor entities14. These non-neoplastic cells modulate the tumor microenvironment and the extracellular matrix15. They are reported to modify tumor progression and therapeutic response. [68Ga]FAPI is reported to concentrate in tumours at a high proportion, whereas it is quickly hived off in normal tissue16 and organs at risk. Particularly, in tumor entities of the head and neck, which are in close vicinity to the nasal sinus, Waldeyer's tonsillar ring or in the region of the upper abdomen such as close to the liver and biliary tract, viz. close to normal tissues with a high physiological [18F]FDG-uptake, target delineation may be challenging17,18. At the same time biliary-tract-carcinomas (BTC), pancreatic-ductal-adenocarcinomas (PDAC) and adenoidcystic-carcinomas (AC) have in common that they are traditionally treated with large clinical-target-volumes. There exists a strong need for a better tumor, and at the same time better target delineation on imaging. Therefore, the present study focusses on the value of [68Ga]FAPI for target delineation and radiation therapy planning of adenoidcystic carcinomas, pancreatic ductal adenocarcinomas (PDAC), and biliary tract cancer.
In adenoidcystic carcinomas, because of the spread along the nerve sheaths, large CTV safety margins are used in radiotherapy to prevent local recurrence. A more sensitive detection of tumor spread along these routes is desirable to individualize, reduce the target volumes and thus allow a higher dose19. In a study of 12 patients with adenoidcystic carcinoma the clinical potential for staging and radiotherapy planning was assessed by means of [68Ga]FAPI-PET/CT20. The authors conclude that [68Ga]FAPI represents a promising imaging modality for adenoidcystic carcinoma, improving the precision of staging and radiotherapy planning compared to CT and MRI20.
For pancreatic ductal adenocarcinomas (PDAC) conventionally fractionated radiotherapy with concurrent chemotherapy using elective nodal irradiation either in the neoadjuvant or adjuvant setting was largely unsuccessful in terms of improving survival21,22. Stereotactic radiotherapy is evolving for locally advanced PDAC, but with small margins a precise determination of tumor spread is mandatory23,24. For biliary tract cancer only phase-II-trials are available, that used large target volumes25.
The SUVmax of [18F]FDG PET/CT is reported to aid differential diagnosis of solitary pancreatic lesions and also in the prediction of proliferative activity of pancreatic cancer26. However, while for many malignant tumors [18F]FDG-uptake correlated with cancer proliferation, for PDAC this correlation remains controversial27. According to a study examining the metabolic landscape of patients with advanced biliary tract cancer lesions, a high SUVmax uptake was associated with a poorer differentiated histology than of those with a low SUVmax uptake28. Likewise, the authors identified SUVmax as a prognostic factor for overall and progression-free survival in biliary tract cancer28. Quite the reverse, accurate delineation of lesions with a low or moderate proliferation may be difficult due to a poor [18F]FDG-uptake.
The aim of the present study is to examine the impact of pre- and posttreatment [68Ga]FAPI-PET/CT on radiotherapy target volume definition and response assessment for patients with adenoidcystic carcinoma, PDAC and biliary tract cancer referred to radiation therapy. Furthermore, the role of [68Ga]FAPI-PET/CT and [18F]FDG-PET/CT in radiation treatment shall be identified and discussed in this specific, for imaging and precise treatment planning challenging, tumor entities.
Methods
Patient cohort
All consecutive patients with PDAC, biliary tract and adenoidcystic carcinoma who were introduced to the department of radiation therapy were reviewed for study purposes in the time period from 01.01.2020 to 01.10.2021. For study examination those patients who received a [68Ga]FAPI-PET/CT prior to radiation therapy admission were included (Consort diagram Fig. 1). [68Ga]FAPI-PET/CT was performed for clinical purposes such as high risk situations, challenging tumor delineation on conventional imaging and the necessity for assessment of complete tumor extension prior to radiation therapy. Patients were enrolled in a prospective observational trial conducted at University Hospital Essen (NCT04571086), which was approved by the local ethics committee of University Hospital Essen (19-8991-BO). Patients gave written informed consent for inclusion. Patients gave written informed consent for anonymized analysis of the data. All research was performed in accordance with relevant guidelines/regulations and in accordance with the Declaration of Helsinki.
Pretreatment imaging and data processing
All included patients were introduced to the Department of Radiation Therapy and received a pretreatment [68Ga]FAPI-PET/CT prior to or at time of admission to radiation therapy. Some patients underwent sequential [68Ga]FAPI-PET/CT and [18F]FDG-PET/CT on the same day or within a narrow time interval prior to treatment planning after patient consent. All examinations were performed on the PET/CT scanner Biograph mCT or Biograph mCT VISION (Siemens Healthineers, Erlangen, Germany). PET acquisition and reconstruction was completed by ordered subset expectation maximization (OSEM) based algorithms. For post-reconstruction filtering a Gaussian filter kernel with a full width at half maximum of 4 mm was applied. Data collected on the PET/CT system were reconstructed with a pixel spacing of 1.65 × 1.65 × 3 and rows and columns of 400 × 400. PET image reconstructions were performed by modeling of resolution degrading phenomena, viz. point-spread function (PSF) reconstruction. Attenuation correction was achieved either by low dose or contrast enhanced, diagnostic computed tomography. Furthermore, the diagnostic CT-component served for morphological correlation. All patients who in interdisciplinary consensus and after radiation therapy specialist assessment were scheduled for radiation therapy underwent a treatment planning simulation. Patients received a planning CT of the area being treated with or without contrast-agent, iterative reconstruction and automatic dose modulation.
Lesion and background definition
The bio-distribution of [68Ga]FAPI- and [18F]FDG was determined in terms of metabolic tumor volumes (MTV) and maximum standardized uptake values (SUVmax). SUVmax was determined by a region grow algorithm for the index lesion. Time interval between examinations of patients who received both, a [68Ga]FAPI- and [18F]FDG-examination, was in mean 5.3 days (median 0 days, range 0–35 days) without treatment changes in-between. In a second step the MTV and SUVmax were separately generated on the basis of [68Ga]FAPI- and [18F]FDG-PET/CT-images. By means of the SUVmax thresholding tool implemented in the treatment planning software ECLIPSE with a standardized threshold of 40% and supervised adaptation the index lesion was measured with respect to the planned radiation treatment.
Physiological tracer activity distribution and the surrounding background uptake was examined for all index lesions by determining SUVmax and SUVmean in a hollow sphere in 5–15 mm perilesional distance (Fig. 2).
Additionally, to consider the background activity concentration in the segmentation of the MTVBackground the respective threshold was calculated as described previously29:
whereby SUVmaxTB = SUVmaxTumor − SUVmaxBackground.
Treatment planning
All available pretreatment PET/CT-images were imported to the treatment planning system ECLIPSE (Varian, Palo Alto, USA). Each [68Ga]FAPI- and [18F]FDG-PET/CT study was reviewed prior to target definition and fused with the standardized treatment planning CT by means of the treatment planning system ECLIPSE. Rigid and deformable image registration was used to fuse the planning CT with the pretreatment [68Ga]FAPI- and/or [18F]FDG PET/CT. The gross tumor volume (GTV) was defined on the planning CT. The clinical target volume (CTV) was delineated according to respective guidelines in order to encompass possible microscopic tumor extension and to consider residual deformations. In general, a CTV expansion of 5 mm or up to a nearer anatomic border was conducted. The planning target volume (PTV) was determined with 5 mm around the CTV to take potential set-up errors into account. Moreover, to control normal tissue complications all organs at risks were defined on the planning CT with restriction of hot spots outside sensitive areas. A separate clinical [68Ga]FAPI- and additional [18F]FDG-based PTV was defined. For all except of one patient the [18F]FDG-based PTV was generated by a 10-mm margin around the MTV with regard to organs at risk and used to develop the 3-dimensional conformal VMAT radiation therapy plan. In one patient who underwent stereotactic lymph node treatment the [18F]FDG-based PTV was generated by a 5-mm margin around the MTV with regard to organs at risk. The two treatment plans for each patient were compared with respect to target volume coverage (GTV, [68Ga]FAPI- and [18F]FDG-MTV).
For tumors in the upper abdomen radiation therapy was planned in plain free breathing delivered during the exhalation phase with gating-windows of 50% of the breathing cycle. By means of a Respiratory Gating System device (RPM) the exact respiration phase was monitored. The minimum dose to the 98% of the target volumes containing the ordered highest dose bins was required to be as at least 95% of the prescribed dose. The Acuros XB algorithm was used to generate either volumetric modulated arc therapy (VMAT) or static-field intensity modulated radiotherapy (IMRT) plans. Patients received radiation therapy once daily with a fractionation dose of 5 × 1.8–3 Gy/w (q.e.d.) at the linear accelerator TrueBeam (Varian, Palo Alto, USA). In case of stereotactic radiation therapy higher fraction doses were applied (3.5 Gy/F). Daily image guidance (IGRT) was an integral part of every radiation therapy sequence and ensured a precise treatment delivery. Online target matching was accomplished with the help of the 6-degrees of freedom table available in the linear accelerator TrueBeam (Varian, Palo Alto, USA).
Post-radiation imaging
Treatment response was reassessed in terms of lesion-to-background ratios [SUVmaxTumor/SUVmeanBackground] by the second and/or third [68Ga]FAPI-PET/CT and [18F]FDG-PET/CT at timepoints t2 and t3 following t1 after treatment completion where available (Diagnostic and treatment timeline highlighted by Fig. 3). Absolute ΔSUVmaxTumor and ΔSUVmaxBackground were examined in dependence of time from radiation therapy start to follow-up imaging. Additionally, to evaluate the impact of the response of perilesional background the background reaction was determined in terms of absolute and percentage lesion-to-background difference ΔSUVmaxTB [SUVmaxTumor − SUVmaxBackground] and %ΔSUVmaxTB [%SUVmaxTumor − %SUVmaxBackground] at timepoints t2 and t3 following t1 after treatment.
Statistical analysis, primary and secondary endpoints
The primary endpoint is to examine the impact of [68Ga]FAPI-PET/CT diagnostics on target volume definition prior to radiation therapy and coverage of morphological GTV by [68Ga]FAPI- and [18F]FDG-PTV based planning. Secondary endpoints represent the assessment of intermodality differences between [68Ga]FAPI- and [18F]FDG PET/CT for target volume definition, for radiation therapy planning and for assessment of post-radiation treatment response.
Intermodality comparison between [68Ga]FAPI- and [18F]FDG-PTV based planning was examined in terms of D100%, MTV, as well as perilesional SUVmax, SUVmean and lesion-to-background ratios [SUVmax_lesion/SUVmean_background] for individual timepoints t1 and t2 by using non-parametric paired t-tests (Wilcoxon signed rank test). Kruskal Wallis test was applied to examine lesion-to-background ratios of the three tumor entities. To test for consistent differences between the percentage change of [68Ga]FAPI- and [18F]FDG-uptake from timepoint t1 to t2 the sign-test was used. All descriptive and statistical analyses were performed using IBM SPSS Statistics version 27 (IBM Corp., Armonk, New York, USA).
Results
Altogether 41 patients with PDAC (n = 14), biliary tract (n = 24) and adenoidcystic carcinoma (n = 3) were introduced to the department of radiation therapy in the time period from 01.01.2020 to 01.03.2022 (Fig. 1). In total, 14/41 patients (34.1%) received a [68Ga]FAPI-PET/CT-examination for clinical purposes prior to radiation therapy after patient consent, 9/41 patients (21.9%) underwent a [18F]FDG PET/CT on the same day or within a narrow time interval prior to treatment planning. Median time of [68Ga]FAPI-PET/CT prior to radiation therapy initiation was 34 days (mean 28.9, range 4–78 days). Overall 11/14 patients who received a [68Ga]FAPI-PET/CT-examination underwent a radiation therapy at the department of radiation therapy introduced. One patient underwent radiation therapy at a different site with carbon ions instead of photons. 2/14 patients underwent no radiation therapy due to different reasons, one patient due to newly diagnosed peritoneal carcinomatosis, the other due to a secondary re-resection with sufficient surgical margins. 9/11 patients who underwent radiation therapy, and 10/14 considering all patients, received a 2nd [68Ga]FAPI-PET/CT. 10/11 patients who underwent radiation therapy, and 11/14 patients considering all patients referred to the Department of Radiation Therapy, received a follow-up [18F]FDG-examination (Fig. 1). 2 patients underwent a 3rd [68Ga]FAPI-PET/CT and 3 patients a 3rd follow-up [18F]FDG-examination. The median activity of the pretreatment [68Ga]FAPI-PET/CT was 95 MBq (mean injected 107 MBq, range 52–177) with images acquired in mean 21 min (range 10–61 min) post-injection. The median activity of the pretreatment [18F]FDG was 307 MBq (mean injected 286 MBq, range 101–431), with images acquired in mean 67 min (range 51–91 min) post injection. The median activity of the follow-up [68Ga]FAPI-PET/CT was 94 MBq (mean injected 92 MBq, range 80–101) with images acquired in mean 28 min (range 10–68 min) post-injection. The median activity of the follow-up [18F]FDG was 289 MBq. (mean injected 297 MBq, range 227–440), with images acquired in mean 71 min (range 54–90 min) post injection. Table 1 summarizes patient characteristics A–N (Table 1 and Supplementary Table 1).
The [68Ga]FAPI-PET/CT-findings altered the radiation therapy volume in 7/8 examined patients (87.5%) in comparison to the [18F]FDG-PET MTV, considering the 8 patients de facto treated at this institution’s department of radiation therapy, who received both, an initial [18F]FDG-PET and [68Ga]FAPI-PET for treatment planning. With regard to the MTV as the basis for treatment planning, [68Ga]FAPI-based MTV was significantly larger compared to [18F]FDG-based MTV (p = 0.008). Tumor lesions were detected by [68Ga]FAPI-PET in all 14 patients. On the contrary, on [18F]FDG-PET in 2 patient with histopathologically confirmed PDAC [18F]FDG-uptake was minimal and only slightly elevated compared to background noise (Fig. 4).
[68Ga]FAPI-PET detected two additional patients with suspected liver metastases, whereas one turned out to be unspecific tracer-uptake in the follow-up imaging. At the same time [18F]FDG-PET detected one additional patient with suspected liver metastases, which turned out to be unspecific tracer-uptake in the follow-up imaging. Intermodality comparison of lesion-to-background ratios in terms of [SUVmax_lesion/SUVmean_background] for individual timepoints t1 and t2 revealed significant differences between [18F]FDG and [68Ga]FAPI (Wilcoxon-test at timepoint t1, p = 0.008; at timepoint t2, p = 0.005). At timepoint t1, mean [68Ga]FAPI lesion-to-background ratio was 11.2 (median 8.5, IQR 7.5–15.2, range 5.7–21.8) and thus, significantly higher than mean [18F]FDG lesion-to-background ratio of 4.4 (median 4.1, IQR 3.1–5.8, range 1.9–7.8). The same relation becomes evident for timepoint t2, where mean [68Ga]FAPI lesion-to-background ratio was 17.1 (median 12.3, IQR 9.7–25.6, range 6.7–35.9) and significantly higher than mean [18F]FDG lesion-to-background ratio of 2.5 (median 2.6, IQR 1.6–3.3, range 0.6–3.8). Comparing the three tumor entities no difference was found considering [68Ga]FAPI lesion-to-background ratios (p = 0.970, Kruskal Wallis test) or considering [18F]FDG lesion-to-background ratios (p = 0.741, Kruskal Wallis test) in this limited size series.
Additionally, to consider the background activity concentration in the segmentation of the MTVBackground the respective threshold was calculated as described by27. According to this formula at timepoint t1 mean [68Ga]FAPI-MTVBackground over background was 7.5 (median 7.2, IQR 5.5–8.4, range 4.8–12.0) and thus, likewise, significantly higher than mean [18F]FDG-MTVBackground over background of 5.2 (median 4.6, IQR 4.2–6.5, range 4.2–6.6) (Wilcoxon-test at timepoint t1, p = 0.038). Intermodality comparison of radiation therapy plans showed that [68Ga]FAPI-based planning resulted in a [18F]FDG MTV target volume dose coverage, characterized by mean D100% values of 97.2% and mean V95% values of 98.8% for [18F]FDG MTV. While [18F]FDG-based planning resulted in mean D100% of 35.9% and V95% of 78.1% for [68Ga]FAPI MTV. The D100% or V95% using [68Ga]FAPI-based planning were significantly higher than the respective values using [18F]FDG-based planning and reading out the coverage of the MTV (p < 0.012 and p < 0.018, Wilcoxon test). [18F]FDG-based planning resulted only in 2 patients in V95% above 95% for [68Ga]FAPI MTV, and in 1 patients in D100% above 97% for [68Ga]FAPI MTV. Plain morphologically delineated GTV coverage was 76.4% by the [18F]FDG-based planning and 99.5% by the [68Ga]FAPI-based planning in terms of V95%.
Altogether 10/14 patients underwent a second [68Ga]FAPI-PET/CT and 11/14 patients a second [18F]FDG-PET/CT at timepoint t2 with mean 50.3 days (range 26–78) from end of radiation therapy to 2nd [68Ga]FAPI-follow-up imaging considering those undergoing radiation therapy and 374 days considering the one patient receiving 2nd [68Ga]FAPI-follow-up imaging from 1st [68Ga]FAPI-PET/CT without radiation therapy. 2 patients underwent a third [68Ga]FAPI-PET/CT and 3 patients a third [18F]FDG-PET/CT at timepoint t3 (mean 111 days, range 103–119 from end of radiation therapy to 3rd [68Ga]FAPI-follow-up imaging).
In 7/9 patients who received radiotherapy SUVmax of the index lesion declined on follow-up [68Ga]FAPI-PET/CT-imaging for more than 40% (mean decline 57.6%, range 41.4–74.8%), PERCIST-criteria suggest 30% cut-off. In 2/9 patients who received radiotherapy and a follow-up [68Ga]FAPI-PET/CT SUVmax increased for more than 20% (Fig. 5a). In both, there was a mismatch of SUVmax uptake between [68Ga]FAPI- and [18F]FDG-PET/CT. In one of these two patients (patient E) the size of the index lesion was regressive and central necrotic at follow-up of 6 months on MRI, on second and third follow-up [18F]FDG-PET/CT, which is considered as treatment response. Thus, in this case [68Ga]FAPI-increase did not indicate tumor progression, but a fibroblastic tissue response after ablative radiation therapy up to 50 Gy at 2.5 Gy/F. On the other hand, the other of the two patients (patient F), with [68Ga]FAPI-uptake increase for more than 90% at timepoint t2, developed a fulminant peritoneal carcinomatosis. Likewise, analyzing treatment response in those patients who underwent radiation therapy showed that [68Ga]FAPI MTV decreased from timepoint t1 to t2 to t3 in most patients (7/9), except of the afore mentioned 2. Analyzing treatment response with [18F]FDG revealed that [18F]FDG-SUVmax and MTV also decayed from t1 to t2 to t3. In all patients (n = 7) who received a pre- and posttreatment [18F]FDG-PET/CT as well as radiotherapy, SUVmax of the index lesion decreased by a mean of 33% on follow-up [18F]FDG-PET/CT-imaging (Fig. 5b).
Additionally, to further examine the impact of the perilesional background on [68Ga]FAPI uptake, the lesion-to-background difference was assessed in terms of %ΔSUVmaxTB, the difference values of [SUVmaxTumor − SUVmaxBackground] at timepoints t2 following t1 after treatment. With baseline SUVmaxTumor at timepoint t1 being 100%, the lesion-to-background difference %ΔSUVmaxTB increased for 14.5% in the respective patient F who developed a peritoneal carcinomatosis. In the only patient (patient I) with follow-up imaging who received no radiotherapy, SUVmax increased for 38.5% and lesion-to-background ratios remained stable on follow-up [68Ga]FAPI-PET/CT (Fig. 5a).
In all patients receiving follow-up imaging the mean change of tumoral [68Ga]FAPI-uptake from timepoint t1 to t2 was − 14.7% (median − 34.7%, IQR − 49.4% to + 25.5%). Mean change of background [68Ga]FAPI-uptake from timepoint t1 to t2 was + 31.3% (median + 39.7%, IQR − 4.4% to + 54.0%). Mean change of tumoral [18F]FDG-uptake from timepoint t1 to t2 was − 32.5% (median − 38.7%, IQR − 51.0% to + 10.8%). Mean change of background [18F]FDG-uptake from timepoint t1 to t2 was − 3.7% (median − 11.4%, IQR − 27.0% to + 22.8%). To test for consistent differences between the percentage change of [68Ga]FAPI- and [18F]FDG-uptake from timepoint t1 to t2 the sign-test was used. While tumoral percentage change showed no significant difference between [68Ga]FAPI- and [18F]FDG-images (p = 1.0, two-sided Exact sign-test), background percentage change from t1 to t2 was significantly different between [68Ga]FAPI- and [18F]FDG-images (p = 0.016, two-sided Exact sign-test). This relation remained the same, when excluding the patient who underwent follow-up, but did not receive radiation therapy (tumoral percentage change p = 1.0, two-sided Exact sign-test; background percentage change p = 0.016, two-sided Exact sign-test). In patients with treatment response there was an apparent relation in tumor and background reaction, whereas absolute perilesional [68Ga]FAPI-uptake difference increased (p = 0.053, two-sided linear regression analysis), absolute tumoral [68Ga]FAPI-uptake difference decreased from radiation therapy start to follow-up [68Ga]FAPI-imaging (p = 0.09, two-sided linear regression analysis) (timepoint t1 to t2, Fig. 6a,b) indicating a time trend (Fig. 6a,b).
Interestingly, SUVmax (Wilcoxon-test, p = 0.037) and SUVmean (Wilcoxon-test, p = 0.012) of perilesional background on [68Ga]FAPI-PET/CT-images significantly increased for all patients receiving follow-up [68Ga]FAPI-PET/CT from timepoint t1 to t2, except for one, with mean values depicted in Table 2. Meanwhile SUVmax (Wilcoxon-test, p = 0.499) and SUVmean (Wilcoxon-test, p = 0.670) of perilesional background on [18F]FDG-PET/CT-images remained stable or slightly decreased without significant changes from timepoint t1 to t2 (Table 2).
Discussion
The primary aim of the present study was to examine the impact of pretreatment [68Ga]FAPI-PET/CT on target volume definition for patients with biliary tract, pancreatic ductal adenocarcinomas (PDAC) and adenoidcystic malignancies presented to radiation therapy. Our results reveal that [68Ga]FAPI-based planning was feasible covering both, plain macroscopic gross tumor volume and [18F]FDG-volume, while [18F]FDG-based planning did not entirely cover [68Ga]FAPI-volume. Lesions were considerably larger and better contrasted with higher lesion-to-background ratios within [68Ga]FAPI-images compared to [18F]FDG-images. But larger MTVs do not automatically mean larger PTVs or higher toxicities30. In a multicentre, open-label, randomised, controlled [18F]FDG-PET/CT trial examining patients with locally advanced non-small-cell lung cancer, the median gross tumor volume was indeed higher in the [18F]FDG PET-based target group compared to the conventional target group; however, there was no significant difference in the median planning target volume (p = 0.180)30. If the detection is more sensitive, then the elective CTV volume, also concerning the lymph node stations, can potentially be reduced.
In line with previous studies16 we observed that [68Ga]FAPI provided high-contrast images. Particularly in tumor entities, which showed a low or absent [18F]FDG-uptake, [68Ga]FAPI enhanced target definition for radiation therapy planning. The present results confirm findings of preceding studies identifying [68Ga]FAPI as an important diagnostic tool for a range of cancer types31,32. A recent study on [68Ga]Ga-DOTA-FAPI-04 PET/CT showed a superior detection efficacy of [68Ga]Ga-DOTA-FAPI-04 PET/CT for detecting various primary and metastatic lesions compared to [18F]FDG PET/CT32. Significantly higher SUVmax uptake values are reported for stomach, liver and pancreatic duct adenocarcinoma compared to [18F]FDG PET/CT32.
Contrary to [18F]FDG which detects pathologies with enhanced glycolysis, [68Ga]FAPI uses other cancer and specific cell-surface targets. It binds to tumor associated fibroblasts rather than to normal adjacent tissue, where it is rapidly degraded. As FAP is a transmembrane glycoprotein on cancer-associated fibroblasts (CAFs) of several tumor entities13, it is probable that radiation treatment planning for a wider range of cancer types may profit31,33. Furthermore, some authors claim that the high, rather selective uptake and excellent image contrast on [68Ga]FAPI PET/CT may allow new applications for noninvasive lesion characterization, staging examinations, or radioligand therapies26. Likewise, Chen et al. report in a study of 59 cancer patients, that 22 patients presented with inconclusive [18F]FDG-PET findings34, while 86.4% (19/22) of these inconclusive lesions, primarily from liver cancer (6/19, 31.6%) and gastric cancer (5/19, 26.3%), showed high [68Ga]FAPI-uptake34. However, other authors argument that [68Ga]FAPI is not more tumor-specific than [18F]FDG, but that it is more sensitive to certain kinds of inflammations, like pancreatic lesions with characteristic storiform fibrosis and IgG4-related disease35. It must not be neglected that [68Ga]FAPI as other radiopharmacons, may be prone to unspecific tracer uptake36. It is reported that degenerative lesions, muscle, head-and-neck, scarring, mammary glands or uterus may show an increased tracer uptake36. According to Chen et al. in the lesion-based analysis sensitivity, specificity, positive predictive value, and negative predictive value of [68Ga]-DOTA-FAPI-04 PET/CT for the diagnosis of suspicious lesions, which were inconclusive on [18F]FDG-PET, were 94.5%, 58.2%, 84.0%, and 82.1%, respectively34. The false-positive findings were attributed to inflammatory-induced fibrosis34. Particularly posttreatment scarring and fibrotic tissues after surgery may represent a challenge for radiation therapy planning. Thus, precise knowledge of surgical operations and maneuvers remains crucial for optimal treatment planning, which may not be replaced by mere PET-imaging demanding morphological information from the CT- or MRI-component.
A second aim of the present study was the evaluation of the post-radiation treatment [68Ga]FAPI-PET/CT for response assessment. First in 1999 the European Organization for Research and Treatment of Cancer (EORTC) recommended response criteria for solid tumors based on PET-imaging37. These criteria are dedicated to [18F]FDG, but the translation to other radiopharmacons seems reasonable. A complete metabolic response on [18F]FDG is defined in cases, where tumor lesions are no longer detectable in contrast to the background uptake. Progressive metabolic disease is defined as an increase in SUVmax of ≥ 25% compared to the pretreatment PET-imaging, while a partial metabolic response is defined as SUVmax-decline for 15–25% or more than 25% after one or more cycles of chemotherapy31. Moreover, the EORTC first proposed PET/CT for treatment response assessment after immunotherapy38. PERCIST 1.0 criteria turned out to be important in evaluating response to novel cancer therapies that stabilize disease39. Additionally, volumetric parameters reported on interim [18F]FDG-PET/CT-imaging are identified as valid prognostic factors5,6,7. Though, as discussed above it is known that both, [68Ga]FAPI- and [18F]FDG-imaging may result in false positive and false negative results, in the present study combined posttreatment tumoral [68Ga]FAPI- and [18F]FDG-uptake after treatment completion showed a continuous decrease in SUVmax in all but 2 patients after radiation therapy helping to determine treatment response (Fig. 7). In the two patients there was a mismatch of SUVmax uptake between [68Ga]FAPI- and [18F]FDG-PET/CT. One of these two patients had a treatment response with regressive and central necrotic index lesion at follow-up of 6 months, thus, in this case [68Ga]FAPI-increase indicates a fibroblastic tissue response after ablative radiation therapy up to 50 Gy at 2.5 Gy/F. On the other hand, the other patient with [68Ga]FAPI-uptake increase for more than 90% at timepoint t2, developed a fulminant peritoneal carcinomatosis. In the one patient who received no radiation therapy and who underwent [68Ga]FAPI-follow-up imaging, SUVmax of the index lesion increased for more than 38%. When assessing treatment response with [68Ga]FAPI-imaging, it is crucial to discuss perilesional background reaction. Our results indicate that posttreatment the tumoral [68Ga]FAPI-uptake and perilesional background [68Ga]FAPI-uptake differ, which harbours a fibroblastic radiation induced stroma response. These results are supported by our observation that absolute perilesional [68Ga]FAPI-uptake difference increased in dependence of time from treatment initiation to follow-up. Previous studies discussed that irradiation of murine subcutaneous stroma leads to retarded tumor growth, an effect called Tumor Bed Effect (TBE)40. TBE is known to impact the sensitivity of stromal tissue to radiation40. While perilesional and tumoral [18F]FDG uptake behaved uniformly, perilesional and tumoral reaction may differ in [68Ga]FAPI-imaging. Complementary [68Ga]FAPI- and [18F]FDG-imaging enhance treatment response assessment.
Finally, the question about radiation dose remains. Giesel et al. report an equivalent dose of ~ 3–4 mSv for a [68Ga]FAPI-examination similar to dose values published for [18F]FDG-, [68Ga]DOTATATE, and [68Ga]PSMA-11-examinations16.
Conclusion
[68Ga]FAPI-PET helped to delineate active primary or recurrent tumor lesions in three tumor entities. Non-tumor specific [68Ga]FAPI-uptake for e.g. degenerative lesions, cicatricial tissue, muscles or in the head-and-neck region have to be considered. The [18F]FDG-based planning did not cover the [68Ga]FAPI-volume in the majority of cases, whereas the [18F]FDG-volume was covered by the [68Ga]FAPI-based planning. Pre- and post-treatment [68Ga]FAPI-PET/CT improved radiotherapy planning and treatment response assessment in this particular patient group.
Data availability
The datasets used and analysed during the current study available from the corresponding author on reasonable request.
References
Kubota, K. et al. Impact of FDG-PET findings on decisions regarding patient management strategies: A multicenter trial in patients with lung cancer and other types of cancer. Ann. Nucl. Med. https://doi.org/10.1007/s12149-015-0963-9 (2015).
Nestle, U. et al. ESTRO ACROP guidelines for target volume definition in the treatment of locally advanced non-small cell lung cancer. Radiother. Oncol. 127(1), 1–5. https://doi.org/10.1016/j.radonc.2018.02.023 (2018).
De Ruysscher, D. et al. European Organization for Research and Treatment of Cancer (EORTC) recommendations for planning and delivery of high-dose, high precision radiotherapy for lung cancer. Radiother. Oncol. 124(1), 1–10. https://doi.org/10.1016/j.radonc.2017.06.003 (2017).
Guberina, M. et al. Patterns of nodal spread in stage III NSCLC: Importance of EBUS-TBNA and 18F-FDG PET/CT for radiotherapy target volume definition. Radiat. Oncol. 16(1), 176. https://doi.org/10.1186/s13014-021-01904-4 (2021).
Kong, F. M. et al. Effect of midtreatment PET/CT-adapted radiation therapy with concurrent chemotherapy in patients with locally advanced non-small-cell lung cancer: A phase 2 clinical trial. JAMA Oncol. 3, 1358–1365 (2017).
Raman, S. et al. Rationale and protocol for a Canadian multicenter phase II randomized trial assessing selective metabolically adaptive radiation dose escalation in locally advanced non-small-cell lung cancer (NCT02788461). Clin. Lung Cancer 19, e699–e770 (2018).
Kong, F. M. S. et al. NRG-RTOG1106/Acrin 6697; 2021 ASCO Meeting. J. Clin. Oncol. 39(15 Suppl), 8548 (2021).
Guberina, M. et al. Prognostic value of post-induction chemotherapy volumetric PET/CT parameters for stage IIIA/B non-small cell lung cancer patients receiving definitive chemoradiotherapy. J. Nucl. Med. 62(12), 1684–1691. https://doi.org/10.2967/jnumed.120.260646 (2021).
Hicks, R. J., Roselt, P. J., Kallur, K. G., Tothill, R. W. & Mileshkin, L. FAPI PET/CT: Will it end the hegemony of 18F-FDG in oncology?. J. Nucl. Med. 62(3), 296–302 (2021).
Calais, J. et al. Phase 3 multicenter randomized trial of PSMA PET/CT prior to definitive radiation therapy for unfavorable intermediate-risk or high-risk prostate cancer [PSMA dRT]: Study protocol. BMC Cancer 21(1), 512. https://doi.org/10.1186/s12885-021-08026-w (2021).
Sanli, Y. et al. Neuroendocrine tumor diagnosis and management: 68Ga-DOTATATE PET/CT. AJR Am. J. Roentgenol. 211(2), 267–277. https://doi.org/10.2214/AJR.18.19881 (2018).
Govaerts, C. W. et al. 11C-methyl-l-methionine PET measuring parameters for the diagnosis of tumour progression against radiation-induced changes in brain metastases. Br. J. Radiol. 94(1125), 20210275 (2021).
Hotta, M., Minamimoto, R. & Miwa, K. 11C-methionine-PET for differentiating recurrent brain tumor from radiation necrosis: Radiomics approach with random forest classifier. Sci. Rep. 9(1), 15666. https://doi.org/10.1038/s41598-019-52279-2 (2019).
Scanlan, M. J. et al. Molecular cloning of fibroblast activation protein alpha, a member of the serine protease family selectively expressed in stromal fibroblasts of epithelial cancers. Proc. Natl. Acad. Sci. U.S.A. 91, 5657–5661 (1994).
Šimková, A., Busek, P., Sedo, A. & Konvalinka, J. Molecular recognition of fibroblast activation protein for diagnostic and therapeutic applications. Biochim. Biophys. Acta Proteins Proteomics 1868, 14040929 (2020).
Giesel, F. L. et al. 68Ga-FAPI PET/CT: Biodistribution and preliminary dosimetry estimate of 2 DOTA-containing FAP-targeting agents in patients with various cancers. J. Nucl. Med. 60, 386–392 (2019).
Ozturk, K., Gencturk, M., Caicedo-Granados, E., Li, F. & Cayci, Z. Utility of FDG PET/CT in the characterization of sinonasal neoplasms: Analysis of standardized uptake value parameters. AJR Am. J. Roentgenol. 211, 1354–1360 (2018).
Wilson, J. M., Mukherjee, S., Brunner, T. B., Partridge, M. & Hawkins, M. A. Correlation of 18F-fluorodeoxyglucose positron emission tomography parameters with patterns of disease progression in locally advanced pancreatic cancer after definitive chemoradiotherapy. Clin. Oncol. (R Coll. Radiol.) 29, 370–377 (2017).
Bakst, R. L. et al. Perineural invasion and perineural tumor spread in head and neck cancer. Int. J. Radiat. Oncol. Biol. Phys. 103(5), 1109–1124 (2019).
Röhrich, M. et al. 68Ga-FAPI-PET/CT improves diagnostic staging and radiotherapy planning of adenoid cystic carcinomas—Imaging analysis and histological validation. Radiother. Oncol. 160, 192–201. https://doi.org/10.1016/j.radonc.2021.04.016 (2021).
Janssen, Q. P. et al. Added value of radiotherapy following neoadjuvant FOLFIRINOX for resectable and borderline resectable pancreatic cancer: A systematic review and meta-analysis. Ann. Surg. Oncol. 28, 8297–8308. https://doi.org/10.1245/s10434-021-10276-8 (2021).
Pasqualetti, F. et al. Adjuvant radiotherapy in patients with pancreatic adenocarcinoma. Is it still appealing in clinical trials? A meta-analysis and review of the literature. Anticancer Res. 41, 4697–4704 (2021).
Nehlsen, A. D. & Goodman, K. A. Controversies in radiotherapy for pancreas cancer. J. Surg. Oncol. 123, 1460–1466 (2021).
Tchelebi, L. T. et al. Conventionally fractionated radiation therapy versus stereotactic body radiation therapy for locally advanced pancreatic cancer (CRiSP): An international systematic review and meta-analysis. Cancer 126, 2120–2131 (2020).
Nara, S. et al. Role of adjuvant and neoadjuvant therapy for resectable biliary tract cancer. Expert Rev. Gastroenterol. Hepatol. 15, 537–545 (2021).
Hu, S. L. et al. Role of SUVmax obtained by 18F-FDG PET/CT in patients with a solitary pancreatic lesion: Predicting malignant potential and proliferation. Nucl. Med. Commun. 34, 533–539 (2013).
Buck, A. C. et al. Ki-67 immunostaining in pancreatic cancer and chronic active pancreatitis: Does in vivo FDG uptake correlate with proliferative activity?. J. Nucl. Med. 42, 721–725 (2001).
Cho, K. M. et al. Metabolic characteristics of advanced biliary tract cancer using 18F-fluorodeoxyglucose positron emission tomography and their clinical implications. Oncologist 20, 926–933 (2015).
Guberina, M. et al. Pretreatment metabolic tumour volume in stage IIIA/B non-small-cell lung cancer uncovers differences in effectiveness of definitive radiochemotherapy schedules: Analysis of the ESPATUE randomized phase 3 trial. Eur. J. Nucl. Med. Mol. Imaging 46, 1439–1447 (2019).
Nestle, U. et al. Imaging-based target volume reduction in chemoradiotherapy for locally advanced non-small-cell lung cancer (PET-Plan): A multicentre, open-label, randomised, controlled trial. Lancet Oncol. 21(4), 581–592 (2020).
Kratochwil, C. et al. 68Ga-FAPI PET/CT: Tracer uptake in 28 different kinds of cancer. J. Nucl. Med. 60, 801–805 (2019).
Lan, L. et al. The potential utility of [68Ga]Ga-DOTA-FAPI-04 as a novel broad-spectrum oncological and non-oncological imaging agent-comparison with [18F]FDG. Eur. J. Nucl. Med. Mol. Imaging 49(3), 963–979 (2022).
Wu, J. et al. Comparison of 68Ga-FAPI and 18F-FDG PET/CT in the evaluation of patients with newly diagnosed non-small cell lung cancer. Front. Oncol. 4(12), 924223. https://doi.org/10.3389/fonc.2022.924223 (2022).
Chen, H. et al. Usefulness of [68Ga]Ga-DOTA-FAPI-04 PET/CT in patients presenting with inconclusive [18F]FDG PET/CT findings. Eur. J. Nucl. Med. Mol. Imaging 48(1), 73–86. https://doi.org/10.1007/s00259-020-04940-6 (2021).
Luo, Y., Pan, Q. & Zhang, W. IgG4-related disease revealed by 68Ga-FAPI and 18F-FDG PET/CT. Eur. J. Nucl. Med. Mol. Imaging 46(12), 2625–2626. https://doi.org/10.1007/s00259-019-04478-2 (2019).
Kessler, L. et al. Pitfalls and common findings in 68Ga-FAPI-PET—A pictorial analysis. J. Nucl. Med. https://doi.org/10.2967/jnumed.121.262808 (2021).
Young, H. et al. Measurement of clinical and subclinical tumour response using [18F]-fluorodeoxyglucose and positron emission tomography: Review and 1999 EORTC recommendations. European Organization for Research and Treatment of Cancer (EORTC) PET Study Group. Eur. J. Cancer 35, 1773–1782 (1999).
Sachpekidis, C. et al. Predictive value of early 18F-FDG PET/CT studies for treatment response evaluation to ipilimumab in metastatic melanoma: Preliminary results of an ongoing study. Eur. J. Nucl. Med. Mol. Imaging 42, 386–396 (2015).
Wahl, R. L., Jacene, H., Kasamon, Y. & Lodge, M. A. From RECIST to PERCIST: Evolving considerations for PET response criteria in solid tumors. J. Nucl. Med. 50(Suppl 1), 122S-150S. https://doi.org/10.2967/jnumed.108.057307 (2009).
Haveman, J., Rodermond, H., van Bree, C., Wondergem, J. & Franken, N. A. Residual late radiation damage in mouse stromal tissue assessed by the tumor bed effect. J. Radiat. Res. 48(2), 107–112 (2007).
Funding
Open Access funding enabled and organized by Projekt DEAL. We acknowledge support of the Open Access Publication Fund of the University of Duisburg-Essen. This research did not receive any specific grant from funding agencies in the public, commercial, or not-for-profit sectors. J.T.S. is supported by the German Cancer Consortium (DKTK); the German Research Foundation (DFG) through SI1549/3-1 (Clinical Research Unit KFO337) and SI1549/4-1; the German Cancer Aid through #70112505, PIPAC and #70113834, PREDICT-PACA.
Author information
Authors and Affiliations
Contributions
Conceptualization, N.G. and M.S.; methodology, N.G. and M.S.; software, N.G. and M.S.; validation, N.G., M.G., and M.S.; formal analysis, M.S.; investigation, N.G.; resources, M.S. and K.H.; data curation, M.S.; writing—original draft preparation, N.G.; writing—review and editing, N.G., M.G., C.P., M.M., J.T.S., M.M., C.R., J.T., D.K., W.P.F., F.I., L.U., S.K., M.S.; visualization, M.S.; supervision, M.S.; project administration, M.S.; funding acquisition, M.S. All authors have read and agreed to the published version of the manuscript.
Corresponding author
Ethics declarations
Competing interests
J.T.S. receives honoraria as consultant or for continuing medical education presentations from AstraZeneca, Bayer, Immunocore, Roche, Servier. His institution receives research funding from Bristol-Myers Squibb, Celgene, Roche; He holds ownership and serves on the Board of Directors of Pharma 15, all outside the submitted work. All authors declare that there is no conflict of interest concerning the submitted work.
Additional information
Publisher's note
Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.
Supplementary Information
Rights and permissions
Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/.
About this article
Cite this article
Guberina, N., Kessler, L., Pöttgen, C. et al. [68Ga]FAPI-PET/CT for radiation therapy planning in biliary tract, pancreatic ductal adeno-, and adenoidcystic carcinomas. Sci Rep 12, 16261 (2022). https://doi.org/10.1038/s41598-022-20447-6
Received:
Accepted:
Published:
DOI: https://doi.org/10.1038/s41598-022-20447-6
- Springer Nature Limited