Radiol Oncol 2024; 58(3): 348-356. doi: 10.2478/raon-2024-0032
348
research article
Quantitative SSTR-PET/CT: a potential 
tool for predicting everolimus response in 
neuroendoctine tumour patients
Homeira Karim1, Michael Winkelmann1, Freba Grawe2, Friederike Völter2,  
Christoph Auernhammer3,4, Johannes Rübenthaler1,3, Jens Ricke1,3, Maria Ingenerf1, 
Christine Schmid-Tannwald1,3
1 Department of Radiology, University Hospital, LMU Munich, Munich, Germany 
2 Department of Nuclear Medicine, University Hospital, LMU Munich, Munich, Germany
3  ENETS Centre of Excellence, Interdisciplinary Center of Neuroendocrine Tumours of the GastroEnteroPancreatic System at 
the University Hospital of Munich (GEPNET-KUM), University Hospital of Munich, Munich, Germany
4 Department of Internal Medicine 4, University Hospital, LMU Munich, Munich, Germany
Radiol Oncol 2024; 58(3): 348-356.
Received 12 March 2024 
Accepted 10 May 2024
Correspondence to: Christine Schmid-Tannwald, P.D., M.D., and Maria Ingenerf, M.D., Department of Radiology, University Hospital, LMU 
Munich, Germany; E-mail: Christine.schmid-tannwald@med.uni-muenchen.de
Disclosure: No potential conflicts of interest were disclosed. 
This is an open access article distributed under the terms of the CC-BY license (https://creativecommons.org/licenses/by/4.0/).
Background. This study aimed to assess 68Ga-DOTA-TATE (-TOC) PET/CT quantitative parameters in monitoring and 
predicting everolimus response in neuroendocrine tumor (NET) patients with hepatic metastases (NELM).
Patients and methods. This retrospective analysis included 29 patients with 62 target lesions undergoing everoli-
mus treatment and pre-therapy, and follow-up 68Ga-DOTA-TATE (-TOC) PET/CT scans. Response evaluation utilized 
progression-free survival (PFS) categorized as responders (R; PFS > 6 months) and non-responders (NR; PFS ≤ 6 months). 
Lesion size and density, along with maximum and median standardize uptake value (SUV) in target lesions, liver, and 
spleen were assessed. Tumor-to-spleen (T/S) and tumor-to-liver (T/L) ratios were calculated, including the tumor-to-
spleen (T/S) ratio and tumor-to-liver (T/L) ratio (using SUVmax/SUVmax, SUVmax/SUVmean, and SUVmean/SUVmean). 
Results. PET/CT scans were acquired 19 days (interquartile range [IQR] 69 days) pre-treatment and 127 days (IQR 74 
days) post-starting everolimus. The overall median PFS was 264 days (95% CI: 134–394 days). R exhibited significant de-
creases in Tmax/Lmax and Tmean/Lmax ratios compared to NR (p = 0.01). In univariate Cox regression, Tmean/Lmax 
ratio was the sole prognostic parameter associated with PFS (HR 0.5, 95% CI 0.28–0.92, p = 0.03). Percentage changes 
in T/L and T/S ratios were significant predictors of PFS, with the highest area under curve (AUC) for the percentage 
change of Tmean/Lmax (AUC = 0.73). An optimal threshold of < 2.5% identified patients with longer PFS (p = 0.003). 
No other imaging or clinical parameters were predictive of PFS.
Conclusions. This study highlights the potential of quantitative SSTR-PET/CT in predicting and monitoring everolimus 
response in NET patients. Liver metastasis-to-liver parenchyma ratios outperformed size-based criteria, and Tmean/
Lmax ratio may serve as a prognostic marker for PFS, warranting larger cohort investigation. 
Key words: neuroendocrine tumors; SSTR-PET/CT; everolimus; response
Introduction
Neuroendocrine tumors (NET) are rare, with an 
incidence of 0.48 per 100,000 population.1-3 These 
tumors are often diagnosed at an advanced stage, 
frequently with liver metastases, limiting curative 
surgical options and shifting the focus of treat-
ment towards symptom control and reducing tu-
Radiol Oncol 2024; 58(3): 348-356.
Karim H et al. /Quantitative SSTR-PET/CT: a potential tool for predicting everolimus response in NET patients 349
mor spread. Targeting and inhibiting the mTOR 
protein, which plays a role in the tumorigenesis of 
NETs of different origins, has emerged as a prom-
ising therapeutic strategy for NETs.1,4 
Everolimus, an mTOR inhibitor, has shown effec-
tiveness as a second-line therapy in advanced pan-
creatic NETs, prolonging progression-free survival 
(PFS) and improving overall survival.1,5-7 However, 
objective tumor response rates to are generally 
low, indicating that tumor growth stabilization 
rather than shrinkage is the primary outcome.5,8 
Conventional response criteria based on tumor 
size change appear to be suboptimal for evaluating 
treatment response to targeted anti-cancer drugs 
in slow-growing tumors like NETs.8-10 However, it 
would be crucial to distinguish responders from 
non-responders early on in clinical practice and 
enhance the design of oncological studies by estab-
lishing a more precise definition of progression-free 
survival (PFS). The Choi criteria, which incorporate 
changes in tumor density on CT in addition to size, 
have demonstrated a better correlation with overall 
survival: A study by Solis-Hernandez analysed 107 
patients with neuroendocrine tumors treated with 
sunitinib: They found out that Median progression-
free survival (PFS) by RECIST and Choi were 11.42 
(95 % confidence interval [CI], 9.7–15.9) and 15.8 
months (95% CI, 13.9–25.7). In addition, PFS by Choi 
exhibited greater correlation with overall survival 
(OS) than PFS by RECIST and RECIST incorrectly 
estimated prognosis in 49.6%.11
PET/CT with 68Ga-labeled somatostatin ana-
logues (SSA) (68Ga-DOTA-TATE, -DOTA-NOC and 
-DOTA-TOC) has potential to provide new imag-
ing biomarkers for NETs: The majority of well to 
moderately differentiated neuroendocrine tumors 
(NETs) (80–95 %) overexpresses somatostatin re-
ceptors (SSTRs) on cell surfaces. PET/CT with 68Ga-
labeled somatostatin analogues (SSA) (68Ga-DOTA-
TATE, -DOTA-NOC and -DOTA-TOC) enables vis-
ualization of SSTRs and correlates with the histo-
pathological expression of SSTRs12-14 and provides 
a comprehensive assessment of NETs, including 
their location, size, and metabolic activity.15 It is 
recommended for initial staging and follow-up of 
gastroenteropancreatic neuroendocrine tumors 
(GEP-NET) by the European Society for Medical 
Oncology Guidelines Working Group.16
However, there is limited research on function-
al imaging response criteria in patients receiving 
everolimus. Therefore, this study aims to assess 
the diagnostic reliability of 68-Ga-DOTA-TATE 
PET/CT to monitor and predict therapy response 
to everolimus in NETs.
Patients and methods
Patients
This retrospective study included consecutive pa-
tients with histologically confirmed NETs of dif-
ferent primary tumor sites who received everoli-
mus between August 2011 and October 2020 at our 
department. Eligible patients had liver metastases 
only or, if not already resected, the primary tumor 
and had undergone both baseline and follow-up 
68Ga-DOTA-TATE (-TOC) PET/CT scans. The selec-
tion for everolimus therapy was based on consen-
sus decisions made in an interdisciplinary tumor 
conference certified for NETs (ENETS Center of 
Excellence). The study received approval from the 
local research ethics committee, and the require-
ment for written informed patient consent was 
waived.
PET/CT
Whole-body PET/CT scans were conducted us-
ing either a GE Discovery 690 (GE Healthcare, 
Little Chalfont, United Kingdom) or a Biograph 64 
TruePoint PET/CT scanner (Siemens Healthcare, 
Erlangen, Germany). Approximately 60 minutes af-
ter intravenous injection of around 220 MBq of 68Ga-
DOTA-TATE (-TOC), emission data were acquired. 
When feasible, 20mg of furosemide were adminis-
tered. The emission data underwent reconstruction 
with attenuation correction using concurrent diag-
nostic CT scans, which covered the neck, thorax, ab-
domen, and pelvis. The diagnostic CT scan param-
eters were set at 100–190 mAs, 120 kV, with a colli-
mation of 2 x 5 mm and a pitch of 1.5. Additionally, 
an iodine-based contrast agent (Ultravist 300TM; 
Bayer Healthcare, Berlin, Germany; 1.5 mL/kg body 
weight) was intravenously injected at a rate of 2.5 
mL/s, with a 50-second delay to capture the portal 
venous phase of the liver.
Image analysis
Two board-certified radiologists with experience 
in nuclear medicine, blinded to the patients’ clini-
cal and follow-up data, conducted a consensus 
review of pre- and post-treatment PET/CT scans. 
Target lesions, including up to two liver metastases 
and the pancreatic NET if not resected, were iden-
tified based on criteria such as increased tracer up-
take exceeding normal physiological activity and 
a minimum size of 1 cm, detectable on CT scans. 
In two separate reading sessions, the radiologists 
measured the maximum lesion size and den-
Radiol Oncol 2024; 58(3): 348-356.
Karim H et al. /Quantitative SSTR-PET/CT: a potential tool for predicting everolimus response in NET patients350
sity (in Hounsfield units) of the normal liver and 
spleen, as well as the liver metastases and NET, on 
CT scans. The uptake of 68Ga-DOTA-TATE was 
quantified by obtaining the maximum and mean 
standardized uptake values (SUVs). Circular vol-
umes of interest (VOIs) were positioned within the 
predefined target lesion and in the normal liver 
and spleen parenchyma to calculate tumor-to-or-
gan ratios, including the tumor-to-spleen (T/S) ra-
tio and tumor-to-liver (T/L) ratio (using SUVmax/
SUVmax, SUVmax/SUVmean, SUVmean/SUVmax 
and SUVmean/SUVmean).
Standard of reference and response to 
treatment
Diagnosis of NET was confirmed by histopathol-
ogy, and Ki-67 labelling index of the primary tu-
mor was obtained for all included patients. Tumor 
grading was rated according to 2017 WHO Tumor 
Classification Guideline (G1: Ki-67 Index was <3%, 
G2: Ki-67 Index was 3–20%, and G3 NET/NEC: Ki-
67 Index was >20%).17
Progression-free survival (PFS) was used as a 
parameter for treatment response, calculated in 
days/ months from the time of everolimus initia-
tion until progression, as evaluated by the local 
interdisciplinary tumor board through the assess-
ment of all performed imaging studies (CT, PET/
CT, MRI). Responder (R) were defined as patients 
with PFS > 6 months and non-responders (NR) as 
patients with PFS ≤ 6 months respectively.
Statistical analysis
Statistical analysis was conducted using com-
mercially available software, including GraphPad 
Prism Version 6 (San Diego, Calif.), SPSS version 25 
(Chicago, IL), and Microsoft Excel v. 16. The level 
of statistical significance was defined as p ≤ 0.05. 
Data were presented as mean with standard devia-
tion (SD) or median values with interquartile range 
[IQR], as appropriate. Normal distribution of con-
tinuous variables was assessed through visual in-
spection of the frequency distribution (histogram).
Quantitative measurements of the target lesions 
before and after therapy were compared using a 
two-tailed, paired t-test, while comparisons of 
target lesions between different response groups 
were performed using a two-tailed, unpaired t-test 
or Wilcoxon rank sum test, depending on the data 
distribution.
Progression-free survival (PFS) was analyzed 
using the Kaplan-Meier method, and survival 
curves were compared using the Log-Rank test. 
Prognostic parameters for PFS were assessed us-
ing Cox proportional hazards regression analysis. 
In the multivariable model, variables with a p-val-
ue ≤ 0.05 in the univariable analysis were included 
using a stepwise approach.
Results 
Patients
A total of 29 patients (12 female, 17 male) with a 
combined count of 62 target lesions (54 liver me-
tastases, 8 primary tumors) were included in this 
retrospective study. The baseline PET/CT scans 
were acquired 19 d (interquartile range (IQR) 69d) 
before treatment initiation, and the first follow-up 
PET/CT scans were performed 127 d (IQR 74d) af-
ter the start of everolimus treatment. Most of the 
included patients had G2 tumors (n = 20), followed 
by G1 tumors (n = 7) and one patient had a high-
TABLE 1. Patients demographics
Sex (male) 17 (59%)
Age (mean + SD ) 63 ± 13.2
Grading
    G1 7 (24%)
    G2 20 (69%)
    G3 1 (3%)
    n/a 1 (3%)
Ki-67 (mean + SD) 9.1 ± 7.6
Primary tumor site
    Pancreas 11 (38%)
    Stomach 1 (3%)
    Liver 1 (3%)
    Lung 1 (3%)
    Small-intestine 11 (38%)
    Kidney 1 (3%)
    Breast 1 (3%)
    Retroperitoneal 1 (3%)
    Rectum 1 (3%)
Bilirubin prior to therapy (mg/dl) 0.6 (0.3–1.3)
Bilirubin after therapy (mg/dl) 0.5 (0.2–2.6)
Median CgA prior to therapy (ng/ml) (range) 487 (10–8983)
Median CgA after therapy (ng/ml) (range) 929 (43–23348)
CgA = chromogranin A; SD = standard deviation 
Radiol Oncol 2024; 58(3): 348-356.
Karim H et al. /Quantitative SSTR-PET/CT: a potential tool for predicting everolimus response in NET patients 351
grade primary tumor (G3), while grading informa-
tion was not available for one patient. Detailed pa-
tient characteristics are presented in Table 1.
Progression-free survival
At the end of the study, 28/29 patients showed pro-
gression on imaging. The overall median PFS was 
264 days (95% CI: 134–394 days). The median PFS 
was 487 days (95% CI: 154–820 days) in the R group 
(n = 16), and 112 d in the NR group (95% CI: 79–145 
days). There was no significant difference in PFS 
between patients with elevated and non-elevated 
baseline chromogranin A (CgA) levels (p > 0.7).
Responder vs. non-responder
There were no differences in pretherapeutic clini-
cal or imaging parameters between the two re-
sponse groups. In responders (R), the absolute 
SUV of the liver metastases (including SUVmax 
and SUVmean) decreased significantly, while 
there was no change in non-responders (NR). 
However, the percentage changes between the 
response groups were not significantly different. 
Tmax/Lmax and Tmean/Lmax of liver metasta-
ses decreased significantly in responders, while 
there was no change in non-responders, and the 
percentage changes were significantly different, 
with -15.5% in responders compared to 5.5% in 
non-responders (p = 0.01) (Figures 1 and 2). There 
were no significant changes in the size of the liver 
metastases. The density of the liver metastases de-
creased significantly in responders, while there 
was no change in non-responders; however, per-
centual changes were not different between both 
response groups. 
Regarding the primary NET, statistical evalua-
tion was limited due to the small sample size and 
different primary tumor sites (pancreas: n = 6, duo-
denum: n = 1, rectum: n = 1), and there were no 
significant changes in response groups. 
SUVmean of the spleen increased significant-
ly in responders (p = 0.02), while it decreased in 
non-responders (P = 0.04). SUVmax of the liver de-
creased in both responders and non-responders, 
while the percentage decrease was slightly higher 
in non-responders (p = 0.04) (Table 2).
Prognostic and predictive factors
In the univariate Cox regression analysis, the 
only prognostic parameter associated with PFS 
was the Tmean/Lmax ratio of the liver metastases 
(HR 0.5, 95% CI 0.28–0.92, p = 0.03). Patients with a 
higher Tmean/Lmax ratio (≥ 2) on baseline imag-
ing showed slightly significantly longer PFS, with 
a median of 410 days compared to 185 days (p = 
0.04). None of the pretherapeutic clinical param-
eters were associated with PFS.
Among the changes after treatment, the percent-
age changes of both tumor-to-liver ratios (Tmax/
Lmax and Tmean/Lmax) and the Tmax/Smean ra-
tio were significant predictors of PFS. In a second-
ary analysis, the area under the curve (AUC) was 
highest for the percentage change of Tmean/Lmax 
FIGURE 1. 63-year-old female with responding liver metastasis of ileal 
neuroendocrine tumor. On the pretherapeutic PETCT (A, B) there were high 
tumor-to- liver (T/L) ratio. After three months of treatment with everolimus, the 
liver metastasis showed no significant shrinkage in size, but a significantly reduced 
uptake of 68Ga-DOTATATE (C, D) compared to pretherapeutic PET/CT (Tmax/Lmax: 
0.94 vs. 2,09 and Tmean/Lmax 1.54 vs. 0.76).
FIGURE 2. 31-year-old male with non-responding liver metastasis of pancreatic 
neuroendocrine tumor. On the pretherapeutic PET/CT (A, B) there were low 
tumor-to- liver (T/L) ratios. After three months of treatment with everolimus, liver 
metastasis (arrow) showed an increase in size on CT (C), but also a significantly 
increased uptake of 68Ga-DOTATATE (D) compared to pretherapeutic PET/CT.
A B
C D
A B
C D
Radiol Oncol 2024; 58(3): 348-356.
Karim H et al. /Quantitative SSTR-PET/CT: a potential tool for predicting everolimus response in NET patients352
TABLE 2. Clinical and imaging parameters at baseline and follow-up with changes
Responder Pre- vs. Post- therapy Non-responder
p-value
R vs. NR Pre- 
treatment
R vs. NR Post- 
treatment
Pre-
treatment
Post-
treatment p
Pre-
treatment
Post-
treatment p p
Clinical parameters
Age 63.5 +- 12.5 62.4 +- 13.4 0.42
Sex (male) 10 (45%) 7 (37%) 0.2
Ki-67 % 7.9 (+- 7.8) 10.5 (+-7) 0.28
Pre Bilirubin 0.6 (0.2) 0.7 (0.3) 0.13
Pre CgA 551(77.6–933.5)
422
(47–1414) 0.11
Imaging parameters
SUVmax Liver 8 (6–9.3) 9.4 (5–10.9) 0.17 6.9 (4.9–9.2) 6.4 (3.5–10) 0.05 0.6 0.1
SUVmean Spleen 12.3(9.9–18.6)
16.4
(9.9–20.1) 0.02
13.8
(10.1–16.9)
11
(9.8–15.1) 0.04 0.3 0.5
SUVmax LM 28.1(15.1–35.3)
22.2
(14.2–31.7) < 0.01
21.3
(12.7–34.7)
22.5
(9.4–29.6) 0.19 0.3 0.6
SUVmean LM 12.4(10.5–19.1)
12.9
(9.3–18.9) 0.03
14.5
(9.3–18.3)
13.5
(7.8–17.4) 0.13 0.4 0.5
Tmax/Lmax LM 3.0 (2.4–4.3) 2.4 (2–3.3) 0.02 2.8 (2.4–3.8) 3 (1.9–4.6) 0.36 0.3 0.8
Tmean/Lmax LM 1.8 (1.4–2.3) 1.6 (1.2–1.9) 0.02 1.9 (1.2–2.2) 1.6 (1.4–2.5) 0.26 0.2 0.7
Tmax/Smean LM 1.6 (1.3–2.4) 1.3 (0.9–1.7) 0.25 1.5 (1.2–2.3) 1.5 (0.9–3.0) 0.3 0.4 0.8
Tmean/Smean LM 1.0(0.8–1.1) 0.8 (0.5–1.0) 0.49 0.9 (0.6–1.6) 0.9 (0.5–1.6) 0.46 0.5 1.0
Size LM 21 (17–29) 20 (15–31.2) 0.64 21 (15–32) 21 (15–32) 0.95 0.7 0.5
Density LM (HU) 101.9 (± 19.9)
90.5
(± 20.5) 0.03
89.4
(± 22.6)
81.7
(± 22.1) 0.1 0.2 0.3
SUVmax NET 32.8(6.9–39.8) 30.4 (10.3–31.5) 0.49
36.4
(28.8–47.4)
43.1
(29.7–53.7) 0.97 0.5 0.3 
SUVmean NET 16(4.6–16.9) 13.4 (7.1–14.7) 0.9
17.6
(14–19.4)
22.3
(13.6–28.5) 0.25 0.4 0.3
Size NET 18 (15-36) 25(11.2–37.3) 0.48
43.5
(24–60.8)
44.5
(25.3–66) 0.37 0.7 0.5
Density NET 83.3 (± 9.1) 81.5 (± 18) 0.9 89.3 (± 17.5) 78.2 (± 11.6) 0.4 0.6 0.8
Change (%)
between pre- and
post-treatment
Responder Non-responder R vs. NRp   
SUVmax Liver -9.5 (-14–19.9) -13 (-37.5–8.7) 0.04   
SUVmean Spleen 13 (-6.6–29.1) -10.7 (-26.3–2.6) 0.01   
SUVmax LM -20.4 (-27–6) -0.9 (-22.8–26.3) 0.21
SUVmean LM -10 (-28.5–12.7) -7 (-23.4–11.1) 0.62
Tmax/Lmax LM -15.5 (-47–5.5) 5.5 (-20.4–20.7) 0.01
Tmean/Lmax LM -16.3 (-37–9) 7 (-22.3–31.1) 0.03
Tmax/Smean LM -16.6 (-44.2–13.6) 4.5 (-16.8–51.4) 0.01
Tmean/Smean LM -16.3 (-39.3–8.8) 0.9 (-17.4–50) 0.04
Size LM -7 (-27.8–6.1) 14.3 (-17.6–28) 0.77
Density LM -5.6 (-12.3–0.2) -7 (-16.5–4.1) 0.8
SUVmax NET -7.3 (-16.2–35.5) -18.1 (-41.6–25.6) 0.77
SUVmean NET 15.6 (-0.6–48) 18.4 (-7.8–40.5) 0.65
Size NET -15.9 (-37.4–11.1) 3.6 (-2.1–13.3) 0.72
Density NET -5.2 (-20–14.5) -18.3 (-22.9– -4.6) 0.69
Bilirubin -33 (-61.7–0) -25 (-66.7–0) 0.43
CgA 56.4 (17.4–144.9) 32.1 (-2.8–72.8) 0.18
CgA = chromogranin A; LR = liver metastases; NET = neuroendocrine tumor; NR = non-responder; R = responder; SUV = standardize uptake value; Tmax/Lmax = tumor max 
to liver max; Tmax/Smean = tumor max to splen max 
Radiol Oncol 2024; 58(3): 348-356.
Karim H et al. /Quantitative SSTR-PET/CT: a potential tool for predicting everolimus response in NET patients 353
(AUC = 0.73), followed by the percentage change 
of Tmax/Lmax (AUC = 0.71). The ROC analysis 
revealed an optimal threshold for Tmean/Lmax 
at >2.5 (sensitivity 62%, specificity 80%) and for 
Tmax/Lmax at >8 (sensitivity 54%, specificity 87%). 
PFS of patients with any decrease of Tmax/Lmax 
less than 2.5% was significantly longer with 322 
days compared to 142 days (p = 0.003). Also, PFS of 
patients with an any decrease of Tmax/Lmax less 
than 8% was significantly longer with 306 days 
compared to 142 days (p = 0.005) (Figure 3). None 
of the other imaging parameters, such as density 
or size, nor any of the clinical parameters, were 
predictive of PFS.
Discussion
In this study we investigated the utility of clinical, 
morphological, and SSTR-PET derived functional 
imaging parameters for evaluating response and 
predicting outcomes in NET patients treated with 
everolimus. Our findings suggest that the use of 
ratios of SUV of the liver metastases (Tmean/Lmax 
and Tmax/Lmax) could serve as valuable tool for 
assessing and even predicting therapy response in 
NET patients receiving everolimus.
We chose progression-free survival (PFS) as the 
primary endpoint for response evaluation, follow-
ing the recommendation of the National Cancer 
Institute Neuroendocrine Tumor Clinical Trials 
Planning Meeting consensus report. The use of 
overall survival (OS) for therapy response evalu-
ation in NETs can be challenging due to the long 
survival times typically associated with these tu-
mors and the range of post-progression salvage 
therapies available.18 The overall median PFS in 
our patient cohort was slightly lower compared to 
the RADIANT-3 and RADIANT-4 trials, with 8.7 
months compared to 11 months, respectively.5,19 
These differences could be attributed to factors 
such as the small size of our study cohort, the use 
of everolimus as a late treatment-line at our clinic, 
and the distribution of tumor grading among pa-
tients. In our patient cohort 69% had G2 tumors 
and 24% had G1 tumors, while in the RADIANT-3 
study 82% of the patients had well differentiated 
tumors and in the RADIANT-4 study 63% had G1 
tumors.5,19
Conventional response assessment based on 
percentage changes in the size of target lesions 
did not show significant differences between the 
response groups on the first follow-up PET/CT. 
However, functional imaging parameters, particu-
larly the percentage changes in tumor-to-organ 
ratios of the liver metastases, were significantly 
different between response groups, with non-
responders showing a median percent increase 
(median 0.9 to 7%) and responders showing a 
median percent decrease (median -15.5 to -16.6%). 
The percentual changes of absolute SUV measure-
ments however, including SUVmax and SUVmean, 
were not significantly different between response 
groups. 
Tumor-to-organ ratios are affected by the 
changes in the specific organs, e.g., liver or spleen 
respectively. Our study revealed a significant in-
crease in spleen SUVmean after treatment in R, 
while NR showed a decrease in splenic SUVmean. 
Previous studies have reported a decrease in SSTR 
uptake in the spleen after long-acting somatosta-
tin analog therapy, accompanied by an increase 
in tumor uptake.20,21 Additionally, after splenec-
tomy, higher uptake of 68Ga DOTA-TOC in tumors 
and some normal tissues has been observed.22,23 
However, these changes’ correlation with tumor 
response has rarely been evaluated.
Quantitative assessment of SSTR PET/CT has its 
challenges, and relying solely on absolute tumor 
uptake for response evaluation might lead to er-
roneous conclusions.20 In this context, tumor-to-
organ ratios offer an advantage, along with the 
normalization of absolute SUV to obtain scanner-
independent parameters. In our study, SUVmax 
of the liver decreased in both responders and 
non-responders, with a slightly greater degree of 
reduction in non-responders (-13% vs. -9.5%). This 
observation could be related to the metabolization 
of everolimus, which mainly occurs in the liver via 
the CYP3A4 system. Although serum enzyme el-
evations may occur in up to 25% of patients, these 
changes are typically mild and self-limiting.24,25 
In a secondary analysis, we evaluated the as-
sociation of different clinical and imaging pa-
rameters with PFS using Cox regression analysis. 
FIGURE 3. Predictive value of %-change of Tmean/Lmax ratio and %-change of 
Tmax/Lmax ratio.
Radiol Oncol 2024; 58(3): 348-356.
Karim H et al. /Quantitative SSTR-PET/CT: a potential tool for predicting everolimus response in NET patients354
Among the prognostic factors, the Tmean/Lmax 
ratio of the liver metastases emerged as the only 
significant parameter associated with PFS (HR 0.5, 
95% CI 0.28–0.92, p = 0.03). Patients with a higher 
Tmean/Lmax ratio (≥ 2) on baseline imaging exhib-
ited longer PFS, while none of the pretherapeutic 
clinical parameters showed a significant asso-
ciation with PFS. These findings are consistent 
with previous studies investigating the prognos-
tic value of SSTR-PET/CT in patients undergoing 
peptide-receptor-radionuclide therapy (PRRT)26-28 
or lanreotide treatment29, which also reported that 
patients with higher baseline tumor-to-liver ratios 
or SUVmax had a better prognosis or were more 
likely to respond to therapy. For PRRT, Kratochwil 
et al. proposed a cut-off value of the tumor-to-
liver ratio > 2.2 to select patients for treatment by 
PRRT.27 The correlation between higher SUV val-
ues and the dose delivered by PRRT may explain 
these findings. However, in the context of a target-
ed therapy like everolimus, the underlying mecha-
nism remains unclear. One possible explanation 
is that a target lesion with higher SSR expression 
might correspond to a more differentiated tumor. 
Further research is needed to elucidate the precise 
mechanisms underlying these observations.
In the univariable Cox regression analysis, the 
percentage change of the tumor-to-organ ratios 
(Tmax/Lmax and Tmean/Lmax) were found to be 
significantly associated with PFS. However, none 
of these parameters remained significant in the 
multivariable analysis, possibly due to the total 
study size being a limiting factor for this analysis. 
ROC analysis was performed on the identified pa-
rameters, and the highest AUC was obtained for 
Tmean/Lmax (AUC = 0.73). Patients with a per-
centual change of Tmax/Lmax of less than 2.5% 
showed a significantly longer PFS with 322 days 
compared to 142 days (p = 0.003). In contrast, none 
of the other imaging parameters, such as density 
or size, nor any of the clinical parameters, were 
predictive of PFS at the first follow-up.
Increasing evidence suggests that conventional 
response assessment based on tumor size change 
is limited in evaluating treatment response to anti-
proliferative or antiangiogenic effects mediated by 
targeted anti-cancer drugs, particularly in slow-
growing tumors such as NETs.8-10 Low objective 
response rates in the RADIANT 3 and RADIANT 
4 trials, with 5% and 2% in the everolimus group, 
respectively, further support this observation.5,19 
It suggests that the benefit of everolimus on PFS 
is mainly attributed to the stabilization of tumor 
growth or minor tumor shrinkage, without reach-
ing the cutoff for partial response as defined by 
RECIST.5,8 Consequently, conventional size-based 
response criteria in this context may not accurately 
classify patients as responders vs. non-responders, 
potentially leading to the inappropriate discontin-
uation of an effective therapy.21
For classical FDG PET/CT, numerous studies 
have demonstrated that a decrease in SUV after 
therapy can predict survival. For instance, in pa-
tients with liver metastasis of pancreatic cancer 
treated with TARE or in breast cancer patients 
receiving targeted therapies, a decrease in SUV 
has been shown to be indicative of improved out-
comes.30,31 However, data regarding SSTR PET/CT 
is more limited. Some studies have indicated that 
a decrease in SUV, corrected for spleen or liver up-
take, is associated with longer time to progression 
after PRRT and even correlated with improved 
clinical symptoms.32,33 Additionally, in a different 
study, the change of T/S and T/L ratios on the first 
follow-up was identified as the best metric to cor-
relate with longer hepatic PFS in NET patients un-
dergoing TARE.34
The main limitation of this study was its small 
sample size, which is related to the low incidence 
of NETs and everolimus representing a second-line 
treatment. Additionally, the retrospective analysis 
represents a limiting factor, as time intervals be-
tween PET/CT scans and everolimus treatment 
were heterogeneous, and prior therapies differed 
among patients. Another limitation is the use of 
different scanners. While the use of quantitative 
SUV is well-established for FDG PET/CT using 
the PERCIST criteria35, the interpretation of SUV 
in SSTR-PET/CT is more complex, as a reduction 
in uptake could be attributed to tumor regression 
or dedifferentiation.26 Therefore, the use of nor-
malized SUV measures by calculating tumor-to-
spleen, liver, or blood pool ratios was suggested by 
various authors.33,36
In conclusion, our study highlights the potential 
value of quantitative SSTR-PET/CT in predicting 
and monitoring response in patients with NETs 
receiving everolimus. The use of liver metastasis-
to-liver parenchyma ratios (Tmean/Lmax and 
Tmax/Lmax) showed promise in assessing therapy 
response, outperforming conventional size-based 
criteria. The Tmean/Lmax ratio emerged as a 
promising prognostic marker for progression-free 
survival (PFS), warranting further investigation 
in larger cohorts. Despite limitations of retrospec-
tive nature and small sample size, functional im-
aging remains crucial for guiding personalized 
treatment strategies in NET patients undergoing 
Radiol Oncol 2024; 58(3): 348-356.
Karim H et al. /Quantitative SSTR-PET/CT: a potential tool for predicting everolimus response in NET patients 355
targeted therapies like everolimus. Prospective 
studies with standardized protocols and larger 
populations are needed to validate these findings’ 
clinical relevance.
References
1. Auernhammer CJ, Spitzweg C, Angele MK, Boeck S, Grossman A, Nölting S, 
et al. Advanced neuroendocrine tumours of the small intestine and pan-
creas: clinical developments, controversies, and future strategies. Lancet 
Diabetes Endocrinol 2018; 6: 404-15. doi: 10.1016/s2213-8587(17)30401-1
2. Dasari A, Shen C, Halperin D, Zhao B, Zhou S, Xu Y, et al. Trends in the inci-
dence, prevalence, and survival outcomes in patients with neuroendocrine 
tumors in the United States. JAMA Oncol 2017; 3: 1335-42. doi: 10.1001/
jamaoncol.2017.0589
3. Klöppel G, Perren A, Heitz PU. The gastroenteropancreatic neuroendocrine 
cell system and its tumors: the WHO classification. Ann NY Acad Sci 2004; 
1014: 13-27. doi: 10.1196/annals.1294.002
4. Briest F, Grabowski P. PI3K-AKT-mTOR-signaling and beyond: the com-
plex network in gastroenteropancreatic neuroendocrine neoplasms. 
Theranostics 2014; 4: 336-65. doi: 10.7150/thno.7851
5. Yao JC, Shah MH, Ito T, Bohas CL, Wolin EM, Van Cutsem E, et al. Everolimus 
for advanced pancreatic neuroendocrine tumors. N Engl J Med 2011; 364: 
514-23. doi: 10.1056/NEJMoa1009290
6. Lee L, Ito T, Jensen RT. Everolimus in the treatment of neuroendocrine 
tumors: efficacy, side-effects, resistance, and factors affecting its place in 
the treatment sequence. Expert Opin Pharmacother 2018; 19: 909-28. doi: 
10.1080/14656566.2018.1476492
7. Akirov A, Larouche V, Alshehri S, Asa SL, Ezzat S. Treatment options for 
pancreatic neuroendocrine tumors. Cancers 2019; 11: 828. doi: 10.3390/
cancers11060828
8. Garcia-Carbonero R, Garcia-Figueiras R, Carmona-Bayonas A, Sevilla I, Teule 
A, Quindos M, et al. Imaging approaches to assess the therapeutic response 
of gastroenteropancreatic neuroendocrine tumors (GEP-NETs): current 
perspectives and future trends of an exciting field in development. Cancer 
Metastasis Rev 2015; 34: 823-42. doi: 10.1007/s10555-015-9598-5
9. Choi JI, Imagawa DK, Bhosale P, Bhargava P, Tirkes T, Seery TE, et al. 
Magnetic resonance imaging following treatment of advanced hepatocel-
lular carcinoma with sorafenib. Clin Mol Hepatol 2014; 20: 218-22. doi: 
10.3350/cmh.2014.20.2.218
10. Krajewski KM, Nishino M, Franchetti Y, Ramaiya NH, Van den Abbeele 
AD, Choueiri TK. Intraobserver and interobserver variability in computed 
tomography size and attenuation measurements in patients with renal cell 
carcinoma receiving antiangiogenic therapy: implications for alternative 
response criteria. Cancer 2014; 120: 711-21. doi: 10.1002/cncr.28493
11. Solis-Hernandez MP, Fernandez Del Valle A, Carmona-Bayonas A, Garcia-
Carbonero R, Custodio A, Benavent M, et al. Evaluating radiological 
response in pancreatic neuroendocrine tumours treated with sunitinib: 
comparison of Choi versus RECIST criteria (CRIPNET_ GETNE1504 study). Br 
J Cancer 2019; 121: 537-44. doi: 10.1038/s41416-019-0558-7
12. Schmid-Tannwald C, Schmid-Tannwald CM, Morelli JN, Neumann R, Haug 
AR, Jansen N, et al. Comparison of abdominal MRI with diffusion-weighted 
imaging to 68Ga-DOTATATE PET/CT in detection of neuroendocrine tumors 
of the pancreas. Eur J Nucl Med Mol Imaging 2013; 40: 897-907. doi: 
10.1007/s00259-013-2371-5
13. Papotti M, Bongiovanni M, Volante M, Allìa E, Landolfi S, Helboe L, et al. 
Expression of somatostatin receptor types 1-5 in 81 cases of gastrointestinal 
and pancreatic endocrine tumors. A correlative immunohistochemical and 
reverse-transcriptase polymerase chain reaction analysis. Virchows Arch 
2002; 440: 461-75. doi: 10.1007/s00428-002-0609-x
14. Versari A, Camellini L, Carlinfante G, Frasoldati A, Nicoli F, Grassi E, et al. 
Ga-68 DOTATOC PET, endoscopic ultrasonography, and multidetector CT 
in the diagnosis of duodenopancreatic neuroendocrine tumors: a single-
centre retrospective study. Clin Nucl Med 2010; 35: 321-8. doi: 10.1097/
RLU.0b013e3181d6677c
15. Singh S, Poon R, Wong R, Metser U. 68Ga PET Imaging in patients with neu-
roendocrine tumors: a systematic review and meta-analysis. Clin Nucl Med 
2018; 43: 802-10. doi: 10.1097/rlu.0000000000002276
16. Pavel M, Öberg K, Falconi M, Krenning EP, Sundin A, Perren A, et al. 
Gastroenteropancreatic neuroendocrine neoplasms: ESMO Clinical practice 
guidelines for diagnosis, treatment and follow-up. Ann Oncol 2020; 31: 844-
60. doi: 10.1016/j.annonc.2020.03.304
17. Kim JY, Hong SM, Ro JY. Recent updates on grading and classification of 
neuroendocrine tumors. Ann Diagn Pathol 2017; 29: 11-6. doi: 10.1016/j.
anndiagpath.2017.04.005
18. Yao JC, Pavel M, Lombard-Bohas C, Cutsem EV, Voi M, Brandt U, et al. 
Everolimus for the treatment of advanced pancreatic neuroendocrine 
tumors: overall survival and circulating biomarkers from the randomized, 
Phase III RADIANT-3 study. J Clin Oncol 2016; 34: 3906-13. doi: 10.1200/
jco.2016.68.0702
19. Yao JC, Fazio N, Singh S, Buzzoni R, Carnaghi C, Wolin E, et al. Everolimus 
for the treatment of advanced, non-functional neuroendocrine tumours 
of the lung or gastrointestinal tract (RADIANT-4): a randomised, placebo-
controlled, phase 3 study. Lancet 2016; 387: 968-77. doi: 10.1016/s0140-
6736(15)00817-x
20. Cherk MH, Kong G, Hicks RJ, Hofman MS. Changes in biodistribution on 
(68)Ga-DOTA-Octreotate PET/CT after long acting somatostatin analogue 
therapy in neuroendocrine tumour patients may result in pseudoprogres-
sion. Cancer Imaging 2018; 18: 3. doi: 10.1186/s40644-018-0136-x
21. Weber M, Telli T, Kersting D, Seifert R. Prognostic implications of PET-derived 
tumor volume and uptake in patients with neuroendocrine tumors. Cancers 
2023; 15: 3581. doi: 10.3390/cancers15143581
22. Kratochwil C, Mavriopoulou E, Rath D, Afshar-Oromieh A, Apostolopoulos 
D, Haufe S, et al. Comparison of 68Ga-DOTATOC biodistribution in patients 
with and without spleenectomy. Q J Nucl Med Mol Imaging 2015; 59: 116-
20. PMID: 24382404
23. Sarikaya I, Sarikaya A, Alnafisi N, Alenezi S. Significance of splenic uptake on 
somatostatin receptor imaging studies. Nucl Med Rev Cent East Eur 2018; 
21: 66-70. doi: 10.5603/NMR.a2018.0012
24. Schieren G, Bölke E, Scherer A, Raffel A, Gerber PA, Kröpil P, et al. Severe 
everolimus-induced steatohepatis: a case report. Eur J Med Res 2013; 18: 
22. doi: 10.1186/2047-783x-18-22
25. Kuhn B, Jacobsen W, Christians U, Benet LZ, Kollman PA. Metabolism of 
sirolimus and its derivative everolimus by cytochrome P450 3A4: insights 
from docking, molecular dynamics, and quantum chemical calculations. J 
Med Chem 2001; 44: 2027-34. doi: 10.1021/jm010079y
26. Öksüz MÖ, Winter L, Pfannenberg C, Reischl G, Müssig K, Bares R, et al. 
Peptide receptor radionuclide therapy of neuroendocrine tumors with 
90Y-DOTATOC: is treatment response predictable by pre-therapeutic up-
take of 68Ga-DOTATOC? Diagn Interven Imaging 2014; 95: 289-300. doi: 
10.1016/j.diii.2013.07.006
27. Kratochwil C, Stefanova M, Mavriopoulou E, Holland-Letz T, Dimitrakopoulou-
Strauss A, Afshar-Oromieh A, et al. SUV of [68Ga]DOTATOC-PET/CT predicts 
response probability of prrt in neuroendocrine tumors. Mol Imag Biol: 
2015; 17: 313-8. doi: 10.1007/s11307-014-0795-3
28. Sharma R, Wang WM, Yusuf S, Evans J, Ramaswami R, Wernig F, et al. (68)
Ga-DOTATATE PET/CT parameters predict response to peptide receptor ra-
dionuclide therapy in neuroendocrine tumours. Radiother Oncol 2019; 141: 
108-115. doi: 10.1016/j.radonc.2019.09.003
29. Kim YI, Yoo C, Oh SJ, Lee SJ, Kang J, Hwang HS, et al. Tumour-to-liver ratio 
determined by [(68)Ga]Ga-DOTA-TOC PET/CT as a prognostic factor of 
lanreotide efficacy for patients with well-differentiated gastroenteropan-
creatic-neuroendocrine tumours. EJNMMI Res 2020; 10: 63. doi: 10.1186/
s13550-020-00651-z
30. Sirico M, Bernocchi O, Sobhani N, Giudici F, Corona SP, Vernieri C, et al. 
Early changes of the standardized uptake values (SUV(max)) predict the 
efficacy of everolimus-exemestane in patients with hormone receptor-
positive metastatic breast cancer. Cancers 2020; 12: 3314 doi: 10.3390/
cancers12113314
31. Michl M, Lehner S, Paprottka PM, Ilhan H, Bartenstein P, Heinemann V, et al. 
Use of PERCIST for prediction of progression-free and overall survival after 
radioembolization for liver metastases from pancreatic cancer. J Nucl Med 
2016; 57: 355-60. doi: 10.2967/jnumed.115.165613
Radiol Oncol 2024; 58(3): 348-356.
Karim H et al. /Quantitative SSTR-PET/CT: a potential tool for predicting everolimus response in NET patients356
32. Haug AR, Auernhammer CJ, Wangler B, Schmidt GP, Uebleis C, Goke B, et al. 
68Ga-DOTATATE PET/CT for the early prediction of response to somatostatin 
receptor-mediated radionuclide therapy in patients with well-differentiated 
neuroendocrine tumors. J Nucl Med 2010; 51: 1349-56. doi: 10.2967/
jnumed.110.075002
33. Opalińska M, Morawiec-Sławek K, Kania-Kuc A, Al Maraih I, Sowa-Staszczak 
A, Hubalewska-Dydejczyk A. Potential value of pre- and post-therapy [68Ga]
Ga-DOTA-TATE PET/CT in the prognosis of response to PRRT in disseminated 
neuroendocrine tumors. Front Endocrinol 2022; 13: 929391. doi: 10.3389/
fendo.2022.929391
34. Ingenerf M, Kiesl S, Karim S, Beyer L, Ilhan H, Rübenthaler J, et al. (68)
Ga-DOTATATE PET/CT and MRI with diffusion-weighted imaging (DWI) in 
short- and long-term assessment of tumor response of neuroendocrine 
liver metastases (NELM) following transarterial radioembolization (TARE). 
Cancers 2021; 13: 4321. doi: 10.3390/cancers13174321
35. O JH, Lodge MA, Wahl RL. Practical PERCIST: a simplified guide to PET 
response criteria in solid tumors 1.0. Radiology 2016; 280: 576-84. doi: 
10.1148/radiol.2016142043
36. Ilan E, Velikyan I, Sandström M, Sundin A, Lubberink M. Tumor-to-blood 
ratio for assessment of somatostatin receptor density in neuroendocrine 
tumors using 68Ga-DOTATOC and 68Ga-DOTATATE. J Nucl Med 2020; 61: 
217-21. doi: 10.2967/jnumed.119.228072