Elba Etchebehere1, Ana Emília Brito2, Kalevi Kairemo3, Eric Rohren3, John Araujo3, Homer Macapinlac3. 1. Universidade Estadual de Campinas (Unicamp), Campinas, SP, Brazil. 2. Real Hospital Português de Beneficência em Pernambuco - Real Nuclear, Recife, PE, Brazil. 3. The University of Texas MD Anderson Cancer Center, Houston, TX, USA.
Abstract
OBJECTIVE: To determine whether an interim 18F-fluoride positron-emission tomography/computed tomography (PET/CT) study performed after the third cycle of radium-223 dichloride (223RaCl2) therapy is able to identify patients that will not respond to treatment. MATERIALS AND METHODS: We retrospectively reviewed 34 histologically confirmed cases of hormone-refractory prostate cancer with bone metastasis in patients submitted to 223RaCl2 therapy. All of the patients underwent baseline and interim 18F-fluoride PET/CT studies. The interim study was performed immediately prior to the fourth cycle of 223RaCl2. The skeletal tumor burden-expressed as the total lesion fluoride uptake above a maximum standardized uptake value of 10 (TLF10)-was calculated for the baseline and the interim studies. The percent change in TLF10 between the baseline and interim studies (%TFL10) was calculated as follows: %TFL10 = interim TLF10 - baseline TLF10 / baseline TLF10. End points were overall survival, progression-free survival, and skeletal-related events. RESULTS: The mean age of the patients was 72.4 ± 10.2 years (range, 43.3-88.8 years). The %TLF10 was not able to predict overall survival (p = 0.6320; hazard ratio [HR] = 0.753; 95% confidence interval [CI]: 0.236-2.401), progression-free survival (p = 0.5908; HR = 1.248; 95% CI: 0.557-2.797) nor time to a bone event (p = 0.5114; HR = 1.588; 95% CI: 0.399-6.312). CONCLUSION: The skeletal tumor burden on an interim 18F-fluoride PET/CT, performed after three cycles of 223RaCl2, is not able to predict overall survival, progression-free survival, or time to bone event, and should not be performed to monitor response at this time.
OBJECTIVE: To determine whether an interim 18F-fluoride positron-emission tomography/computed tomography (PET/CT) study performed after the third cycle of radium-223 dichloride (223RaCl2) therapy is able to identify patients that will not respond to treatment. MATERIALS AND METHODS: We retrospectively reviewed 34 histologically confirmed cases of hormone-refractory prostate cancer with bone metastasis in patients submitted to 223RaCl2 therapy. All of the patients underwent baseline and interim 18F-fluoride PET/CT studies. The interim study was performed immediately prior to the fourth cycle of 223RaCl2. The skeletal tumor burden-expressed as the total lesion fluoride uptake above a maximum standardized uptake value of 10 (TLF10)-was calculated for the baseline and the interim studies. The percent change in TLF10 between the baseline and interim studies (%TFL10) was calculated as follows: %TFL10 = interim TLF10 - baseline TLF10 / baseline TLF10. End points were overall survival, progression-free survival, and skeletal-related events. RESULTS: The mean age of the patients was 72.4 ± 10.2 years (range, 43.3-88.8 years). The %TLF10 was not able to predict overall survival (p = 0.6320; hazard ratio [HR] = 0.753; 95% confidence interval [CI]: 0.236-2.401), progression-free survival (p = 0.5908; HR = 1.248; 95% CI: 0.557-2.797) nor time to a bone event (p = 0.5114; HR = 1.588; 95% CI: 0.399-6.312). CONCLUSION: The skeletal tumor burden on an interim 18F-fluoride PET/CT, performed after three cycles of 223RaCl2, is not able to predict overall survival, progression-free survival, or time to bone event, and should not be performed to monitor response at this time.
Baseline whole-body 18F-fluoride PET/CT is ideal for staging and restaging
prostate cancer and has been shown to be an independent prognostic imaging biomarker
of patients undergoing radium-223 dichloride (223RaCl2)
therapy(1). However,
although treatment with 223RaCl2 improves survival in prostate
cancer patients(2-4), not all patients respond to this
therapy. It would be beneficial to identify nonresponders early in the course of
treatment, thereby reducing morbidity and unnecessary costs.After successful treatment of osteoblastic bone metastases, an osteoblastic reaction
(flare) can occur, which increases bone uptake even in responsive cases. That can be
confused with the osteoblastic reaction and inflammation that occur in response to
tumor-associated growth factors during progression. This phenomenon has been well
described in conventional bone scintigraphy, and that method is therefore not
recommended for use as the sole means of determining the response to
treatment(5,6).Although interim studies performed with 18F-FDG PET/CT can change the
management of patients with a variety of cancer types(7-10), the exact role of 18F-fluoride PET/CT in
evaluating the early response to therapy (interim study) is not well established.
The importance of 18F-fluoride PET/CT has extended beyond the diagnosis
of metastases to the evaluation of optimal strategies for use in patients submitted
to treatment with new therapeutic agents. Chemotherapy, hormone therapy,
immunotherapy, and radionuclide therapies such as those involving
223RaCl2(11) are costly approaches. Therefore, the ability to predict
response, thereby avoiding overtreatment and reducing costs, will improve patient
management. The purpose of this study was to determine whether an interim
18F-fluoride PET/CT study is able to evaluate treatment responses in
prostate cancer patients submitted to 223RaCl2 therapy.
MATERIALS AND METHODS
The local institutional review board approved this retrospective analysis (reference
no. PA14-0848). We retrospectively reviewed histologically confirmed cases of
hormone-refractory prostate cancer with bone metastasis in patients receiving
223RaCl2 therapy and undergoing two
18F-fluoride PET/CT studies-a baseline study and an interim study
(immediately prior to the fourth cycle of 223RaCl2)-at our
facility. All patients completed at least four cycles of
223RaCl2 (Xofigo; Bayer Pharma AG, Berlin, Germany),
receiving intravenous infusions of 50 kBq/kg (1.4 µCi/kg) of
223RaCl2 at monthly intervals.
18F-fluoride PET/CT acquisition
18F-fluoride PET/CT images were acquired immediately prior to
initiation of the 223RaCl2 therapy (baseline study) and
immediately before the fourth cycle (interim study). True whole-body PET images
were obtained 50-60 min after intravenous injection of 158-370 MBq of
18F-sodium fluoride in dedicated PET/CT scanners (Discovery STe,
RX, or VCT; 16 or 64 channel; GE Healthcare, Milwaukee, WI, USA, or Siemens mCT
Flow; 64 channel; Siemens Healthcare, Knoxville, TN, USA), and whole-body
noncontrast CT scans were used for attenuation correction.
18F-fluoride PET/CT interpretation and quantification
Two board-certified nuclear medicine physicians evaluated baseline and interim
18F-fluoride PET/CT images. Visual and quantitative analyses were
performed.
Visual analysis
In the visual analysis, we compared the baseline and interim studies,
classifying the responses as follows:Complete response - Osteoblastic bone metastases identified in
the baseline study no longer being present in the interim
study.Partial response - Interim study showing decreased uptake in
pre-existing bone metastases.Stable disease - No difference between the interim and baseline
scans in terms of the uptake in pre-existing bone
metastases.Progressive disease - Interim study showing an increase in the
uptake or volume of a pre-existing bone metastases or new
osteoblastic metastases.The patients were followed for confirmation of these response
classifications. The follow-up reference standards used in order to
determine if the response classification was correct (i.e., to identify
true-positive, true-negative, false-positive, and false-negative responses)
included clinical parameters-such as clinical worsening, disease
progression, bone events, and death; biochemical parameters-such as the
levels of alkaline phosphatase (ALP) and prostate-specific antigen (PSA);
and imaging findings-such as those obtained with 18F-fluoride
PET/CT, 18F-FDG PET/CT, bone scans, or CT scans. On the interim
18F-fluoride PET/CT study, images that demonstrated stable
disease, a partial response, or a complete response were all considered to
represent a true-positive response to therapy if the reference standards
also indicated that the patient had responded to therapy (no clinical
worsening, progression, or increase in the levels of the biochemical
markers) or a false-positive response to therapy if those same standards
demonstrated progressive disease (new areas of disease, clinical worsening,
or death). In contrast, images that demonstrated progressive disease were
considered to represent a true-negative response to therapy if the reference
standards also indicated that the patient had not responded to therapy and
it was confirmed during follow-up that there was no response to therapy or a
false-negative response to therapy (flare response) if those same standards
demonstrated a response (no clinical worsening, progression, or increase in
the levels of the biochemical markers).
Quantitative analysis
Using quantitative analysis, we determined the whole-body skeletal tumor
burden in the baseline and interim 18F-fluoride PET/CT images.
The skeletal tumor burden was determined after establishing the maximum
standardized uptake value (SUVmax) threshold ≥ 10 to
exclude normal bone(12). To that end, we initially obtained the volume
(in milliliters) of total fluoride activity, defined as the fluoride tumor
volume above an SUVmax of 10 (FTV10), within the
volume of interest (VOI). The FTV10 calculation is equivalent to
the metabolic tumor volume calculation used in 18F-FDG PET/CT
studies. The total fluoride lesion uptake above an SUVmax of 10
(TLF10) was then calculated as the product of mean
SUVmax × FTV10. The TLF10 is
equivalent to the total lesion glycolysis used in 18F-FDG PET/CT
studies. To evaluate the performance of interim 18F-fluoride
PET/CT, the percent change in the skeletal tumor burden between the baseline
and interim studies was calculated as follows:%TLF10 = interim TLF10 - baseline TLF10 /
baseline TFL10
Statistical analyses
Categorical variables were expressed as absolute and relative frequencies,
whereas continuous variables were expressed as mean ± standard deviation
when presenting normal distribution and as median (minimum-maximum) when
presenting non-normal distribution. All outcome measures were correlated with
the %TFL10 values obtained. The primary end point was overall
survival (OS), which was calculated from the first
223RaCl2 cycle to the date of death or last follow-up.
Secondary end points were progression-free survival (PFS), time to a bone event
(TTBE), and bone marrow failure (BMF). PFS was calculated from the first
223RaCl2 cycle to the date of progression, death, or
last follow-up. The TTBE was calculated as the time from the date of the first
223RaCl2 cycle to the next bone event. Lastly, BMF was
defined as the development of hematologic toxicity (World Health Organization
grade 3 or 4), together with no recovery after six weeks or death due to BMF
after the last 223RaCl2 cycle.Kaplan-Meier survival curves were generated, and Cox proportional hazards
regression was used in order to analyze predictors of survival. Backward
stepwise selection was performed for multivariate Cox models. Logistic
regression was used in order to model the odds of a bone event as a function of
all of the PET variables. We used Spearman's correlation coefficient to assess
the level of agreement between the PET variables. For the statistical analyses,
we used the Statistical Analysis System, version 9.3 for Windows (SAS Institute
Inc., Cary, NC, USA).
RESULTS
We analyzed the cases of 34 patients, with a mean age of 72.4 ± 10.2 years
(median, 72.5 years; range, 43.3-88.8 years) (Table
1), who had had prostate cancer for a mean of 6 ± 4 years (range,
2-20 years). The mean Gleason score was 7 ± 3. Prior to the initiation of
223RaCl2 therapy, 26.9% of the patients had received
chemotherapy, 5% had received radiotherapy, 59% had received hormone therapy, and 9%
had received blood transfusion. At the first 223RaCl2 cycle,
the mean ALP was 193.9 IU/L and the mean PSA was 103.2 ng/mL. The median time of
follow-up after the interim study was 28.1 months (range, 11-52 months). The 34
patients were submitted to a collective total of 179 223RaCl2
cycles: 55.9% of the patients received six cycles of 223RaCl2;
14.7% received five cycles; and 29.4% received four cycles. The principal causes of
treatment interruption were progression (in 44.4%), hematologic toxicity (in 17.8%),
a significant decline of the Eastern Cooperative Oncology Group performance status
(in 13.3%), and a bone event (in 2.2%).
Table 1
Demographic and clinical characteristics of 34 patients prior to
223RaCl2 therapy.
Characteristic
Median
Range
Age
72.4
43.3-88.8
Prostate specific antigen (ng/mL)
103.2
2.1-761.1
Alkaline phosphatase (IU/L)
193.9
48.0-913.0
Hemoglobin (g/dL)
11.2
6.6-13.6
Platelets (K/µL)
215.8
114-413
Absolute neutrophils (K/µL)
5.7
1.5-21.4
Demographic and clinical characteristics of 34 patients prior to
223RaCl2 therapy.
Visual analysis of interim 18F-fluoride PET/CT
A complete response was not perceived in any of the interim
18F-fluoride PET/CT studies or on the basis of the follow-up
reference standards. A partial response was identified in 16 (47%) of the
patients in the interim 18F-fluoride PET/CT studies (Figure 1), and the reference standards
demonstrated that a partial response had indeed been achieved in eight of those
patients (true-positive cases), whereas the other eight patients had progressed
(false-positive cases), as shown in Figure
2. Stable disease was noted in five (15%) of the patients in the
interim 18F-fluoride PET/CT studies, although only three of those
patients were categorized as true-positive cases (showing stable disease or a
partial response), whereas the two remaining patients progressed. Progressive
disease was identified in 13 (38%) of the patients in the interim
18F-fluoride PET/CT studies, 12 (35.3%) of whom were categorized as
true-negative cases (Figure 3), the
remaining patient (3.0%) being categorized as a false-negative case because the
increased uptake noted on the interim 18F-fluoride PET/CT (when
compared with that observed in the baseline study) was actually due to a flare
phenomenon (Figure 4). Therefore, the
responses were categorized as true positive in 11 cases (32.4%), false positive
in 10 (29.4%), true negative in 12 (35.3%), and false negative in 1 (2.9%).
Figure 1
A patient with hormone-refractory prostate cancer, accompanied by
bone metastasis, who showed a partial response to
223RaCl2, and the interim
18F-fluoride PET/CT study demonstrating a true-positive
response. A: The baseline 18F-fluoride
PET/CT study revealing widespread osteoblastic metastases.
B: The interim 18F-fluoride PET/CT
study, performed after the third 223RaCl2
cycle, showing a reduction in osteoblastic metastases, especially in
the rib cage, pelvis, and right femur, consistent with a partial
response to 223RaCl2. There was a 70%
reduction in the %TLF10. During follow-up, the ALP levels
dropped and no new bone lesions appeared. After the last
223RaCl2 cycle, the patient resumed
enzalutamide to control lymph node metastases that had been present
prior to the first 223RaCl2 cycle.
Figure 2
A patient with hormonerefractory prostate cancer, accompanied by bone
metastasis, who showed progression during
223RaCl2 therapy but was categorized as a
false-positive case on the basis of the imaging findings.
A: The baseline 18F-fluoride PET/ CT
study showing osteoblastic metastases. B: The interim
18Ffluoride PET/CT study, performed after the third
223RaCl2 cycle, showing a slight reduction
in uptake by the known osteoblastic metastases and no new lesions,
consistent with a partial response. Although the %TLF10
decreased by 44%, the PSA and ALP levels continued to rise and there
was rapid progression of the bone metastases. Therefore, the patient
was started on cyclophosphamide and subsequently on dasatinib. C: A
follow-up 18F-fluoride PET/ CT study, conducted after the
sixth 223RaCl2 cycle, showed wide- A B C
spread osteoblastic metastases.
Figure 3
A patient with hormone-refractory prostate cancer, accompanied by
bone metastasis, who showed progression during
223RaCl2 therapy. A: The
baseline 18F-fluoride PET/CT study showing widespread
osteoblastic metastases. B: The interim
18F-fluoride PET/CT study, performed after the third
223RaCl2 c ycle, s howing i ncreased u
ptake i n t he k nown o steoblastic metastases and new lesions,
especially in the pelvis, consistent with progression. The
%TLF10 increased by 104%; PSA and ALP levels
continued to rise; new bone metastases developed; a liver metastasis
developed; and there was further enlargement of previously enlarged
lymph nodes. The patient started a new chemotherapy regimen but died
eight months after the last 223RaCl2
cycle.
Figure 4
A patient with hormone-refractory prostate cancer, accompanied by
bone metastasis, who responded to 223RaCl2 but
was categorized as a falsenegative case on the basis of the imaging
findings. A: The baseline 18F-fluoride
PET/CT study showing osteoblastic metastases. B: The
interim 18F-fluoride PET/CT study, performed after the
third 223RaCl2 cycle, showing increased uptake
in the known osteoblastic metastases but no new lesions. Although
that pattern is consistent with progression (with a
%TLF10 increase of 65%), the PSA and ALP dropped
remarkably, after which the patient responded and was stable at 12
months after the last 223RaCl2 cycle.
Therefore, the images were clearly due to a flare (false-negative)
response.
A patient with hormone-refractory prostate cancer, accompanied by
bone metastasis, who showed a partial response to
223RaCl2, and the interim
18F-fluoride PET/CT study demonstrating a true-positive
response. A: The baseline 18F-fluoride
PET/CT study revealing widespread osteoblastic metastases.
B: The interim 18F-fluoride PET/CT
study, performed after the third 223RaCl2
cycle, showing a reduction in osteoblastic metastases, especially in
the rib cage, pelvis, and right femur, consistent with a partial
response to 223RaCl2. There was a 70%
reduction in the %TLF10. During follow-up, the ALP levels
dropped and no new bone lesions appeared. After the last
223RaCl2 cycle, the patient resumed
enzalutamide to control lymph node metastases that had been present
prior to the first 223RaCl2 cycle.A patient with hormonerefractory prostate cancer, accompanied by bone
metastasis, who showed progression during
223RaCl2 therapy but was categorized as a
false-positive case on the basis of the imaging findings.
A: The baseline 18F-fluoride PET/ CT
study showing osteoblastic metastases. B: The interim
18Ffluoride PET/CT study, performed after the third
223RaCl2 cycle, showing a slight reduction
in uptake by the known osteoblastic metastases and no new lesions,
consistent with a partial response. Although the %TLF10
decreased by 44%, the PSA and ALP levels continued to rise and there
was rapid progression of the bone metastases. Therefore, the patient
was started on cyclophosphamide and subsequently on dasatinib. C: A
follow-up 18F-fluoride PET/ CT study, conducted after the
sixth 223RaCl2 cycle, showed wide- A B C
spread osteoblastic metastases.A patient with hormone-refractory prostate cancer, accompanied by
bone metastasis, who showed progression during
223RaCl2 therapy. A: The
baseline 18F-fluoride PET/CT study showing widespread
osteoblastic metastases. B: The interim
18F-fluoride PET/CT study, performed after the third
223RaCl2 c ycle, s howing i ncreased u
ptake i n t he k nown o steoblastic metastases and new lesions,
especially in the pelvis, consistent with progression. The
%TLF10 increased by 104%; PSA and ALP levels
continued to rise; new bone metastases developed; a liver metastasis
developed; and there was further enlargement of previously enlarged
lymph nodes. The patient started a new chemotherapy regimen but died
eight months after the last 223RaCl2
cycle.A patient with hormone-refractory prostate cancer, accompanied by
bone metastasis, who responded to 223RaCl2 but
was categorized as a falsenegative case on the basis of the imaging
findings. A: The baseline 18F-fluoride
PET/CT study showing osteoblastic metastases. B: The
interim 18F-fluoride PET/CT study, performed after the
third 223RaCl2 cycle, showing increased uptake
in the known osteoblastic metastases but no new lesions. Although
that pattern is consistent with progression (with a
%TLF10 increase of 65%), the PSA and ALP dropped
remarkably, after which the patient responded and was stable at 12
months after the last 223RaCl2 cycle.
Therefore, the images were clearly due to a flare (false-negative)
response.The interim 18F-fluoride PET/CT study was found to have a sensitivity
of 91.6%, a specificity of 54.5%, a positive predictive value of 52.4%, a
negative predictive value of 92.3%, and an accuracy of 67.6% (Figure 5). For distinguishing between
responders and nonresponders, a reduction in the ALP level had a sensitivity of
38% and a specificity of 85% when the follow-up parameters were taken as the
reference.
Figure 5
Visual analysis and evolution of the 34 patients.
Visual analysis and evolution of the 34 patients.
Quantitative analysis of interim 18F-fluoride PET/CT
Figure 6 illustrates the quantitative method
employed to obtain the TLF10 and FTV10 values. Spearman's
correlation coefficient showed that the %TLF10 and %FTV10
values correlated strongly with each other (rho = 0.95). Therefore, only the
%TLF10 values were applied to subsequent analyses. The median
TLF10 was 7374 (range, 391-46,550) in the baseline
18F-fluoride PET/CT study and 5632 (range, 486-30,200) in the interim
study.
Figure 6
Example of determination of TLF10 and FTV10.
A: A semi-automatic VOI (orange rectangle) is
placed within the whole-body maximum intensity projection image. A
threshold SUVmax of 10 is then established as the cut-off
to separate normal bone from abnormal bone. Consequently, the
software will automatically delineate only SUVmax regions
above the set threshold of 10, defining the VOI with an isocontour
threshold set at 41% of the SUVmax. After all regions
have been defined, a careful inspection should be performed to
exclude all non-tumor-related VOIs. The sum of all the VOIs outlined
with the SUVmax of 10 provides the FTV10. To
obtain the TLF10, the FTV10 is multiplied by
the SUVmean10 (VOI10 ×
mean10), which is also measured in milliliters.
B: In this particular example, the patient had only
one lesion with an SUVmax higher than 10, which
corresponded to a rib metastasis with an SUVmax of 25.
The TLF10 was 65.8, and the FTV10 was 4.2.
Example of determination of TLF10 and FTV10.
A: A semi-automatic VOI (orange rectangle) is
placed within the whole-body maximum intensity projection image. A
threshold SUVmax of 10 is then established as the cut-off
to separate normal bone from abnormal bone. Consequently, the
software will automatically delineate only SUVmax regions
above the set threshold of 10, defining the VOI with an isocontour
threshold set at 41% of the SUVmax. After all regions
have been defined, a careful inspection should be performed to
exclude all non-tumor-related VOIs. The sum of all the VOIs outlined
with the SUVmax of 10 provides the FTV10. To
obtain the TLF10, the FTV10 is multiplied by
the SUVmean10 (VOI10 ×
mean10), which is also measured in milliliters.
B: In this particular example, the patient had only
one lesion with an SUVmax higher than 10, which
corresponded to a rib metastasis with an SUVmax of 25.
The TLF10 was 65.8, and the FTV10 was 4.2.At the end of the follow-up period, 32 (94%) of the patients had progressed and
17 (53%) had died (Table 2). The average
time to progression was 4.7 ± 2.9 months (median, 3.1 months; range,
0.9-12.1 months), and the most common type of progression was metastasis to the
bone (in 39.1%), followed by nodal metastases (in 25.0%) and visceral metastases
(in 21.9%).
Table 2
%TLF10 variation and outcome measures.
OS
PFS
TTBE
BMF
Patient
%TLF10
Status
Months
Status
Months
Status
Months
Status
Months
1
46.9%
Alive
17.4
Yes
3.0
No
17.4
No
9.9
2
-44.0%
Alive
11.8
Yes
2.8
No
11.8
No
8.8
3
-22.4%
Alive
18.7
Yes
11.9
No
18.7
No
13.2
4
-70.0%
Alive
11.4
Yes
0.9
No
11.4
No
8.0
5
-7.3%
Deceased
8.6
Yes
6.5
Yes
6.5
No
6.6
6
-33.0%
Deceased
8.7
Yes
3.4
No
8.7
Yes
3.4
7
-35.1%
Alive
9.0
Yes
5.2
No
9.0
Yes
7.7
8
-33.8%
Deceased
10.4
Yes
3.0
No
10.4
No
6.7
9
17.8%
Deceased
11.1
Yes
2.8
No
11.1
No
10.5
10
-51.3%
Deceased
9.0
Yes
2.2
Yes
2.2
No
4.5
11
-9.8%
Alive
13.9
Yes
2.8
Yes
6.2
No
9.5
12
39.6%
Alive
3.7
Yes
2.8
No
3.7
No
3.7
13
-24.5%
Deceased
6.0
Yes
3.1
No
6.0
Yes
4.5
14
-17.1%
Alive
10.7
Yes
7.7
No
10.7
No
7.6
15
34.6%
Alive
11.5
Yes
8.1
No
11.5
No
10.3
16
-22.4%
Alive
15.4
Yes
9.3
No
15.4
No
11.4
17
14.2%
Alive
4.8
Yes
2.8
Yes
2.8
Yes
4.3
18
-20.4%
Alive
11.9
Yes
7.1
No
11.9
No
6.1
19
-25.6%
Alive
9.5
Yes
4.2
No
9.5
No
7.9
20
-8.8%
Alive
13.9
Yes
8.1
No
13.9
No
11.7
21
16.1%
Deceased
8.7
Yes
2.8
No
8.7
No
3.7
22
65.5%
Alive
16.3
No
12.1
No
16.3
No
8.1
23
-26.0%
Deceased
4.7
Yes
1.8
No
4.7
No
3.5
24
-66.3%
Alive
17.7
Yes
10.0
Yes
4.5
No
12.1
25
-11.6%
Deceased
5.9
Yes
2.0
No
5.9
Yes
5.1
26
-18.9%
Deceased
5.0
Yes
2.8
No
5.0
Yes
2.8
27
104.0%
Deceased
12.1
Yes
3.2
No
12.1
Yes
11.9
28
-43.8%
Deceased
8.2
Yes
5.1
Yes
8.2
No
5.1
29
-28.8%
Alive
9.6
Yes
4.6
No
9.6
No
4.6
30
19%
Deceased
8.2
Yes
5.0
No
8.2
No
5.0
31
65.5%
Deceased
6.8
Yes
2.8
No
6.8
Yes
6.4
32
-84.5%
Deceased
5.8
Yes
2.8
No
5.8
Yes
5.6
33
-62.8%
Alive
9.3
No
4.9
No
9.3
No
4.8
34
8.4%
Deceased
5.4
Yes
3.1
No
5.4
No
4.2
%TLF10 variation and outcome measures.In our study sample, the %TLF10 on the interim 18F-fluoride
PET/CT was not able to predict OS (p = 0.6320; HR = 0.753; 95%
CI: 0.236-2.401) or PFS (p = 0.5908; HR = 1.248; 95% CI:
0.557-2.797). Six patients had a bone event, and %TLF10 was also
unable to predict the TTBE (p = 0.5114; HR = 1.588; 95% CI:
0.399-6.312). Nine patients developed BMF after 223RaCl2,
and %TLF10 was also not a significant univariate predictor of the
odds of developing that condition (p = 0.6071; HR = 1.401; 95%
CI: 0.387-5.070). We found that OS did not correlate with the SUVmax
(p = 0.7989), any nodal disease (p =
0.1342), or visceral disease (p = 0.1496).
DISCUSSION
We have demonstrated that an interim 18F-fluoride PET/CT study is unable
to predict outcomes after 223RaCl2 therapy. Novel therapies
for osteoblastic metastases, including 223RaCl2 therapy, are
costly, and it is therefore important to establish a diagnostic test to predict
responses to these new, expensive treatments. In one study evaluating treatment
responses after six cycles of 223RaCl2 in ten
patients(13),
conventional bone scintigraphy demonstrated that increased areas of uptake were due
not only to treatment response but also to reparative bone changes after therapy (a
flare response).Previous studies have shown that a baseline 18F-fluoride PET/CT study
plays a prognostic role in patients with breast or prostate cancer treated with
223RaCl2(1,14).
However, 18F-fluoride PET/CT is not traditionally used in evaluating the
response to any therapy, because the process of bone healing involves an
osteoblastic reaction than can increase 18F-fluoride uptake, as in
conventional bone scintigraphy(15). Because of comparable pharmacokinetics between
223RaCl2(2) and 18F-fluoride(16), we hypothesized that
18F-fluoride would be able to evaluate osteoblastic metastases
before, during, and after 223RaCl2 therapy.In our study sample, the interim study demonstrated that a decrease in uptake was
generally due to a response (partial or stable disease) to therapy. However, we find
it interesting that, in six (17.6%) of the patients, the decreased uptake was caused
by extensive tumor infiltration of the bone marrow, ultimately leading to BMF. To
our knowledge, there have been no previous studies describing the latter imaging
pattern (caused by BMF) in interim studies. In contrast, although the interim study
was able to demonstrate that increased uptake was due to progression, that pattern
of uptake was in fact a flare phenomenon in one case. This increased uptake most
likely occurred because of the bone healing process after successful
223RaCl2 treatment, which involves an osteoblastic
reaction. In the subset of patients in which the flare phenomenon occurred, the CT
portion of the study revealed reparative changes with increased extent of the
sclerotic lesions. However, even on CT, it was not possible to determine which
patients were progressing and which were responding. Although we hypothesized that
bone levels of ALP could help evaluate patient outcomes, it demonstrated higher
specificity and lower sensitivity than did the interim 18F-fluoride
PET/CT study.Quantitative analyses of 18F-fluoride PET/CT images have been conducted to
assess its role in predicting outcomes, by determining the peak SUVmax
values of bone metastases. Apolo et al.(17) performed 18F-fluoride PET/CT after 6 and 12
months of standard therapy in prostate cancer patients, reporting that progression
was associated with SUV increases of more than 57%, as well as that a greater
increase in SUV was associated with worse survival. Yu et al.(18) evaluated responses to therapy
with dasatinib using SUVmax in five target lesions on
18F-fluoride PET/CT and detected only a borderline correlation with PFS;
the changes also correlated with the ALP level. Another study, involving only five
patients, showed a reduction in SUVmax at 6 and 12 weeks after the use of
223RaCl2(19). In our population, the SUVmax did not
correlate with OS. Although the above mentioned studies performed
18F-fluoride PET/CT for therapeutic evaluation, its precise role in
determining the early response to therapy has yet to be extensively studied,
especially in terms of assessing survival as an end point.The reported frequency of the flare phenomenon in prostate cancer patients undergoing
conventional bone scintigraphy ranges from 6% to 25%(20,21). Although the flare phenomenon has also been described in
patients undergoing 18F-fluoride PET/CT(15), there have been no reports of its frequency in
patients treated with 223RaCl2 and undergoing
18F-fluoride PET/CT. Although we identified the flare phenomenon on
18F-fluoride PET/CT in only a small proportion of our patient sample
(3%), that proportion is probably higher than in conventional bone scintigraphy,
given the greater sensitivity of PET/CT. The most likely explanation for the fact
that the frequency of the flare phenomenon was not higher is that our study sample
was composed of patients with extensive disease, in whom the likelihood of
progression is greater than is that of a response to therapy. In addition, the
number of patients might have been insufficient to detect this phenomenon.In our patient sample, the interim 18F-fluoride PET/CT (%TLF10)
after three cycles of 223RaCl2 was not able to predict OS,
PFS, TTBE, or BMF. These findings are quite similar to those of a previous study,
involving ten prostate cancer patients treated with
223RaCl2(22), although the interim 18F-fluoride PET/CT
studies were performed at different time points: at baseline; after one (or two)
cycles of 223RaCl2; and at the end of treatment. A correlation
with outcome was only noted between baseline and end-of-treatment
18F-fluoride PET/CT results were found to correlate with outcomes, as
previously reported(1).One major limitation of our study was the relatively small number of patients. We
believe that the interim 18F-fluoride PET/CT could have potential for the
prediction of BMF, given that 6 of the 9 patients who evolved to BMF showed a
reduction in uptake. However, due to the small sample size, those results were not
significant. Another limitation was the fact that it was not possible to obtain
histological confirmation in the patients who showed progression. Although the
18F-fluoride PET/CT images were acquired in different scanners, the
same software was employed in all quantifications, guaranteeing uniformity in the
metrics.To our knowledge, this is the first study to evaluate the role of interim
18F-fluoride PET/CT in predicting the response to
223RaCl2 therapy, using quantitative methods to determine
the skeletal tumor burden. It would be interesting to know whether these findings
could be replicated in other populations, such as that of breast cancer patients
treated with 223RaCl2.
CONCLUSION
In prostate cancer patients undergoing 223RaCl2 therapy,
interim 18F-fluoride PET/CT performed after three cycles of
223RaCl2 does not seem able to predict outcomes. It also
appears to be unable to differentiate a flare response from progressive disease, and
we therefore discourage the use of interim 18F-fluoride PET/CT to
evaluate the response to 223RaCl2 therapy in prostate cancer
patients. There is a need for studies involving a larger number of patients and
patients with other types of cancer, in order to verify our findings.
Authors: Karen A Kurdziel; Joanna H Shih; Andrea B Apolo; Liza Lindenberg; Esther Mena; Yolanda Y McKinney; Stephen S Adler; Baris Turkbey; William Dahut; James L Gulley; Ravi A Madan; Ola Landgren; Peter L Choyke Journal: J Nucl Med Date: 2012-06-22 Impact factor: 10.057
Authors: Gary Cook; Chris Parker; Sue Chua; Bernadette Johnson; Anne-Kirsti Aksnes; Val J Lewington Journal: EJNMMI Res Date: 2011-06-07 Impact factor: 3.138
Authors: Paul G Kluetz; William Pierce; V Ellen Maher; Hui Zhang; Shenghui Tang; Pengfei Song; Qi Liu; Martin T Haber; Eldon E Leutzinger; Ali Al-Hakim; Wei Chen; Todd Palmby; Elleni Alebachew; Rajeshwari Sridhara; Amna Ibrahim; Robert Justice; Richard Pazdur Journal: Clin Cancer Res Date: 2013-11-04 Impact factor: 12.531
Authors: C Parker; S Nilsson; D Heinrich; S I Helle; J M O'Sullivan; S D Fosså; A Chodacki; P Wiechno; J Logue; M Seke; A Widmark; D C Johannessen; P Hoskin; D Bottomley; N D James; A Solberg; I Syndikus; J Kliment; S Wedel; S Boehmer; M Dall'Oglio; L Franzén; R Coleman; N J Vogelzang; C G O'Bryan-Tear; K Staudacher; J Garcia-Vargas; M Shan; Ø S Bruland; O Sartor Journal: N Engl J Med Date: 2013-07-18 Impact factor: 91.245
Authors: Tim E Phelps; Jyoti Roy; Michael V Green; Jurgen Seidel; Kwamena E Baidoo; Stephen Adler; Elijah F Edmondson; Donna Butcher; Jennifer L Matta; Anita T Ton; Karen Wong; Shan Huang; Ling Ren; Amy K LeBlanc; Peter L Choyke; Elaine M Jagoda Journal: Cancer Biother Radiopharm Date: 2021-02-25 Impact factor: 3.099
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