2Deparment of Nuclear Medicine, Hacettepe University Hospital, Ankara-Türkiye
3Deparment of Radiology, Hacettepe University Hospital, Ankara-Türkiye
4Deparment of Oncology, MKA Breast Cancer Clinic, Ankara-Türkiye DOI : 10.5505/tjo.2022.3701
Summary
OBJECTIVENeoadjuvant chemotherapy (NAC) is applied in locally advanced breast cancers (LABCs). Pathological complete response (PCR) after NAC is associated with prognosis. This prospective study aimed to compare the predictive value of semi-quantitative parameters obtained by dynamic contrast-enhanced (DCE) magnetic resonance imaging (MRI) and dual-phase 18F-FDG PET/CT in LABC patients receiving NAC.
METHODS
Thirty-nine patients with LABC underwent DCE-MRI and 18F-FDG PET/CT at baseline, and 38 after
2-3 cycles of NAC (interim). Tumor diameter, spherical volume (SV), angiographic volume, peak signal
intensity (PSI), the rapid and medium component of initial rise, and percentage of Type I, Type II, and
Type III curves were calculated. SUVmax, total lesion glycolysis (TLG), and metabolic tumor volume
(MTV) were measured using adaptive (adp) and 42% thresholding methods in whole-body and late
prone images. Baseline and interim studies calculated percentage changes and compared the surgery
results, PCR, and non-PCR. ROC curves were obtained to calculate the area under the curve for PCR
prediction. Optimal threshold values to discriminate between PCR and non-PCR were calculated.
RESULTS
Late prone images had higher sensitivity and specificity to detect the residual tumor (91%, 71.4%) than
MRI (84%, 37.5%). 18F-FDG PET/CT parameters differed significantly between PCR and non-PCR
groups, except for MTV-42 values. Optimal cutoff values were-65% for SV%, 73% for MTV-adp%, and
88% for TLG-adp%.
CONCLUSION
Semi-quantitative parameters for 18F-FDG PET/CT and volumetric changes obtained with DCE-MRI
can predict response to NAC. Percentage changes in SV, MTV, and TLG can identify non-responding
patients better than other parameters.
Introduction
Neoadjuvant chemotherapy (NAC) is essential in treating locally advanced breast cancer patients (LABC) to reduce tumor size and stage.[1] In breast cancer patients receiving NAC, pathological complete response (PCR) is an important prognostic indicator for long-term diseasefree and overall survival.[2,3] Prediction of response to NAC is critical at an early stage. In patients who do not respond to NAC, it is possible to change ineffective chemotherapy to minimize its toxic effects and prevent unnecessary costs. Successful results have been obtained in predicting the response to NAC with 18F-FDG PET/CT, which evaluates the metabolic activity of the tumor. Routine PET/CT is performed in the supine position. It has been shown that dual-time imaging in the prone position contributes to evaluating primary tumors in breast cancer patients.[4-6] Dynamic contrast-enhanced (DCE) magnetic resonance imaging (MRI) of the breast is also an available method that offers high diagnostic accuracy in primary tumor therapy response assessment.[7-10]The purpose of this prospective study was to investigate the success of dual time supine prone position 18F-FDG PET/CT and DCE-MRI in predicting NAC response in patients with LABC.
Methods
Research Ethics Standards ComplianceOur institute ethics committee approved this study (GO 13/45-29). The written informed consent form was obtained from the patients.
Study Cohort
We included patients diagnosed with LABC and
planned to receive NAC. Patients Stage IIB, IIIA, IIIB,
or IIIC diseases were included according to the American
Joint Committee on Cancer 7th edition.[11] Patients
were scanned with 18F-FDG PET/CT and DCE-MRI
before treatment (baseline), after 2-3 cycles of NAC (interim),
and after the end of treatment, before surgery.
We did not have patients with dose infiltration, suboptimal image quality, and a feature that would prevent PET/CT or MRI. Breast cancer diagnosis in all patients was confirmed histopathologically from biopsy materials. We recorded the size of the residual tumor from the pathology results of patients who underwent a mastectomy after NAC. We accepted the absence of invasive tumor in the surgical specimen as a complete pathological response, including carcinoma in situ.[12-14] We grouped the patients as those with a complete pathological response (PCR) or residual tumor according to the results of the histopathological evaluation (non-PCR).
Imaging Protocol
DCE MRI and 18F-FDG PET/CT have been performed
sequentially within 3 days (0-6 days).
Whole-Body 18F-FDG PET/CT Imaging
A dedicated PET/CT scanner (GE Medical Systems
Discovery ST PET/CT scanner, LLC 3000 N, Grandview
Blvd, Waukesha, Wisconsin, USA) was used for
18F-FDG PET/CT imaging. All patients were requested
to fast for at least 4-6 h before the PET/CT examination,
and their blood glucose levels were ≤180 mg/dl before
the 18F-FDG injection. Patients were scanned from the
skull base to the mid-thigh in the supine position, at six
to seven-bed positions (3 min per bed position) with
a 128×128 matrix. Iterative image processing was applied
to the images (2 iterations, 21 subsets). A lowdose
CT scan (4-slice, 120 kV, 300 mA) was obtained
for attenuation correction and anatomic localization.
Late Prone Imaging
We produced a dense sponge material coil for PET/CT
prone imaging based on the breast MRI unit's breast
coil. We have optimized its dimensions so that the patient
is not trapped in the PET/CT gantry. Late prone
images were obtained using that breast coil. In baseline
PET/CT late prone images, FDG uptake time was a median
of 142 min (99-191 min), and in interim late prone
images, FDG uptake time was 126.5 min (88-199 min).
MRI
MRI was performed on a 1.5 Tesla (General Electric)
device using an 8-channel breast coil. Pre-contrast
axial T1W (3 mm), axial (3 mm), and sagittal (4 mm)
T2 fat-suppressed STIR sequences were obtained in
the prone position. After intravenous administration
of gadolinium contrast agent (0.5 mmol/kg), 6 times
T1W (3 mm) fat-suppressed gradient echo dynamic
sequences in the axial plane were obtained. After the
extraction images were obtained, AngioMap and 3D
reconstructed images were obtained using Computer-
Aided Diagnosis (CADstream) software.
Data Analysis
Data Analysis in 18F-FDG PET/CT
Visual evaluation
Two nuclear medicine physicians with over 20 years
of expertise and a research assistant evaluated the images
at the AW-46 workstation with a consensus. We recorded the localization and primary tumor focus and
excluded patients with distant metastases.
Semi-quantitative Analysis
FDG PET/CT whole-body and late prone imaging
We calculated the tumor's SUVmax, SUVmean, and SULpeak
values. Metabolic volumes (MTVs) were measured
with VOI. To measure MTV, we used two different evaluation
methods: The volume of the lesion measured
using the threshold value of 42% of the SUVmax (MTV-
42) and the volume of the metabolically active part of
the tumor visually (MTV-adp).[15] We calculated total
lesion glycolysis (TLG) using SUVmean (bw)×MTVs formula.
The percentage change of all measured numerical
parameters after 2-3 cycles was calculated according
to the following formula (% change=value after 2-3
cycles of chemotherapy-baseline/baseline value×100).
Data Analysis in MRI
Two experienced breast radiologists with over 20 years
of expertise performed the visual and semi-quantitative
analysis of the MRI images. Subtraction image
was obtained by subtracting the images obtained before
and after intravenous gadolinium. Contrast areas
were detected. Tumor size, volume, and time-contrast
curves were obtained using AngioMap and 3D reconstructed
images using CADstream software.
Parameters Measured by MRI
(1) Number of tumors, (2) three dimensions, (3) spherical
volume (SV=length × height × thickness×0.52), (4)
perfusion volume (angiovolume [AV]), (5) time-contrast
curves. a-Type 1-2-3 contrast enhancement percentages.
b-Percentages of "rapid" and "medium" at the
beginning of the contrast curve. c-PSI (PSI, maximum
value of the contrast curve). The parameters change after
2-3 cycles of chemotherapy was calculated according
to the formula used in PET/CT. The difference values
were calculated since Types I, II, and III, and "rapid"
and "medium" values were given as percentages.
Statistical Analysis
The conformity of the variables to the normal distribution
was examined with the Kolmogorov-Smirnov
test. Continuous variables were expressed as median
(min-max) and mean with standard deviation. The parameters
calculated in the whole-body and late studies
were compared using parametric or non-parametric
tests. As a non-parametric test, Kruskal-Wallis analysis
(K-W) and Jonckheere-Terpstra (J-P) trend analysis
were performed in multiple groups. Chi-square, Fisher, t-test, or Mann-Whitney U tests were used when examining
the response to NAC with univariate analyses.
The diagnostic decision-making properties of the calculated
parameters in predicting the surgical response
were analyzed by ROC curve analysis. In the presence
of significant threshold values, the sensitivity, specificity,
and positive and negative predictive values were calculated.
p<0.05 was considered statistically significant.
Statistical analyses were performed using SPSS 18.
Results
Study CohortWe evaluated baseline 18F-FDG PET/CT images of 46 patients (mean age 46±10 years) before NAC. Two patients were excluded from the study later because they did not come for imaging after the baseline imaging. One patient died of colitis after the first course, and another patient progressed while chemotherapy was continuing. Two patients were excluded due to liver and lung metastasis. One patient did not undergo surgery voluntarily, although the imaging was completed. As a result, the data of 39 patients were analyzed to evaluate NAC response. The histopathological diagnosis of 39 patients was invasive ductal carcinoma; tumor size ranged from 22 to 120 mm (median=57 mm). PCR was observed in 12 patients (30.8%), while residual tumors were detected in 27 patients (69.2%).
The clinical data of patients are given in Table 1.
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Table 1: Clinical information of patients
NAC Regimen
The chemotherapy regimen included four cycles of
adriamycin and cyclophosphamide every 21 days, followed
by weekly paclitaxel for 12 weeks. Patients with
HER2+breast cancer also received concomitant weekly
trastuzumab with paclitaxel.
Surgical Response Assessment
All patients underwent modified radical mastectomy
following the end of NAC. The complete pathological
response was detected in the primary tumor in 12 patients
(30.8%). In the remaining 27 patients (69.2%),
residual tumors ranging in size from 5 to 70 mm (median:
25 mm) were observed.
Visual Evaluation
18F-FDG PET/CT
We evaluated the primary tumor"s whole-body (n=39)
and late prone (n=37) images at baseline. In 19 patients,
additional tumors were detected with late prone images.
After NAC, while the size and metabolic activity
of the lesions decreased at different levels, no primary tumor was observed in whole-body images in six patients
and late images in three patients. In one patient,
the metabolic activity of the tumor increased. Two unifocal
and one multifocal tumor not observed in wholebody
images were detected in three patients with late
images. We performed whole-body imaging in 34 patients
at the end of NAC. Late images were present in 32
patients. While the residual tumor was observed in 19
patients with whole-body images, the residual tumor
was detected in 24 patients with late images. Compared
with the surgical response, the sensitivity, specificity,
and positive and negative predictive values of wholebody
imaging and late prone imaging were 62.5% versus
91.3%, 80% versus 71.4%, 62.6% versus 91.3%, and
47% versus 62.5%, respectively. While the highest sensitivity
and positive and negative predictive values were
obtained in late images, the specificity value was high
with whole-body images detecting residual tumors.
Contrast-enhanced Dynamic MRI
Baseline DCE-MRI was obtained in 39 patients. While a
single tumor focus (57 mm [17-200 mm]) was observed
in 60% of the patients, two tumor foci were observed
in 35%, and more than 2 tumor foci were observed in
5% of the patients. A significant reduction in tumor size was observed in the interim study (32 mm [5-100 mm])
(p<0.0001), and the major focus disappeared in one of
the patients with two tumor foci. After NAC, the primary
lesion completely disappeared in seven patients, while the
lesion size (27 mm [11-85 mm]) decreased significantly
in other patients. According to the surgical outcome, the
sensitivity, specificity, and positive and negative predictive
values of MRI for residual tumors were 84%, 37.5%,
80.7%, and 42.8%, respectively, Figure 1.
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Quantitative Evaluation
18F-FDG PET/CT
Interim images of 38 patients were evaluated. The %
change values between the interim and baseline images
are given in Table 2.
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Response to NAC
When the % changes were compared to surgical response,
%TLG-adp and % MTV-adp were significantly
different according to surgical response in the wholebody
and late images. These values showed more variation
in the group with the complete surgical response.
We found no difference in whole-body and late prone
images for %MTV-42.
DCE MRI
Interim MRI was performed on 38 patients. Baseline
and interim MRI parameters were not significantly different
between receptor subgroups and grades. When
the PCR and non-PCR groups were compared, rapid
(p=0.044), medium (p=0.044), and peak (p=0.034) values
were statistically different and changed on baseline
MRI. Long diameter (p=0.035) and volume (p=0.02)
in interim MRI were significantly lower in the PCR
group. MRI parameters changes are given in Table 3.
When the % change values calculated in 34 patients
were compared according to the surgical response,
long diameter (p=0.041), volume (0.001), and curve
peak (0.03) showed more changes in the PCR group
compared to the non-PCR group, Figure 2.
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Predictive Value of Parameters
Between the interim and baseline studies, percent change
values of PSI and SV from MRI, SULpeak, MTV-adp, and
TLG-adp from PET/CT could predict PCR with high
accuracy. The list of parameters for which ROC analysis
was performed to evaluate NAC response and whose
p-value was significant is given in Table 4. In addition,
the sensitivity, specificity, positive and negative predictive
values, and accuracy values calculated for the determined
threshold values are given in the same table (Table 4).
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Discussion
This study compared 18F-FDG PET/CT and DCE-MRI parameters in predicting NAC response in patients with LABC. We compared baseline, after the second or third cycle of NAC, and at the end of NAC, pre-surgical imaging, and histopathological results.When comparing standard whole-body imaging with late prone imaging in the visual evaluation of 18FFDG PET/CT, we found that the assessment of primary tumor was most successfully performed with late prone images. The breast was evaluated more easily in the prone position using a breast coil. We detected additional primary lesions in late imaging due to the increase in 18F-FDG uptake in the tumor with time, the decrease in the level of 18F-FDG in the normal breast tissue, and the increase in the tumor/ground activity contrast. In primary tumor evaluation, prone imaging is recommended to increase 18F-FDG PET/ CT sensitivity. Other authors have also described the use of breast coils which are also used to fuse MRI/ PET images to increase the specificity of MRI images. [6,16] Late prone 18F-FDG PET/CT images were more compatible with MRI. It is known that the late component of dual imaging increases not only specificity but also sensitivity, and our finding is consistent with the literature.[4,17]
While different tumor metabolic activity reduction levels were observed with interim 18F-FDG PET/ CT, we detected a reduction in lesion size with MRI. When the post-NAC, pre-surgery, 18F-FDG PET/CT, and MRI images were compared with the histopathological results, the sensitivity of MRI was higher than that of whole-body supine 18F-FDG PET/CT images. However, late images were more successful than MRI. Positive predictive values were higher than negative predictive values.
It is known that quantitative parameters are more successful than visual evaluation. The changes in SUVmax values were examined most frequently in the studies.[18-20] TLG and MTVs changes have been used. [21,22] In some of the studies, the predictive value of TLG was reported to be higher than SUVmax values. [22] On the other hand, while a study reports that SUV max change is a more significant predictor than TLG change, a study also says that both MTVs changes are equally successful.[21,23] The % TLG-adp and %MTV-adp values showed significant differences between the PCR and non-PCR groups in whole-body and late images. No statistically significant difference was found with %MTV-42. We found the "adapted" method superior to the method in which 42% was used as the threshold value. In the literature, parameters are generally used to predict NAC response. In this study, we also examined TLG and MTV differently. In a meta-analysis of 19 articles and 920 patients, the sensitivity of PET/CT was 84%, the specificity was 66%, the positive predictive value was 50%, and the negative predictive value was 91%.[24] In the articles in this meta-analysis, the sensitivity ranged from 33% to 100%, while the specificity values were reported between 30% and 100%. In another metaanalysis, which included 745 patients and evaluated 15 studies, the values were 80.5%, 78.8%, 79.8%, and 79.5%, respectively.[25] Values ranging from 40% to 88% in SUVmax have been reported to predict NAC in these studies. One of the reasons why different values were detected is that imaging timing for the prediction of NAC response is not standard. Some authors imaged after one cycle, while others imaged after 2 or 3 cycles. For ease of comparison, we studied after 2-3 cycles, which is the most frequently used time in our study. Contrary to this, Humbert et al.[26] suggested that a SUVmax <2.1 after the first cycle had an accuracy of 76%. The heterogeneity of the groups in the studies, the differences in PET/CT imaging times, and the lack of many patients lead to different results.
The volume change measured in standard MRI has been defined as a sensitive parameter in predicting NAC response. The contrast enhancement curve and dynamic parameters obtained by dynamic MRI with contrast provide information about the angiogenesis of the tumor. A study comparing MRI and 18F-FDG PET/CT in TN and non-TN breast tumors found that MRI enhancement kinetics and SUVmax change were correlated. It was emphasized that MRI measured angiogenesis/ perfusion and PET measured metabolism were correlated, which was more robust in the more aggressive TN group.[27] In a study comparing MRI and PET/CT, Pengel et al.[28] found the % SUVmax and tumor diameter change to be equally successful in predicting NAC. However, when analyzed according to receptor subgroups, the diameter change was significant only in the TN group, while the SUVmax change was significant in the TN and luminal groups. Using SUVmax and MRI enhancement parameters together, Lim et al.[29] showed that the combined enhancement curve (at least 6%) and SUVmax (at least 41%) change after one cure is a successful predictor of disease-free survival. A study comparing PET and MRI reported that both methods were not sensitive enough but had high specificity. SUVmax, SULmax, SULpeak, and TLG parameters of FDG PET/CT, and enhancement parameters of MRI were compared. While TLG did not differ between groups according to surgical response, SUV values differed; only SUVmax change was determined as an independent predictor in multivariate analysis.[23] In our study, the baseline PSI, % PSI change, and % SV change from MRI parameters differed in PCR and non-pCR groups. The highest predictive value among these parameters is % SV. Volume change was correlated with metabolic parameters, and the highest correlation was found between % MTV-adp and % TLG-adp. In addition, it has been reported that hybrid 18F-FDG PET/ MRI imaging may provide more satisfactory results than 18F-FDG PET and MRI for the early assessment of NAC response in patients with breast cancer.[30]
Limitations
Although the study started with 46 patients, we had to
exclude some patients due to a lack of data. Our study
group was heterogeneous as the response differed according
to the receptor groups. Separate statistical
evaluation according to receptor subgroups could not
be made due to the low number of patients.
Conclusion
Late prone imaging is successful in evaluating breast tumors; therefore, late imaging should be used in the late period in addition to standard whole-body imaging. Percentage changes in SV, MTV, and TLG can identify non-responding patients better than other parameters. There is no standard for when interim imaging to predict NAC response.Peer-review: Externally peer-reviewed.
Conflict of Interest: All authors declared no conflict of interest.
Ethics Committee Approval: The study was approved by the Hacettepe University Non-interventional Clinical Research Ethics Committee (no: GO 13/45-29, date: 23/01/2013).
Financial Support: None declared.
Authorship contributions: Concept - M.T., M.G.A., K.A., F.B.D., B.E.; Design - O.K., M.T., P.Ö.K., M.G.A., K.A., F.B.D., B.E.; Supervision - M.T., F.B.D., B.E.; Funding - None; Materials - None; Data collection and/or processing - M.T., P.Ö.K., M.G.A., K.A., F.B.D., B.E.; Data analysis and/or interpretation - O.K., M.T., B.E.; Literature search - O.K., M.T., K.A., B.E.; Writing - O.K., M.T., K.A., F.B.D., B.E.; Critical review - O.K., M.T., P.Ö.K., M.G.A., K.A., F.B.D., B.E.
References
1) Wolff AC, Davidson NE. Primary systemic therapy in
operable breast cancer. J Clin Oncol 2000;18(7):1558-69.
2) Fayanju OM, Ren Y, Thomas SM, Greenup RA, Plichta
JK, Rosenberger LH, et al. The clinical significance
of breast-only and node-only pathologic complete
response (pCR) after neoadjuvant chemotherapy
(NACT): A review of 20,000 breast cancer patients
in the National Cancer Data Base (NCDB). Ann Surg
2018;268(4):591-601.
3) Buzdar AU, Ibrahim NK, Francis D, Booser DJ,
Thomas ES, Theriault RL, et al. Significantly higher
pathologic complete remission rate after neoadjuvant
therapy with trastuzumab, paclitaxel, and epirubicin
chemotherapy: results of a randomized trial in human
epidermal growth factor receptor 2-positive operable
breast cancer. J Clin Oncol 2005;23(16):3676-85.
4) Imbriaco M, Caprio MG, Limite G, Pace L, De Falco
T, Capuano E, et al. Dual-time-point 18F-FDG PET/
CT versus dynamic breast MRI of suspicious breast
lesions. AJR Am J Roentgenol 2008;191(5):1323-30.
5) Malhotra A, Tincey S, Naidu V, Papagiorcopulo C,
Ghosh D, Tan PH, et al. Characterisation of MRI indeterminate
breast lesions using dedicated breast
PET and prone FDG PET-CT in patients with
breast cancer-a proof-of-concept study. J Pers Med
2020;10(4):148.
6) Abramson RG, Lambert KF, Jones-Jackson LB, Arlinghaus
LR, Williams J, Abramson VG, et al. Prone versus
supine breast FDG-PET/CT for assessing locoregional
disease distribution in locally advanced breast cancer.
Acad Radiol 2015;22(7):853-9.
7) Fowler AM, Mankoff DA, Joe BN. Imaging neoadjuvant
therapy response in breast cancer. Radiology
2017;285(2):358-75.
8) Schmitz AMT, Teixeira SC, Pengel KE, Loo CE, Vogel
WV, Wesseling J, et al. Monitoring tumor response
to neoadjuvant chemotherapy using MRI and 18FFDG
PET/CT in breast cancer subtypes. PLos One
2017;12(5):e0176782.
9) Gu YL, Pan SM, Ren J, Yang ZX, Jiang GQ. Role of
magnetic resonance imaging in detection of pathologic
complete remission in breast cancer patients
treated with neoadjuvant chemotherapy: a meta-analysis.
Clin Breast Cancer 2017;17(4):245-55.
10) Pahk K, Kim S, Choe JG. Early prediction of pathological
complete response in luminal B type neoadjuvant
chemotherapy-treated breast cancer patients: comparison
between interim 18F-FDG PET/CT and MRI.
Nucl Med Commun 2015;36(9):887-91.
11) Edge SB, Compton CC. The American Joint Committee
on Cancer: the 7th edition of the AJCC cancer staging
manual and the future of TNM. Ann Surg Oncol
2010;17(6):1471-4.
12) Cortazar P, Zhang L, Untch M, Mehta K, Costantino JP,
Wolmark N, et al. Pathological complete response and
long-term clinical benefit in breast cancer: the CTNeoBC
pooled analysis. Lancet 2014;384(9938):164-72.
13) Mazouni C, Peintinger F, Wan-Kau S, Andre F, Gonzalez-
Angulo AM, Symmans WF, et al. Residual ductal
carcinoma in situ in patients with complete eradication
of invasive breast cancer after neoadjuvant chemotherapy
does not adversely affect patient outcome. J Clin
Oncol 2007;25(19):2650-5.
14) Guarneri V, Broglio K, Kau SW, Cristofanilli M, Buzdar
AU, Valero V, et al. Prognostic value of pathologic
complete response after primary chemotherapy in relation
to hormone receptor status and other factors. J
Clin Oncol 2006;24(7):1037-44.
15) Kupik O, Akin S, Tuncel M, Eren G, Türker A, Kars
A, et al. Comparison of clinical and PET-derived
prognostic factors in patients with non-Hodgkin lymphoma:
a special emphasis on bone marrow involvement.
Nucl Med Commun 2020;41:540-9.
16) Moy L, Ponzo F, Noz ME, Maguire GQ Jr, Murphy-
Walcott AD, Deans AE, et al. Improving specificity of breast MRI using prone PET and fused MRI and PET
3D volume datasets. J Nucl Med 2007;48(4):528-37.
17) Schillaci O. Use of dual-point fluorodeoxyglucose
imaging to enhance sensitivity and specificity. Semin
Nucl Med 2012;42(4):267-80.
18) Humbert O, Berriolo-Riedinger A, Riedinger JM,
Coudert B, Arnould L, Cochet A, et al. Changes in 18FFDG
tumor metabolism after a first course of neoadjuvant
chemotherapy in breast cancer: influence of
tumor subtypes. Ann Oncol 2012;23(10):2572-7.
19) Groheux D, Giacchetti S, Hatt M, Marty M, Vercellino
L, de Roquancourt A, et al. HER2-overexpressing
breast cancer: FDG uptake after two cycles of chemotherapy
predicts the outcome of neoadjuvant treatment.
Br J Cancer 2013;109(5):1157-64.
20) Andrade WP, Lima EN, Osório CA, do Socorro Maciel
M, Baiocchi G, Bitencourt AG, et al. Can FDG-PET/CT
predict early response to neoadjuvant chemotherapy in
breast cancer? Eur J Surg Oncol 2013;39(12):1358-63.
21) Lee SM, Bae SK, Kim TH, Yoon HK, Jung SJ, Park JS,
et al. Value of 18F-FDG PET/CT for early prediction of
pathologic response (by residual cancer burden criteria)
of locally advanced breast cancer to neoadjuvant
chemotherapy. Clin Nucl Med 2014;39(10):882-6.
22) Hatt M, Groheux D, Martineau A, Espié M, Hindié E,
Giacchetti S, et al. Comparison between 18F-FDG PET
image-derived indices for early prediction of response
to neoadjuvant chemotherapy in breast cancer. J Nucl
Med 2013;54:341-9.
23) Tateishi U, Miyake M, Nagaoka T, Terauchi T, Kubota
K, Kinoshita T, et al. Neoadjuvant chemotherapy in
breast cancer: prediction of pathologic response with
PET/CT and dynamic contrast-enhanced MR imaging-
-prospective assessment. Radiology 2012;263(1):53-63.
24) Wang Y, Zhang C, Liu J, Huang G. Is 18F-FDG PET
accurate to predict neoadjuvant therapy response in
breast cancer? A meta-analysis. Breast Cancer Res
Treat 2012;131(2):357-69.
25) Mghanga FP, Lan X, Bakari KH, Li C, Zhang Y. Fluorine-
18 fluorodeoxyglucose positron emission tomography-
computed tomography in monitoring the response
of breast cancer to neoadjuvant chemotherapy:
a meta-analysis. Clin Breast Cancer 2013;13(4):271-9.
26) Humbert O, Berriolo-Riedinger A, Cochet A, Gauthier
M, Charon-Barra C, Guiu S, et al. Prognostic
relevance at 5 years of the early monitoring of neoadjuvant
chemotherapy using (18)F-FDG PET in luminal
HER2-negative breast cancer. Eur J Nucl Med Mol
Imaging 2014;41(3):416-27.
27) Bolouri MS, Elias SG, Wisner DJ, Behr SC, Hawkins
RA, Suzuki SA, et al. Triple-negative and non-triplenegative
invasive breast cancer: association between
MR and fluorine 18 fluorodeoxyglucose PET imaging.
Radiology 2013;269(2):354-61.
28) Pengel KE, Koolen BB, Loo CE, Vogel WV, Wesseling
J, Lips EH, et al. Combined use of ¹?F-FDG PET/CT
and MRI for response monitoring of breast cancer
during neoadjuvant chemotherapy. Eur J Nucl Med
Mol Imaging 2014;41(8):1515-24.