nach oben

European Journal of Nuclear Medicine and Molecular Imaging

Erschienen in:

Open Access 02.08.2018 | Original Article

Prognostic value of posttreatment ¹⁸F-FDG PET/CT and predictors of metabolic response to therapy in patients with locally advanced cervical cancer treated with concomitant chemoradiation therapy: an analysis of intensity- and volume-based PET parameters

verfasst von: Giacomo Maria Lima, Antonella Matti, Giulio Vara, Giulia Dondi, Nicoletta Naselli, Eugenia Maria De Crescenzo, Alessio Giuseppe Morganti, Anna Myriam Perrone, Pierandrea De Iaco, Cristina Nanni, Stefano Fanti

Erschienen in: European Journal of Nuclear Medicine and Molecular Imaging | Ausgabe 12/2018

Abstract

Purpose

To investigate the prognostic value of posttreatment ¹⁸F-FDG PET/CT in patients with locally advanced cervical cancer (LACC) treated with concomitant chemoradiation therapy (CCRT). The secondary aim was to assess the possible role of intensity-based and volume-based PET parameters including SUVmax, SUVmean, MTV and TLG, and clinical parameters including age, pathology, FIGO stage and nodal involvement as factors predicting response to treatment.

Methods

This retrospective study included 82 patients affected by LACC treated with CCRT. All patients underwent ¹⁸F-FDG PET/CT both before and after treatment. The posttreatment PET/CT scans were used to classify patients as complete metabolic responders (CMR) or non-complete metabolic responders (N-CMR) according to the EORTC criteria. Kaplan-Meier analysis was used to evaluate differences in overall survival (OS) between the CMR and N-CMR groups. Student’s t test, Pearson’s chi-squared test and logistic regression were used to investigate the possible value of PET and clinical parameters as predictors of metabolic response to therapy.

Results

KaplanMeier analysis showed a highly significant difference in OS between the CMR and N-CMR groups (log-rank test p < 0.0001). Significant independent predictors of response to therapy were MTV (p = 0.019, odds ratio = 1.015, 95% CI = 1.002–1.028, Nagelkerke R² = 0.110), TLG (p = 0.045, odds ratio = 1.001, 95% CI = 1.000–1.002, Nagelkerke R² = 0.081) and nodal involvement (p = 0.088, odds ratio = 2.361, 95% CI = 0.879–6.343, Nagelkerke R² = 0.051).

Conclusion

Introduction

Background

Cervical cancer is the fourth most common cancer in women with an estimated 528,000 new cases reported in 2012. A major part (around 85% of cases) of the global burden occurs in developing countries [1, 2]. This is due to a lack of screening that is the most important public health intervention to reduce both the incidence and mortality of the disease [3‐6]. Cervical tumours are staged using the International Federation of Gynecology and Obstetrics (FIGO) classification [7]. Surgery is considered only in patients with earlier stages of cervical cancer (up to FIGO stage IIa) without risk factors. Otherwise the standard of care for locally advanced cervical cancer (LACC; FIGO Ib2–IVa) is concomitant chemoradiation therapy (CCRT) [8].

¹⁸F-FDG PET/CT has a well-established role in the management of patients with cervical cancer, especially in staging, radiotherapy planning, response assessment and recurrence of LACC as stated in American National Comprehensive Cancer Network (NCCN) guidelines [9‐11].

Detection, staging and radiation therapy planning

Clinical suspicion of cervical cancer is confirmed by pathology findings, and imaging examinations are routinely used for locoregional and distance staging and follow-up [8]. Pelvic MRI imaging is the best tool to assess locoregional disease. It can evaluate tumour size, stromal penetration and parametrial invasion [12, 13] and the potential involvement of the bladder, rectum and pelvic sidewall [14]. CT and PET/CT imaging are used for whole-body staging [13]. PET/CT has a limited role in local primary staging [15]. The most important role is in the detection of distant metastasis and pathological lymph nodes with better performance than CT, especially for nonpathological enlarged lymph node metastases [16, 17]. In patients with LACC, PET/CT is often used to plan the correct radiation therapy field. PET/CT has been shown to influence external-beam radiotherapy planning by allowing modification of the treatment field and customization of the radiation dose [18‐21].

Treatment response

Depending on stage, cervical carcinoma is treated with surgery, radiation therapy or chemotherapy. Several studies have shown the value of PET/CT in the assessment of treatment response [22, 23]. With regard to chemoradiation therapy, the NCCN guidelines recommend that PET/CT be performed 3–6 months after the end of treatment. The key role of posttreatment PET/CT is the early detection of locoregional therapy failure that indicates the need for salvage therapy, and the identification of unsuspected asymptomatic distant metastasis. Radiotherapy-induced inflammatory changes can lead to false-positive ¹⁸F-FDG uptake, and thus the timing of the posttreatment PET/CT examination is crucial [24‐26]. Persistent FDG uptake at the end of chemoradiotherapy is associated with a poor 5-year survival prognosis [22, 27]. The role of interim PET performed during radiation therapy is not yet unequivocally defined [28].

Recurrent disease

The accurate localization of recurrent disease is critical and guides management and the selection of appropriate therapies. In these patients, earlier intervention leads to a better outcome [29]. In this setting, the role of PET/CT is to localize the recurrence so that patients can be properly referred to surgery (in those with pelvic recurrence) or salvage radiotherapy (in those with extrapelvic recurrence) [30‐32].

Aim

The aim of this study was to determine the prognostic value of posttreatment ¹⁸F-FDG PET/CT in patients with LACC treated with CCRT. For this purpose, the prognostic value of the criteria developed by the European Organization for Research and Treatment of Cancer (EORTC criteria) was evaluated with a survival analysis. We also assessed the possible role of pretreatment intensity-based and volume-based PET parameters and clinical data including maximum and mean standardized uptake values (SUVmax, SUVmean), metabolic tumour volume (MTV), total lesion glycolysis (TLG), age, pathology findings, FIGO stage and nodal involvement as factors predicting response to treatment.

Materials and methods

Population characteristics

The clinical records of all patients referred to our centre for cervical cancer from January 2008 to January 2018 were analysed. Among these patients, 82 affected by LACC and treated with CCRT were retrospectively enrolled. Other inclusion criteria were: proven diagnosis of cervical cancer, FIGO stage IIA–IVA (with or without positive paraaortic nodes), availability of full clinical history and follow-up data, CCRT to the pelvis (with or without an external beam boost to positive pelvic or para-aortic nodes together with a brachytherapy boost to the tumour as a single treatment option), and ¹⁸F-FDG PET/CT scans performed before and after treatment. Exclusion criteria were: previous surgical treatment of the cervical tumour, and FIGO stage IB2 (because the treatment is not unequivocally defined). After the end of therapy all patients were clinically evaluated by a gynaecologist (physical examination and ultrasonography or MRI where indicated). All patients gave permission to use their clinical data for scientific purposes.

Radiopharmaceuticals and imaging protocol

Each patient underwent a ¹⁸FFDG PET/CT for both staging and restaging at least 3 months after the end of treatment (range 3–12 months, mean 6.7 ± 3.0 months). All PET/CT scans were reviewed by two experienced nuclear medicine physicians.

Whole-body FDG PET/CT was performed using standard procedures. Briefly, 3 MBq/kg of ¹⁸F-FDG was intravenously injected. All patients were required to fast for 6 h. The uptake time was 60 min in all patients. Images were acquired on a 3-D tomograph (Discovery STE; GE) for 2 min per bed position. A low-dose CT scan (120 kV, 80 mA) was performed both for attenuation correction and to provide an anatomical map. PET images were reconstructed using an iterative 3-D ordered subsets expectation maximization method with two iterations and 20 subsets, followed by smoothing (with a 6-mm 3-D gaussian kernel) with CT-based attenuation, scatter and random coincidence event correction.

Image analysis and interpretation criteria

For each scan, SUVmax, SUVmean, MTV and TLG were measured both in the primary cervical lesion and in nodal or distant lesions (when present).

MTV measurement was calculated on FDG PET/CT images using a semiquantitative (40% threshold) analysis, corrected with visual evaluation of the tracer uptake in the neoplastic lesions to avoid missing tumour at the boundaries. SUVmax and SUVmean normalized to body weight were calculated within the MTV defined as above. TLG values of the primary lesions were calculated as the product of MTV and SUVmean [33]. SUVmean, MTV and TLG were measured both in the primary lesion and in distant lesions. The final MTV value was the sum of the MTVs of every lesion and the final TLG value was the sum of the TLGs of every lesion. When the bladder (filled with radioactive urine even after voiding) was very close to the primary lesion, visual correction of the adjacent region of interest margin was necessary.

The posttreatment PET/CT scans were used to classify patient responses into four categories according to EORTC criteria: complete metabolic response (CMR, no FDG uptake within the tumour volume), partial metabolic response (PMR, SUVmax reduction greater than 25% after treatment), stable metabolic disease (SMD, SUVmax increase or decrease less than 25%), progressive metabolic disease (PMD, SUVmax increase greater than 25% or increase in the extension of tumour uptake greater than 20% in the longest dimension or the appearance of new ¹⁸F-FDG uptake) [34]. Patients with PMR, SMD and PMD were then grouped as non-complete metabolic responders (N-CMR) (Fig. 1).

Chemoradiotherapy

External beam radiotherapy

All patients underwent pelvic 3-D conformal external beam radiotherapy. The prescribed dose to the pelvis was 46 Gy in fractions of 2 Gy. The treatment volumes were delineated as follows. The clinical target volume (CTV) was defined as the gross tumour volume, uterus, parametria, upper third of the vagina, obturator, and presacral, iliac (common, internal and external) and paraaortic lymph nodes (if PET-positive) with an expansion of 7 mm. The CTV boost was defined as lymphadenopathies with high FDG uptake plus an expansion of 7 mm. The planning target volumes (PTV and PTV boost) were obtained by adding a 1-cm CTV to PTV isotropic expansion.

Chemotherapy

Cisplatin (40 mg/m²) was administered once a week during the period of external radiotherapy.

Brachytherapy

After radiochemotherapy all patients underwent a brachytherapy boost, with the high dose-rate or pulsed dose rate technique. The dose was prescribed according to the International Commission on Radiation Units (ICRU) Report 38 recommendations.

Statistical analysis

All statistical analyses were performed using SPSS version 24 (IBM Corp., Armonk, NY). Kaplan-Meier analysis was used to evaluate differences in overall survival (OS) between the CMR and N-CMR groups and the log-rank test was used to evaluate the significance of differences between survival curves [35]. We also investigated whether SUVmax, SUVmean, MTV and TLG (measured on the pretreatment scan), age, pathology findings, FIGO stage and nodal involvement could predict the metabolic response to therapy. According to the data distribution, Student’s t test was used to compare the means of continuous variables, and Pearson’s chi-squared test was used to compare the frequencies of categorical variables. Univariate logistic regression was used to evaluate the associations between independent variables and the metabolic response to therapy (CMR vs. N-CMR, dependent variable) [36]. Independent variables are reported in terms of odds ratios (OR) and their 95% confidence intervals (CI). Significant independent variables (p < 0.1) were included in the multivariate backward logistic regression.

Results

The main characteristics of the study population, including age, body mass index, pathology, FIGO stage, nodal involvement and follow-up, are presented in Table 1. Of the 82 patients, 23 died during the observation period. The timing of the posttherapy PET/CT scans did not differ significantly between the CMR group (6.9 ± 2.7 months) and the non-CMR group (6.5 ± 3.5 months).

Table 1

Characteristics of the 82 enrolled patients

Characteristic	Value
Clinical data, n (range)
Age (years), mean (range)	61.3 (28–94)
BMI (kg/m²), mean (range)	25.4 (18–42)
Died during observation period, n (%)	23 (28)
FIGO stage, n (%)
IIA	3 (3.7)
IIB	54 (65.8)
IIIA	4 (4.9)
IIIB	12 (14.6)
IVA	9 (11.0)
Nodal involvement, n (%)
Nodal disease at staging	44 (53.6)
Lumboaortic nodal disease at staging	11 (13.4)
Pathology, n (%)
Squamous	64 (78)
Adenocarcinoma	15 (18.3)
Other	3 (3.7)
Follow-up (months), mean (range)	50.8 (8.6–98.4)

According to EORTC criteria, of the 82 patients, 57 had CMR, 8 had PMR, 2 had SMD and 15 had PMD. The N-CMR group (those with PMR, SMD and PMD) included 25 patients. All patients were also clinically evaluated after chemoradiation treatment. Of the 57 patients in the CMR group, 48 were classified as clinical responders (84.2% concordance), and of the 25 patients in the N-CMR group, 10 were classified as clinical nonresponders (40% concordance). Even though clinical response is routinely assessed in LACC patients, in our study, the PET/CT scan led to reclassification of 24 of the 82 patients (29.3%).

Survival analysis

KaplanMeier analysis showed a highly significant difference in OS between the CMR and N-CMR groups (log-rank test p < 0.0001; Fig. 2). Of the 57 patients in the CMR group and the 25 patients in the N-CMR group, 9 (15.78%) and 14 (56.00%), respectively, died during follow-up.

Comparison of variables between CMR and N-CMR groups

Student’s t test and Pearson’s chi-squared test results are presented in Tables 2 and 3, respectively. The mean pretreatment MTV and TLG values were significantly different between the CMR and N-CMR groups (p = 0.008 and p = 0.046). The mean MTV and TLG values were 35.74 ± 31.23 cm³ and 360.02 ± 427.84 in the CMR group and 62.49 ± 57.86 cm³ and 621.37 ± 566.54 in the N-CMR group, respectively. The frequencies of nodal involvement were also different between the CMR and N-CMR groups (27 of 57 patients, 47.36%, and 17 of 25 patients, 68.00%, respectively; p = 0.085). There were no significant differences in the mean SUVmax, SUVmean and age between the two groups (p = 0.292, p = 0.624, p = 0.778, respectively), nor in the frequencies of pathology findings, FIGO stage or lumboaortic nodal involvement (p = 0.936, p = 0.236 and p = 0.649, respectively).

Table 2

Comparison of continuous variables between the CMR and N-CMR groups (Student’s t test results)

Variable	Group		p value
Variable	CMR	N-CMR	p value
Metabolic PET parameters
SUVmax	16.57 ± 10.18	18.73 ± 7.58	0.292
SUVmean	9.27 ± 4.83	9.73 ± 3.33	0.626
MTV (cm³)	35.74 ± 31.23	62.49 ± 57.86	0.008
TLG	360.02 ± 427.84	621.37 ± 566.54	0.046
Clinical parameters
Age at diagnosis (years)	56.8 ± 13.5	55.8 ± 16.1	0.763

The data presented are means ± SD

Table 3

Comparison of categorical variables between the CMR and N-CMR groups (Pearson’s chi-squared test results)

Variable	Group		p value
Variable	CMR	N-CMR	p value
Pathology
SCC	44 (53.7)	20 (24.4)	0.936
AC	11 (13.4)	4 (4.9)
Non-SCC, non-AC	2 (2.4)	1 (1.2)
FIGO stage
IIA	1 (1.8)	2 (8.0)	0.236
IIB	37 (64.9)	17 (68.0)
IIIA	4 (7.0)	0 (0.0)
IIIB	10 (17.5)	2 (8.0)
IVA	5 (8.8)	4 (16.0)
Nodal status
LN (any site)
LN+	27 (47.4)	17 (68.0)	0.085
LN−	30 (52.6)	8 (32.0)	0.085
LN (lumboaortic)
LN+	7 (12.3)	4 (16.0)	0.649
LN−	50 (87.7)	21 (84.0)	0.649

The data presented are number (%) of patients

SCC squamous cell carcinoma, AC adenocarcinoma, LN lymph nodes

Logistic regression

All the variables were tested in a univariate logistic regression analysis to evaluate their relationship with the metabolic response to therapy (Table 4).

Table 4

Logistic regression analysis: associations with metabolic response to treatment

Independent variables	p value	Odds Ratio	95% CI	Nagelkerke R²
MTV	0.019	1.015	1.002–1.028	0.110
TLG	0.045	1.001	1.000–1.002	0.081
SUVmax	0.349	–	–	–
SUVmean	0.669	–	–	–
Age	0.759	–	–	–
FIGO stage	0.692	–	–	–
SCC	0.936	–	–	–
AC	0.729	–	–	–
Non-SCC, non-AC	0.939	–	–	–
LN involvement
Any site	0.088	2.361	0.879–6.343	0.051
Lumboaortic	0.650	–	–	–

Variables with values in bold are independent predictors of response to therapy assuming significance at p < 0.1

SCC squamous cell carcinoma, AC adenocarcinoma, LN lymph nodes

Accepting p < 0.1 as the level of significance, the only independent predictors of response to therapy were MTV (p = 0.019, OR = 1.015, 95% CI = 1.002–1.028, Nagelkerke R² = 0.110), TLG (p = 0.045, OR = 1.001, 95% CI = 1.000–1.002, Nagelkerke R² = 0.081) and nodal involvement (PET-positive lymph nodes at any site; p = 0.088, OR = 2.361, 95% CI = 0.879–6.343, Nagelkerke R² = 0.051). It was not possible to perform a multivariate logistic regression using both MTV and TLG as variables because, as expected, they were correlated (correlation test p < 0.0001, Pearson correlation = 0.786). MTV and nodal involvement were included in the multivariate backward logistic regression. However, the best logistic model was a model with only MTV as independent variable.

Discussion

SUVmax is the most used PET parameter in the restaging of LACC patients. In our study, the EORTC classification was able to predict the OS in these patients, as demonstrated by Kaplan-Meier survival analysis. Patients with CMR after CCRT showed a better OS than patients with N-CMR (PMR, SMD, PMD). This observation could lead physicians to consider other adjuvant treatments in N-CMR patients (e.g. adjuvant chemotherapy) to improve prognosis and survival. Our findings are similar to those reported by Grigsby et al. [22]. In their study they evaluated 152 LACC patients who had undergone FDG PET/CT before and after treatment, : a CMR on PET was predictive of good survival (92% 5-year survival) while a PMR was predictive of poor survival (46% 5-year survival) and a PMD in 18 patients was predictive of death from cervical cancer in 17. These results indicating a good clinical outcome in LACC patients with a CMR to treatment as assessed by PET/CT were confirmed by Beriwal et al. [25] in a study in 155 patients.

We then sought to determine if some pretreatment PET parameters (SUVmax, SUVmean, MTV and TLG) and clinical parameters (age, pathology findings, FIGO stage and nodal involvement) could predict response to treatment. Although numerous published studies have investigated the prognostic value of FDG PET/CT in LACC, few of them assessed the role of volume-based and intensity-based PET parameters including MTV and TLG. In our cohort of patients, the statistical analysis indicated that pretreatment MTV and TLG and nodal involvement were predictors of response to therapy (MTV OR = 1.015, TLG OR = 1.001, nodal involvement OR = 2.361). Higher MTV and TLG values increase the risk of a non-complete metabolic response to CCRT. The presence of pretreatment PET-positive lymph nodes also increases the risk of a non-complete metabolic response to therapy. Pretreatment MTV was found to be the most significant predictor. However, the Nagelkerke R² value in the univariate logistic regression analysis of the association between MTV and metabolic response was 0.110. This value indicates that the added value of MTV in predicting response to therapy is low. This could be due to the fact that there were relatively few patients in the N-CMR group (25 out 82). Further investigations including a larger number of patients are needed to assess the value of pretreatment MTV as a predictor of metabolic response to CCRT.

Liang et al. [37] found that pretreatment TLG was able to independently predict survival in patients with LACC. Ueno et al. [38] found that MTV and TLG of the primary tumour were significantly higher in nonresponders than in responders. In our study, SUVmax, SUVmean, age, pathology findings, FIGO stage and lumboaortic nodal involvement were not predictors of response to treatment. Although NCCN guidelines recommend that a restaging FDG PET/CT scan be performed 3–6 months after the end of CCRT, there is no complete agreement regarding the timing.

As in the largest studies in the literature, a limitation of our study was also the timing of the posttreatment PET/CT scan that ranged from 3 to 12 months (mean 6.7 months) after completion of treatment. Grisby et al. [22] performed restaging PET/CT at 1 to 12 months (mean 3 months) after treatment, and Onal et al. [39] performed FDG PET/CT at 3 to 10 months (median 4 months) after treatment. Another limitation of our study concerns patient classification: although patients were originally classified using the EORTC criteria into four groups (patients with CMR, PMR, SMD and PMD), we had to group those with PMR, SMD and PD together in the N-CMR group because of the small numbers of patients with PMR (eight) and SMD (two). A larger study, including more patients could better explore the benefit of grouping patients using the EORTC criteria.

Conclusion

¹⁸F-FDG PET/CT-based response assessment using the EORTC criteria reliably predicts OS in LACC patients treated with CCRT. In our cohort of patients, pretreatment MTV and TLG and nodal involvement were predictors of response to treatment. MTV was the best predictor of response. However, its additional risk value seems to be low (MTV OR = 1.015). Further studies including a larger number of patients are needed to confirm our preliminary findings about the value of MTV, TLG and nodal involvement in response prediction.

Acknowledgements

The publication of this article was supported by funds of the European Association of Nuclear Medicine (EANM).

Compliance with ethical standards

Conflict of interests

None.

Ethical approval

All procedures performed in studies involving human participants were in accordance with the ethical standards of the institutional and/or national research committee and with the principles of the 1964 Declaration of Helsinki and its later amendments or comparable ethical standards.

Informed consent was obtained from all individual participants included in the study.

Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made.

Unsere Produktempfehlungen

e.Med Interdisziplinär

Kombi-Abonnement

Für Ihren Erfolg in Klinik und Praxis - Die beste Hilfe in Ihrem Arbeitsalltag

Mit e.Med Interdisziplinär erhalten Sie Zugang zu allen CME-Fortbildungen und Fachzeitschriften auf SpringerMedizin.de.

Jetzt testen ¹

e.Med Radiologie

Kombi-Abonnement

Mit e.Med Radiologie erhalten Sie Zugang zu CME-Fortbildungen des Fachgebietes Radiologie, den Premium-Inhalten der radiologischen Fachzeitschriften, inklusive einer gedruckten Radiologie-Zeitschrift Ihrer Wahl.

Jetzt testen ²

Ferlay J, Soerjomataram I, Dikshit R, Eser S, Mathers C, Rebelo M, et al. Cancer incidence and mortality worldwide: sources, methods and major patterns in GLOBOCAN 2012. Int J Cancer. 2015;136(5):E359–86CrossRefPubMed

Jemal A, Bray F, Center MM, Ferlay J, Ward E, Forman D. Global cancer statistics. CA Cancer J Clin. 2011;61(2):69–90.CrossRefPubMed

Peirson L, Fitzpatrick-Lewis D, Ciliska D, Warren R. Screening for cervical cancer: a systematic review and meta-analysis. Syst Rev. 2013;2(1):35.CrossRefPubMedCentralPubMed

Spadea T, Bellini S, Kunst A, Stirbu I, Costa G. The impact of interventions to improve attendance in female cancer screening among lower socioeconomic groups: a review. Prev Med. 2010;50(4):159–64.CrossRefPubMed

Vaccarella S, Lortet-Tieulent J, Plummer M, Franceschi S, Bray F. Worldwide trends in cervical cancer incidence: impact of screening against changes in disease risk factors. Eur J Cancer. 2013;49(15):3262–73.CrossRefPubMed

Rees I, Jones D, Chen H, Macleod U. Interventions to improve the uptake of cervical cancer screening among lower socioeconomic groups: a systematic review. Prev Med. 2018;111:323–35.CrossRefPubMed

FIGO Committee on Gynecologic Oncology. FIGO staging for carcinoma of the vulva, cervix, and corpus uteri. Int J Gynaecol Obstet. 2014;125(2):97–8.CrossRef

Marth C, Landoni F, Mahner S, McCormack M, Gonzalez-Martin A, Colombo N, et al. Cervical cancer: ESMO Clinical Practice Guidelines for diagnosis, treatment and follow-up. Ann Oncol. 2017;28(suppl_4):iv72–83.CrossRefPubMed

Narayanan P, Sahdev A. The role of 18F-FDG PET CT in common gynaecological malignancies. Br J Radiol. 2017;90(1079):20170283.CrossRefPubMedCentralPubMed

10.

The Royal College of Radiologists, Royal College of Physicians of London, Royal College of Physicians and Surgeons of Glasgow, Royal College of Physicians of Edinburgh, British Nuclear Medicine Society, Administration of Radioactive Substances Advisory Committee. Evidence-based indications for the use of PET-CT in the United Kingdom 2016. Clin Radiol. 2016;71(7):e171–88.CrossRef

11.

National Comprehensive Cancer Network. NCCN Clinical Practice Guidelines in Oncology: cervical cancer, V.2. 2015. http://www.nccn.org/professional/physician_gls/PDF/cervicalcancer.pdf.

12.

Park JJ, Kim CK, Park SY, Park BK. Parametrial invasion in cervical cancer: fused T2-weighted imaging and high-b-value diffusion-weighted imaging with background body signal suppression at 3 T. Radiology. 2014;274(3):734–41.CrossRefPubMed

13.

Freeman SJ, Aly AM, Kataoka MY, Addley HC, Reinhold C, Sala E. The revised FIGO staging system for uterine malignancies: implications for MR imaging. Radiographics. 2012;32(6):1805–27.CrossRefPubMed

14.

Rauch GM, Kaur H, Choi H, Ernst RD, Klopp AH, Boonsirikamchai P, et al. Optimization of MR imaging for pretreatment evaluation of patients with endometrial and cervical cancer. Radiographics. 2014;34(4):1082–98.CrossRefPubMed

15.

Magné N, Chargari C, Vicenzi L, Gillion N, Messai T, Magné J, et al. New trends in the evaluation and treatment of cervix cancer: the role of FDG-PET. Cancer Treat Rev. 2008;34(8):671–81.CrossRefPubMed

16.

Raithatha A, Papadopoulou I, Stewart V, Barwick TD, Rockall AG, Bharwani N. Cervical cancer staging: a resident’s primer: women’s imaging. Radiographics. 2016;36(3):933–4.CrossRefPubMed

17.

James RM, Cruickshank ME, Siddiqui N. Management of cervical cancer: summary of SIGN guidelines. BMJ. 2008;336(7634):41–3.CrossRefPubMedCentralPubMed

18.

Lazzari R, Cecconi A, Jereczek-Fossa BA, Travaini LL, Dell’ Acqua V, Cattani F, et al. The role of [18F]FDG-PET/CT in staging and treatment planning for volumetric modulated Rapidarc radiotherapy in cervical cancer: experience of the European Institute of Oncology, Milan, Italy. Ecancermedicalscience. 2014;8:405.PubMed

19.

Cima S, Perrone AM, Castellucci P, Macchia G, Buwenge M, Cammelli S, et al. Prognostic impact of pretreatment fluorodeoxyglucose positron emission tomography/computed tomography SUVmax in patients with locally advanced cervical cancer. Int J Gynecol Cancer. 2018;28(3):575–80.CrossRefPubMed

20.

Salem A, Salem A-F, Al-Ibraheem A, Lataifeh I, Almousa A, Jaradat I. Evidence for the use of PET for radiation therapy planning in patients with cervical cancer: a systematic review. Hematol Oncol Stem Cell Ther. 2011;4(4):173–81.CrossRefPubMed

21.

Belhocine T, Thille A, Fridman V, Albert A, Seidel L, Nickers P, et al. Contribution of whole-body 18FDG PET imaging in the management of cervical cancer. Gynecol Oncol. 2002;87(1):90–7.CrossRefPubMed

22.

Grigsby PW, Siegel BA, Dehdashti F, Rader J, Zoberi I. Posttherapy [18F] fluorodeoxyglucose positron emission tomography in carcinoma of the cervix: response and outcome. J Clin Oncol. 2004;22:2167–71.CrossRefPubMed

23.

Mirpour S, Mhlanga JC, Logeswaran P, Russo G, Mercier G, Subramaniam RM. The role of PET/CT in the management of cervical cancer. AJR Am J Roentgenol. 2013;201(2):W192–205.CrossRefPubMed

24.

Schwarz JK, Siegel BA, Dehdashti F, Grigsby PW. Metabolic response on post-therapy FDG-PET predicts patterns of failure after radiotherapy for cervical cancer. Int J Radiat Oncol Biol Phys. 2012;83(1):185–90.CrossRefPubMed

25.

Beriwal S, Kannan N, Sukumvanich P, Richard SD, Kelley JL, Edwards RP, et al. Complete metabolic response after definitive radiation therapy for cervical cancer: patterns and factors predicting for recurrence. Gynecol Oncol. 2012;127(2):303–6.CrossRefPubMed

26.

Schwarz JK, Siegel BA, Dehdashti F, Grigsby PW. Association of posttherapy positron emission tomography with tumor response and survival in cervical carcinoma. JAMA. 2007;298(19):2289–95.CrossRefPubMed

27.

Schwarz JK, Grigsby PW, Dehdashti F, Delbeke D. The role of 18F-FDG PET in assessing therapy response in cancer of the cervix and ovaries. J Nucl Med. 2009;50(Suppl 1):64S–73.CrossRefPubMed

28.

Ferrari M, Travaini LL, Ciardo D, Garibaldi C, Gilardi L, Glynne-Jones R, et al. Interim 18FDG PET/CT during radiochemotherapy in the management of pelvic malignancies: a systematic review. Crit Rev Oncol Hematol. 2017;113:28–42.CrossRefPubMed

29.

Zhou Z, Liu X, Hu K, Zhang F. The clinical value of PET and PET/CT in the diagnosis and management of suspected cervical cancer recurrence. Nucl Med Commun. 2018;39(2):97–102.PubMed

30.

Herrera FG, Prior JO. The role of PET/CT in cervical cancer. Front Oncol. 2013;3:34. https://doi.org/10.3389/fonc.2013.00034. eCollection 2013.

31.

Brooks RA, Powell MA. Novel imaging modalities in gynecologic cancer. Curr Oncol Rep. 2009;11(6):466–72.CrossRefPubMed

32.

Son H, Kositwattanarerk A, Hayes MP, Chuang L, Rahaman J, Heiba S, et al. PET/CT evaluation of cervical cancer: spectrum of disease. Radiographics. 2010;30(5):1251–68.CrossRefPubMed

33.

Lee JA. Segmentation of positron emission tomography images: some recommendations for target delineation in radiation oncology. Radiother Oncol. 2010;96(3):302–7.CrossRefPubMed

34.

Young H, Baum R, Cremerius U, Herholz K, Hoekstra O, Lammertsma AA, et al. Measurement of clinical and subclinical tumour response using [18F]-fluorodeoxyglucose and positron emission tomography: review and 1999 EORTC recommendations. Eur J Cancer. 1999;35(13):1773–82.CrossRefPubMed

35.

Bland JM, Altman DG. The logrank test. BMJ. 2004;328(7447):1073.CrossRefPubMedCentralPubMed

36.

Bagley SC, White H, Golomb BA. Logistic regression in the medical literature: standards for use and reporting, with particular attention to one medical domain. J Clin Epidemiol. 2001;54(10):979–85.CrossRefPubMed

37.

Liang Y, Li X, Wan H, Fang Y, Zheng R, Zhang W, et al. Prognostic value of volume-based metabolic parameters obtained by 18F-FDG-PET/CT in patients with locally advanced squamous cell cervical carcinoma. J Comput Assist Tomogr. 2018;42(3):429–34CrossRefPubMed

38.

Ueno Y, Lisbona R, Tamada T, Alaref A, Sugimura K, Reinhold C. Comparison of FDG PET metabolic tumour volume versus ADC histogram: prognostic value of tumour treatment response and survival in patients with locally advanced uterine cervical cancer. Br J Radiol. 2017;90(1075):20170035.CrossRefPubMedCentralPubMed

39.

Onal C, Reyhan M, Guler OC, Yapar AF. Treatment outcomes of patients with cervical cancer with complete metabolic responses after definitive chemoradiotherapy. Eur J Nucl Med Mol Imaging. 2014;41(7):1336–42.CrossRefPubMed

Titel: Prognostic value of posttreatment 18F-FDG PET/CT and predictors of metabolic response to therapy in patients with locally advanced cervical cancer treated with concomitant chemoradiation therapy: an analysis of intensity- and volume-based PET parameters
verfasst von: Giacomo Maria Lima
Antonella Matti
Giulio Vara
Giulia Dondi
Nicoletta Naselli
Eugenia Maria De Crescenzo
Alessio Giuseppe Morganti
Anna Myriam Perrone
Pierandrea De Iaco
Cristina Nanni
Stefano Fanti
Publikationsdatum: 02.08.2018
Verlag: Springer Berlin Heidelberg
Erschienen in: European Journal of Nuclear Medicine and Molecular Imaging / Ausgabe 12/2018
Print ISSN: 1619-7070
Elektronische ISSN: 1619-7089
DOI: https://doi.org/10.1007/s00259-018-4077-1

Springer Medizin

Abstract

Purpose

Methods

Results

Conclusion

Introduction

Background

Detection, staging and radiation therapy planning

Treatment response

Recurrent disease

Aim

Materials and methods

Population characteristics

Radiopharmaceuticals and imaging protocol

Image analysis and interpretation criteria

Chemoradiotherapy

External beam radiotherapy

Chemotherapy

Brachytherapy

Statistical analysis

Results

Survival analysis

Comparison of variables between CMR and N-CMR groups

Logistic regression

Discussion

Conclusion

Acknowledgements

Compliance with ethical standards

Conflict of interests

Ethical approval

Informed consent

Unsere Produktempfehlungen

e.Med Interdisziplinär

e.Med Radiologie

Weitere Artikel der Ausgabe 12/2018

Diagnostic performance of 18F-PSMA-1007 PET/CT in patients with biochemical recurrent prostate cancer

Quantification of myocardial blood flow with dynamic SPECT acquisitions: ready for prime time?

Can integrated 18F-FDG PET/MR replace sentinel lymph node resection in malignant melanoma?

Correction to: PET imaging of EGFR expression using an 18F-labeled RNA aptamer

18F-NaF and 18F-FDG as molecular probes in the evaluation of atherosclerosis

68Ga-PSMA PET/CT in patients with recurrent prostate cancer after radical treatment: prospective results in 314 patients