Diagnostic utility of a conventional MRI-based analysis and texture analysis for discriminating between ovarian thecoma-fibroma groups and ovarian granulosa cell tumors
Journal of Ovarian Research volume 15, Article number: 65 (2022)
To evaluate the diagnostic utility of conventional magnetic resonance imaging (MRI)-based characteristics and a texture analysis (TA) for discriminating between ovarian thecoma-fibroma groups (OTFGs) and ovarian granulosa cell tumors (OGCTs).
This retrospective multicenter study enrolled 52 patients with 32 OGCTs and 21 OTFGs, which were dissected and pathologically diagnosed between January 2008 and December 2019.
MRI-based features (MBFs) and texture features (TFs) were evaluated and compared between OTFGs and OGCTs. A least absolute shrinkage and selection operator (LASSO) regression analysis was performed to select features and construct the discriminating model. ROC analyses were conducted on MBFs, TFs, and their combination to discriminate between the two diseases.
We selected 3 features with the highest absolute value of the LASSO regression coefficient for each model: the apparent diffusion coefficient (ADC), peripheral cystic area, and contrast enhancement in the venous phase (VCE) for the MRI-based model; the 10th percentile, difference variance, and maximal correlation coefficient for the TA-based model; and ADC, VCE, and the difference variance for the combination model. The areas under the curves of the constructed models were 0.938, 0.817, and 0.941, respectively. The diagnostic performance of the MRI-based and combination models was similar (p = 0.38), but significantly better than that of the TA-based model (p < 0.05).
The conventional MRI-based analysis has potential as a method to differentiate OTFGs from OGCTs. TA did not appear to be of any additional benefit. Further studies are needed on the use of these methods for a preoperative differential diagnosis of these two diseases.
Ovarian granulosa cell tumors (OGCTs) and ovarian thecoma-fibroma groups (OTFGs) are both uncommon neoplasms that originate from the sex cord-stromal cells of the ovary [1, 2]. The clinical manifestations of these two groups overlap, and include vaginal bleeding, endometrial hyperplasia, and carcinoma, which are related to excessive estrogen production [3, 4]. OGCTs are regarded as a low-grade malignancy, but with a modest risk of metastasis or the potential to recur years after the initial diagnosis [5, 6]. In the advanced stages of OGCT, chemotherapy is recommended as adjuvant treatment . Follow-ups are also recommended for all patients with OGCTs due to the modest to high rate of recurrence (17–50%). In contrast, OTFGs are benign tumors that rarely metastasize or recur and often may be treated conservatively . Therefore, an accurate preoperative diagnosis between OGCTs and OTFGs has significant implications for clinical treatment and management strategies.
Magnetic resonance imaging (MRI) is a feasible method for providing important diagnostic information on pelvic lesions, such as OGCTs and OTFGs. A high signal intensity on T1-weighted images (T1WI) representing hemorrhage, a high signal intensity on diffusion-weighted imaging (DWI), a low apparent diffusion coefficient (ADC) value, and moderate enhancement are characteristic MRI features of OGCTs [8,9,10]. In contrast, a low signal intensity on T1WI and T2-weighted images (T2WI) indicating a fibrous tissue component, a high ADC value, and minimal or mild enhancement are the predominant features of OTFGs [11, 12]. Although previous studies reported characteristic MRI findings for these two tumors, quantitative or semi-quantitative assessments with MRI have been limited.
A texture analysis (TA) is an image analysis technique that allows for the quantification of image characteristics using the distribution of pixels and their surface intensity or patterns [13, 14]. These image characteristics are based on the microstructures of a background tissue and are sometimes imperceptible to the human visual system . TA has been applied to a number of medical image assessments, including oncologic imaging [15, 16], neuroimaging [17, 18], and musculoskeletal imaging [19, 20]. In pelvic MRI on ovarian sex cord-stromal tumors, recent radiomics studies reported the differentiation of OTFGs from uterine fibroids in the adnexal area . A discriminative analysis of OGCTs and OTFGs using imaging-based models and TA-based models was conducted by Li et al. . Although there are clinical merits to predictive models for these adnexal lesions, the number of related studies is still limited, which may be due to the rarity of these diseases.
Therefore, the present study was performed to assess MRI-based features (MBFs) and texture features (TFs), identify the most favorable features for discriminating between OGCTs and OTFGs, and evaluate the combined diagnostic performance of MBFs and TFs.
This was a retrospective multicenter study; each Institutional Review Board provided approval, and informed consent was obtained in the form of an opt-out on the website. All experiments were performed in accordance with the relevant guidelines and regulations.
Data were collected from the Saitama Medical University International Medical Center (SMUIMC) and Tokyo Metropolitan Komagome Hospital (TMKH). We searched their pathology databases for consecutive patients with pathologically confirmed OTFGs and OGCTs between January 2008 and December 2019.
Inclusion and exclusion criteria were summarized as a flow chart shown in Fig. 1. Based on these criteria, 52 patients with 32 OTFGs and 21 OGCTs were ultimately enrolled in the present study.
MRI was performed using the 3.0-T system (Achieva, Philips (SMUIMC); and Skyra, Siemens Healthcare (TMKH)). The principal MRI protocol included T2WI in the axial plane, T1WI in the axial plane, DWI in the axial plane, and multiphasic contrast-enhanced fat-suppressed T1WI in the axial, sagittal, or coronal plane. Representative scanning sequences and parameters are shown in Table 1. An intravenous injection of 20 mg of butyl-scopolamine was administered to all patients to relax the bowel wall and reduce peristaltic bowel movement before MRI examinations.
Conventional MRI-based analysis
The evaluation of MBFs was performed by two radiologists (K.I. and K.N.) with 20 and 6 years of experience in gynecological imaging who were blinded to the pathological results. The two radiologists independently assessed MBFs, which were used for inter-reader reproducibility tests. They then reached a consensus for any discrepancies to be resolved and consensus data were used in the construction of classification models.
The following MBFs of the two types of diseases were recorded:
Lesion size: the maximum lesion diameter of the three dimensions measured.
Multiple nodular: may be divided into many nodules or locules
Oval: may be approximated as a round or ellipse shape
Shallow lobulated: may consist of lobules, not having a nodular appearance
Capsule: the presence of a uniformly thin layer covering the whole lesion.
Solid and cystic components:
Solid: without cystic degeneration found by the naked eye
Predominantly solid: the area of cystic degeneration was < 1/3 of the total area
Solid and cystic: the area of cystic degeneration was 1/3–2/3 of the total area
Predominantly cystic: the area of cystic degeneration was > 2/3 of the total area
Mainly large cysts: the area of large cysts was > 1/2, large cysts were ≥ 1 cm
Mainly small cysts: the area of small cysts was > 1/2, small cysts were < 1 cm
Mixed: the areas of large and small cysts were almost equal
Cyst size: the longest diameter of the cystic region.
Peripheral cystic area: the presence of cystic areas in the peripheral zone of the lesion.
Hemorrhagic component: the presence of a high signal intensity on T1WI within the lesion.
Endometrial hyperplasia: an endometrial thickness of more than 16 and 5 mm in premenopausal and postmenopausal women, respectively.
Uterine fibroids or adenomyosis: the presence of uterine nodules or ill-defined thickening of the myometrium with small foci of hemorrhage or cystic changes.
Small: ascites localized in the pelvic cavity
Large: ascites extending beyond the pelvic cavity into the peritoneal cavity
T1WI, T2WI, and DWI: the signal intensity in solid regions was examined.
Hypo-, iso-, or hyperintense relative to the uterine myometrium
ADC value: the mean value within solid regions was obtained after three measurements.
Contrast enhancement: the degree of contrast enhancement within the lesion was examined in the arterial, venous, and delayed phases.
Minimal: clearly less than the myometrium
Mild: less than the myometrium
Moderate: similar to the myometrium
Marked: more than the myometrium
To avoid data heterogeneity bias, all MRI data were subjected to imaging normalization (the intensity of the image was scaled to 0–100), resampled to the same resolution (3 × 3 × 3 mm), and discretized before feature extraction. Segmentation was performed using open-source software (ITK-SNAP version 3.8.0). One slice of axial T2WI that harbored the largest solid region of the tumor was selected for each case. A radiologist with 6 years of experience (K.N.) selected an appropriate slice and then asked two radiologists, both with 3 years of experience (T.K. and F.Y.), to draw on the identified slice. An irregular two-dimensional ROI was manually drawn to contain the outline borders of the solid region of the tumor on each selected image, and the cystic region was avoided as much as possible (see Fig. 2c or 3c). All three radiologists were blinded to clinical information. The ROI data delineated by T.K. and F.Y. were used for an inter-reader reproducibility test, while those delineated by T.K. were used to construct classification models.
TFs were extracted using the open-source python package (PyRadiomics version 2.1.0 (www.radiomics.io/pyradiomics.html)). Extracted TFs were as follows: 18 first-order statistics, 24 Gy-level co-occurrence matrix (GLCM), 16 Gy-level run-length matrix, 16 Gy-level size zone matrix, 14 Gy-level dependence matrix, and 5 neighboring gray-tone difference matrix features.
Quantitative data were summarized in our dataset as means ± standard deviations. Qualitative data were summarized as the total number of cases in our dataset (or percentages). In univariate analyses, the Mann–Whitney U test was used for quantitative data, while Fisher’s exact test or the x2 test was used for qualitative data.
Before the consecutive statistical analysis, all numeric values were standardized using the Python scikit-learn package “RobustScaler” to minimize the effects associated with differences in the MRI machines and protocols between two centers.
To construct discriminant models that differentiate between OTFGs and OGCTs, we performed feature selection. We adopted the least absolute shrinkage and selection operator (LASSO) algorithm, which may be a suitable method for the regression of high dimensional data with a small sample size, such as that in the present study . All variables were included in each attempt of feature selection, and their LASSO regression coefficients were obtained by tenfold cross-validation. To avoid over-fitting, only three features with the highest absolute values of the LASSO regression coefficient were selected each time. Model development was conducted using a linear discriminant analysis. ROC analyses were performed on independent discriminative features to assess the overall diagnostic performance of the discriminant models.
We constructed the MRI-based model (using selected MBFs), TA-based model (using selected TFs), and combination model (using the best features selected from all MBFs and TFs), and compared their performance. In consideration of the small sample size, we adopted tenfold cross-validation repeated 100 times to construct the final model. The performance of classifiers was evaluated by the area under the curve (AUC). Accuracy, sensitivity, specificity, precision, and the F-measure were calculated based on the confusion matrix of classification results.
Interobserver reproducibility was evaluated for each feature; Kappa values were used in the assessment of qualitative data among MBFs (k ≥ 0.75 was indicative of almost perfect agreement): the intraclass correlation coefficient (ICC) was measured in the assessment of quantitative data among MBFs and TFs (ICC ≥ 0.75 and lower 95%CI ≥ 0.6 indicated good reproducibility). The collinearity status between each feature was analyzed using Pearson’s correlation coefficient (r ≥ 0.7 indicated high collinearity).
Statistical analyses were performed using an opensource software package (Python scikit-learn 0.22.1). Statistical values of p < 0.05 were considered to be significant.
The clinical characteristics of all of the lesions examined are summarized in Table 2. No significant differences were observed in variables, such as age, side of the lesion, body mass index, the menopausal status, parity, or clinical symptoms, between OTFGs and OGCTs.
Conventional MRI-based characteristics
MRI-based characteristics were compared between OTFGs and OGCTs, as shown in Tables 3 and 4. Representative cases of the two diseases are shown in Figs. 2 and 3. The univariate analysis identified the following ten variables: capsule, solid and cystic components, peripheral cystic areas, the cystic pattern, intratumoral hemorrhage, pelvic fluid, the ADC value, and contrast enhancement in the arterial, venous, and delayed phases, as significant factors for differentiating between the two disease groups (p < 0.05).
All variables were included in the LASSO regression analysis. To establish a discriminating model using representative MBFs, we selected 3 features with the highest absolute value of the LASSO regression coefficient: the ADC value, peripheral cystic area, and contrast enhancement in the venous phase (VCE). The AUC of the discriminating model using these representative MBFs was 0.938, with an accuracy of 0.905, sensitivity of 0.857, and specificity of 0.937 (Table 6).
We used Kappa values to investigate interobserver variability and found that the observers were in agreement on most of the conventional MR features. Kappa values ranged between 0.76 and 0.96, as shown in Tables 3 and 4. The collinearity status between each feature is shown in Supplementary Fig. 1.
The mean sizes of the ROIs placed by two radiologists (T.K. and F.Y.) were 118.31 ± 86.78 and 125.19 ± 92.43 cm2, respectively. Among 93 TFs, the mean ICC value was 0.864 ± 0.124 in the inter-observer reproducibility test. The number of features with good reproducibility (ICC ≥ 0.75 and lower 95%CI ≥ 0.6) was 80. All variables were included in the LASSO regression analysis. TFs with LASSO regression coefficients other than 0 were summarized in Table 5 and their distribution was shown in Fig. 4. To establish a discriminating model using representative TFs, we selected 3 features with the highest absolute values of LASSO regression coefficients: the histogram-based 10th percentile, GLCM-based difference variance, and maximal correlation coefficient. The AUC of the discriminating model using these representative TFs was 0.817, with an accuracy of 0.791, sensitivity of 0.618, and specificity of 0.904 (Table 6). The collinearity status between each feature is shown in Supplementary Fig. 1.
Combination of conventional MRI-based characteristics and TA
We evaluated the performance of the diagnostic model using the best parameters of MRI-based characteristics and TA. All MBFs and TFs were included in the LASSO regression analysis. Features with LASSO regression coefficients other than 0 are summarized in Supplementary Table 1. We selected the best 3 features with the highest absolute value of the LASSO regression coefficient: ADC, VCE, and difference variance. The AUC of the discriminating model using these representative features was 0.941, with an accuracy of 0.901, sensitivity of 0.893, and specificity of 0.906 (Table 6).
Comparison of representative classification models
The performance of representative classification models (MRI-based, TA-based, and combination models) was compared using bootstrap likelihood ratio tests. The AUCs for these models in each of 100 bootstrap samples are shown in Supplementary Table 2. The diagnostic performance of the MRI-based and combination models was similar (p = 0.38), but significantly better than that of the TA-based model (p < 0.05). All results are summarized in Table 6, with representative ROC curves in Fig. 5.
In the present study, we assessed the ability of a conventional MRI-based analysis and TA to distinguish between OGCTs and OTFGs. We found that several MBFs were important for differentiating between the two disease groups. The peripheral cystic area, ADC values, and VCE were the most valuable differentiators. We also showed that TA may be helpful for distinguishing between OGCTs and OTFGs, but were unable to identify its advantages over MBFs in the present study.
Previous studies reported that conventional MRI findings may facilitate the differentiation of OGCTs from OTFGs [8,9,10,11,12]. An assessment of the cystic component is important for the diagnosis of OTFGs and OGCTs. In the present study, cystic areas were more frequently detected in OGCTs than in OTFGs. The maximum diameter of cysts was similar between the two groups in the present study; however, a significant difference was reported in a previous study . We showed that the presence of peripheral cystic areas may be an important indicator in the differential diagnosis of OTFGs and OGCTs. In OTFGs, cystic changes are mainly caused by degeneration, and occur in the peripheral zone in approximately 50% of cases [11, 21]. Regarding OGCTs, the present results demonstrated that cystic areas were always present peripherally and more frequently than in OTFGs, and contralateral or distal to the adnexal vascular inflow site in most cases. The frequency of capsules was previously reported to be significantly higher in OGCTs than in OTFGs [8, 10, 11, 24], and this was confirmed in the present study. Morphology was also examined in a previous study, with OTFGs showing multiple nodular lesions and OGCTs mostly exhibiting oval lesions . However, in the present study, no significant differences were observed between the two groups. Hemorrhage is a distinctive feature in OGCTs . In the present study, a hemorrhagic component was observed in 61.9% of cases, which was consistent with previous findings [10, 25].
On T2WI in the present study, more than 50% of OGCTs showed hyperintense signals, while OTFGs had various signal intensities. OTFGs in conventional MRI findings often had a low signal intensity on T2WI, representing the fibrous component of the tumor . However, the extent of the low signal may be affected by edema, degenerative changes, or the amount of theca cells and fibrous content, resulting in various degrees of signal intensity . On DWI in the present study, OGCTs and OTFGs both exhibited a high or mixed signal intensity. The ADC value of the solid component was significantly higher in OTFGs than in OGCTs. DWI reflects the motion of water molecules, and water diffusivity may be quantitatively calculated using the ADC value. Increased cellularity in lesions generally causes the ADC value to decrease, and this has potential for differentiating between benign and malignant lesions. Regarding OGCTs and OTFGs, the ADC value may be affected by the degree of cellularity (the number of granulosa cells or fibroblasts), minor degeneration, or edematous changes. Previous studies reported that a high density of granulosa cells in OGCTs may be related to reduced values, while the likelihood of degeneration in OTFGs may result in an increase in the ADC value; however, there is an overlap between the two diseases [8, 10, 27].
OGCTs and OTFGs have been suggested to have different blood supplies, with the former being more hypervascular than the latter [8, 10]. In the present study, OTFGs always exhibited minimal to mild enhancement, while OGCTs mostly showed mild to moderate enhancement. Regarding contrast phases, according to one study, the distinction between thecomas and OGCTs was more apparent in the venous and delayed periods than in the arterial period of multiphasic contrast enhancement . These findings were confirmed in the present study, with VCE being identified as a more significant independent differentiator of the two disease groups than that in the other phases. This result may be attributed to the variability of enhancement degrees in lesions as well as in the myometrium (used as a reference), which may be emphasized in the early contrast phase.
The present results implied that the extent and pattern of signal intensities differ between the two disease groups. Although it is of high clinical value for these differences to be made explicit, difficulties are associated with assessing them in a quantitative manner. In comparisons with visual assessments of texture, computational TA techniques are reportedly more objective and sensitive to changes that are imperceptible to the human visual system [13, 14]. In the present study, the following TFs on T2WI were particularly important for differentiating between OGCTs and OTFGs: the 10th percentile (a histogram-based value below which 10% of all data in a set fall) and the difference variance (a GLCM-based feature that measures the deviation from the mean value) [28,29,30]. OTFGs showed a lower 10th percentile, indicating a predominant area with a low signal intensity (fibrous component). In contrast, OGCTs displayed a higher signal intensity (granulosa cell component) and higher difference variance (implying heterogeneity caused by hemorrhage or fibrosis).
The present results revealed that the diagnostic performance of the MRI-based and combination models was similar, and no additional benefit was obtained in TA. These results were contradictory to recent findings reported by Li et al. showing that TA-based and combination models were superior to the MBF-based model . However, there were important differences between that study and the present study; (1) The number of parameters they initially applied in TA was 1,316, which was too big for the small sample size of their study (46 cases). It may have led to over-fitting, even if they used multi-step feature selection including the LASSO algorithm. (2) The present study was conducted at two institutions, whereas theirs was a single-center study. Although we performed image preprocessing and data standardization, variations between the two centers may have resulted in inferior results for TA. (3) The present study considered the solid portion of the lesion in only one slice of axial T2WI for TA instead of the whole area throughout all slices of the tumor in their study. Therefore, the extracted data may have differed, and their data may have contained more texture information than ours.
The present study had a number of limitations that need to be addressed. The sample size was small because the rarity of these disorders prevented us from collecting a large number of patients. In addition, this study was retrospective, which inevitably increases the risk of bias. Future prospective studies with a large sample size and independent training and test cohorts will further underline the diagnostic value of the present results. Moreover, the present study lacked other ovarian tumors (particularly other sex-cord tumors, such as sclerosing stromal tumors). Another limitation is that our TA study only considered the solid region of the tumor on each selected image, while the cystic region was avoided as much as possible. By omitting these regions, we may have lost some important TA information. Similarly, we only used T2WI axial images for TA in the present study. We did not include additional TA on T1WI or contrast-enhanced images because these sequences were sometimes taken in only the coronal, sagittal, or oblique plane, and axial images were not available in all patients. Furthermore, as discussed above, we delineated the ROI in a single slice because it contained representative information on tissue texture and may be a substitute for all slice data. This methodology has been applied in many studies on TA. Furthermore, it is time-consuming to delineate all slices. However, in a recent study, good findings were obtained for TA-based models using all slice data ; therefore, further studies are needed. The further development of our models will be achieved by addressing these issues in the future.
The conventional MRI-based analysis may be used to differentiate OTFGs from OGCTs. TA did not appear to have any additional benefits. Further studies are needed to verify their reproducibility and feasibility for the non-invasive preoperative diagnosis of these two diseases.
Availability data and materials
The authors declare that all data supporting the results of the present study are available within the article.
Apparent diffusion coefficient
Area under the curve
Gray-level co-occurrence matrix
Intraclass correlation coefficient
Least absolute shrinkage and selection operator
Magnetic resonance imaging
Ovarian granulosa cell tumor
Ovarian thecoma-fibroma group
Region of interest
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The authors wish to acknowledge Dr. Akira Kunimatsu, Professor of the International University of Health and Welfare (IUHW) Mita Hospital, for his help in interpreting the significance of the results of this study.
The authors declare that they have no competing interests.
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Nagawa, K., Kishigami, T., Yokoyama, F. et al. Diagnostic utility of a conventional MRI-based analysis and texture analysis for discriminating between ovarian thecoma-fibroma groups and ovarian granulosa cell tumors. J Ovarian Res 15, 65 (2022). https://doi.org/10.1186/s13048-022-00989-z