MR findings of primary ovarian granulosa cell tumor with focus on the differentiation with other ovarian sex cord-stromal tumors

Between December 2009 and December 2015, 1217 consecutive patients with clinically suspected adnexal disease prospectively underwent 1.5 T MRI examinations before pelvic or laparoscopic surgery at our institution. The time interval between the MRI evaluation and surgery was less than one month (2–27 days; mean, 5 ± 12 days).

Among them, 18 patients with histologically proven OGCT (24–79 years of age; average age, 45.9 ± 15.3 years) were included in this study when we retrospectively retrieved the database on the Picture Archiving and Communication System (PACS). Two recurrent OGCTs were excluded for further analysis because the primary imaging data was evaluated in another hospital. Thirty four patients with OSCs, including histologically proven sclerosing stroma tumors (SST, n = 4), fibrothecomas (n = 21), and fibromas (n = 9), were included as the comparative group. Patients with any previous pelvic surgery or radiation history were arbitrarily excluded because the inherent structure of the uterus may has been altered. Details of the samples studied are summarized in Table 1.

MRI was performed using a 1.5-T MR system (Magnetom Avanto, Siemens, Erlangen, Germany) with a phased-array coil. The routine MRI protocols used for assessment of pelvic masses included axial turbo spin-echo (TSE) T1WI, sagittal TSE T2WI, and axial/sagittal TSE fat-suppressed T2WI (FS T2WI). For axial images, the transverse plane was perpendicular to the long axis of uterine body; for sagittal images, the longitudinal plane was parallel to the main body of uterus. DWI using an echo-planar imaging two-dimensional (EP2D) sequence performed in the axial plane with parallel acquisition technique by using b value = 0, 100, and 800 s/mm². Contrast-enhanced pelvic imaging was acquired at multiple phases of contrast medium enhancement in both sagittal and axial planes.

The location, size (the largest dimension in two orthogonal planes), margin (regular or irregular); visibility of hemorrhagic component (high signal on T1WI) within the lesion; and presence of capsule, pelvic-free fluid and lymph node were also noted. On T1WI, hypo-, iso-, and hyperintensity were similar for the pelvic fluid, pelvic wall muscle, and fat signal; on T2WI, hypo-, iso-, and hyperintensity were similar for the pelvic bone, pelvic wall muscle, and fat signal; on b = 800 mm^− 2/s DWI images, the low, intermediate, and high-signal intensity were similar for the pelvic bone, myometrium, and endometrium. After the intravenous injection of the contrast medium, the lesion enhancement type was graded as follows: 1, minor enhancement (clearly less than the myometrium); 2, mild enhancement (less than the myometrium); 3, moderate enhancement (similar to the myometrium); or 4, avid enhancement (more than the myometrium). ADCs were measured manually on post-processing workstation (Leonardo, Siemens, Germany) by one reviewer (H.Z.). Two observers (S. X. G. and H.Z., with 6 and 10 years of experience in gynecological imaging, respectively), who were blinded to the histological results independently, analyzed MRI datasets of each participant. At the end of the study, two observers were also required to determine the tumor etiology (benign or malignant) according to previous established criteria [14‐16]. For interobserver discrepancies in the evaluation of uterine lesions, consensus was achieved.

Continuous variables were expressed as the means ± standard deviation (S.D.) and compared with the unpaired t test if normally distributed or the Mann–Whitney test if not normally distributed. A nonparametric test (Mann–Whitney) was used to test other nonparametric variables within each group. The area under the receiver operating characteristic (ROC) curve (AUC) was calculated for ADCs to discriminate OGCTs from OSCs. SPSS (version 13.0, SPSS, Chicago, USA) was used to perform statistical analyses. P values ≤0.05 were considered statistically significant.

Neoplastic bleeding can be seen in six OGCTs, appearing as the patchy high signal intensity on T1WI images in the tumor body (Fig. 3), which was not identified in OSC group (p = 0.000). Seventeen OGCTs were round or oval masses with regular margin (17/20) and intact capsule (16/20), while 33 (33/34) and 34(34/34) observed in OSCs, respectively (p = 0.015). Regarding the tumor component, OGCTs mostly appeared as the solid or mostly solid component (16/20, Fig. 4), while OSCs always showed purely solid component (28/34) (p = 0.000). On the post-contrast images, fourteen lesions (14/20) in OGCT group displayed mild enhancement and six showed moderate enhancement. In OSC group, most of fibromas showed minor enhancement and 4 SSTs appeared inhomogeneously avid enhancement (Fig. 5). On DWI images, 80 % of OGCTs (16/20, 80.0%) showed high signal intensities in comparison with 47% (16/34, 47.1%) in OCS group. The average ADC value (817 ± 144 × 10^− 3 s/m²) in OGCT group was obviously less than OSC group (1223 ± 473 × 10^− 3 s/m², p = 0.002) and fibrothecoma (1209 ± 437 × 10^− 3 s/m², p = 0.001, Fig. 6). When use the ADC cutoff value as 619 × 10^− 3 s/m², MRI could yield a sensitivity of 79.4% and a specificity of 60.0% for diagnosis of OGCT, respectively; the AUC is 0.784(95% CI:0.658–0.910) (Fig. 7). Enlarged lymph nodes were not observed in all OGCTs at MRI images. Pathological fluid was only noted in one OGCT, obviously less than 11 cases in OSCs group. At multivariate analysis, neoplastic hemorrhagic contents (OR: 3.429), component (OR: 2.50) and no pathological fluid (OR: 8.130) are more indicative of OGCT diagnosis (Table 2). On MRI, two readers accurately determined the malignant condition in 17 cases. If combining ADC values, then they could yield a sensitivity of 95.0% and a specificity of 94.1% for OGCT diagnosis. Three lesions were misdiagnosed as uterine fibroids and two lesion as fibrothecoma before invasive procedures. The overall diagnostic performance of MRI for diagnosing OGCT is listed as Table 3.