Jung Mi Byun, MD is an Assistant Professor of Obstetrics and Gynecology at Inje University, School of Medicine. Dr. Byun received her medical degree from the Inje University in 2004 and completed her residency training in Obstetrics & Gynecology at Busan Paik hospital, Inje University in Busan from 2005 to 2009. She continued with subspecialty training as a fellow in Gynecology Oncology at the Inje University. She is an expert in laparoscopic operation and management of gynecologic cancer. Her clinical research interests include management and epidemiology of gynecologic cancer. Dr. Byun is a member of the International Gynecological Cancer Society (IGCS) and Korean Cancer Association for gynecologic oncology.
Uterine tumors resembling ovarian sex cord tumors (UTROSCTs) are a rare group of stromal neoplasms containing prominent sex cord-like elements. Since they were first described in 1945 by Morehead and Bowman [1], no more than 100 such tumors have been reported [2]. In a report by Clement and Scully [3], these neoplasms were divided into 2 groups on the basis of clinical and histologic patterns. The first group (group I) included endometrial stromal tumors with less than 50 % sex cord-like elements, and the second group (group II) included UTROSCTs exhibiting sex cord-like differentiation of more than 50 %. In the latest, according to the World Health Organization classification of uterine neoplasms, UTROSCTs were placed in a miscellaneous category of tumors of the uterine corpus because of their different morphology and benign clinical behaviors [4]. More recently, UTROSCTs have been suggested to be unusual neoplasms of uncertain malignancy with polyphenotypic immunohistochemical expression, characterized by positivity for sex cord, epithelial, and myoid markers [5, 6]. These tumors usually occur in premenopausal or menopausal women. Most patients have symptoms such as abnormal vaginal bleeding, abdominal pain, and enlarged uterus or a palpable uterine mass on physical examination [7]. In most cases, UTROSCT is diagnosed incidentally after hysterectomy for a clinical diagnosis of an endometrial polyp [8, 9] or sometimes leiomyoma [10].
We report a case of UTROSCT in a postmenopausal woman with vaginal bleeding who was diagnosed with uterine sarcoma at a local clinic.
A 56-year-old woman, gravida 4, para 2, was admitted to our institute in August 2012 for management of abnormal vaginal bleeding and uterine malignancy tumor. She had reached menopause 2 years previously and had experienced irregular vaginal bleeding for 1 year. She visited a local gynecologic clinic underwent endometrial curettage. Pathology indicated malignant tumor with rhabdoid features, and the patient was referred to our clinic. Her body mass index was 20.5 kg/m2, and her medical history was unremarkable. Transvaginal ultrasonography examination revealed a lesion in the uterine fundus, which showed an irregular hyperechoic mass, and there was not clear margin between the myometrium and the mass. Fluid collection was noted in the endometrial cavity (Fig. 1). Computed tomography of the abdomen and pelvis showed a 2 cm mildly enhanced nodular mass, which was suspected to be malignant mixed Mu¨llerian tumor or endometrial cancer with myometrial invasion, but no metastasis was noted (Fig. 2). Abdominal hysterectomy with bilateral salpingo-oophorectomy was performed, and the removed organs were submitted for pathologic examination. The removed uterus measured 7.5 9 5.0 9 3.0 cm and weighed 74.8 g. The cervix, fallopian tubes, and both ovaries were unremarkable on gross observation. Macroscopic examination, showed that the lesion was projecting into the uterine cavity. On section, the uterine mass was located submucosally with relatively good margination and yellowish color that was more intense than that for usual leiomyoma. The uterine mass measured 2.2 cm in diameter (Fig. 3). Microscopically, the tumor consisted of compactly packed, elongated, or rounded cells and irregular trabeculae, cords, or clusters of larger or foamy cells (Fig. 4a). Immunohistochemical stains were positive for smooth muscle actin and negative for CD10, a marker of endometrial stromal cells, and desmin in the elongated or rounded cells and positive for a-inhibin and calretinin in the larger cells (Fig 4b). Histologic and immunohistochemical findings indicated a mixture of smooth muscle elements and sex cordlike elements, suggesting a diagnosis of UTROSCT. The patient was discharged on the 8th postoperative day without complications. Follow-up based on clinical examination and imaging studies and laboratory tests was planned.
UTROSCTs are considered as neoplasms and show benign behavior: they are different from endometrial stromal tumors with sex cord-like elements (ESTSCLEs or group I), which are associated with metastasis and recurrence. The clinical behavior of ESTSCLEs is similar to that of low-grade endometrial stromal sarcoma, which has a locoregional or distant relapsing rate of approximately 50 % [3, 11]. Although most UTROSCTs follow a benign course, some cases have shown recurrence, with omental, retroperitoneal extension, or subcutaneous suprapubic and abdominal metastases [12–14]. These neoplasms usually occur in middle-aged women with an average age of 50 years who are premenopausal or menopausal [7]. Clinical manifestations include abnormal uterine bleeding, enlarged uterus, palpable mass, or pelvic pain [7–9]. Therefore, most patients undergo hysterectomy with or without bilateral salpingo-oophorectomy. Because of the low recurrence rate, conservative management with fertility-sparing tumor resection has been suggested as an alternative to hysterectomy [10]. Although the exact pathogenesis of UTROSCTs yet been established, some researchers have hypothesized that UTROSCTs originate from an uncommitted stem cell enabling both epithelial and sex cord differentiation, whereas others have postulated that UTROSCTs can be considered a variant of endometrial stromal neoplasm [6, 15]. In most cases, UTROSCTs were diagnosed incidentally after hysterectomy for a treatment after clinical diagnosis of an endometrial polyp [8, 9] or a leiomyoma [10]. In our case, the patient was a menopausal woman diagnosed with uterine sarcoma by biopsy at a local clinic. However, she was diagnosed with UTROSCT on final pathology after hysterectomy in our hospital. UTROSCT can present some diagnostic difficulties when healthcare practitioners examine a small biopsy specimen, because this neoplasm can be similar to other benign or malignant lesions with mesenchymal or epithelial structures. Because UTROSCT shows a large variety of histological features, it is necessary to differentiate it from a large number of neoplasms. Epithelioid leiomyomas, stromal tumors, perivascular epithelioid cell tumors, melanoma, and endometrioid carcinoma should be differentiated from UTROSCT [7]. Therefore, immunohistochemical analysis is useful for differentiating UTROSCT from leiomyoma, ESTSCLE, and other malignant epithelial neoplasms such as endometrioid adenocarcinoma and uterine mesonephric carcinoma. According to Irving et al. [5], reliable histochemical markers for UTROSCT are calretinin, inhibin, CD99, and Melan-A, and positivity for calretinin and at least one of the other 3 markers is suggestive of UTROSCT. In our case, tumor cells were positive for calretinin and a-inhibin.
UTROSCTs are usually benign [3] and have low recurrence rates, and they are generally treated with hysterectomy alone. If patients desire to have children, fertility-sparing tumor resection can be suggested [10]. Few cases of recurrence of UTROSCT have been reported [14]. Therefore, close long-term follow-up with imaging studies such as vaginal ultrasonography, computed tomography, pelvic magnetic resonance image, and chest X-ray is required [16].
In our case, the patient received total abdominal hysterectomywith bilateral salpingo-oophorectomy inAugust 2012 and has been followed-up thereafter. This patient was initially diagnosed with uterine sarcoma by endometrial biopsy, at a local clinic, and her symptomwas abnormal vaginal bleeding in a menopausal state. Therefore, we had good reason to be suspicious of a malignancy, but her final diagnosis was confirmed as UTROSCT by immunohistochemical analysis. UTROSCT is a rare tumor, and it can sometimes be misdiagnosed as malignancy in postmenopausal women. Furthermore, radical surgery or overtreatment can be performed after misdiagnosis. UTROSCT is diagnosed using immunohistochemical analysis, which is justified because it prevents overtreatment and the need for long-term follow-up.
Conflict of interest The authors have no conflicts of interest to declare.
