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Review

Uterine Tumors Resembling Ovarian Sex Cord Tumors (UTROSCTs): A Scoping Review of 511 Cases, Including 2 New Cases

by
Rafał Watrowski
1,2,*,†,
Mario Palumbo
3,†,
Serena Guerra
3,
Alessandra Gallo
3,
Brunella Zizolfi
3,
Pierluigi Giampaolino
3,
Giuseppe Bifulco
3,
Attilio Di Spiezio Sardo
3 and
Maria Chiara De Angelis
3
1
Department of Obstetrics and Gynecology, Helios Hospital Müllheim, 79379 Müllheim, Germany
2
Faculty of Medicine, University of Freiburg, 79106 Freiburg, Germany
3
Department of Public Health, School of Medicine, University of Naples Federico II, 80138 Naples, Italy
*
Author to whom correspondence should be addressed.
These authors contributed equally to this work.
Medicina 2024, 60(1), 179; https://doi.org/10.3390/medicina60010179
Submission received: 2 December 2023 / Revised: 10 January 2024 / Accepted: 15 January 2024 / Published: 19 January 2024
(This article belongs to the Special Issue Uterine Smooth-Muscle Tumors)
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Abstract

:
Uterine Tumors Resembling Ovarian Sex Cord Tumors (UTROSCTs) are rare uterine mesenchymal neoplasms with uncertain biological potential. These tumors, which affect both premenopausal and postmenopausal women, usually have a benign clinical course. Nevertheless, local recurrences and distant metastases have been described. By analyzing 511 cases retrieved from individual reports and cases series, we provide here the most comprehensive overview of UTROSCT cases available in the literature, supplemented by two new cases of UTROSCTs. Case 1 was an asymptomatic 31-year-old woman who underwent a laparoscopic resection of a presumed leiomyoma. Case 2 was a 58-year-old postmenopausal woman with abnormal vaginal bleeding who underwent an outpatient hysteroscopic biopsy of a suspicious endometrial area. In both cases, immunohistochemical positivity for Calretinin and Inhibin was noted, typical for a sex cord differentiation. In both cases, total laparoscopic hysterectomy with bilateral salpingo-oophorectomy was performed. In light of the available literature, no pathognomonic clinical or imaging finding can be attributed to UTROSCT. Patients usually present with abnormal uterine bleeding or pelvic discomfort, but 20% of them are asymptomatic. In most cases, a simple hysterectomy appears to be the appropriate treatment, but for women who wish to become pregnant, uterus-preserving approaches should be discussed after excluding risk factors. Age, tumor size, lymphovascular space invasion, nuclear atypia, and cervical involvement are not reliable prognostic factors in UTROSCT. The current research suggests that aggressive cases (with extrauterine spread or recurrence) can be identified based on a distinct genetic and immunohistochemical phenotype. For instance, UTROSCTs characterized by GREB1::NCOA1-3 fusions and PD-L1 molecule expression appear to be predisposed to more aggressive behaviors and recurrence, with GREB1::NCOA2 being the most common gene fusion in recurrent tumors. Hence, redefining the criteria for UTROSCTs may allow a better selection of women suitable for fertility-sparing treatments or requiring more aggressive treatments in the future.

1. Introduction

Uterine Tumors Resembling Ovarian Sex Cord Tumors (UTROSCTs) are rare mesenchymal neoplasms uniquely classified within the group of “Mesenchymal tumors specific to the uterus” with “unspecified, borderline, or uncertain behavior” according to the WHO [1] and ICD-O [2] classifications. Their histologic features recapitulate the appearance of ovarian sex cord tumors [1]. The initial UTROSCT description dates back to 1945 when Morehead and Bowman reported a uterine neoplasm closely resembling a granulosa cell tumor in a 44-year-old woman [3]. A defining series published in 1976 by Clement and Scully detailed this novel histopathological entity [4]. Based on the quantity of sex cord elements, these tumors have been categorized into two subtypes: type 1 and type 2. Type 1 tumors, referred to as endometrial stromal tumors with sex cord-like elements (ESTSCLE), display a higher malignant potential compared to type 2 tumors. The latter encompasses classic UTROSCTs, which generally exhibit low-grade malignant potential with typically benign behavior, albeit with occasional recurrences. In 2008, Czernobilsky introduced an immunohistochemical algorithm that established the diagnostic criteria for UTROSCTs [5]. Four antibodies, including Calretinin, Inhibin, CD99, and Melan A, have been recognized as the most characteristic markers for confirming a UTROSCT diagnosis (type 2 tumors), while ESTSCLE typically only expresses a single sex cord marker, predominantly Calretinin [5]. Some authors, noting morphological and molecular distinctions, as well as differing clinical behaviors, argue against conflating ESTSCLE and UTROSCT into a single tumor category [6], leading to some studies excluding ESTSCLE, while others including it. Recent molecular discoveries support considering UTROSCT as a separate entity; however, the cellular precursor of UTROSCT remains unknown [7].
To date, UTROSCT is among the rarest uterine tumor types [1,4,5,7,8], with no literature review covering more than 80 cases. The established knowledge about UTROSCT is summarized in Table 1.
The diagnosis and treatment of UTROSCTs present challenges due to their rarity and the fact that their symptoms and imaging findings closely mimic those of leiomyomas. The impossibility of conducting large prospective studies and the limited feasibility of long-term follow-up observations often lead to intuitive treatment protocols, which can potentially result in overtreatment. Additionally, there is a low (20–25%) but significant risk of malignant progression in an ill-defined subset of UTROSCT cases. Therefore, there is an urgent need to refine histological criteria and prognostic factors by incorporating recent molecular findings. This will enable personalized treatment protocols that avoid overtreatment and reduce patient uncertainty, especially in cases with benign clinical behavior, and will clearly delineate tumors with aggressive potential.
In this review, by analyzing 511 cases from individual reports and case series, we offer the most exhaustive overview of UTROSCT to date. Based on a data set spanning 78 years, including significant advancements from 2022–2023, we emphasize the necessity of updating diagnostic and prognostic criteria to incorporate molecular tumor characteristics. Moreover, we propose new criteria for fertility-sparing treatments, marking a significant contribution in this field. In addition, we report two cases of UTROSCTs, one identified through hysteroscopic biopsy and another during laparoscopic surgery, both of which were managed with laparoscopic hysterectomy with bilateral salpingo-oopherectomy (BSO).

2. Case Reports

2.1. Case 1

In 2022, a 31-year-old asymptomatic woman was referred to our center (University of Naples Federico II) for a routine gynecological ultrasound check. The patient had two spontaneous deliveries and experienced two spontaneous abortions; therefore, she had no desire for further pregnancies. She reported regular menstrual cycles in terms of duration and quantity and had no family history of cancer. At the time of admission, the patient had a BMI of 23.8 kg/m2. Transvaginal and transabdominal ultrasound examination, performed by an expert ultrasound gynecologist (B.Z.), revealed a normal anteverted uterus with regular margins and an inhomogeneous echo pattern. The endometrial echo pattern was regular with a normal endometrial thickness. Both ovaries appeared regular in size, shape, and echotexture. A well-defined, oval-shaped mass measuring 27.8 × 26.5 × 19 mm occupied the posterior uterine wall. The mass showed regular margins and non-uniform echogenicity due to the presence of some anechoic cystic areas (Figure 1). Moderate edge shadowing was present, while fan-shaped shadowing was absent. On color Doppler ultrasound, the lesion appeared not to be richly vascularized. No pelvic fluid was observed (Figure 2). A diagnostic hysteroscopy performed by the expert hysteroscopist (A.D.S.S.) revealed a regular uterine cavity without myoma imprints.
The radiological examination was performed externally by the patient and then was examined by an expert gynecologist oncologist (G.B.). Pelvic MRI confirmed the presence of an intramural-subserous “myoma” measuring 34 × 30 mm, with a screening intermediate signal T1-T2 and a peripheral ring of low signal T2. The mass was hypovascularized and exhibited a contextual millimeter cystic areola (see Figure 3). A red degeneration of uterine leiomyoma was suspected.
Consequently, a laparoscopic myomectomy was conducted by an experienced gynecological surgeon (P.G.). The exploration of the abdomen and of the pelvis showed no macroscopic abnormalities; however, the uterus appeared irregular in shape for the presence of the uterine posterior mass of about 30 mm (Figure 4). The surgical specimen was extracted using an endobag to prevent dispersion in the abdominal cavity.
Surprisingly, the mass was diagnosed as an UTROSCT upon the final pathological examination. Microscopic examination revealed a hypercellular tumor with a solid growth pattern and focal glandular and trabecular differentiation. The cells were small to medium in size, with scant cytoplasm and regular, ovoid nuclei. Mitotic activity was low, with approximately 2 mitoses per 10 high-power fields, and there was no evidence of necrosis. An infiltrative growth pattern into the myometrium was apparent, and this was suggestive of lymphovascular space invasion.
As described in Table 2, the immunohistochemical examination demonstrated tumor cells positivity for ER, PR, WT1, Calretinin, CD56, CD99, Smooth Muscle Actin, and Desmin, with focal positivity for E-cadherin and p16. The tumor was negative for Cyclin D1, BCOR, EMA, CK7, TTF1, GATA3, Chromogranin, Synaptophysin, Caldesmon, Cathepsin k, and Inhibin. Following the immunohistochemical criteria outlined by Czernobilsky [5], the co-expression of Calretinin and at least one other sex cord marker confirmed the diagnosis of UTROSCT (type 2).
Despite the patient’s young age and her lack of desire for fertility, a total laparoscopic HE with BSO was planned after multidisciplinary consultation.

2.2. Case 2

In 2019, a 58-year-old post-menopausal multiparous woman presented with abnormal vaginal bleeding that did not respond to medical therapy. Sonographic examination revealed an increased uterine volume, with two fibroids located in the anterior and posterior uterine wall, measuring 3.5 cm and 5 cm, respectively, and an endometrial thickness of 8 mm (despite the patient’s postmenopausal status). The woman underwent an ambulatory hysteroscopy (Naples), utilizing a vaginoscopic approach with a 5 mm continuous-flow hysteroscope (Bettocchi Office Hysteroscopes; KARL STORZ, Tuttlingen, Germany) equipped with an incorporating 5-Fr operating channel. During the procedure, an area of suspicion was identified on the anterior wall of the endometrium, measuring 1.5 cm, characterized by an irregular, yellow-colored surface. The presence of diffuse hypervascularization along with areas of necrosis was suggestive of malignancy, and a grasp biopsy was performed (see Figure 5).
The microscopic examination of the tissue revealed stretched and branched endometrial glands, surrounded by cells with abundant and foamy cytoplasm, suggesting the presence of sex cord-like elements. Following the recommendations of the pathology team, a second hysteroscopic examination was conducted to obtain deeper tissue samples. Using a 5-Fr Twizzle Versapoint™ bipolar system (Olympus, Hamburg, Germany) inserted through the operating channel of the hysteroscope, the suspicious area was completely resected (Figure 5D). The subsequent immunohistochemical studies were performed, confirming that the tumor was diffusely positive for Calretinin and Inhibin, focally positive for CD99, and negative for CD10 (see Table 2). Based on the immunohistochemical phenotype suggestive of the presence of sex cord components, the tumor was diagnosed as a UTROSCT (type 2). Staging examinations revealed neither locoregional spread nor distant metastases. Finally, a laparoscopic total HE with BSO was performed by the surgical-gynecological team (G.B. and P.G.), and the final histological diagnosis confirmed UTROSCT. The post-operative course was uneventful, and the patient was discharged on the third post-operative day, with a total regression of the initial symptoms.
Currently, three years after the initial diagnosis, the patient is relapse-free.

3. Literature Review

3.1. Materials and Methods

This exhaustive review meets the criteria of a scoping review as outlined by Paré et al.: (a) a broad scope of questions, (b) a comprehensive search strategy, (c) the inclusion of both conceptual and empirical primary sources, (d) explicit study selection criteria, (e) the absence of quality appraisal, and (f) the lack of meta-analytic tools, distinguishing our review from both narrative and systematic reviews [9]. Its cornerstone is the literature collection compiled by the first author (R.W.) over the last ten years. Consequently, the review was not prospectively registered per protocol. The final literature selection occurred during several rounds of literature searches performed in 2023: an electronic search of databases PubMed, SciELO, and Scopus; the scientific search engine Google Scholar; and publisher platforms such as ScienceDirect, Wiley Online Library, Taylor & Francis Online, Nature Publishing Group, SAGE Publications, and SpringerLink, was conducted up to November 2023. This was complemented by a meticulous review of reference lists. Our search algorithm combined terms like “uterine tumor resembling ovarian sex cord tumors”, “UTROSCT”, “ESTSCLE”, “sex-cord”, and “sex-cord like” with all relevant counterparts such as “immunohistochemistry”, “diagnosis”, “fertility-sparing”, “treatment”, “myomectomy”, “hysteroscopy”, “laparoscopy”, “ultrasound”, “imaging”, etc. There were no restrictions on language or geographic location. We recorded relevant aspects of each article, with special emphasis on histopathological findings, types of treatment applied, and reported outcomes. Our exclusion criteria included cases with no clinical information for data extraction, such as those lacking details on symptoms and/or survival, as well as duplicate reports. However, conference abstracts providing relevant information (in at least three categories) and published as supplements to established scientific journals were included. Two cases reported as UTROSCTs were excluded due to an immunohistochemical profile and a histological appearance that were not compatible with those of UTROSCT. Age differences between study groups were analyzed using the Student’s t-test, with a two-sided p-value of ≤ 0.05 considered statistically significant. Statistical analyses were conducted using JASP statistical software v.0.17.3 for Windows.

3.2. Characteristics of Included Publications

We selected 104 case reports (studies with up to 3 cases) [3,10,11,12,13,14,15,16,17,18,19,20,21,22,23,24,25,26,27,28,29,30,31,32,33,34,35,36,37,38,39,40,41,42,43,44,45,46,47,48,49,50,51,52,53,54,55,56,57,58,59,60,61,62,63,64,65,66,67,68,69,70,71,72,73,74,75,76,77,78,79,80,81,82,83,84,85,86,87,88,89,90,91,92,93,94,95,96,97,98,99,100,101,102,103,104,105,106,107,108,109,110,111,112] and 24 case series (including between 4 and 75 cases) [4,6,113,114,115,116,117,118,119,120,121,122,123,124,125,126,127,128,129,130,131,132,133,134]. For a better readability, the cases are summarized in Table 2 (studies reporting 1–3 cases without recurrence), Table 3 (individual aggressive cases with extrauterine spread or recurrence), Table 4 (all series with more than 4 cases), and Table A1 (detailed data on patients who became pregnant with or after UTROSCT). The publications were mostly in English, two in German [15,79], two in Portuguese [23,48], and one in Spanish [19].
What makes our review the largest available review on UTROSCT is that we identified a total of 511 UTROSCT cases, including 93 individual cases with benign behavior (no extrauterine growth at the first diagnosis or recurrence, or with no reported recurrence) as listed in Table 3, 28 individual cases with aggressive behavior (extrauterine spread or metastasis at first diagnosis, or recurrent disease) listed in Table 4, and a further 373 cases reported in case series (starting with the seminal study by Clement and Scully [4] with 14 cases, up to the largest cohorts by Boyraz et al. [129] with 75 cases and Moore and McCluggage [122] with 34 cases), as shown in Table 5.
The year 2023 could be groundbreaking for UTROSCT research, as until November 2023, six series with a total of 156 cases, focusing on novel genetic and immunohistochemical insights, as well as 7 reports (including the present study) with a total of 8 cases, were published.
Some studies did not differentiate between UTROSCT type 1 and type 2, others included only type 2, and some studies used criteria for sex cord elements different from those of Czernobilsky [5]. In addition, recent research indicates that, in light of genetic heterogeneity, the dichotomous classification may be obsolete. With these facts in mind, we included both types of UTROSCTs to maintain comparability between older and newer studies.

3.3. Patient Characteristics

For patients reported individually, the mean age of women with a non-aggressive disease course (48.7, SD 14.66, range 18–77 years) and malignant disease course (46.8, SD 15.4, range 18–68 years) did not differ significantly (p = 0.53). Women aged 40 or younger accounted for 33% (31/93) of benign cases and 32% (9/28) of clinically aggressive cases. The age distribution is displayed in Figure 6.
The mean age and age range in our evaluation are similar to those reported in the landmark 1976 study by Clement and Scully, as well as in recent case series, e.g., Boyraz et al., 53 years (range 21–84) [129], and Goebel et al., 49.6 years (range 20–74) [125]. The youngest patient (12 years old) and the oldest (86 years old) were reported in the large case series by Moore and McCluggage [122].
The proportion of benign to malignant disease courses in our evaluation was 3:1, acknowledging the possibility of publication bias. There were 19 nulliparous women in the cohort, presenting a therapeutic challenge due to the uncertainty about the safety of fertility-sparing treatments and the dilemma of the potential overtreatment, including unnecessary hysterectomy and oophorectomy [114,127].

3.4. Clinical Presentation

The most common symptom across all ages and menopausal statuses was abnormal uterine bleeding (AUB), followed by pelvic pain or abdominal discomfort. In some cases, the tumor was asymptomatic and discovered incidentally during routine check-ups or infertility evaluations [25,50,56]. Hormonal disturbances such as galactorrhea [95], hyperprolactinemia [95,107], or hypercalcemia [20], resulting from ectopic prolactin or PTH-related peptide production, were the initial symptoms in other cases. Notably, in two cases, an emergency involving intraabdominal bleeding from the tumor led to the diagnosis of UTROSCT [89,93].
UTROSCTs typically mimic leiomyomas in their submucosal or intramural presentation. In around 15% of cases, the tumors present as intracavitary polyps. Pretherapeutic curettage sometimes yielded falsely negative results [75,76,111] or abnormal but misleading findings, such as low-grade endometrial stromal sarcoma (LG-ESS) [49,92,110], rhabdoid tumor [52], carcinosarcoma [14], or adenocarcinoma [100]. The value of preoperative targeted biopsy remains uncertain. It can either provide the definitive result (as in our Case 2 or [56]) or be misleading, as in [100], where image-guided omental biopsy revealed high-grade adenocarcinoma suggestive of epithelial ovarian carcinoma. The reason for the uncertainty may be the heterogenous composition of the tumor itself or a sampling error due to the presence of several similar lesions.
In all but one reported cases, the diagnosis of UTROSCT was always unexpected and was made through the evaluation of the final surgical specimen. Intriguingly, the intraoperative appearance (via hysteroscopy or laparoscopy) often did not alter the initial assumption of the lesion being a leiomyoma or a polyp.
In only one case was UTROSCT suspected preoperatively, based on a cervical liquid biopsy. However, even in that case, the diagnosis was facilitated by the presence of a polypoid tumor protruding into the vagina, and it was confirmed using extensive immunohistochemical staining, as the initial diagnosis was “atypical glandular cells consistent with adenocarcinoma, NOS” [69].
The coexistence of UTROSCT with other tumors at the time of surgery was not unusual, mostly with typical leiomyomas [18,27,41,42,43,45,48,60,103], but also with other neoplasms such as a second UTROSCT [29,60], ovarian sex cord stromal tumors [41], gastrointestinal stromal tumors [94], endometrial adenoacanthoma [17], cervical intraepithelial neoplasia [120], or cervical metastasis from breast cancer [40].
Information on the diagnostic utility of tumor markers for UTROSCT is scarce. Elevated CA-125 (up to 2210 U/L in [100]) levels have been occasionally reported [60,88,100,135], linking with extrauterine tumor spread [60,100,110] or accompanying conditions like adenomyosis [135]. Notably, CA-125, HE4, and CEA, which were normal in some reports [66,77,111], are not typical markers for sex cord tumors. Interestingly, serum Inhibin levels, a marker for sex cord tumors, have not been reported, reflecting the oversight of sex cord differentiation during perioperative consideration. Nevertheless, if elevated at the initial diagnosis, tumor markers (CA125, prolactin) might be useful for monitoring recurrence and response to therapy [100,110].
The usefulness of imaging in UTROSCT is limited, presenting no specific sonomorphologic or MRI features that would facilitate preoperative diagnosis. While there are detailed MRI reports, none have resulted in the correct preoperative identification of UTROSCT [17,30,49,71,72,81]. Intratumoral cystic degeneration, intratumoral hemorrhage, and necrosis are often seen on MRI, but are not pathognomonic [81], and can be mistaken for a liquid degeneration within a leiomyoma [63,71]. Unfortunately, imaging has sometimes led to the incorrect suspicions of UTROSCT relapse. For example, Hermsen et al. [49] reported a suspected early myometrial recurrence during pregnancy, which was monitored using MRI until the 34th week of gestation. The patient underwent a cesarean hysterectomy due to the presumed recurrence, but the lesion turned out to be adenomyosis. Carbone et al. [127] described lymphadenectomies performed due to suspected lymph node metastasis on imaging, which were not confirmed histologically.
Few cases were diagnosed with distant metastases at the time of diagnosis (see Table 4). Intraabdominal relapse and pulmonary metastases were the most common relapse sites [4,93,101,114,122]. Among all 511 cases, 18 patients died from or with the disease [4,93,100,111,112,114,122,129,130]. Those who died often experienced rapid disease progression, were metastatic at diagnosis, or progressed despite adjuvant therapies [93,111,112]. This raises the question of whether the application of unproven chemotherapeutic or hormonal therapies in UTROSCT could potentially worsen prognosis. Generally, survival data should be interpreted with caution due to the uncertain degree of underreporting, as follow-up times, when available, were often reported in months rather than years.

3.5. Gross and Ultrastructural Appearances

The mean size of tumors behaving benignly was 5.4 cm (SD: 4 cm, range: 0.9–20 cm), and for those behaving aggressively, it was 6.6 cm (SD: 3 cm, range: 1.5–11 cm), which was not significantly different (p = 0.27). Tumor growth limited to the cervix was observed infrequently, in approximately 10 cases. Most tumors presented as yellow to tan-yellow, tan-pink, or tan-gray masses, occasionally with hemorrhage or cystic areas. Microscopically, most tumors were well-circumscribed, but up to one-quarter exhibited an infiltrative growth pattern [121,129]. By definition, UTROSCTs mainly comprise cells resembling ovarian sex cord elements which are arranged in cords or trabeculae, or form tubular structures with central lumina. Occasional cases demonstrate retiform appearances [116]. Indeed, in the largest series by Boyraz et al., the following architectural patterns were present: cords, diffuse, hollow tubules, nests, trabeculae, retiform, solid tubules, pseudoangiomatoid, pseudopapillary, and whorled [129]. Typically, more than one pattern was seen. Cytologic atypia ranged from absent to mild in the majority of cases, and it was moderate in 21% and moderate-to-severe in 2.7% of tumors [129].
UTROSCTs exhibit a diverse immunohistochemical profile reflecting their complex histogenesis. The widely accepted immunohistochemical signature of UTROSCT is defined by a panel comprising Calretinin, Inhibin, CD99, and Melan A—markers indicative of sex cord lineage. Positivity for Calretinin, in conjunction with at least one other marker from this panel, is diagnostic for UTROSCT, whereas ESTSCLE generally express a single sex cord marker, predominantly Calretinin [5]. Other popular antibodies used in the diagnosis of UTROSCT are those immunoreactive for mesenchymal and epithelial elements, including Vimentin, Desmin, Cytokeratin, Epithelial Membrane Antigen (EMA), CD10, and estrogen/progesterone receptors (ER/PR) [5,41]. However, several studies rely on alternative algorithms [42,96,97,100,101,135,136], considering tumors such as UTROSCT to be negative for Calretinin but positive for other sex cord markers. Nogales et al. emphasize that UTROSCTs are not “a discrete entity but a group of tumors that do not necessarily have a stereotyped morphology and are only defined by comparison with histologically equivalent ovarian tumors. Morphologically, they imperfectly reproduce the histology and immunohistochemistry of a variety of patterns (trabecular, tubular, pseudoglandular, luteinized, etc.) of sex-cord stromal tumors of the ovary. Moreover, some exhibit a mixed sex cord and predominantly myoid phenotype, which can also be part of the tumor proliferation in sex-cord-like structures of UTROSCTs” [137].
Some authors favor CD56 as the most reliable immunohistochemical UTROSCT marker [41,42]. A review on the immunohistochemical features of the 44 cases of UTROSCT reported by Abdullazade et al. showed CD56 expression in 100%, followed by positivity for Calretinin in 94%, AE1/AE3 in 73%, CD10 in 50%, Inhibin in 49%, Desmin in 46%, EMA in 29%, and Caldesmon in 7% of cases [41]. In addition, Stewart et al. explored both older and newer immunohistochemical markers of sex cord-like elements in UTROSCT and confirmed that Calretinin was more sensitive than Inhibin, FOXL2, and steroidogenic factor-1 (SF1), but SF1 was the only marker specific to UTROSCT, as it was negative in all potential histological mimics that were investigated [121]. These results were confirmed by Croce et al., who found that 53% (10/19) of investigated UTROSCT samples exhibited nuclear immunoreactivity with FOXL2, and 58% (11/19) showed nuclear staining with SF1 [123].
Apart from the polyphenotypic histomorphologic appearance of UTROSCT itself, in some cases, UTROSCT displayed partial sarcomatous features [77], myxoid features [87], or osteoid metaplasia [12]. Conversely, UTROSCT elements can be incorporated into other tumors, e.g., adenomyosis [135], true endometrial polyps [138], endometrioid carcinomas [139], or LG-ESS [136,140]. Two intriguing cases reported 32 years apart (1989 and 2021) involved the initial tumors diagnosed (or misdiagnosed?) as LG-ESS, but recurrences with significantly abundant sex cord-like elements met the diagnostic criteria of UTROSCT [92,110]. In the first case, speculation about the misdiagnosis of the initial tumor could be justified (even the report’s title uses of confusing terminology); however, the latter case is substantiated by meticulous molecular analysis showing a UTROSCT-typical genetic rearrangement in the recurrent tumor (GREB1-NCOA2 fusion) [110].

3.6. Gene Fusions in UTROSCT

Recent studies have highlighted the significant role of specific gene fusions in UTROSCT, particularly those combining genes relevant to sex hormone pathways with (co)activator oncogenes. These include estrogen receptor 1 (ESR1) and growth regulation by estrogen in breast cancer 1 (GREB1) genes, which fuse with nuclear receptor coactivators NCOA1-3 [76,104,105,124,125,131,134]. GREB1 encodes for a protein driven transcriptionally by estrogen-bound ER, being a crucial component of the canonical estrogen/ER signaling pathway. Binding with estrogen, ESR1 is essential for a broad range of physiological functions, but is also involved in pathologic processes, including breast cancer, endometrial cancer, or osteoporosis [76,104,105,132,133,134]. Mutations in ESR1′s ligand-binding domain have been correlated with resistance to hormone therapy in ER-positive breast cancer. Notably, UTROSCTs with ESR1 rearrangements may be resistant to estrogen blockade as the ER ligand-binding domain is lost in these fusions, potentially explaining the resistance to anti-hormonal treatments reported in relapsed UTROSCT [96,99,112].
The NCOA family, a part of the p160 steroid receptor coactivators (SRC1/2/3), interacts with ligand-dependent hormone nuclear receptors, including estrogen receptor-alpha (ERα). It mediates transcriptional programs promoting cellular proliferation, metabolism, growth, and survival [109]. In UTROSCTs with NCOA rearrangements, the chimeric fusion protein expressed is under the transcriptional control of the 5′ fusion partner promoter, retaining the 3′ NCOA fusion partner’s nuclear receptor co-activator and transcriptional activation domains [105,109,141]. Recent research has specifically focused on NCOA1, NCOA2, and NCOA3 gene fusions in UTROSCT [76,104,105,124,125,131,134]. Bi et al. reported that in recurrent UTROSCT cases, the GREB1::NCOA2 fusion was the most common, accounting for 57% of cases, with GREB1::NCOA1 and ESR1 fusions also detected. These GREB1-rearranged tumors were typically more advanced, larger, and occurred in older patients [132]. Lu et al. reported recurrent NCOA1-3 rearrangements in 87.5% (14/16) of their series, without JAZF1, PHF1, BCOR, or YWHAE rearrangements, underscoring the diagnostic value of these rearrangements in distinguishing UTROSCT from endometrial stromal tumors [131]. In Goebel et al.’s study of 26 UTROSCT cases, NCOA1/3 rearrangement was identified in 81.8% (18/22) of cases, with ESR1-NCOA3 being the most common fusion, followed by GREB1-NCOA1, ESR1-NCOA2, and GREB1-NCOA2 rearrangements. Only one case experienced recurrence 66 months after the initial diagnosis, and this was the only case with a GREB1-NCOA2 fusion [125]. In the recent case series by Quji et al., six types of fusion genes were identified: ESR1::NCOA3 (found in 4 cases), ESR1::NCOA2 (2 cases), ESR1::CITED2 (2 cases), GREB1::NCOA2 (2 cases), GREB1::NCOA1 (1 case), and GREB1::NCOA3 (1 case). Notably, the three cases with recurrence and metastasis were associated with the fusion genes GREB1::NCOA2, ESR1::NCOA3, and ESR1::CITED2 [134]. Additionally, Croce et al. reported a novel translocation t(2;3) involving GREB1 and CTNNB1 (encoding β-catenin), activating the Wnt/β-catenin signaling pathway and presenting a potential new therapeutic target [105,123]. These gene fusions, especially those involving NCOA genes, interact with hormone nuclear receptors and mediate essential cellular functions, hinting at the oncogenic potential when these are dysregulated [109]. The partner genes of GREB1- or ESR1-rearranged UTROSCT, including NCOA1–3, NR4A3, GTF2A1, and CTNNB1, are described in Table 6.
To mention the negative findings in UTROSCT, which can be useful in differentiation from other uterine neoplasms, it has been consequently shown that UTROSCTs lack the JAZF1-JJAZ1 translocation that is frequently seen in endometrial stromal tumors [87,97,117]. Furthermore, the Bcl-2 and MALT1 genes are unlikely to be involved in the pathogenesis of UTRSCT, although they are located close to the frequently observed translocation points t(X;6)(p22.3;q23.1) and t(4;18)(q21.1;q21.3) [22,31]. Finally, UTRSCTs frequently exhibit positivity for sex cord markers FOXL2 and SF-1 without showing any mutations in the FOXL2 and DICER1 genes [123].

3.7. Risk Factors and Prognostic Factors

Considering the small number of cases, there are no established risk factors for UTROSCT, and reports on their hereditary background are absent. Seven UTROSCT cases have been reported in patients treated with tamoxifen [28,36,40,46,70,116,126]. A causal association should be approached with caution, as the majority of UTROSCT cases developed without tamoxifen exposure, and the number of women exposed to tamoxifen—due to the high incidence of breast cancer—is disproportionately large in comparison to the rarity of UTROSCT. Furthermore, some gene rearrangements seen in UTROSCT (GREB1-fusions) are known to make the tumors responsive to tamoxifen therapy.
Factors such as age, menopausal status, or the extent of surgery (whether uterus-preserving or not) have not been predictive of relapse. Accordingly, in our review, age and tumor size have not been associated with more aggressive disease course.
Traditionally, based on the series by Clement and Scully, recurrences are more commonly associated with type 1 tumors than with type 2 tumors [4,113]. Certain histological features have been identified as prognostic factors in UTROSCT. Boyraz et al. observed five recurrences among 58 patients over an average follow-up time of 73 months (ranging from 22 to 192 months) and concluded that malignant UTROSCTs exhibited more than three of the following five features compared to their benign counterparts: size greater than 5 cm, at least moderate cytologic atypia, three or more mitoses per 10 high-power fields (HPF), infiltrative borders, and necrosis. One of the five malignant tumors displayed extensive rhabdoid morphology [129]. Additionally, tumor size, lymphovascular space involvement, nuclear atypia, cervical involvement, or the proliferation index (Ki67) could not be confirmed as prognostic factors in UTROSCT by various authors [54,91,94,95,97,98,99,122].
Myometrial invasion and serosal involvement are traditional pathological risk factors evaluated, though their utility in UTROSCT has been supported by individual observations without comparators [54,95,97,98,99]. In contrast, tumors with infiltrating growth patterns and no recurrences during follow-ups are well-documented [47,50]. Some immunophenotypes, like those with a predominant epithelial retiform component (RUTROSCT), seem to be associated with a good prognosis and could help in preventing overtreatment in selected patients [116]. Due to the relative overrepresentation of malignant cases in the dataset of Moore and McCluggae, their findings are particularly insightful regarding the malignant potential of individual UTROSCT cases, i.e., 8 of 34 patients (23.5%) developed extraterine metastases in various sites, including the pelvic and abdominal peritoneum, ovary, lymph nodes, bone, liver, and lung, and three patients (8.8%) died due to the tumors [122]. Neoplasms exhibiting malignant behavior that occurred on average in older patients were larger and more likely to show necrosis, lymphovascular invasion, cervical involvement, significant nuclear atypia, and significant mitotic activity. Finally, only the presence of necrosis and a significant mitotic activity were statistically significant [122].
Given the overlap in pathological parameters between clinically benign and malignant neoplasms, some authors proposed considering all UTROSCTs as potentially malignant until proven otherwise [122]. This somewhat fatalistic view has been significantly clarified in recent years by numerous studies equivocally pointing to specific genetic changes within UTROSCT as the most important predictors of malignancy and recurrence. Gene rearrangements involving key genes in sex hormone pathways appear to be the best predictors of recurrence. As demonstrated in [105,125], UTROSCTs with GREB1 rearrangement may have a high risk of recurrence or metastasis. Regarding prognosis, GREB1-rearranged tumors tended to occur in significantly older women than UTROSCT with ESR1 fusions; moreover, GREB1-rearranged tumors tended to be larger and more mitotically active and behave more aggressively [105]. Recently, Yin et al. [86] described novel fusion genes involving ESR1 and GREB1 as the 5′ partner and NCOA1-3 as the 3′ partner. Genotype and phenotype correlation has suggested that GREB1-rearranged UTROSCTs may have a higher tendency to behave aggressively.
Particularly, tumors with GREB1::NCOA2 fusions are more likely to recur than those with any other genetic alteration [132]. The suggestive study by Xiong et al. combined classical histomorphological, immunohistochemical, and molecular–genetic predictors, and finding a significant mitotic activity, a high expression of stromal PD-L1, and an NCOA2 gene alteration may help in identifying the subset of UTROSCT with aggressive behavior and shorter disease-free survival (DFS) [130].

3.8. Treatment Strategies

Total abdominal hysterectomy with BSO was the most common treatment, followed by total abdominal hysterectomy without BSO. Other forms of hysterectomy, such as (laparoscopically assisted) vaginal hysterectomy, were also reported [4,63,118,120].
For women who have completed their reproductive plans, a total HE, whether abdominal or laparoscopic, and depending on menopausal status, with or without ovariectomy, appears to be an adequate treatment for tumors confined to the uterus.
Supracervical hysterectomy, although mentioned incidentally in reports by Bakula-Zalewska et al. [119] and Carbone et al. [127], does not appear to be appropriate for UTROSCT because of its potential for cervical involvement and the need for tumor morcellation, which can increase the risk of recurrence [109]. The scarcity of intraoperative details in most cases and documented recurrences following tumor disintegration [58,60,109] should prompt surgeons to be particularly vigilant.
When bulky lymph nodes are present, removing the nodes and performing regional lymphadenectomy is a straightforward decision. However, for cases with histologically aggressive tumors in preoperative specimens, there is no established strategy. The use of indocyanine green for sentinel lymph node detection, while aligning with current trends to minimize perioperative morbidity [142], has not been specifically studied in UTROSCT. Consequently, routine systematic lymphadenectomy or non-specific sampling in UTROSCT lacks robust support from existing evidence. Individual decisions, taking into account patient preferences, are advisable in such scenarios.
Given the fact that around 15% of all reported cases occurred in nulligravidas, the possibility of uterus-preserving treatments and, on the other hand, the identification of tumors with aggressive behavior (where conservative treatments could potentially lead to worse prognosis) are critical. Confusingly, among nulliparous patients, only 30% underwent fertility-sparing treatments. Notably, the recurrence rate does not appear to be higher following fertility-sparing treatments compared to hysterectomy or more radical approaches. In the youngest reported case, a 12-year-old patient underwent uterus-sparing removal of a 19.5 cm tumor and remained recurrence-free at a 27-month follow-up [122]. Conversely, cases of nulliparous patients aged 18 [92] and 19 [114] who underwent hysterectomy and BSO raise concerns about the potential overtreatment.

3.9. UTROSCT and Fertility

Ten cases of pregnancy associated with UTROSCT have been reported, including two pregnancies in one patient both during and after UTROSCT treatment [127]. Interestingly, three cases of UTROSCT were identified during evaluations for primary or secondary infertility [25,50,56], and another case was detected following a miscarriage curettage [127]. In three instances, conception occurred while the tumor was present [93,127] or shortly after tumor resection [49]. Seven nulliparous women successfully conceived following fertility-sparing treatments for UTROSCT [25,34,49,50,56,58,127], and each experienced an uncomplicated pregnancy. Except for one in vitro fertilization [50], all pregnancies occurred spontaneously. One patient, diagnosed with an advanced tumor in the 35th week of pregnancy [93], died nine months later due to disease progression; however, all other patients remained alive. Some women underwent hysterectomy at or after delivery [49,58], while others did not [34,56,127]. These cases are summarized in Table A1.
A viable approach appears to be delayed hysterectomy, undertaken immediately after fulfilling reproductive plans. This strategy was employed in cases [49,50,58]. Schraag et al. reported a successful pregnancy in a patient who had undergone two organ-preserving treatments (initially for tumor persistence and subsequently for relapse), eventually followed by a hysterectomy [58]. Considering the potential for late local recurrences and the absence of long-term cohort studies, offering a hysterectomy upon the completion of family planning seems advisable [25,58].

3.10. Follow-Up

Follow-up protocols for UTROSCT differ between authors. Common imaging modalities like transvaginal ultrasound or MRI can be used, since the problem with UTROSCT is not that it is not visible on imaging, but only indistinguishable from common pathologies by ultrasound or MRI. Accordingly, most recurrences were detected through ultrasound or MRI. While there are no established serum tumor markers specific to UTROSCT, markers that were elevated at initial diagnosis and responsive to treatment should be monitored during follow-up. Notably, increases in serum CA125 [100,110] or prolactin [95,107] levels have preceded some recurrences.
In cases where the initial approach was hysteroscopic, performing repeat hysteroscopy to exclude intracavitary tumor residues after local resection [34] or as a part of follow-up can enhance the safety of conservative strategies [37,56]. Garuti et al. proposed a follow-up regimen of clinical examinations and transvaginal sonography at 6-month intervals, supplemented by office hysteroscopy every 12 months for the first three years [37]. whereas Similarly, De Franciscis et al. recommended transvaginal ultrasound examinations every six months and diagnostic hysteroscopy annually for five years [56]. The duration of follow-up remains undefined due to low number of recurrent cases, no established patterns of recurrence, and PFSs of 7 [112], 11 [96], 14 [110], 23 [99] or 32 [104] years being not uncommon.

3.11. Recurrence Treatments

Surgery aimed at the complete removal of any tumor residues key to long-term survival, even in the cases of recurrence, with singular follow-ups reaching 32 years [104]. Cömert et al. [102] calculated the average recurrence rate of UTROSCT at 6.3%. The response to chemotherapy and hormonal treatments is generally poor. Reported chemotherapeutic regimens include ifosfamide, carboplatin, and CYVADIC (cyclophosphamide, vincristine, doxorubicin, and dacarbazine), with no response in a patient who subsequently died 9 months after the initial diagnosis [93]. BEP (bleomycin, etoposide, cisplatin) was used in a 43-year-old patient with recurrence [60], as well as megestrol acetate and letrozole, with recurrence occurring 3 months after the completion of adjuvant therapy. Letrozole and medroxyprogesterone acetate were abandoned after 3 months due to no response [99]. Blinmann et al. [96] applied tamoxifen, warfarin, and doxorubicin with minimal response and anastrazol with uncertain effect. Another patient received BEP and relapsed 8 months after the completion of therapy. They continued with carboplatin, paclitaxel, and ombrabulin, with repeated disease progression. The subsequent treatments included epirubicin with pazopanib, letrozole, trabectedin, paclitaxel, BI860585, and exemestane and rechallenged with epirubicin, BMS-986148, and nivolumab until the final progression and death [112].

4. Discussion

This review represents the largest aggregation of UTROSCT cases to date, with 511 cases reported from the initial description in 1945 to late 2023. We also contribute two new cases of UTROSCT: one mimicking a myoma FIGO type 4, diagnosed after laparoscopic “myomectomy,” and another manifesting as a submucous mass with endometrial thickening, diagnosed via office hysteroscopy with endometrial biopsy [143]. For both individuals, a hysterectomy was the chosen definitive treatment.
Although our review provides several insights into UTROSCT’s clinical presentation and management, the level of available evidence is still unsatisfactory, due to relying on case reports and retrospective case series (the largest comprising 75 cases). The available knowledge about UTROSCT suffers from insufficient case numbers and the impossibility of randomized controlled trials, but also publication bias. The latter shortcoming can lead to an overrepresentation of aggressive cases (as stated in [122]) or an assumption of cases to be prematurely benign, as cases with a follow-up of few months or simply not reporting a recurrence are commonly classified as “not recurrent” (the latter limitation may apply also to the present review). The quality of reporting, e.g., lacking histological description [71], further contributes to the uncertainty of available evidence.
AUB is the most common symptom for leiomyomas, endometrial polyps, and other endometrial proliferations [144]. The symptoms and the sonographic appearance of UTROSCT are identical with those of very common uterine pathologies responsible for AUB or pelvic pain. In addition, a significant proportion of UTROSCTs become asymptomatic, a characteristic shared with uterine myomas. The sonographic or MRI appearance is usually suggestive of uterine leiomyoma or, less commonly, adenomyosis. Neither the size (ranging from 1 to 20 cm), nor the relationship to the myometrium (whether submucosal or intramural) or endometrium (such as polypoid intracavitary growth), facilitates the differentiation of UTROSCT from myomas or polyps. Additionally, it is noteworthy that UTROSCT often coexists with one or more leiomyomas in the same patient [18,27,41,103].
The difficulty in differentiating between uterine tumors with a sonographic appearance similar to myomas is well known [145,146,147]. In the study by Russo et al., no significant differences were observed between benign and malignant lesions in terms of echogenicity, the presence of shadowing, or size; however, cystic areas within the lesion were seen in 31% of typical leiomyomas and in 55% of leiomyoma variants, adenomyomas, and smooth muscle tumors of uncertain malignant potential (STUMP) or leiomyosarcoma. Lesion borders were regular in 99% of benign lesions and 40% of malignant lesions [145]. Similarly, intratumoral cystic areas, poor or moderate vascularization, and the absence of shadowing were more common in sarcomas [146] and in STUMP [147]. In this context, the observation by Chiappa et al. that sparse edge shadowing and a lesser degree of vascularization, especially intralesional, might be more common in UTROSCT than in typical leiomyomas is not surprising. However, these findings cannot be interpreted as UTROSCT specific [73].
Our review confirmed that age and tumor size do not differ between patients with UTROSCT presenting aggressive behavior (defined by the initial extrauterine tumor spread or recurrence) and those with benign clinical course. The unspecific symptomatic and sonographic appearance, grossly overlapping with those of uterine myomas or intracavitary polyps, are the inherited features of UTROSCT and therefore not modifiable. Nevertheless, progress has been achieved in the areas of individualized therapy planning and immunohistochemical and molecular diagnosis.
The analysis of gene fusions is a new tool in the differential diagnosis of UTROSCT, offering novel prognostic factors that facilitate tailored therapy planning. For example, UTROSCT differs from endometrial stromal neoplasms (including those with sex cord stromal differentiation) in that it typically does not exhibit the JAZF1-SUZ12 fusion or PHF1 rearrangements [7]. Furthermore, UTROSCT is not associated with FOLX2 and DICER1 mutations, which are indicative of ovarian adult-type granulosa cell tumors and Sertoli–Leydig cell tumors, respectively [7]. On the other hand, recent findings have identified recurrent fusions involving NCOA2 and NCOA3 (such as ESR1-NCOA3, ESR1-NCOA2, or GREB1-NCOA2) in UTROSCT. These genes, NCOA2 and NCOA3, are known to be involved in steroid hormone regulation, and the disruptions in their nuclear receptor coactivator domains are thought to play a crucial role in the development of UTROSCT [7,76,104,105,124,125,131,132,133,134].
Recent research has provided molecular features that aid in a more personalized approach. We assume that the future of UTROSCT diagnosis and treatment—including the decision to preserve the uterus or not—will be the molecular–genetic testing, as it has become common in other gynecologic malignancies, e.g., endometrial carcinoma [148,149]. This hypothesis is supported by numerous recent studies [86,105,109,123,124,125,126,128,129,130,131,132] that identified factors associated with aggressive clinical behavior and recurrence. In UTROSCT, GREB1 or ESR1 often fuse with members of the p160 steroid receptor coactivator family, which includes NCOA1, NCOA2, and NCOA3. These gene fusions, such as GREB1::NCOA2 and ESR1::NCOA2, result in the aberrant activation of estrogen signaling pathways, driving the proliferation and survival of tumor cells. The fusion proteins maintain the transcriptional activation function, which may lead to the dysregulated expression of genes that are normally regulated by sex hormones, potentially contributing to the tumorigenesis of UTROSCT. The specific fusion types, particularly GREB1::NCOA2, are associated with a higher recurrence risk. Furthermore, the GREB1 rearrangements can be detected both in aggressive primary and relapsed tumors [105,125]. Since specific gene fusions, a high expression of stromal PD-L1, and a significant mitotic activity have been shown to predict aggressive UTROSCT [130], we postulate to include these parameters into the standard evaluation of UTROSCT. Along with these findings, the most recent WHO classification concludes that “although data is limited, features that may be associated with aggressive behavior include a mitotic count >2 per 2 mm2 (>2 mitoses per 10 HPFs if field diameter is 0.55 mm), necrosis, extensive (>50%) rhabdoid morphology and potentially tumors with GREB1 rearrangement” [1].

Criteria for Fertility-Sparing UTROSCT Treatments

A significant strength of the paper is the accumulation of cases with a favorable outcome despite uterus-preserving strategies. In 2015, Watrowski et al. recommended to consider uterus preservation—after counseling about the unpredictable course of the disease—in young patients with small, well-circumscribed tumors limited to the intrauterine cavity, with a hysteroscopic follow-up or at least a regular transvaginal ultrasound [47].
As of 2023, in light of the current literature, we suggest following criteria for considering fertility-preserving treatments:
  • Desire for pregnancy.
  • Evaluation and documentation of risk factors:
    Tumor size/extrauterine spread;
    Presence of necrosis;
    Mitotic activity;
    Presence of GREB1::NCOA-1/3 fusions.
  • No tumor residues after last treatment (e.g., negative re-hysteroscopy).
  • Possibility and adherence to follow-up.
  • Offering hysterectomy after the completion of family planning.

5. Conclusions

Our review of literature comprises the largest data extraction from 511 cases, two of them being reported for the first time. UTROSCT is not associated with specific clinical presentations or pathognomonic findings; the symptoms and sonographic appearance of UTROSCT largely overlap with those of leiomyoma, and less commonly, with those of adenomyosis or endometrial polyps. Therefore, it is usually discovered accidentally, often after a disintegrating surgical modality performed for benign pathology. Fertility-preserving initial treatment does not seem to worsen the prognosis. Common parameters, like patient age, tumor size, lymphovascular space invasion, nuclear atypia, and cervical involvement, are not prognostic factors in UTROSCT. However, current research suggests that aggressive cases (with extrauterine spread or recurrence) can be identified based on a distinct genetic and immunohistochemical phenotype. Particularly, UTROSCT with GREB1::NCOA2 gene fusions or the expression of the PD-L1 molecule seem to be predisposed to metastasize and relapse. Hence, we advocate a subclassifcation of UTROSCT according to molecular criteria to allow a better selection of women suitable for fertility-sparing treatments and, on the other hand, with an increased risk of relapse, possibly requiring more radical treatments.

Author Contributions

Conceptualization, M.P., R.W., M.C.D.A. and A.D.S.S.; methodology, M.C.D.A., M.P., R.W. and S.G.; formal analysis, R.W.; investigation, R.W., M.P., S.G. and M.C.D.A.; resources, R.W. and M.P.; data curation, R.W., M.P. and M.C.D.A.; writing—original draft preparation, R.W., M.P., S.G. and M.C.D.A.; writing—review and editing, R.W., M.P., A.D.S.S. and M.C.D.A.; visualization, M.P., M.C.D.A., A.G. and G.B.; supervision, G.B., B.Z., P.G., A.D.S.S. and M.C.D.A. All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

Not applicable.

Informed Consent Statement

Written informed consent has been obtained from the patients to publish this paper.

Data Availability Statement

The data presented in this study are available on request from M.P. and R.W.

Conflicts of Interest

The authors declare no conflicts of interest.

Appendix A

Table A1. Patients with pregnancy concurrent to or following UTROSCT.
Table A1. Patients with pregnancy concurrent to or following UTROSCT.
First Author, YearAge SymptomsSize (cm)TreatmentInfiltrative MarginsConceptionTime from dgn (mo)Delivery ModeRecurrenceHE after Childbearing Total FU, mo
Di Vagno, 1995 [93]N/aHemoperitoneum at 35 weeks5Caesarean HEYesSpoCo, concurrent with UTROSCT0CS, 35 weeksPDYes9
Hillard, 2004 [25]32Infertility; AUBN/aLsc TR SpoCo15N/aNo 15
Anastasakis, 2008 [34]28AUBN/aHsc TRNoSpoCo6VDNoNo27
Hermsen, 2015
(Case 1) [49]		36AUBN/aHsc TRYesSpoCo, concurrent with UTROSCT0CS (with HE), 34 weeksNoCaesarean HE at 34 weeks (no reisdual tumor)24
Jeong, 2015 [50]32Infertility, AUB3Hsc TRYesIn vitro fertilization3CS, 36 weeks, 3070gYesLsc HE (residual tumor on specimen)47
De Franciscis, 2016 [56]38Infertility, AUB1Hsc TRYesSpoCo2CS, 39 weeksNoNo60
Schraag, 2017(Case 2) [58]28Pelvic pain10Open TRNoSpoCo (after second surgery for residual tumor)19CS (with HE) at 39 weeksYes (20 mo after CS)Caesarean HE at 39 weeks55
Carbone, 2021
(Case 1) [127]		25AUB0.2D&C (for miscarriage) followed by Hsc TRN/a1st: SpoCo concurrent with UTROSCT, 2nd: SpoCo24VD, 39 weeks, 3590 gNoNo96
Carbone, 2021
(Case 2) [127]		30AUB4open TRNoSpoCo13CS, 38 weeks, 3080 gNoNo16
ys—years, mo—months, AUB—abnormal uterine bleeding, N/a—not available, HE—hysterectomy, Hsc—hysteroscopic, Lsc—laparoscopic, TR—tumor resection, and SpoCo—spontaneous conception.

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Figure 1. Sonographic appearance and measurements in three dimensions of the UTROSCT in Case 1.
Figure 1. Sonographic appearance and measurements in three dimensions of the UTROSCT in Case 1.
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Figure 2. Sonographic Power-Doppler appearance of the UTROSCT in Case 1.
Figure 2. Sonographic Power-Doppler appearance of the UTROSCT in Case 1.
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Figure 3. Magnetic resonance imaging of the UTROSCT in Case 1.
Figure 3. Magnetic resonance imaging of the UTROSCT in Case 1.
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Figure 4. Intraoperative view: (A) typical intramural leiomyoma with a slight serosal protrusion of the posterior uterine wall and smooth Douglas peritoneum and (B) after incision, the tumor still presents as an intramural myoma.
Figure 4. Intraoperative view: (A) typical intramural leiomyoma with a slight serosal protrusion of the posterior uterine wall and smooth Douglas peritoneum and (B) after incision, the tumor still presents as an intramural myoma.
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Figure 5. The arrows indicate the intraoperative appearance of UTROSCT on the anterior uterine wall (AC) during hysteroscopy, and the post-biopsy view (D) of Case 2.
Figure 5. The arrows indicate the intraoperative appearance of UTROSCT on the anterior uterine wall (AC) during hysteroscopy, and the post-biopsy view (D) of Case 2.
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Figure 6. Age distribution of benign and clinically aggressive cases.
Figure 6. Age distribution of benign and clinically aggressive cases.
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Table 1. Clinical and histological characteristics of UTROSCT (adopted from [7] and [8]).
Table 1. Clinical and histological characteristics of UTROSCT (adopted from [7] and [8]).
Age DistributionAdult women (third to sixth decades)
Equal distribution among parous and non-parous women
Clinical FeaturesAbnormal uterine bleeding
Pain
Often asymptomatic
Gross FindingsWell circumscribed, variable size (median 6 cm; >10 cm in 20%)
Infrequent cervical involvement (<10%)
Infrequent extrauterine spread (<10%)
Homogeneous yellow to tan cut surface
Microscopic FindingsUsually well-demarcated; irregular border with infiltration may occur
Cords trabeculae, nests, gland-like structures, tubules, and retiform growth reminiscent of sex cord stromal tumors
Bland, uniform cells with scant to abundant eosinophilic cytoplasm
Relatively frequent: mitosis (56%), atypia (40%), and plemorphism (40%)
Infrequent: lympho-vascular space invasion (<10%) and necrosis (<7%)
Immunohistochemical FeaturesCalretinin (>95%), CD99 (>90%), CD 56 (>90%), inhibin, WT1, and FOXL2 positive
ER (>70%) and PR (90%) positive
Smooth muscle markers, Melan-A, CD10, and epithelial markers frequently positive
SF1 can be positive
HMB45 negative
Differential DiagnosisEndometrial stromal tumor (nodule or low-grade sarcoma)
Endometrial carcinoma with sex cord differentiation
Perivascular epithelioid cell tumor
Epithelioid smooth muscle tumor
Table 2. Immunohistochemical characteristics of tumors.
Table 2. Immunohistochemical characteristics of tumors.
AntibodyMarker forCase 1 (31 y.o.)Case 2 (58 y.o.)
CalretininSex cordPositive (++)Positive (++)
CD99 Sex cordPositive (++)Focally positive (+)
CD56 (NCAM)Sex cordPositive (++)N/a
InhibinSex cordNegativePositive (++)
Wilms tumor protein (WT1)Mesothelioma/serous differentiationPositive (++)N/a
Cytokeratin (CK 7)Epithelium (e.g., ovarian adenocarcinoma)NegativeNegative
EMAEpithelial membraneNegativeNegative
Alpha-SMC Smooth muscle cellsPositive (++)Focally positive (+)
DesminMuscle-type intermediate filamentsFocally positive (+)Focally positive (+)
CaldesmonMyogenic markerNegativeNegative
E-CadherinEpithelial markerFocally positive (+)Focally positive (+)
P16HPV-related carcinomasFocally positive (+)Negative
Cyclin D1Different cancersNegativeNegative
BCORSoft tissue sarcomas, ESSNegativeNegative
TTF1Lung adenocarcinoma, thyroid carcinomaNegativeNegative
GATA3Breast cancerNegativeNegative
ChromograninNeuroendocrine markerNegativeNegative
SynaptophysinNeuroendocrine markerNegativeNegative
Cathepsin KBreast, lung, prostate, kidneyNegativeNegative
Estrogen receptorGenital and breast carcinomasPositive (++)Positive (++)
Progesterone receptorGenital and breast carcinomasPositive (++)Positive (++)
alpha-SMA: alpha-Smooth Muscle Actin, ER: estrogen receptor, PR: progesterone receptor, WT1: Wilms tumor 1, BCOR: BCL6 corepressor, EMA: epithelial membrane antigene, CK7: cytokeratin 7, TTF1: thyroid transcription factor-1. NCAM: neural cell adhesion molecule (=CD56); and ESS: endometrial stromal sarcoma; (+) and (++) indicate the intensity of staining, with ‘(+)’ denoting a lower intensity and ‘(++)’ indicating a higher intensity.
Table 3. Case reports with benign outcome (no evidence or no reporting of extrauterine spread or relapse).
Table 3. Case reports with benign outcome (no evidence or no reporting of extrauterine spread or relapse).
First AuthorYearAge ParitySymptomSiteSize, cmTreatmentsFU (mo)Associated with
Morehead [3]194544G7, P5AUBUterine mass2vaginal HEN/a
Tang [10]197928N/aAUBIntramural9HE8“indistinguishable from UTROSCT” (but referred to as “stromomyoma”)
Fekete [11]1985 N/a Submucosal HEN/a
Iwasaki [12]198633 TAH Osteoid metaplasia
Erhan [13]199240N/apainIntramural9TAH, BSO Stromomyoma; D&C: normal
Moll [14]199273G2/P1AUB, painPolypoid5TAH, BSO12D&C: carcinosarcoma
Horn [15]199554N/a Uterine mass7.6HE, BSO27Partially retroperitoneal
Miliaras [16]199757N/aAUBIntramural7.5HE, BSO30
Okada [17]2001 Intramural Endometrial adenoacanthoma
Hauptmann [18] 200149N/aAUBIntramural4.5HE 7Multiple leiomyomas
Ribau Díez [19] 200136G3, P3AUBUterine mass5.7HE94
Suzuki [20]200266G1, P1HypercalcemiaCervix8HE, BSON/aHypercalcemia, hyper-PTH-emia
Kuruvila [21]200350N/aAUBPolypoid D&C in both cases12
Wang [22]200334G2, P1AUBSubmucosal 4.7HE, BSO12
Franco [23]200369G7, P4AUBUterine mass7D&C, HE, BSO, LN samplingN/a
Kabbani [24] 200324G0, P0AUBCervix11HE, irradiation, PLN sampling12
Hillard [25]200432G0, P0AUBIntramuralN/aLsc TR15Pregnancy after treatment
Sutak [26] 200572N/aAUBIntramural2.2HE + BSO15
Motiwala [27]200663N/aAUBIntramural11HE + BSON/aMultiple leiomyomas
Oztekin [28] 200658G13, P3PainIntramural6TAH, BSO8Tamoxifen therapy
Zámecník [29]200639N/aN/aIntramural2HEN/aDouble tumor
Calisir [30] 200765N/aPelvic massIntramural8.5HE, BSON/aMazabraud’s syndrome
Sitic [31]200776N/aAUBUterine mass7.5HE, BSO48
Kunz [32]200738G1, P0asymptomaticIntramural12Open TRN/a
Dede [33]200837 AUBIntramural3.5HE, LN samplingN/a
Anastasakis [34]200828G0, P0AUBPolypoidN/aHsc TR27Pregnancy 6 mo after diagnosis
Berretta [35]200926G0, P0AUBUterine mass Hsc TRN/a
Stolnicu [36]200971N/aAUBPolypoid2.5HE, BSO36Adenosarcoma
Stolnicu [36]200964N/aAUBPolypoid8HE, BSO60Adenosarcoma, tamoxifen
Garuti [37]200929G0, P0AUBSubmucosal5Hsc TR13
Aziz [38]200962N/aPMBPolypoid2TAH, BSON/aUneventful “yearly checkups”
Carta [39]201074N/aAUBIntramural17HE, BSO8
Giordano [40]201026G0, P0AUBSubmucosal2.2Hsc TR15
Giordano [40] 201046G2/P2AUBPolypoidN/aHE, BSO (finally)N/aTamoxifen, breast cancer metastasis to the cervix
Abdullazde [41]201046N/aAUB, PainIntramural2HE, BSO24Multiple leiomyomas
Abdullazde [41]201030N/aAUB“myoma”2“myomectomy”N/a
Abdullazde [41]201042N/aAUBPolypoid1.5HEN/a
Özer [42]201338G4/P3AUB, painIntramural18TAHN/aMultiple leiomyomas
Abid [43]201443N/aAUBPolypoid and Intramural1.5D&C, HE, BSO12Multiple leiomyomas
Hashmi [44]201448N/aAUBIntramural7HE, BSON/a
Ehdaivand [45] 201447G0, P0AUBIntramuralN/aLsc HE, BSO, morcellation24Multiple leiomyomas
Gutierrez-Pecharroman [46]201449 Polypoid2HE18Tamoxifen
Watrowski [47] 201522G0, P0AUBSubmucosal2Hsc TR28
Coelho [48]201535G0, P0AUBSubmucosal1.5Hsc TR, followed by TAHN/aMultiple leiomyomas
Hermsen [49] (1)201536N/aAUBSubmucosalN/aHsc TR, Caesarean HE in 34 wop24Pregnancy
Hermsen [49] (2)201568N/aAUBPolypoid1.5D&C, TAH + BSO6 (probably)D&C misleading: ESS
Jeong [50] 201532G0, P0Infertility, AUBSubmucosal3.6Hsc TR, then Lsc HE after 5 mo 47Pregnancy
Lin [51]201537G2, P2AUBSubmucosal5.7Hsc TR, TAHN/a
Byun [52] 201556G4, P2AUButerine mass2.2HE, BSO36
Uçar [53] 201665G6, P5AUBIntramural8TAH, BSO, PLND, PALND12
Gomes [54]201653N/aAUBUterine mass12LASH, BSO, Cervix, OMx, parametrectomy, PLNDN/a
Cetinkaya [55] 201652G2, P2AUBSubmucosal2HE, BSO, PLND, PALND17
De Franciscis [56] 201638G0, P0AUBPolypoid1Hsc TR60Pregnancy
Cho [57]201750N/aAUB 8.7HE, BSON/a
Schraag [58] (3)201772N/aAUBNo macroscopic tumorN/aTAH, BSO 46
Stefanovic [59]201759Multi-PAUBPolypoid10TAH, BSON/aTwo D&Cs (benign polyp) in 5 years prior to UTROSCT
Viau [60] (1)201749G1, P1PainIntramural1.8HE, BSO16Multiple myomas of 8 cm
Sadeh [61]201757N/aAUBPolypoid0.9Lsc HE, BSO36
Varban [62]201846N/aAUBIntramural7HE, BSON/aSubserosal myoma of 3.5 cm
Vilos [63] (1)201852G3, P3AUBSubmucosal1Hsc TR; EMABL; LAVH, BSO 36HE 9 mo after Dgn, no residues
Vilos [63] (2)201847G4, P3AUBSubmucosal2Hsc TR, EMABL; LAVH, BS12
Fan [64] 201862N/aAUBUterine tumor3.8Extended HE, BSO, PLND, PALNDN/a
Thakur [65] 201837G1, P1InfertilityIntramural1.1Hsc/Lsc TRN/a
Rozário Garcia [66]201846G1, P1AUBProlapsed myoma4vaginal TR, then TAH, BSO12
Natarajan [67]201858Multi-PAUBSubmucosal4TAH, BSON/a
Zhang [68] (1)201964N/aAUBUterine mass10HE, BSO12
Zhang [68] (2)201933G2, P1AUBUterine mass3.5HE, BS144
Dubruc [69]201956N/aAUBCervix2.6HE4
Segala [70]201962N/aN/aIntramural7TAH10Tamoxifen; multiple leiomyomas
Takeuchi [71]201948N/aAbdominal fullnessCervix20HE, BSON/aThoracic lymphadenopathy
Li [72]201943N/aasymptomaticPolypoid + Intramural3.1Lsc HE, BS (after HSc, D&C)3Endometriosis
Chiappa [73]201928G0, P0AUBSubmucosal5.5Hsc TR N/a
Kim [74] (1)202029G1, P1PainSubserosal6.5Lsc HE, BSO, PLND3
Kim [74] (2)202049G2, P2AUBUterine mass9HE, BSO12
Nguyen [75]202061N/aAUBPolypoid5.3Extended Lsc HE, BSO, PLND1
Grither [76] 202069N/aAUBUterine mass5.2Robotic HE + BSO8
Sato [77]202057G2, P2PainIntramural2.5HE, BSO, OMx, PLND, PALND39Sarcomatous features
Zhou [78]202156N/aAUBPelvic mass10TAH + BSO58
Müller [79]202118G0, P0AUBSubmucosal4.5Hsc TR (2×)9
Pereira [80]202137G0, P0AUBSubmucosal3.5Hsc TR20
Pang [81] (1)202246N/aAUBSubmucosal4.5Lsc HE35
Pang [81] (2)202242N/aPainIntramural5Lsc HE4
Wang [82] 202242N/aAUBUterine mass3.9Lsc HE, BSON/a
Xu [83] 202240N/aasymptomaticUterine mass10open TR12
Shibahara [84]202277G4/P2AUBUterine mass3TAH + BSO12
Sahraoui [85]202319G0, P0PainCervix3cervical TR24
Yin [86]202351 AUBSubmucosal8.5HE, BSO, LNE12GREB1-NCOA2 fusion
Ise [87]202375 AUB 8 Myxoid features
Zhou [88]202349N/aN/aIntramural14HE, BSO1Increase in CA125
EL Hayek [89]202358G2, P2HemoperitoneumIntramural10HE, BSON/aUterine rupture
Ferrara [90]202373G4, P2AUBIntramural2.5Lsc HE, BSO12
Present study202331G4, P4AsymptomaticIntramural3Lsc HE, BSON/a
Present study202358Multi-PAUBSubmucosal1.5Lsc HE, BSO36Flat submucosal area
AUB—abnormal uterine bleeding, N/a—not available, G—gravida, P—para, Hsc—hysteroscopic, Lsc—laparoscopic, TR—tumor resection, HE—hysterectomy, TAH—total abdominal HE, BSO—bilateral salpingo-oophorectomy, VH—vaginal HE, LND—lymphonodectomy, EMABL—endometrial ablation, and OMx—omentectomy; “uterine mass”—used when the exact localization within the uterus was not reported.
Table 4. Aggressive cases (extrauterine spread or metastasis at the first diagnosis or recurrence).
Table 4. Aggressive cases (extrauterine spread or metastasis at the first diagnosis or recurrence).
First AuthorYearAgeSite (Extrauterine Extension)Size, cmPrimary TreatmentRecurrence and PFSTotal FULast Status
Kantelip [91]198686Intramural, left ovary, two epiploic nodules10TAH, BSO, partial cystectomy, epiploic resectionNo recurrence60 moNED
Malfetano [92]198918Intramural5TR, followed by TAH, PALND, OmxSigmoid, mesentery, ovary (nodules up to 6 cm), abdominal wall nodules 1–2 cm, PFS 72N/aTumor initially diagnosed as LG-ESS, recurrence as UTROSCT, G0, P0
Di Vagno [93]1996 Pelvic tumor, lung metastasis, carcinomatosis (35th gw) Caesarean HE, debulking, two CHT regimens (nonresponsive)PD 9 moDOD, 9 mo after dgn
Biermann [94]200768Intramural4.5HE10 cm, small bowel, PFS 48 mo48 mo2 benign gastrointestinal stromal tumors
O’Meara [95]200935Intramural9.9HERetropubic mass with bladder invasion, 8.3 cm, PFS 3 ys48 moNED 1 ys after secondary treatement with surgery and CHx, galactorrhea and hyperprolactinemia (at first and second dgn)
Blinman [96]200949 6.5HE8 cm retroperitoneal mass, PFS 11 ys Response to second-line anastrazole, lost for follow-up 10 ys after FD
Macak [97]201453Uterine mass1.5HE, BSO, PALNDNo recurrence10 moNED
Umeda [98] (1)201438Submucosal4.5 HE, BSO, PLND No recurrence11 moNED
Umeda [98] (2)201457Submucosal6.4HE, BSONo recurrence8 ysNED
Endo [99]201562N/aN/aHEPelvic recurrence, 14 cm, 23 ys after HE (PFS 276 mo)24.5 ysSD (recurrent tumor not completely resected)
Kuznicki [100]201749Ovary, omental cake6Neoadjuvant CHx, optimal cytoreductionPD, death 15 mo after dgn15 moDOD (CA125: 2210 U/mL)
Schraag [58] (1)201724SubmucosalN/aHsc TR, followed by re-Hsc, followed by open TRUterus, PFS 9 mo65 moNED, 56 mo from last surgery. False positive MRI (8 mm nodule) after 3 mo
Schraag [58]201728Myoma10open TRPelvis, PFS 20 mo55 moTumor rupture during first surgery; pregnancy after second surgery
Viau [60]201743Double tumor: pedunculated uterine mass (13 cm), myometrial mass (5.5 cm); peritoneum TAH, BSO, debulking, CHTx (bleomycin, etoposide, cisplatin).Pelvic tumor 5.5 cm, PFS 40 mo64 moNED, 2 years after second surgery Tumor rupture during first surgery
Kondo [101]201769Uterine mass TAH, BSO Lung, PFS 26 mo NED
Cömert [102]201861Pelvic mass7TAH, BSO Pelvic mass, spleen, omentum, PFS 60 mo83 moNED, 7 mo after last surgery
Marrucci [103]201954Uterine mass9HE, BSOvaginal vault, PFS 50 mo74 moNED 24 mo after recurrence, Coexistence with multiple leiomyomas
Bennett [104] (1)202032IntramuralN/aHE(1) Pelvic sidewall, PFS 7 ys, and (2) second subtotal debulking, PFS 11 mo8 ysAWD (Second subtotal debulking 11 mo later)
Bennett [104] (2)202054Intramural (multiple tumors 1.5–6.5 cm)1.5–6.5LASH, followed by trachelectomyPelvis, PFS 9 ys, debulking, CHx10 ys NED
Bennett [104] (3)202030N/aN/aHEOmentum, PFS 32 ys6 ysPD (2 further recurrences, 2 and 4 years later)
Chang [105]202057Intramural10TAH, BSO Pelvic mass, PFS 30 mo35 moGREB1-NCO2 rearranged
Sh Hassan [106]202041IntramuralN/aTAHVaginal vault, PFS “few weeks”24 moNED
Dimitriadis [107]202046Uterine mass11TAHIntraabdominal recurrence, PFS 2 ys2 ysN/a (report at the time of relapse)
Dondi [108]202124Submucosal3Hsc TR Uterus, PFS 20 mo30 moNED after secondary Lsc HE
Devereaux [109]202142Intramural8.8TR with morcellation; at recurrence: TAH, BSO, debulkingUterus, PFS 6 mo6 moLost for FU after second surgery
Chen [110]202133Uterus, pelvic lymph nodesN/aRadical HE, BSO, PLND, CHx, RTxRetroperitoneal mass in the upper abdomen 10 × 7 cm, PFS 14 ys14 ysInitially diagnosed as LG-ESS with pelvic LN metastases
Wei [111]202146Uterus11TAH, BS20cm pelvic tumor adherent to intestine, PFS 53 mo.62 moDOD (9 mo after relapse); Ki67 25%, p53 positive; D&C 2 mo earlier: normal
Massa [112]202256Intramural, among multiple myomasN/aHE10 peritneal nodules up to 8 cm, PFS 7 ys17 ysDOD, 10 CHTx, antibody and hormonal therapies
ys—years, mo—months, N/a—not available, HE—hysterectomy, TAH—total abdominal hysterectomy, LASH—laparoscopic supracervical hysterectomy, LAVH—laparoscopically assisted vaginal hysterectomy, BSO—bilateral salpingo-oophorectomy, BS—bilateral salpingectomy, Hsc—hysteroscopic, Lsc—laparoscopic, TR—tumor resection, OMx—omentectomy, Rx—radiotherapy, CHx—chemotherapy, LN—lymph nodes, LND—lymphonodectomy, PFS—progression-free survival, DOD—dead of disease, NED—no evidence of disease, PD—progressive disease, and FU—follow-up.
Table 5. Case series with clinical data (in ≥ 3 categories).
Table 5. Case series with clinical data (in ≥ 3 categories).
First AuthorYear No.Age SymptomsLocalizationSize
(cm)		Primary TreatmentRecurrence, PFSTotal FU Outcome by Last-SeenComments
Clement [4]19761444 (type 1, n = 6)
49 (type 2, n = 8)		AUB (n = 9)
Pelvic discomfort (n = 2)
Asymptomatic (n = 3)		Intracavitary (n = 1 type 1, n = 3 type 2)
Submucous (n = 1, type 1)
Intramural (n = 3, type 1, n = 2, type 2)
Subserosal (n = 3 type 2)
Extrauterine spread (n = 1, type 1)		2–15Type 1: TAH, BSO (n = 5); VH (n = 1)
Type 2: TAH, BSO (n = 7), TAH (n = 1)		Type1: Yes (n = 3): (a) PFS 12 ys, irradiation; (b) PFS 2 ys, lung metastases, no therapy; (c) PFS 2 ys, CHx-, Rx; Type 2: NoType 1: 22 mo–15 ys
Type 2: 4 mo–7 ys		Type 1: DOD: n = 2,
NED: n = 1 after relapse; NED: n = 2 w/o relapse; lost for FU: n = 1
Type 2: NED (all)
Baker [113]19991550 (30–78), (type 1, n = 10)
51 (34–77) (type 2, n = 5)		AUB (n = 5)
Pelvic mass (n = 8); Asymptomatic (n = 2)		Intramural or polypoid (no details)N/aN/aN/aN/aN/a
Irving [114]2006842 (19–69)AUB (n = 8)Intracavitary polyp (n = 3)
Intramural (n = 4)
n/a (n = 1)		3.5–14TAH, BSO (n = 2); TAH, BSO, Rx (n = 1), TAH, BSO, CHx (n = 1), HE (n = 4)No (n = 7)
Yes (n = 1; Lung, bone, PFS N/a, death 10 mo after dgn		10–62 moNED (n = 7)
DOD (n = 1, type 1)
Rollins [115]20073747 (21–66)N/aSubmucosal (“majority”)2.9 (0.7–17)N/aN/aN/aN/a
Hurrel [6]2007443, 51, 73, 84 Intramural (n = 3)
Pedunculated/subserosal (n = 1)		0.8–19.5HE (4 times), BSO (2×), ULSO (1×)N/aN/a
Nogales [116]2009665 (42–76)AUB (n = 4)
Asymptomatic (n = 2)		Polypoid (n = 4)
Intramural (n = 2)		0.7–8TAH, BSO (n = 5)
Rx (n = 1)		No1–15 ysNEDPelvic endometriosis: n = 1
tamoxifen: n = 1
Staats [117]20092451 (29–84)N/aEndocervical polyp (n = 1); Submucous (n = 7); Intramural (n = 10); Subserosal (n = 2)6.6 (2–22)N/aN/aN/aN/aUltrastructural study; cases from the Collection of Scully
de Leval [118]20101250 (29–59)AUB (n = 5)
Asymptomatic (n = 4)
N/a (n = 3)		Intramural (n = 5),
Polyp or submucous (n = 4), subserosal (n = 1); N/a (n = 2)		5.5 (3–10)TAH, BSO (n = 6), TAH (n = 1), VH (n = 1); D&C (n = 1), N/a (n = 3)N/aN/aN/aUltrastructural study; cases from the Collection of Scully
Bakula-Zalewska [119]2014650,25, 51,63, 24,62N/aUterine mass3–24 LASH + BSO (4 times), HSC TR (Case 2 and 5), adjuvant gestagene (4 times, nos)No3–14.5 ysNED
Liu [120]2015545 (35–50)AUB (n = 4)
Asymptomatic (n = 2)		Intramural (n = 3); Polypoid/submucous (n = 2); Protruding mass (n = 1)5.6 (3–10.2) TAH (n = 3); VH (n = 1); TAH, BSO (n = 1); TR (n = 1)Yes (n = 2)
No (n = 4)		3 mo–7 ysNED (n = 4)
AWD (n = 1)
N/a (n = 1)		CIN (n = 1); 1 recurrence after Hsc TR, one after TAH.
Stewart [121]2016660 (42–67) AUB (n = 6)Intramural (n = 5)
Endocervial (n = 1)		4.6 (1–10) N/aNo65.5 (39–96) moNED
Moore [122]20173452 (12–86)N/aUterine mass
Metastasis (n = 1)		6.1 (0.4–19.5)HE (n = 30)
TR (n = 2)
CHx and Rx (n = 1, metastatic disease at first diagnosis)		No (n = 26)
Yes (n = 7; LN, pelvis, lung, bone, liver; PFSs 11–78 mo)		39 (6–135) moDOD (n = 3; 12, 23 and 23 after diagnosis);
PD (n = 5)
NED (n = 26)
Croce [123]20191270 (n = 1)
N/a (n = 11)		Pelvic mass (n = 1)
N/a (n = 11)		N/a10 (n = 1)
N/a (n = 11)		TAH, BSO; posterior exenteration for recurrence (n = 1);
N/a (n = 11)		Yes (n = 1, PFS 17 mo, pelvis, lung)
N/a (n = 11)		29N/a11/12 cases only as ultrastructural study
Dickson [124]2019453 (38–68)N/aIntramural (n = 3)
Polypoid (n = 1)		2.4 (0.7–3.3)HE (n = 3), D&C (n = 1)N/aN/aN/aAdenomyosis
Goebel [124]20202649.6 (20–74)N/aPolypoid (n = 4)
Intramural (n =11)
(data available for 15 tumors)		5.1 (0.5–15)HE (n = 17), TR (n = 3), D&C (n = 6) (numbers refer to the specimen source) *No (n = 10)
Yes (n = 1, pelvis, DFS 66 mo.)
N/a (n = 16)		94.4 (1–319) moNED (n = 11)
Kaur [126]2020642, 43, 46, 47, 49, 50. AUB (n = 6)Intramural (n = 5)
N/a (n = 1)		1–9.3TAH, BSO (n = 4);
TAH, BSO, CHTx (n = 1); radical HE Type 3, BSO (n = 1)		Yes (n = 1, PFS 7 mo),
No (n = 5)		4 weeks–2 ysNED (n = 4)
N/a (n = 1)		Tamoxifen: n = 1
Carbone [127]20211048.5 (30–69)AUB (n = 8)
Miscarriage (n = 1)
Asymptomatic (n = 1)		Intramural (n = 10)2 (0.2–8)HE, BSO (n = 4), HE, BSO, LNE (n = 3), LASH, BSO, Hsc TR (n = 1), open TR (n = 1) No25 (3–97) moNEDBoth conservatively treated patients became pregnant
Ye [128]2022553 (39–65)AUB (n = 5)Polypoid (n = 3)
Intramural (n = 2)		1.5–5 HE, BSO (n = 4), HSC TR (n = 1)No20 (4–72) moNED
Boyraz [129]20237553 (21–84)AUB (n = 35)
Pelvic pain (n = 6)
Asymptomatic (n = 16)
N/a (n = 18)		Intramyometrial (n = 38)
Submucosal (n = 34) cervical (n = 3)
Lung metastasis (n = 1)		3.5 (0.6–20)
HE (n = 18), HE, BSO (n = 53), TR (n = 4)Yes (n = 4); 1. peritoneum, PFS 60 mo; 2. peritoneum, PFS 144 mo; 3. peritoneum, PFS 60 mo; 4. brain and femur, PFS 30 and 48.64 (22–192) mo NED (n = 53),
AWD (n = 3),
DOD (n = 2)
Xiong [130]20231942.8 (19–58)N/aN/a4.1 (1.5–15)HE (n = 11)
No treatment (n = 1)
N/a (n = 7)		No (n = 13), Yes (n = 6): 1. Peritoneum, PFS 99 mo; 2. pelvis, colon, PFS 2 mo, death; 3. Site n/a, PFS 54 mo; 4. lung, pelvis; PFS 13 mo; 5. pelvis, colon; 189 mo; 6. lung, PFS 14 mo)40.9 (1.2–195.3) moNED (n = 18, incl. n = 5 after recurrence)
DOD (n = 1)
Lu [131]20231845 (27–60)AUB, pelvic mass (n not indicated) HE (n = 3)
HE, BSO (n = 8)
Hsc TR (n = 5)
Lsc TR (n = 2)
Bi [132]20232343 (23–65)N/aIntramyometrial (n = 14)
Polypoid/submucosal (n = 7)
Protuberant mass (n = 2)		5.4 (1–15)TAH (n = 4)
TAH, BSO (n = 13)
TAH, BSO, LND (n = 2); TR (myomectomy) (n = 2); TR (polypectomy) (n = 2) 		Yes (n = 8)
No (n = 15)		8–177 moNED (n = 21)
DOD (n = 2)
Bini [133]20234 N/aMetastatic tumorsN/aN/aYes (n = 4)13.5 (6–34) ysDOD (n = 3)
NED (n = 1)
Qijun [134]20231747 (19–67)AUB (n = 15)
Asymptomatic (n = 2)		Intramural (n = 10)
Submucosal (n = 7)		4.6 (0.6–14.7)TAH or Lsc HE (n = 13)
Hsc TR (n = 4)
CHx (n = 1)		Yes (n = 3) plevis/abdomen, PFS 16 and 17 mo; lung PFS 12 mo;
No (n = 14)		20.2 (1–68) moNED (n = 14)
N/a (n = 3)
* (mean or median, range), ys—years, mo—months, Rx—radiotherapy, CHx—chemotherapy, AUB—abnormal uterine bleeding, N/a—not available, HE—hysterectomy, TAH—total abdominal hysterectomy, LAVH—laparoscopically assisted vaginal hysterectomy, BSO—bilateral salpingo-oophorectomy, Hsc—hysteroscopic, Lsc—laparoscopic, TR—tumor resection, VH—vaginal hysterectomy, LN—lymph nodes, LND—lymphonodectomy, PFS—progression-free survival, DOD—dead of disease, NED—no evidence of disease, and AWD—alive with disease.
Table 6. Common partner genes related to GREB1 and ESR1 rearrangement in UTROSCT.
Table 6. Common partner genes related to GREB1 and ESR1 rearrangement in UTROSCT.
GeneEncoded ProteinFunctionReference
GREB1Growth Regulation by Estrogen in Breast Cancer 1Transcriptionally driven by estrogen-bound ER, important in the estrogen/ER signaling pathway. GREB1-rearranged UTROSCT may be more aggressive [76,86,104,105,110,125,132,134,141]
ESR 1Estrogen Receptor 1Ligand-dependent transcription factor involved in sexual development, reproduction, and bone formation. ESR1-rearranged UTROSCT may be resistant to estrogen blockade due to loss of the ER ligand-binding domain[76,104,105,132,133,134,141]
NCOA1–3Nuclear Receptor Coactivator 1–3Enhance the activity of nuclear hormone receptors and mediate transcriptional effects of steroid/sex-hormone receptor pathways. Fusions involving NCOA genes have oncogenic potential when dysregulated [76,104,105,124,125,131,134,141]
CTNNB1β-CateninKey in Wnt/β-catenin signaling pathway, coactivator for TCF/LEF, involved in transcription initiation and chromatin remodeling. [105,123]
NR4A3Nuclear Receptor Subfamily 4 Group A Member 3Transcriptional activator for the steroid/thyroid hormone nuclear receptor family, regulating proliferation, survival, and differentiation.[105]
GTF2A1General Transcription Factor IIA, subunit 1Component of the RNA polymerase II transcription-initiation complex, interacting with steroid hormone receptors, including ERα, to facilitate transcription initiation.[109]
CITED2CBP/p300 interacting transactivator with Glu/Asp-rich carboxyl-terminal domain 2Transcriptional co-activator that modulates interactions between DNA-binding proteins and histone modifying enzymes, influencing the transcription of genes involved in embryonic development or cellular response to hypoxia.[134]
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Watrowski, R.; Palumbo, M.; Guerra, S.; Gallo, A.; Zizolfi, B.; Giampaolino, P.; Bifulco, G.; Di Spiezio Sardo, A.; De Angelis, M.C. Uterine Tumors Resembling Ovarian Sex Cord Tumors (UTROSCTs): A Scoping Review of 511 Cases, Including 2 New Cases. Medicina 2024, 60, 179. https://doi.org/10.3390/medicina60010179

AMA Style

Watrowski R, Palumbo M, Guerra S, Gallo A, Zizolfi B, Giampaolino P, Bifulco G, Di Spiezio Sardo A, De Angelis MC. Uterine Tumors Resembling Ovarian Sex Cord Tumors (UTROSCTs): A Scoping Review of 511 Cases, Including 2 New Cases. Medicina. 2024; 60(1):179. https://doi.org/10.3390/medicina60010179

Chicago/Turabian Style

Watrowski, Rafał, Mario Palumbo, Serena Guerra, Alessandra Gallo, Brunella Zizolfi, Pierluigi Giampaolino, Giuseppe Bifulco, Attilio Di Spiezio Sardo, and Maria Chiara De Angelis. 2024. "Uterine Tumors Resembling Ovarian Sex Cord Tumors (UTROSCTs): A Scoping Review of 511 Cases, Including 2 New Cases" Medicina 60, no. 1: 179. https://doi.org/10.3390/medicina60010179

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