Next Article in Journal
Percutaneous Computed Tomography (CT) Fluoroscopy-Guided Biopsy of the Spleen Using Fibrin Glue as a Sealant
Next Article in Special Issue
Assessment of Cervicovaginal Smear and HPV DNA Co-Test for Cervical Cancer Screening: Implications for Diagnosis and Follow-Up Strategies
Previous Article in Journal
A Quantitative Evaluation of the Effectiveness of the Metal Artifact Reduction Algorithm in Cone Beam Computed Tomographic Images with Stainless Steel Orthodontic Brackets and Arch Wires: An Ex Vivo Study
Previous Article in Special Issue
A Glimmer of Hope for Patients with a T3 Transformation Zone: miRNAs Are Potential Biomarkers for Cervical Dysplasia
 
 
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Article

Dedifferentiated Leiomyosarcoma of the Uterine Corpus with Heterologous Component: Clinicopathological Analysis of Five Consecutive Cases from a Single Institution and Comprehensive Literature Review

1
Department of Pathology and Translational Genomics, Samsung Medical Center, Sungkyunkwan University School of Medicine, Seoul 06351, Republic of Korea
2
Pathology Center, Seegene Medical Foundation, Seoul 04805, Republic of Korea
*
Authors to whom correspondence should be addressed.
Diagnostics 2024, 14(2), 160; https://doi.org/10.3390/diagnostics14020160
Submission received: 13 December 2023 / Revised: 4 January 2024 / Accepted: 8 January 2024 / Published: 10 January 2024
(This article belongs to the Special Issue Pathology and Diagnosis of Gynecologic Diseases, 2nd Edition)

Abstract

:
Dedifferentiation is a very rare phenomenon in uterine leiomyosarcoma (LMS). The aim of this study was to comprehensively analyze the clinicopathological characteristics of uterine dedifferentiated LMS (DDLMS). We reviewed electronic medical records and pathology slides from five patients with uterine DDLMS and performed immunostaining. The mean age of the patients was 56 years. Two patients presented with abdominal discomfort, while in three cases the uterine tumors were detected on routine medical examination. The mean size of the tumors was 17.0 cm. Four patients underwent hysterectomy. The initial stages were distributed as IB (2/5), IIIC (2/5), and IVC (1/5). Post-operative concurrent chemoradiation therapy, radiation therapy, and chemotherapy were administered in one, one, and two patients, respectively. Despite post-operative treatment, three patients developed metastatic recurrences in the abdominal and pelvic organs. Recurrence-free survival time ranged between 4 and 30 months. Histologically, the differentiated areas demonstrated the classic morphology of malignant smooth muscle differentiation, whereas the dedifferentiated areas resembled undifferentiated pleomorphic sarcoma and were characterized by large pleomorphic tumor cells admixed with haphazardly arranged atypical cells with marked nuclear pleomorphism. All cases also exhibited heterologous components, including chondrosarcoma (CSA; 3/5) and rhabdomyosarcoma (2/5). In two cases, the heterologous components were initially detected in primary tumors. In three cases, the primary tumors did not exhibit any dedifferentiated or heterologous components. Instead, more than half of the recurrent tumors consisted of heterologous components. Three cases showed a sharp demarcation between the LMS and CSA components, while in two cases the dedifferentiated area imperceptibly merged with the differentiated component. Immunostaining revealed that the dedifferentiated components exhibited a lack of desmin immunoreactivity in three of the four examined cases. A subset of uterine LMS represents various amounts and types of dedifferentiation and heterologous components in both primary and recurrent tumors. Routine recognition of DDLMS and distinction from its mimickers are required for accurate diagnosis and further characterization of these rare tumors.

1. Introduction

Leiomyosarcoma (LMS) is a mesenchymal malignancy that primarily develops from smooth muscle cells in both visceral organs and non-visceral structures [1,2]. It is the most common malignant soft tissue tumor, comprising 15% of all sarcomas in adults [3]. The most common primary sites in which LMS develops include the uterus, retroperitoneum, gastrointestinal tract, and extremities, although its distribution is broad [2,4]. Its clinical behavior has a wide range of outcomes, primarily based on histological grade, stage, and distant metastasis [5].
Uterine sarcoma is one of the rarest female genital tumors, representing only 1% of all gynecological malignancies [6,7]. Arising from the myometrium or the connective tissue elements of the endometrium, uterine sarcoma includes a heterogeneous group of tumors derived from mesenchymal cells, comprising three main histological types: LMS, endometrial stromal sarcoma, and undifferentiated uterine sarcoma [8]. Uterine LMS constitutes 50–70% of uterine mesenchymal malignancies, with an annual incidence of approximately 1 per 100,000 women in United States [9,10]. The majority of uterine LMS is identified in perimenopausal women aged 50–55 years, although 15% is found in women aged <40 years [11,12]. It is more prevalent in younger women, with increasing incidence at 30 years and a peak at 50 years [2]. Uterine LMS is often aggressive, with a worse prognosis than endometrial endometrioid carcinoma. Typically presenting as a large pelvic mass, its signs and symptoms include vaginal bleeding, pelvic pain, a sense of fullness in the pelvis or abdomen, dyspareunia, and dysuria, although some patients are asymptomatic. Since uterine LMS is rarely suspected before surgery, this tumor is often diagnosed upon routine pathological examination after hysterectomy or myomectomy performed to treat presumed uterine leiomyoma [13,14].
Dedifferentiation has been documented in several malignant mesenchymal tumors, such as liposarcoma, chondrosarcoma (CSA), rhabdomyosarcoma (RMS), chordoma, and solitary fibrous tumor [15]. These dedifferentiated sarcomas are more aggressive than those without the dedifferentiated component [16]. Histologically, dedifferentiation is defined as an abrupt transition from the differentiated area to the undifferentiated tumor [3]. The term dedifferentiated LMS (DDLMS) was first coined by Shmookler and Lauer in 1983 [17], who determined that DDLMS is morphologically characterized by the abrupt transition from classic LMS to high-grade undifferentiated pleomorphic sarcoma (UPS). The latter does not express immunohistochemical smooth muscle markers [18,19].
Although a small number of DDLMS cases has been reported in the retroperitoneum, trunk, and extremities [20,21], uterine DDLMS is relatively rare [22]. Its clinical features, pathological characteristics, and immunophenotypes have yet to be clarified. Previous studies have shown that, in some uterine DDLMS cases, the non-myogenic tumor component presents heterologous differentiation. The heterologous components, such as RMS, CSA, and osteosarcoma, frequently display severe nuclear pleomorphism, while those exhibiting low-grade cytological atypia have seldom been reported [23]. We recently experienced some cases of primary uterine DDLMS with a heterologous component and initiated a comprehensive review of previously published cases with thorough analysis of their clinicopathological characteristics. In this study, we investigated the clinical manifestations, histological features, and immunostaining results of uterine DDLMS. Our comprehensive analysis will improve the understanding of this rare condition and help pathologists to make accurate diagnoses.

2. Materials and Methods

With the approval of the Institutional Review Board at the Samsung Medical Center (Seoul, Republic of Korea), the pathology database was queried for all cases of primary uterine LMS between January 2021 and December 2023. During the 3 years of the study period, a total of 103 patients in the database underwent surgery for primary uterine LMS. Two board-certified gynecological pathologists examined all available hematoxylin and eosin (H&E)-stained slides to confirm the diagnosis and select the most representative formalin-fixed, paraffin-embedded (FFPE) tissue blocks for immunohistochemical staining. Upon a thorough slide review, we identified five patients with primary uterine DDLMS and reviewed their electronic medical records to collect the following clinical information: patient’s age at initial diagnosis; presenting symptoms; previous medical history; imaging findings; pre-operative clinical impression; pathological diagnosis; greatest dimension of uterine tumor; surgical procedure for uterine tumor; extension to the adnexa, pelvic peritoneum, abdominal peritoneum, rectum, and bladder; lymph node metastasis; initial stage; post-operative treatment and recurrence; pathological diagnosis of recurrent tumor; treatment for recurrence; recurrence-free survival; survival status; and overall survival. We also reviewed all available H&E-stained slides to analyze the following pathological characteristics: dominant morphology of the differentiated component; nuclear pleomorphism; mitotic count per 10 high-power fields; tumor cell necrosis; tumor border; intratumoral lymphocytic infiltrate; and histological type and proportion of the dedifferentiated component.
Immunostaining was performed using whole-tissue sections containing >80% viable tumor tissue, as previously described [24,25,26,27,28,29,30,31,32]. In brief, 4 μm thick FFPE tissue sections were deparaffinized and rehydrated using a xylene and alcohol solution. We used an automated instrument (BOND-MAX immunostainer; Leica Biosystems, Deer Park, IL, USA) with a biotin-free polymeric horseradish peroxidase-linker antibody conjugate system (BOND Polymer Intense Detection System; Leica Biosystems) [33,34,35,36]. After antigen retrieval, endogenous peroxidases were quenched with hydrogen peroxide. The sections were incubated with the primary antibodies listed in Table 1. After chromogenic visualization, the sections were counterstained with hematoxylin and coverslipped. The appropriate positive controls listed in Table 1 were stained, while the negative control was prepared by substituting non-immune serum for the primary antibodies, resulting in no detectable staining. For desmin and S100 protein, staining in the cytoplasm or membrane was interpreted as positive expression. For myogenin, myoD1, and special AT-rich sequence-binding protein 2 (SATB2), nuclear staining was interpreted as positive expression [24,28,37]. The staining intensity was graded as strong, moderate, or weak, while the staining proportion was graded as either diffuse (≥50%) or focal (<50%). For retinoblastoma protein (RB), even weak nuclear staining indicated preserved expression, whereas loss of expression was defined as the complete absence of nuclear immunoreactivity. p53 expression was interpreted as a mutation pattern when one of the following staining patterns was observed [38]: diffuse (≥75%) and strong nuclear immunoreactivity (overexpression); no nuclear immunoreactivity in any of the tumor cells (complete absence); or unequivocal cytoplasmic staining (cytoplasmic). In contrast, p53 expression was interpreted as a wild-type pattern if a variable proportion of nuclear expression with mild-to-moderate staining intensity was observed.

3. Results

Figure 1 summarizes the patients’ treatment timelines. In case 1, the patient underwent hysterectomy and adjuvant concurrent chemoradiation therapy (CCRT). Thirty-three months after surgery, she developed a recurrent tumor in the pelvic peritoneum and underwent repeated surgeries and radiation therapy to treat the peritoneal metastatic recurrence. After 7 disease-free months, the abdominal metastases progressed again. The patient then underwent surgical excision and received chemotherapy for 26 months. She has survived with this disease for 96 months after a hysterectomy. In case 2, the patient underwent hysterectomy with post-operative chemotherapy. The pulmonary and peritoneal metastases developed 10 months after the hysterectomy. Surgical mass excision was performed, and chemotherapy was administered for 12 months. In case 3, the patient was prescribed post-operative radiation therapy, but the treatment was interrupted due to exacerbation of her health condition. Nevertheless, 17 months after the operation, she is alive with no signs of recurrent disease. In case 4, the patient underwent hysterectomy with adjuvant chemotherapy but developed a recurrent tumor in the left paracolic gutter 8 months later. She then underwent surgical excision. In case 5, the patient with advanced-stage disease was lost to follow-up immediately after extensive surgery.
Table 2 summarizes the clinical features of patients with uterine DDLMS. Patient age ranged between 51 and 63 years (mean, 56 years). Two patients presented with abdominal discomfort (cases 1 and 5), one with constipation (case 1), and another with a palpable pelvic mass (case 5), while in the remaining three asymptomatic patients the uterine tumors were detected during routine medical examinations. Ultrasonography revealed single (cases 2 and 4) or multiple (case 3) uterine masses occupying the abdominal or pelvic cavity. Two patients had previous medical histories of thyroid carcinoma and umbilical hernia (case 3) and hyperthyroidism (case 4), respectively. Imaging findings were available for four patients. Abdominopelvic magnetic resonance imaging revealed various radiological features, including a mixed solid and cystic mass (case 2), multiple solid masses (case 3), a heterogeneous mass with intratumoral necrosis (case 4), and adnexal extension (case 5). Four patients were suspected of having uterine leiomyoma, while the remaining patient (case 5) was presumed to have uterine sarcoma. Four patients underwent total hysterectomy. One and two patients underwent bilateral salpingectomy (case 3) and salpingo-oophorectomy (cases 2 and 4), respectively. In one patient (case 2), pelvic and para-aortic lymph node dissection was performed. The remaining patient (case 5), who did not undergo hysterectomy, received uterine mass excision with left oophorectomy, left hemicolectomy, and left nephrectomy. Two patients (cases 2 and 5) were initially diagnosed with primary uterine DDLMS with a heterologous component, while in the remaining cases, the uterine tumors were diagnosed as LMS (cases 1 and 3) and DDLMS (case 2), respectively. The dimensions of the uterine tumors ranged between 8.3 and 27.8 cm (mean, 17.0 cm). The initial stages were distributed as IB (2/5; cases 1 and 2), IIIC (2/5; cases 3 and 4), and IVC (1/5; case 5). Lymph node metastases were detected in two patients (cases 3 and 4), while pelvic and abdominal peritoneal metastases were identified in one (case 3) and two (cases 3 and 5) cases, respectively.
Follow-up information was available for all but one patient (case 5; Table 2). Post-operative chemotherapy, CCRT, and radiation therapy were administered to two (cases 2 and 4), one (case 1), and one (case 3) patients, respectively. The latter patient was initially prescribed radiation therapy for the whole pelvis and para-aortic area (at an intended dose of 5400 cGy in 30 fractions), but the treatment was interrupted after receiving 2700 cGy when the patient’s health worsened. Two patients received six cycles of post-operative chemotherapy, including cyclophosphamide, vincristine, adriamycin, and dacarbazine (case 2), and ifosfamide and doxorubicin (case 4), respectively. One patient (case 1) received post-operative radiation therapy (5040 cGy in 28 fractions) with six cycles of weekly cisplatin. Despite the post-operative treatment, three of the four patients (cases 1, 2, and 4) developed metastatic recurrences in the abdominal and pelvic organs, including the vagina, ovary, bladder, colon, mesentery, omentum, and abdominopelvic peritoneum. Four metastatic tumors had heterologous components. One patient (case 3) did not experience any recurrent or metastatic disease during 15 months after hysterectomy; however, one of the patients (case 2) experienced distant metastases in the lungs, and three patients underwent surgical excision for metastatic tumors. Two patients also received CCRT (case 1) and chemotherapy (case 2), respectively. The recurrence-free survival time ranged between 4 and 30 months (mean, 13.3 months). One of the three patients who developed recurrences is currently alive with disease.
Table 3 summarizes the pathological characteristics of uterine DDLMS. Figure 2 and Figure 3 are photomicrographs showcasing the histological features of case 1 (Figure 2A–C), case 2 (Figure 2D–F), case 3 (Figure 2G–J), case 4 (Figure 3A–C), and case 5 (Figure 3D–F), respectively. Dedifferentiated, undifferentiated, or heterologous morphology was included in the initial pathological diagnosis in all cases. The absence of a benign and malignant epithelial tumor component excluded the possibility of adenosarcoma and carcinosarcoma of endometrial origin. All uterine tumors exhibited varying amounts of LMS types (20–80%), including spindle cell and epithelioid. There was no evidence of co-existing leiomyoma or smooth muscle tumor of uncertain malignant potential (STUMP). The histologically differentiated areas of these tumors demonstrated the morphology typical of malignant smooth muscle differentiation, including intersecting fascicles of atypical spindle cells with eosinophilic cytoplasm, variably well-defined cell borders, broad or blunt-ended nuclei (spindle cell LMS), as well as round or polygonal cells with eosinophilic or clear cytoplasm arranged in nested, corded, nodular, and diffuse patterns (epithelioid LMS). Three tumors (cases 1, 3, and 5) showed mixed spindle cell and epithelioid morphologies, while the remaining two tumors were compatible with epithelioid LMS (case 2) and spindle cell LMS (case 4), respectively. High-grade histological features, including multifocal tumor cell necrosis and brisk mitotic activity, were identified in the differentiated areas of all tumors. The dedifferentiated tumors resembled UPS or malignant fibrous histiocytoma (MFH) of the soft tissue and were characterized by large pleomorphic tumor cells admixed with haphazardly arranged atypical cells with marked nuclear pleomorphism in a background of myxoid or collagenous stroma. The heterologous components, including RMS (case 3) and CSA (case 5), were first detected in the primary uterine tumors. In cases 1, 2, and 4, no dedifferentiated or heterologous component was identified in the primary tumors, but the heterologous components comprised more than half of the metastatic tumor volume. Three cases (cases 1, 4, and 5) showed a sharp demarcation between the differentiated and dedifferentiated components, while in two cases (cases 2 and 3) the dedifferentiated area imperceptibly merged with the differentiated component. The dedifferentiated and heterologous components exhibited an expansile but focally infiltrative, scalloped tumor border; severe nuclear pleomorphism; occasional bizarre, monstrous, or multinucleated tumor cells; and frequent mitoses (range, 21–46 per 10 high-power fields). One case (case 2) contained multinucleated tumor giant cells.
Table 3 summarizes the immunophenotypes of uterine DDLMS, while the photomicrographs in Figure 4 show the immunophenotypical features. Regarding the differentiated component, three cases were diffusely positive for desmin. A few microscopic foci were weakly positive for S100 protein and SATB2 in one case. In all examined cases, myogenin and myoD1 expression was negative, p53 protein expression was wild type, and RB protein expression was preserved. Regarding the dedifferentiated and heterologous components, three cases were completely negative for desmin. In one case, the dedifferentiated area exhibited patchy faint-to-weak staining for desmin. CSA was strongly positive for S100 protein in two cases. Some areas of RMS were weakly positive for myogenin. The dedifferentiated and heterologous components were negative for myoD1 in all cases. One case exhibited diffuse and intense nuclear immunoreactivity for SATB2. p53 protein was overexpressed in one case. RB1 protein expression was preserved in two cases.

4. Discussion

DDLMS is defined by the presence of an undifferentiated tumor component, which lacks the histological and immunophenotypical features of smooth muscle differentiation, in proximity with differentiated LMS [20]. DDLMS displays pleomorphic atypical cells with brisk mitotic activity and extensive necrosis, with characteristics similar to UPS. DDLMS of the soft tissue presents as highly aggressive tumors with a 50–65.2% mortality rate and 89% likelihood of metastasis [21,39]. It has also been reported that the loss of myogenic differentiation in LMS could be a significant prognostic factor accounting for the aggressiveness of these tumors [40]. Among soft tissue tumors, dedifferentiation is an infrequent but well-known phenomenon observed in pleomorphic RMS, dedifferentiated chordoma, and dedifferentiated liposarcoma [41]. However, the dedifferentiation of uterine LMS was not mentioned in the most recent World Health Organization Classification of female genital tumors [42].
For a comprehensive review of the literature on uterine DDLMS with a heterologous component, we searched the Medline bibliographic database via the PubMed retrieval service using the keywords “uterus”, “leiomyosarcoma”, “dedifferentiation”, “dedifferentiated leiomyosarcoma”, “heterologous”, “osteosarcoma,” “chondrosarcoma”, and “rhabdomyosarcoma”. We found that 42 previously published cases of primary uterine LMS with a heterologous component have been reported to date [3,16,20,41,43,44,45,46] and subsequently collected the clinicopathological information of these cases. Table 4 summarizes the clinical characteristics of 42 patients with uterine DDLMS. The mean age at diagnosis was 57.7 years (range, 38–90 years). Only a few individual case reports described the initial symptoms or signs, including pelvic or abdominal pain, vaginal bleeding, hypermenorrhea, and infertility. Imaging findings and clinical impressions were available for only a few individual cases. Imaging studies revealed several variable-sized fibroids or solid heterogeneous masses measuring up to 18.9 cm. Staging information was available for 27 cases, more than half of which were classed as stage I (15/27; 55.6%). Six patients had stage IV disease at the time of initial diagnosis. Most patients underwent surgery, including total hysterectomy, bilateral salpingo-oophorectomy, and myomectomy, and approximately one-third received post-operative chemotherapy or radiation therapy. Three of the six patients with stage IV disease were initially prescribed chemotherapy. Of the 17 patients whose post-treatment recurrence data were available, 13 (76.5%) developed locoregional or metastatic recurrences. Similarly, 16 of the 18 patients with available relevant clinical radiological information experienced distant metastases in the lungs, pleura, liver, peritoneum, brain, bones, heart, and kidneys.
Follow-up information was available for 32 of the 42 previously reported patients with uterine DDLMS. Although most of these tumors were classed as stage I at presentation, 62.5% (20/32) of patients died of the disease, with a mean overall survival of 26.7 months. Brief clinical presentations of patients described in each of the previously published articles are as follows: Iihara et al. [46] reported in their single case report that the patient received gamma knife radiotherapy for brain metastasis detected 16 months after initial therapy. She died of metastatic disease at 20 months after initial therapy. According to the case series reported by Chen et al. [20], one of the two patients who underwent mass excision died 12 months after initial presentation, and the other patient who underwent hysterectomy was alive without evidence of disease 28 months after initial presentation. In a single case report by Rawish and Fadare [44], despite hysterectomy with adjuvant chemotherapy, the patient developed a large pelvic mass with multiple peritoneal seeding at 6 months after surgery. She underwent debulking surgery and chemotherapy, and was alive with disease 8 months after hysterectomy. Yu and Hornick [3] recently documented a series of 15 DDLMS cases, in which 10 cases were of uterine origin. Eight patients developed distant metastases in the lungs, liver, bone, small bowel, peritoneum, and so on. Among nine patients whose follow-up information was available, six patients died of disease with a mean overall survival of 10.5 months and three patients were alive with disease with a mean overall survival of 32 months. In another recent case series reported by Chapel et al. [16], survival data were available for 19 patients. Twelve patients died of disease with a median disease-specific survival of 14 months (range, 2–73 months). Four patients were alive with disease at 4, 12, 44, and 50 months, and three patients were alive without evidence of disease at 56, 109, and 114 months. Interestingly, only one patient experienced RFS > 24 months. They stated that the proportion of dedifferentiated component and immunoreactivity were not significantly associated with survival. Kousar et al. [47] reported in their single case report that the patient was treated with hysterectomy with adjuvant chemotherapy. Abdominopelvic computed tomography after completing chemotherapy indicated that she developed multiple peritoneal and liver metastases.
Detailed information on the histological types of differentiated and dedifferentiated components was available for all 42 previously published DDLMS cases. Table 5 summarizes their histological characteristics. Although all tumors contained variable epithelioid, spindled, and pleomorphic tumor cells, the dominant morphology of the differentiated component was spindle cell LMS in more than two-thirds of cases (32/42; 76.2%). One case (2.4%) showed dominant epithelioid LMS in the differentiated areas. Cellular leiomyoma, leiomyoma with bizarre nuclei, and STUMP were identified in three (7.1%), one (2.4%), and two (4.8%) cases, respectively. Three cases (7.1%) showed a transition from benign to high-grade poorly differentiated components. Notably, benign components (leiomyoma, cellular leiomyoma, and leiomyoma with bizarre nuclei) co-existed with spindle cell LMS in two cases, while in another case, areas of frank LMS and undifferentiated component were imperceptibly blended into more recognizable smooth muscle (leiomyoma-like) areas. The tumor size ranged between 3.0 and 30.0 cm. In 23 cases (54.8%), the dedifferentiated component showed MFH- or UPS-like morphology, characterized by large non-cohesive polygonal cells possessing moderate-to-abundant eosinophilic to amphophilic cytoplasm, large pleomorphic nuclei with coarse vesicular-to-smudged chromatin, and one or more macronucleoli. The proportion of dedifferentiated component ranged between 5% and 70%. Although we did not include a case of uterine DDLMS showing an OSA component in this study, our comprehensive review of the previous literature revealed that 13 tumors (31.0%) had areas of OSA as a heterologous component. Particularly, Yu and Hornick [3] reported a series of 10 uterine DDLMS cases showing an OSA component. Some of those tumors also included areas of CSA or RMS.
In their study of 18 DDLMS cases, Chen et al. [7] stated that the delineation of pleomorphic LMS and DDLMS can be challenging, especially in cases where an abrupt morphological transition occurs with no observable shift in immunophenotype. Pleomorphic LMS and DDLMS may represent a histological spectrum of LMS transitioning from classic LMS to high-grade UPS. One of the cases included in their study showed faint-to-weak desmin immunoreactivity in a few microscopic areas of the dedifferentiated component. However, those areas comprised less than 1% of the entire tumor volume, and most tumor tissues did not express desmin. Since the histological features of the dedifferentiated and heterologous components corresponded to UPS and CSA, respectively, a diagnosis of DDLMS was established.
LMS encompasses tumors that demonstrate a wide range of differentiation with loss of smooth muscle marker expression, extending from well-differentiated to poorly differentiated LMS, resembling UPS [48]. The vast majority of patients with uterine LMS carry at least one mutation in either tumor protein 53 (TP53), retinoblastoma (RB1), phosphatase and tensin homolog deleted on chromosome 10 (PTEN), or alpha-thalassemia/mental retardation, X-linked (ATRX) [49]. It has been also documented that a small subset of uterine LMS harbors somatic mutations in the breast cancer gene (BRCA) and alterations in homologous recombination repair genes [50]. Guo et al. [51] identified three molecular subtypes of LMS and confirmed their findings by analyzing The Cancer Genome Atlas (TCGA) datasets. Subtype III almost entirely corresponded with uterine LMS, with 92% of subtype III samples derived from the uterus [48]. Genes enriched in subtype III involved biological processes regulating transcription and the metabolic pathways and indicated that uterine LMS comprises a molecularly and clinically distinct cluster from soft tissue LMS (subtype I), which frequently overexpresses genes associated with normal smooth muscle function and differentiation [51]. In contrast, subtype II showed significantly fewer muscle-specific genes than other subtypes and indicated a more dedifferentiated molecular subtype [48]. Importantly, this dedifferentiated subtype was shown to cluster with UPS and characterized by significantly higher genomic instability and worse outcome. We consider that these genomically distinct subtypes can partially explain the significant phenotypic and morphological differences between conventional LMS and DDLMS of the uterus.
The phenomenon of cellular plasticity, the ability of cells to change their phenotype in a reversible fashion, is involved in tissue regeneration as well as epithelial homeostasis [52,53]. Cellular plasticity also plays an important role in tumor development and progression [54], and it is closely related to intratumoral heterogeneity and variable degrees of phenotypic interconversion [55]. It is not surprising that malignant tumors present with phenotypes and molecular features of either retrodifferentiated, dedifferentiated, or transdifferentiated states, suggestive of cellular plasticity. Among these, retrodifferentiation and dedifferentiation are often used interchangeably [56]. Retrodifferentiation is characterized by a reversion of maturated properties and expression patterns of a differentiated phenotype to a precursor or stem-like cell [57]. Cancer stem cells (CSCs), which are generated by retrodifferentiation from differentiated tumor cells, regain the capacity for self-renewal and may thus be able to maintain tumorigenicity [58]. Accumulating evidence suggests that certain tumor cells can adopt a CSC state associated with the epithelial–mesenchymal transition, higher transdifferentiation potential, and increased resistance to chemotherapy or radiation therapy [59,60]. While retrodifferentiation implies the acquisition of a stem cell/progenitor phenotype, dedifferentiation of tumor cells is characterized by loss of phenotypic specialization, i.e., morphological loss of lineage identity and expression patterns with tumor progression [61,62]. Some cases of conventional LMS with pleomorphic foci retain smooth muscle marker expression, while others show undifferentiated morphology and no or at most very focal smooth muscle marker immunoreactivity. It has been suggested that the latter might be most rigorously regarded as DDLMS [16,39] and that the former might be categorized as pleomorphic LMS. In this study, all except one examined case was negative for desmin, and the remaining case exhibited only rare cells faintly expressing desmin.
There have been some case reports describing loss and gain of certain morphologies and immunophenotypes in the process of dedifferentiation [63,64,65]. In a case of intracranial anaplastic hemangiopericytoma reported by Tan et al. [65], the dedifferentiated component displayed a focal area of glandular formation with the acquisition of epithelial immunophenotypes. Watts et al. [63] described a rare case of succinate dehydrogenase (SDH)-deficient dedifferentiated gastrointestinal stromal tumor (GIST) of the stomach, exhibiting loss of SDH subunit A expression and gain of the smooth muscle immunophenotype. Dedifferentiation of GIST is a rare but well-recognized phenomenon [66]. It is characterized by transition to a frankly sarcomatoid morphology and frequently accompanied by loss of immunoreactivity for KIT and discovered for GIST 1. In a recent case report written by Shah et al. [64], the patient who was initially diagnosed as having grade 1 endometrioid carcinoma of the endometrium developed an isolated breast metastasis. The tumor underwent dedifferentiation to undifferentiated carcinoma at the metastatic site. Particularly, the metastatic lesion showed undifferentiated morphology and loss of PAX8 expression, without a residual low-grade component. It also demonstrated loss of immunoreactivities for AT-rich interaction domain 1A (ARID1A) and ARID1B, which was not observed in the primary endometrial tumor. To the best of our knowledge, the alteration in stem cell/progenitor phenotype or the acquisition of certain immunophenotypes has never been investigated in uterine DDLMS. Although a recent genomic database analysis by Astolfi et al. [49] revealed that PTEN mutation was more frequent in metastatic uterine LMS than in primary ones, this finding was not exactly about DDLMS. It is unclear which genetic and molecular differences may contribute to the distinction between uterine LMS and DDLMS. In order to gain insight about their differences and enlighten differential management, further investigations are warranted to reveal the distinct expression profiles and mutation patterns between conventional LMS and DDLMS of the uterus.
This study has several limitations. First, since we enrolled patients with uterine DDLMS who underwent surgery at a single institution, the cohort was relatively small. Second, comparative molecular analysis was beyond the scope of this study. Third, due to the small number of cases, we did not analyze the statistical differences in survival. Further investigations using more detailed prognostic information obtained from larger cohorts of uterine DDLMS are necessary. Fourth, the divergent criteria used to define DDLMS in previous studies were noted, although we have addressed this through a fair and rational approach, as discussed above.
In conclusion, we demonstrated that dedifferentiation occurs in primary uterine LMS or in recurrent or metastatic tumors. Our findings suggest that a subset of uterine LMS represents various types and amounts of dedifferentiation. Routine prospective recognition of DDLMS and distinction from its mimickers are advocated for accurate diagnosis and further characterization of these rare tumors.

Author Contributions

Conceptualization, S.K., H.B. and H.-S.K.; methodology, H.-S.K.; validation, S.K.; formal analysis, H.B.; investigation, S.K.; resources, H.-S.K.; data curation, H.-S.K.; writing—original draft preparation, S.K. and H.B.; writing—review and editing, H.B. and H.-S.K.; visualization, H.-S.K.; supervision, H.-S.K.; funding acquisition, H.-S.K. All authors have read and agreed to the published version of the manuscript.

Funding

This work was supported by the Samsung Medical Center Grant (SMO1230291) and the National Research Foundation of Korea (NRF) grant funded by the Korean Government (MSIT) (2023R1A2C2006223).

Institutional Review Board Statement

This study was conducted in accordance with the Declaration of Helsinki and approved by the Institutional Review Board (approval number: 2023-12-057; date of approval: 11 December 2023).

Informed Consent Statement

Regarding the retrospective nature of this study, the Institutional Review Board waived the requirement for the investigators to obtain signed informed consent.

Data Availability Statement

Data is contained within the article.

Conflicts of Interest

The authors declare no conflicts of interest.

References

  1. Asano, H.; Isoe, T.; Ito, Y.M.; Nishimoto, N.; Watanabe, Y.; Yokoshiki, S.; Watari, H. Status of the current treatment options and potential future targets in uterine leiomyosarcoma: A Review. Cancers 2022, 14, 1180. [Google Scholar] [CrossRef]
  2. Devaud, N.; Vornicova, O.; Abdul Razak, A.R.; Khalili, K.; Demicco, E.G.; Mitric, C.; Bernardini, M.Q.; Gladdy, R.A. Leiomyosarcoma: Current clinical management and future horizons. Surg. Oncol. Clin. N. Am. 2022, 31, 527–546. [Google Scholar] [CrossRef]
  3. Yu, S.; Hornick, J.L. Malignant mesenchymoma revisited: A clinicopathologic study of leiomyosarcomas with osteosarcomatous differentiation. Am. J. Surg. Pathol. 2022, 46, 1430–1435. [Google Scholar] [CrossRef] [PubMed]
  4. Penel, N.; Coindre, J.M.; Giraud, A.; Terrier, P.; Ranchere-Vince, D.; Collin, F.; Guellec, S.L.E.; Bazille, C.; Lae, M.; de Pinieux, G.; et al. Presentation and outcome of frequent and rare sarcoma histologic subtypes: A study of 10,262 patients with localized visceral/soft tissue sarcoma managed in reference centers. Cancer 2018, 124, 1179–1187. [Google Scholar] [CrossRef] [PubMed]
  5. Gronchi, A.; Strauss, D.C.; Miceli, R.; Bonvalot, S.; Swallow, C.J.; Hohenberger, P.; Van Coevorden, F.; Rutkowski, P.; Callegaro, D.; Hayes, A.J.; et al. Variability in patterns of recurrence after resection of primary retroperitoneal sarcoma (RPS): A report on 1007 patients from the multi-institutional collaborative RPS Working Group. Ann. Surg. 2016, 263, 1002–1009. [Google Scholar] [CrossRef] [PubMed]
  6. Buzinskiene, D.; Mikenas, S.; Drasutiene, G.; Mongirdas, M. Uterine sarcoma: A clinical case and a literature review. Acta Med. Litu. 2018, 25, 206–218. [Google Scholar] [CrossRef] [PubMed]
  7. Abeler, V.M.; Royne, O.; Thoresen, S.; Danielsen, H.E.; Nesland, J.M.; Kristensen, G.B. Uterine sarcomas in Norway. A histopathological and prognostic survey of a total population from 1970 to 2000 including 419 patients. Histopathology 2009, 54, 355–364. [Google Scholar] [CrossRef]
  8. D’Angelo, E.; Prat, J. Uterine sarcomas: A review. Gynecol. Oncol. 2010, 116, 131–139. [Google Scholar] [CrossRef] [PubMed]
  9. Hosh, M.; Antar, S.; Nazzal, A.; Warda, M.; Gibreel, A.; Refky, B. Uterine sarcoma: Analysis of 13,089 cases based on Surveillance, Epidemiology, and End Results Database. Int. J. Gynecol. Cancer 2016, 26, 1098–1104. [Google Scholar] [CrossRef]
  10. Toro, J.R.; Travis, L.B.; Wu, H.J.; Zhu, K.; Fletcher, C.D.; Devesa, S.S. Incidence patterns of soft tissue sarcomas, regardless of primary site, in the Surveillance, Epidemiology and End Results Program, 1978–2001: An analysis of 26,758 cases. Int. J. Cancer 2006, 119, 2922–2930. [Google Scholar] [CrossRef]
  11. Sparic, R.; Andjic, M.; Babovic, I.; Nejkovic, L.; Mitrovic, M.; Stulic, J.; Pupovac, M.; Tinelli, A. Molecular insights in uterine leiomyosarcoma: A systematic review. Int. J. Mol. Sci. 2022, 23, 9728. [Google Scholar] [CrossRef]
  12. Roberts, M.E.; Aynardi, J.T.; Chu, C.S. Uterine leiomyosarcoma: A review of the literature and update on management options. Gynecol. Oncol. 2018, 151, 562–572. [Google Scholar] [CrossRef] [PubMed]
  13. Juhasz-Boss, I.; Gabriel, L.; Bohle, R.M.; Horn, L.C.; Solomayer, E.F.; Breitbach, G.P. Uterine leiomyosarcoma. Oncol. Res. Treat. 2018, 41, 680–686. [Google Scholar] [CrossRef] [PubMed]
  14. Zhang, F.; Liu, Y.; Quan, Q.; Meng, Y.; Mu, X. Diagnostic value of preoperative CA125, LDH and HE4 for leiomyosarcoma of the female reproductive system. Cancer Manag. Res. 2021, 13, 4657–4664. [Google Scholar] [CrossRef] [PubMed]
  15. Henricks, W.H.; Chu, Y.C.; Goldblum, J.R.; Weiss, S.W. Dedifferentiated liposarcoma: A clinicopathological analysis of 155 cases with a proposal for an expanded definition of dedifferentiation. Am. J. Surg. Pathol. 1997, 21, 271–281. [Google Scholar] [CrossRef]
  16. Chapel, D.B.; Maccio, L.; Bragantini, E.; Zannoni, G.F.; Quade, B.J.; Parra-Herran, C.; Nucci, M.R. Dedifferentiated leiomyosarcoma of the uterus: A clinicopathologic and immunohistochemical analysis of 23 cases. Histopathology 2023, 82, 812–825. [Google Scholar] [CrossRef] [PubMed]
  17. Shmookler, B.M.; Lauer, D.H. Retroperitoneal leiomyosarcoma. A clinicopathologic analysis of 36 cases. Am. J. Surg. Pathol. 1983, 7, 269–280. [Google Scholar] [PubMed]
  18. Dekanic, A.; Jonjic, N.; Savic Vukovic, A. Dedifferentiated leiomyosarcoma of the auricle with heterologous osteosarcoma component: Case report and literature review. Case Rep. Otolaryngol. 2022, 2022, 3684461. [Google Scholar] [CrossRef]
  19. Gaeta, R.; Matera, D.; Muratori, F.; Roselli, G.; Baldi, G.; Campanacci, D.A.; Franchi, A. Dedifferentiated soft tissue leiomyosarcoma with heterologous osteosarcoma component: Case report and review of the literature. Clin. Sarcoma Res. 2020, 10, 6. [Google Scholar] [CrossRef]
  20. Chen, E.; O’Connell, F.; Fletcher, C.D. Dedifferentiated leiomyosarcoma: Clinicopathological analysis of 18 cases. Histopathology 2011, 59, 1135–1143. [Google Scholar] [CrossRef]
  21. Nicolas, M.M.; Tamboli, P.; Gomez, J.A.; Czerniak, B.A. Pleomorphic and dedifferentiated leiomyosarcoma: Clinicopathologic and immunohistochemical study of 41 cases. Hum. Pathol. 2010, 41, 663–671. [Google Scholar] [CrossRef] [PubMed]
  22. Matsuda, K.; Akazawa, Y.; Yamaguchi, Y.; Mussazhanova, Z.; Kurohama, H.; Ueki, N.; Kohno, M.; Fukushima, A.; Kajimura, I.; Hiraki, H.; et al. Immunofluorescence analysis of DNA damage response protein p53-binding protein 1 in a case of uterine dedifferentiated leiomyosarcoma arising from leiomyoma. Pathol. Res. Pract. 2019, 215, 152640. [Google Scholar] [CrossRef] [PubMed]
  23. Zuo, X.; Wu, W.L.; Shi, P.; Liu, T.M.; Yu, N.; Li, L. A case report of recurrent leiomyosarcoma with chondrosarcoma differentiation in the abdominal wall and a review of the literature. Pathol. Oncol. Res. 2023, 29, 1611109. [Google Scholar] [CrossRef] [PubMed]
  24. Park, S.; Park, E.; Kim, H.S. Mesonephric-like carcinosarcoma of the uterine corpus: Clinicopathological, molecular and prognostic characteristics in comparison with uterine mesonephric-like adenocarcinoma and conventional endometrial carcinosarcoma. Cancer Genom. Proteom. 2022, 19, 747–760. [Google Scholar] [CrossRef] [PubMed]
  25. Chu, J.; Yeo, M.K.; Lee, S.H.; Lee, M.Y.; Chae, S.W.; Kim, H.S.; Do, S.I. Clinicopathological and prognostic significance of programmed death ligand-1 SP142 expression in 132 patients with triple-negative breast cancer. In Vivo 2022, 36, 2890–2898. [Google Scholar] [CrossRef]
  26. Sohn, J.; Lee, Y.; Kim, H.S. Endometrioid carcinomas of the ovaries and endometrium involving endocervical polyps: Comprehensive clinicopathological analyses. Diagnostics 2022, 12, 2339. [Google Scholar] [CrossRef] [PubMed]
  27. Chung, Y.; Kim, S.; Kim, H.S.; Do, S.I. High receptor-interacting serine/threonine-protein kinase 3 (RIP3) expression serves as an independent poor prognostic factor for triple-negative breast carcinoma. Anticancer. Res. 2022, 42, 2753–2761. [Google Scholar] [CrossRef]
  28. Koh, H.H.; Park, E.; Kim, H.S. Mesonephric-like adenocarcinoma of the ovary: Clinicopathological and molecular characteristics. Diagnostics 2022, 12, 326. [Google Scholar] [CrossRef]
  29. Yoo, H.; Kim, H.S. Clinicopathological and prognostic values of telomerase reverse transcriptase (TERT) promoter mutations in ovarian clear cell carcinoma for predicting tumor recurrence, platinum resistance and survival. Cancer Genom. Proteom. 2023, 20, 626–636. [Google Scholar] [CrossRef]
  30. Park, S.; Cho, Y.; Kim, H.S. Mesonephric-like adenocarcinoma of the uterine corpus: Clinicopathological and prognostic significance of L1 cell adhesion molecule (L1CAM) over-expression. Anticancer. Res. 2023, 43, 4559–4571. [Google Scholar] [CrossRef]
  31. Koh, H.H.; Park, E.; Kim, H.S. Mesonephric-like adenocarcinoma of the uterine corpus: Genomic and immunohistochemical profiling with comprehensive clinicopathological analysis of 17 consecutive cases from a single institution. Biomedicines 2023, 11, 2269. [Google Scholar] [CrossRef] [PubMed]
  32. Kim, H.; Kim, H.S. Mesonephric-like adenocarcinoma of the uterine corpus: Comparison between mismatch repair protein immunostaining and microsatellite instability testing. Anticancer Res. 2023, 43, 1785–1795. [Google Scholar] [CrossRef] [PubMed]
  33. Lee, Y.; Oh, Y.L. Thyroid pathology, a clue to PTEN hamartoma tumor syndrome. J. Pathol. Transl. Med. 2023, 57, 178–183. [Google Scholar] [CrossRef] [PubMed]
  34. Park, S.; Kim, J.; Jang, W.; Kim, K.M.; Jang, K.T. Clinicopathologic significance of the delta-like ligand 4, vascular endothelial growth factor, and hypoxia-inducible factor-2alpha in gallbladder cancer. J. Pathol. Transl. Med. 2023, 57, 113–122. [Google Scholar] [CrossRef]
  35. Chang, S.; Choi, Y.L.; Shim, H.S.; Lee, G.K.; Ha, S.Y.; Korean Cardiopulmonary Pathology Study Group. Usefulness of BRAF VE1 immunohistochemistry in non-small cell lung cancers: A multi-institutional study by 15 pathologists in Korea. J. Pathol. Transl. Med. 2022, 56, 334–341. [Google Scholar] [CrossRef] [PubMed]
  36. Koh, H.H.; Oh, Y.L. Papillary and medullary thyroid carcinomas coexisting in the same lobe, first suspected based on fine-needle aspiration cytology: A case report. J. Pathol. Transl. Med. 2022, 56, 301–308. [Google Scholar] [CrossRef]
  37. Kim, H.; Na, K.; Bae, G.E.; Kim, H.S. Mesonephric-like adenocarcinoma of the uterine corpus: Comprehensive immunohistochemical analyses using markers for mesonephric, endometrioid and serous tumors. Diagnostics 2021, 11, 2042. [Google Scholar] [CrossRef]
  38. Kobel, M.; Ronnett, B.M.; Singh, N.; Soslow, R.A.; Gilks, C.B.; McCluggage, W.G. Interpretation of p53 immunohistochemistry in endometrial carcinomas: Toward increased reproducibility. Int. J. Gynecol. Pathol. 2019, 38, S123–S131. [Google Scholar] [CrossRef]
  39. Oda, Y.; Miyajima, K.; Kawaguchi, K.; Tamiya, S.; Oshiro, Y.; Hachitanda, Y.; Oya, M.; Iwamoto, Y.; Tsuneyoshi, M. Pleomorphic leiomyosarcoma: Clinicopathologic and immunohistochemical study with special emphasis on its distinction from ordinary leiomyosarcoma and malignant fibrous histiocytoma. Am. J. Surg. Pathol. 2001, 25, 1030–1038. [Google Scholar] [CrossRef]
  40. Demicco, E.G.; Boland, G.M.; Brewer Savannah, K.J.; Lusby, K.; Young, E.D.; Ingram, D.; Watson, K.L.; Bailey, M.; Guo, X.; Hornick, J.L.; et al. Progressive loss of myogenic differentiation in leiomyosarcoma has prognostic value. Histopathology 2015, 66, 627–638. [Google Scholar] [CrossRef]
  41. Nosaka, K.; Komatsu, H.; Oishi, T.; Horie, Y.; Harada, T.; Umekita, Y. A Case of dedifferentiated leiomyosarcoma of the uterus. Int. J. Pathol. Clin. Res. 2016, 2, 49. [Google Scholar] [CrossRef]
  42. WHO. WHO Classification of Tumours: Female Genital Tumours, 5th ed.; WHO Classification of Tumors Editorial Board, Ed.; WHO: Lyon, France, 2020. [Google Scholar]
  43. Sadiq, Q.; Khan, F. High grade sarcoma with chondrosarcomatous differentiation in primary uterine leiomyosarcoma; A rare case and review of literature. Gynecol. Oncol. Rep. 2022, 39, 100905. [Google Scholar] [CrossRef] [PubMed]
  44. Rawish, K.R.; Fadare, O. Dedifferentiated leiomyosarcoma of the uterus with heterologous elements: A potential diagnostic pitfall. Case Rep. Obstet. Gynecol. 2012, 2012, 534634. [Google Scholar] [CrossRef]
  45. Parikh, P.; Maheshwari, A.; Rekhi, B. Two uncommon cases of uterine leiomyosarcomas displaying heterologous osteosarcomatous de-differentiation. J. Cancer Res. Ther. 2015, 11, 654. [Google Scholar] [CrossRef] [PubMed]
  46. Iihara, K.; Hirano, K.; Fujioka, Y.; Sakamoto, A. Leiomyosarcoma with dedifferentiation in a premenopausal patient discovered after uterine artery embolization. Pathol. Int. 2007, 57, 681–687. [Google Scholar] [CrossRef]
  47. Kousar, A.; Wald, A.I.; Heayn, M.; Cardillo, N.D.; Elishaev, E.; Bhargava, R. Dedifferentiated leiomyosarcoma: Morphology, immunohistochemistry, and molecular findings of a case and review of literature. Int. J. Gynecol. Pathol. 2023. online ahead of print. [Google Scholar] [CrossRef] [PubMed]
  48. Cope, B.M.; Traweek, R.S.; Lazcano, R.; Keung, E.Z.; Lazar, A.J.; Roland, C.L.; Nassif, E.F. Targeting the molecular and immunologic features of leiomyosarcoma. Cancers 2023, 15, 2099. [Google Scholar] [CrossRef]
  49. Astolfi, A.; Nannini, M.; Indio, V.; Schipani, A.; Rizzo, A.; Perrone, A.M.; De Iaco, P.; Pirini, M.G.; De Leo, A.; Urbini, M.; et al. Genomic database analysis of uterine leiomyosarcoma mutational profile. Cancers 2020, 12, 2126. [Google Scholar] [CrossRef]
  50. Ciccarone, F.; Bruno, M.; De Paolis, E.; Piermattei, A.; De Bonis, M.; Lorusso, D.; Zannoni, G.F.; Normanno, N.; Minucci, A.; Scambia, G.; et al. Role of homologous recombination repair (HRR) genes in uterine leiomyosarcomas: A retrospective analysis. Cancers 2022, 14, 1934. [Google Scholar] [CrossRef]
  51. Beck, A.H.; Lee, C.H.; Witten, D.M.; Gleason, B.C.; Edris, B.; Espinosa, I.; Zhu, S.; Li, R.; Montgomery, K.D.; Marinelli, R.J.; et al. Discovery of molecular subtypes in leiomyosarcoma through integrative molecular profiling. Oncogene 2010, 29, 845–854. [Google Scholar] [CrossRef]
  52. Hass, R.; von der Ohe, J.; Ungefroren, H. The intimate relationship among EMT, MET and TME: A T(ransdifferentiation) E(nhancing) M(ix) to be exploited for therapeutic purposes. Cancers 2020, 12, 3674. [Google Scholar] [CrossRef]
  53. Varga, J.; Greten, F.R. Cell plasticity in epithelial homeostasis and tumorigenesis. Nat. Cell Biol. 2017, 19, 1133–1141. [Google Scholar] [CrossRef]
  54. Meacham, C.E.; Morrison, S.J. Tumour heterogeneity and cancer cell plasticity. Nature 2013, 501, 328–337. [Google Scholar] [CrossRef] [PubMed]
  55. Hammerlindl, H.; Schaider, H. Tumor cell-intrinsic phenotypic plasticity facilitates adaptive cellular reprogramming driving acquired drug resistance. J. Cell Commun. Signal. 2018, 12, 133–141. [Google Scholar] [CrossRef] [PubMed]
  56. Hass, R. Retrodifferentiation: A mechanism for cellular regeneration? Biol. Chem. 2009, 390, 409–416. [Google Scholar] [CrossRef] [PubMed]
  57. Hass, R. Retrodifferentiation and cell death. Crit. Rev. Oncog. 1994, 5, 359–371. [Google Scholar] [CrossRef] [PubMed]
  58. Cabillic, F.; Corlu, A. Regulation of transdifferentiation and retrodifferentiation by inflammatory cytokines in hepatocellular carcinoma. Gastroenterology 2016, 151, 607–615. [Google Scholar] [CrossRef]
  59. Lu, W.; Kang, Y. Epithelial-mesenchymal plasticity in cancer progression and metastasis. Dev. Cell 2019, 49, 361–374. [Google Scholar] [CrossRef]
  60. Easwaran, H.; Tsai, H.C.; Baylin, S.B. Cancer epigenetics: Tumor heterogeneity, plasticity of stem-like states, and drug resistance. Mol. Cell 2014, 54, 716–727. [Google Scholar] [CrossRef]
  61. Yamada, Y.; Haga, H.; Yamada, Y. Concise review: Dedifferentiation meets cancer development: Proof of concept for epigenetic cancer. Stem Cells Transl. Med. 2014, 3, 1182–1187. [Google Scholar] [CrossRef]
  62. Dubois-Pot-Schneider, H.; Fekir, K.; Coulouarn, C.; Glaise, D.; Aninat, C.; Jarnouen, K.; Le Guevel, R.; Kubo, T.; Ishida, S.; Morel, F.; et al. Inflammatory cytokines promote the retrodifferentiation of tumor-derived hepatocyte-like cells to progenitor cells. Hepatology 2014, 60, 2077–2090. [Google Scholar] [CrossRef] [PubMed]
  63. Watts, F.; Stewart, P.; Gill, A.J.; Krishnaswamy, M. SDHA deficient dedifferentiated gastrointestinal stromal tumour with a smooth-muscle immunophenotype. Pathology 2023. online ahead of print. [Google Scholar] [CrossRef]
  64. Shah, V.I.; Morgan, S.E.; Kobel, M.; Lee, C.H.; McCluggage, W.G. Dedifferentiation in breast metastasis of endometrial carcinoma: A diagnostic dilemma. Int. J. Gynecol. Pathol. 2022, 41, 35–39. [Google Scholar] [CrossRef]
  65. Tan, N.J.H.; Sun, I.S.Y.; Low, S.W.; Kuick, C.H.; Chang, K.T.E.; Tan, C.L. A rapidly fatal intracranial anaplastic hemangiopericytoma with de-novo dedifferentiation: Emphasis on diagnostic recognition, molecular confirmation and discussion on treatment dilemma. Brain Tumor Pathol. 2019, 36, 20–26. [Google Scholar] [CrossRef] [PubMed]
  66. Pauwels, P.; Debiec-Rychter, M.; Stul, M.; De Wever, I.; Van Oosterom, A.T.; Sciot, R. Changing phenotype of gastrointestinal stromal tumours under imatinib mesylate treatment: A potential diagnostic pitfall. Histopathology 2005, 47, 41–47. [Google Scholar] [CrossRef] [PubMed]
Figure 1. Timelines of patients’ clinical course. #—cycle of chemotherapy; CCRT—concurrent chemoradiation therapy; NED—no evidence of disease; PD—progressive disease; PR—partial response; RT—radiation therapy; SD—stable disease.
Figure 1. Timelines of patients’ clinical course. #—cycle of chemotherapy; CCRT—concurrent chemoradiation therapy; NED—no evidence of disease; PD—progressive disease; PR—partial response; RT—radiation therapy; SD—stable disease.
Diagnostics 14 00160 g001
Figure 2. Histological features of uterine DDLMS (cases 1−3). Case 1: (A) The metastatic lesion exhibits variable-sized multinodular tumors. Each nodule consists of a peripheral rim of dedifferentiated component (blue asterisks) and CSA (yellow asterisk) at the center. (B) The dedifferentiated component is characterized by UPS-like morphology. (C) The heterologous component displays CSA. Case 2: (D) The dedifferentiated component shows non-cohesive polygonal cells with moderate eosinophilic cytoplasm and large pleomorphic nuclei. (E) Some multinucleated tumor giant cells can also be observed (blue arrows). Brisk mitotic activity (green circle) with occasional atypical mitotic figures (yellow circles) is noted in the dedifferentiated component. (F) High-power magnification reveals large polygonal cells possessing abundant eosinophilic cytoplasm and eccentrically placed nuclei with marked pleomorphism, compatible with RMS. Some tumor cell nuclei display one or more conspicuous nucleoli (red circle). Case 3: (G,H) The differentiated components show the histological features of (G) spindle cell LMS and (H) epithelioid LMS. (I,J) The dedifferentiated component shows scattered pleomorphic tumor cells possessing (I) abundant eosinophilic cytoplasm (blue arrows) and (J) eccentrically placed nuclei with conspicuous macronucleoli (red circle). Original magnification: (A) 20×; (B), 40×; (CE), 200×; (F), 400×; (G,H) 40×; (I,J) 200×.
Figure 2. Histological features of uterine DDLMS (cases 1−3). Case 1: (A) The metastatic lesion exhibits variable-sized multinodular tumors. Each nodule consists of a peripheral rim of dedifferentiated component (blue asterisks) and CSA (yellow asterisk) at the center. (B) The dedifferentiated component is characterized by UPS-like morphology. (C) The heterologous component displays CSA. Case 2: (D) The dedifferentiated component shows non-cohesive polygonal cells with moderate eosinophilic cytoplasm and large pleomorphic nuclei. (E) Some multinucleated tumor giant cells can also be observed (blue arrows). Brisk mitotic activity (green circle) with occasional atypical mitotic figures (yellow circles) is noted in the dedifferentiated component. (F) High-power magnification reveals large polygonal cells possessing abundant eosinophilic cytoplasm and eccentrically placed nuclei with marked pleomorphism, compatible with RMS. Some tumor cell nuclei display one or more conspicuous nucleoli (red circle). Case 3: (G,H) The differentiated components show the histological features of (G) spindle cell LMS and (H) epithelioid LMS. (I,J) The dedifferentiated component shows scattered pleomorphic tumor cells possessing (I) abundant eosinophilic cytoplasm (blue arrows) and (J) eccentrically placed nuclei with conspicuous macronucleoli (red circle). Original magnification: (A) 20×; (B), 40×; (CE), 200×; (F), 400×; (G,H) 40×; (I,J) 200×.
Diagnostics 14 00160 g002
Figure 3. Histological features of uterine DDLMS (cases 4 and 5). Case 4: (A) The differentiated area exhibits the classic morphology of malignant smooth muscle differentiation, including intersecting fascicles of atypical spindle cells with eosinophilic cytoplasm (spindle cell LMS). (B) The dedifferentiated (blue asterisk) and heterologous (yellow asterisk) components are sharply delineated. (C) The heterologous component is morphologically compatible with high-grade CSA. Case 5: (D) The dedifferentiated component shows extreme hypercellularity and severe-to-marked nuclear pleomorphism. (E) The heterologous component comprises variable-sized islands of malignant cartilage. (F) In a few areas showing CSA, extensive tumor necrosis is observed. Original magnification: (A) 100×; (B) 40×; (C) 200×; (DF) 100×.
Figure 3. Histological features of uterine DDLMS (cases 4 and 5). Case 4: (A) The differentiated area exhibits the classic morphology of malignant smooth muscle differentiation, including intersecting fascicles of atypical spindle cells with eosinophilic cytoplasm (spindle cell LMS). (B) The dedifferentiated (blue asterisk) and heterologous (yellow asterisk) components are sharply delineated. (C) The heterologous component is morphologically compatible with high-grade CSA. Case 5: (D) The dedifferentiated component shows extreme hypercellularity and severe-to-marked nuclear pleomorphism. (E) The heterologous component comprises variable-sized islands of malignant cartilage. (F) In a few areas showing CSA, extensive tumor necrosis is observed. Original magnification: (A) 100×; (B) 40×; (C) 200×; (DF) 100×.
Diagnostics 14 00160 g003
Figure 4. Immunostaining results of uterine DDLMS. Case 1: (A) In the dedifferentiated component, desmin immunoreactivity is either (B) absent or (C) faint in a few tumor cells. The dedifferentiated component shows (D) strong S100 protein expression, (E) preserved RB protein expression, and (F) wild-type p53 protein expression. Case 2: (G) The dedifferentiated component resembling UPS shows (H) a lack of desmin immunoreactivity, (I) strong SATB2 expression, and (J) p53 overexpression. Case 4: (K) Low-power magnification reveals differentiated LMS (white asterisk), DDLMS (blue asterisk), and CSA (yellow asterisk). (L) Desmin expression is uniform and strong in the differentiated component (white asterisk), while the dedifferentiated (blue asterisk) and heterologous (yellow asterisk) components show no signs of desmin expression. Original magnification: (AF) 40×; (GJ) 100×; (K,L) 20×.
Figure 4. Immunostaining results of uterine DDLMS. Case 1: (A) In the dedifferentiated component, desmin immunoreactivity is either (B) absent or (C) faint in a few tumor cells. The dedifferentiated component shows (D) strong S100 protein expression, (E) preserved RB protein expression, and (F) wild-type p53 protein expression. Case 2: (G) The dedifferentiated component resembling UPS shows (H) a lack of desmin immunoreactivity, (I) strong SATB2 expression, and (J) p53 overexpression. Case 4: (K) Low-power magnification reveals differentiated LMS (white asterisk), DDLMS (blue asterisk), and CSA (yellow asterisk). (L) Desmin expression is uniform and strong in the differentiated component (white asterisk), while the dedifferentiated (blue asterisk) and heterologous (yellow asterisk) components show no signs of desmin expression. Original magnification: (AF) 40×; (GJ) 100×; (K,L) 20×.
Diagnostics 14 00160 g004
Table 1. Antibodies used.
Table 1. Antibodies used.
AntibodyDilutionCloneCompanyPositive Control
Desmin1:200D33Agilent Technologies, Santa Clara, CA, USANormal myometrium
S100 protein1:5000polyclonalAgilent Technologies, Santa Clara, CA, USAVulvar malignant melanoma
Myogenin1:50F5DCell marque, Rocklin, CA, USAUterine rhabdomyosarcoma
MyoD11:50EP212Cell marque, Rocklin, CA, USAUterine rhabdomyosarcoma
SATB21:2000EPNCIR130AAbcam, Cambridge, UKColonic adenocarcinoma
p531:800DO-7Leica Biosystems, Deer Park, IL, USAOvarian HGSC
Retinoblastoma protein1:4004H1Cell Signaling Technology, Beverly, MA, USAOcular retinoblastoma
Abbreviations: HGSC—high-grade serous carcinoma; SATB2—special AT-rich sequence-binding protein 2.
Table 2. Clinical characteristics of five patients with uterine DDLMS.
Table 2. Clinical characteristics of five patients with uterine DDLMS.
Case No12345
Age (years)6055515163
Presenting symptomsAbdominal discomfort, constipationUterine mass detected on routine examinationUterine masses detected on routine examinationUterine mass detected on routine examinationAbdominal discomfort and pain, palpable pelvic mass
Previous medical historyNoneNoneThyroid cancer, umbilical herniaHyperthyroidismNone
Imaging findings of uterine tumorNAA large solid cystic massMultiple solid uterine masses measuring up to 8.9 cmAn 8.3 cm lobulated, heterogeneous mass with hypodense necrotic areaA 23.0 cm large heterogeneous mass with adnexal extension
Clinical impressionUterine leiomyomaUterine leiomyomaUterine leiomyomaUterine leiomyomaUterine sarcoma
Surgical procedure for uterine tumorTHTH, BSO, PLND, PALND, OMT, APPTH, bilateral salpingectomyTH, BSO, OMTUterine mass excision, LO, LHC, left nephrectomy
Pathological diagnosis of uterine tumorLMSDDLMSDDLMS-HLMSDDLMS-H
Greatest dimension of uterine tumor (cm)NA27.88.98.323.0
Adnexal extensionAbsentAbsentAbsentAbsentPresent
Pelvic extensionAbsentAbsentPresentAbsentPresent
Abdominal extensionAbsentAbsentAbsentAbsentPresent
LN metastasisAbsentAbsentPresent (para-aortic)Present (left pelvic)Absent
Initial stageIBIBIIICIIICIVC
Post-operative treatmentCCRTChemotherapyRTx (interrupted)ChemotherapyNA (lost to follow-up)
Post-treatment recurrencePresent (ovary, colon, bladder, peritoneum, mesentery, omentum)Present (vagina, bladder, peritoneum, lungs)AbsentPresent (left paracolic gutter)NA (lost to follow-up)
Pathological diagnosis of recurrent tumorMetastatic DDLMS-HMetastatic DDLMS-HNoneMetastatic DDLMS-HNA (lost to follow-up)
Treatment for recurrenceExcision, RTx, chemotherapyExcision, chemotherapyNoneExcisionNA (lost to follow-up)
RFS (months)306154NA (lost to follow-up)
Survival statusAlive with diseaseNA (lost to follow-up)No evidence of diseaseNA (lost to follow-up)NA (lost to follow-up)
OS (months)93NA (lost to follow-up)15NA (lost to follow-up)NA (lost to follow-up)
Abbreviations: APP—appendectomy; BSO—bilateral salpingo-oophorectomy; CCRT—concurrent chemoradiation therapy; DDLMS-H—dedifferentiated leiomyosarcoma with heterologous component; LHC—left hemicolectomy; LO—left oophorectomy; NA—not applicable; OMT—omentectomy; RTx—radiation therapy; PALND—para-aortic lymph node dissection; PLND—pelvic lymph node dissection; TH—total hysterectomy.
Table 3. Pathological characteristics of five patients with uterine DDLMS.
Table 3. Pathological characteristics of five patients with uterine DDLMS.
Case No12345
Dominant morphology of differentiated componentSpindle cell and epithelioid LMSEpithelioid LMSSpindle cell and epithelioid LMSSpindle cell LMSSpindle cell and epithelioid LMS
Nuclear pleomorphismSevereSevereSevereSevereSevere
Mitotic count per 10 HPFs2340462221
Tumor cell necrosisPresentPresentPresentPresentPresent
Tumor borderInfiltrativeInfiltrativeInfiltrativeInfiltrativeInfiltrative
Lymphocytic infiltrateAbsentPresentPresentPresentAbsent
Histological type and proportion of heterologous componentCSA (80%)RMS (60%)RMS (20%)CSA (60%)CSA (30%)
DesminDifferentiatedDMPDSPDSPNegativeNA
DedifferentiatedFWPNegativeNegativeNegativeNA
S100 proteinDifferentiatedFWPNegativeNANegativeNA
DedifferentiatedDSPNegativeNAFSPNA
MyogeninDifferentiatedNegativeNegativeNegativeNANA
DedifferentiatedNegativeNegativeFWPNANA
MyoD1DifferentiatedNegativeNegativeNegativeNANA
DedifferentiatedNegativeNegativeNegativeNANA
SATB2DifferentiatedFWPNegativeNANANA
DedifferentiatedNegativeDSPNANANA
p53DifferentiatedWTWTWTNANA
DedifferentiatedWTOEWTNANA
RB proteinDifferentiatedNo lossNo lossNANANA
DedifferentiatedNo lossNo lossNANANA
Abbreviations: CSA—chondrosarcoma; DMP—diffuse moderate positive; DSP—diffuse strong positive; FSP—focal strong positive; FWP—focal weak positive; HPFs—high-power fields; NA—not applicable; OE—overexpression; RMS—rhabdomyosarcoma; WT—wild type.
Table 4. Clinical characteristics of 42 previously reported uterine DDLMS cases.
Table 4. Clinical characteristics of 42 previously reported uterine DDLMS cases.
Authors (Year
Published)
Case NoAge (Years)Presenting SymptomInitial StageTreatmentRecurrenceDistant
Metastasis
DFS (Months)OutcomeOS or DSS (Months)
Iihara et al., (2007) [46]148Hypermenorrhea for 4 yearsIBUAE, TH, CTx, GKRSNAPresent (lungs, brain)NADOD20 a
Chen et al., (2011) [20]259Pelvic painNATH, BSOAbsentAbsent28NED28 a
380PMBNAExcisionNANANADOC12 a
Rawish and Fadare (2012) [44]448NAIASH, BSO, CTxPresentAbsent6AWD8 a
Parikh et al., (2015) [45]560Abdominal pain for 4 monthsNATH, BSNANANANANA
638InfertilityNAMyomectomyNANANANANA
Nosaka et al., (2016) [41]763Bloody vaginal discharge for 2 monthsIVBTH, BSO, CTxNAPresent (lungs)NANANA
Yu and Hornick (2022) [3]863NANASurgery, CTxPresentPresent (lungs, diaphragm, heart, SVC, kidney)NADOD7.5 a
940NANASurgery, CTxPresentPresent (colon, retroperitoneum)NADOD18 a
1048NANASurgery, CTx, RTxPresentPresent (lungs, liver, peritoneum, colon, small bowel)NADOD6.5 a
1155NANACTxAbsentPresent (pancreas, bone, lungs)NADODNA
1252NANASurgery, CTxPresentPresent (lungs, abdomen)NAAWD36 a
1361NANASurgery, CTx, RTxPresentPresent (lungs, pleura)NADOD17 a
1453NANASurgeryAbsentNANADOD3.5 a
1562NANANANANANANANA
1643NANASurgery, CTxPresentPresent (small bowel)NAAWD32 a
1752NANASurgery, CTxPresentPresent (liver, small bowel)NAAWD28 a
Sadiq and Khan (2022) [43]1868Vaginal bleedingNATH, BSONANANANANA
Chapel et al., (2023) [16]1988NAIBSurgeryNANA2DOD2 b
2066NAIBSurgeryNANA7DOD11 b
2168NAIBSurgery, CTxPresentNA3DOD20 b
2242NAIBSurgeryNANANADOD23 b
2361NAIBSurgeryNANANADOD5 b
2457NAIIIBSurgeryNANANANANA
2546NAIISurgeryNANA23DOD31 b
2654NAIBSurgeryNANANADOD73 b
2759NAIBCTxNANA114NED114 b
2850NAIIIBSurgeryNANA12AWD12 b
2953NAIASurgeryNANA21AWD50 b
3063NAIVCTxNAPresent8DOD16 b
3153NAIVCTxNAPresentNADOD15 b
3254NAIVSurgeryNAPresentNADOD3 b
3352NAIVCTxNAPresentNADOD10 b
3457NAIBCTx for recurrencePresentPresent4NED109 b
3590NAIISurgeryNANANANANA
3654NAIICTx and RTx for recurrencePresentNA2NED56 b
3770NAIBRTxNANA15AWD44 b
3875NAIBSurgeryNANANANANA
3955NAIBCTx for recurrencePresentNA4AWD4 b
4060NAIBCTx for recurrencePresentNA8DOD13 b
4163NAIISurgeryNANANANANA
Kousar et al., (2023) [47]4242Acute abdominal pain and vaginal bleedingIVSurgery, CTxPresentPresent (liver, peritoneum)NANANA
Abbreviations: AWD—alive with disease; BSO—bilateral salpingo-oophorectomy; CTx—chemotherapy; DFS—disease-free survival; DSS—disease-specific survival; DOD—died of disease; GKRS—gamma knife radiosurgery; NA—not applicable; NED—no evidence of disease; OS—overall survival; PMB—postmenopausal bleeding; SH—subtotal hysterectomy; SVC—superior vena cava; TH—total hysterectomy; UAE—uterine artery embolization. a OS; b DSS.
Table 5. Pathological characteristics of 42 previously reported uterine DDLMS cases.
Table 5. Pathological characteristics of 42 previously reported uterine DDLMS cases.
Authors
(Year Published)
Case NoTumor Size (cm)Dominant Morphology of Differentiated ComponentHistological Type of Heterologous
Component (Proportion)
Iihara et al., (2007) [46]114.0Spindle cell LMSMixed proliferation of scattered bizarre cells and spindle cells without specific structures (NA)
Chen et al., (2011) [20]26.8Spindle cell LMSMFH-like morphology (NA)
318.0Spindle cell LMSMFH-like morphology (NA)
Rawish and Fadare (2012) [44]418.0Spindle cell LMSOSA (10%)
Parikh et al., (2015) [45]530.0Spindle cell LMSOsteochondroid differentiation and MNGCs (NA)
612.5Spindle cell LMSOSA (NA)
Nosaka et al., (2016) [41]714.0Spindle cell LMSUndifferentiated pleomorphic sarcoma (NA)
Yu and Hornick (2022) [3]811.7Spindle cell LMSOSA (NA)
9NASpindle cell LMSOSA (NA)
1012.0Spindle cell LMSOSA (NA)
119.0Spindle cell LMSOSA (NA)
1220.0Spindle cell LMSOSA (NA)
1318.0Spindle cell LMSOSA (NA)
1416.0Spindle cell LMSOSA (NA)
1518.0Spindle cell LMSOSA (NA)
1617.0Spindle cell LMSOSA (NA)
1718.8Spindle cell LMSOSA (NA)
Sadiq and Khan (2022) [43]18Up to 4.0Spindle cell LMSCSA (NA)
Chapel et al., (2023) [16]19NASpindle cell LMSMFH-like morphology (30%)
206.5Spindle cell LMSMFH-like morphology (20%)
218.5Spindle cell LMS and CLMMFH-like morphology (40%)
2210.0CLMMFH-like morphology (50%)
237.0Epithelioid LMSMFH-like morphology (5%)
2412.0Spindle cell LMSMFH-like morphology (15%)
2512.1Spindle cell LMSMFH-like morphology and OSA (20%)
268.2Spindle cell LMSMFH-like morphology (10%)
276.8Spindle cell LMSMFH-like morphology (40%)
283.0Spindle cell LMSMFH-like morphology (50%)
294.5STUMPMFH-like morphology (30%)
3011.7Spindle cell LMSMFH-like morphology and OSA (10%)
318.0Spindle cell LMSMFH-like morphology (25%)
3225.0Spindle cell LMSMFH-like morphology (20%)
3320.0Spindle cell LMSMFH-like morphology, OSA, and CSA (70%)
349.0CLMMFH-like morphology (50%)
3520.0LBNMFH-like morphology (50%)
3614.5CLMMFH-like morphology (20%)
3711.0STUMPMFH-like morphology (40%)
386.1Spindle cell LMSMFH-like morphology (70%)
3910.0Spindle cell LMSMFH-like morphology (40%)
4014.3LM, LBM, and spindle cell LMSMFH-like morphology (10%)
417.7Spindle cell LMSMFH-like morphology (70%)
Kousar et al., (2023) [47]4210.5, 6.7 (fundus); 1.7 (body)LM-like areas, STUMP, and frank LMSAreas showing extreme hypercellularity and large polygonal cells with significant cytological atypia and brisk mitotic activity
Abbreviations: CLM—cellular leiomyoma; LBN—leiomyoma with bizarre nuclei; LM—leiomyoma; MFH—malignant fibrous histiocytoma; MNGCs—multinucleated giant cells; NA—not applicable; STUMP—smooth muscle tumor of uncertain malignant potential.
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content.

Share and Cite

MDPI and ACS Style

Kim, S.; Bae, H.; Kim, H.-S. Dedifferentiated Leiomyosarcoma of the Uterine Corpus with Heterologous Component: Clinicopathological Analysis of Five Consecutive Cases from a Single Institution and Comprehensive Literature Review. Diagnostics 2024, 14, 160. https://doi.org/10.3390/diagnostics14020160

AMA Style

Kim S, Bae H, Kim H-S. Dedifferentiated Leiomyosarcoma of the Uterine Corpus with Heterologous Component: Clinicopathological Analysis of Five Consecutive Cases from a Single Institution and Comprehensive Literature Review. Diagnostics. 2024; 14(2):160. https://doi.org/10.3390/diagnostics14020160

Chicago/Turabian Style

Kim, Suyeon, Hyunsik Bae, and Hyun-Soo Kim. 2024. "Dedifferentiated Leiomyosarcoma of the Uterine Corpus with Heterologous Component: Clinicopathological Analysis of Five Consecutive Cases from a Single Institution and Comprehensive Literature Review" Diagnostics 14, no. 2: 160. https://doi.org/10.3390/diagnostics14020160

APA Style

Kim, S., Bae, H., & Kim, H. -S. (2024). Dedifferentiated Leiomyosarcoma of the Uterine Corpus with Heterologous Component: Clinicopathological Analysis of Five Consecutive Cases from a Single Institution and Comprehensive Literature Review. Diagnostics, 14(2), 160. https://doi.org/10.3390/diagnostics14020160

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop