Background
Rhabdomyosarcomas can be classified as embryonal, alveolar and pleomorphic subtypes [
1‐
3]. Embryonal rhabdomyosarcoma (ERMS) is the most common soft tissue sarcoma of the lower urogenital tract in children [
4,
5] from birth to 15 years of age [
6]. In adults ERMS is very rare. There are only individual case reports of ERMS in adulthood. In contrast to infants and children prognosis is poor in this age group [
7‐
13]. Spindle cell rhabdomyosarcoma is considered a rare variant of ERMS that shows spindle cell morphology [
9,
14]. In the latest WHO classification scheme spindle cell rhabdomyosarcoma is grouped together with sclerosing rhabdomyosarcoma [
15]. ERMS shows a striking male predominance and arises most commonly from the paratesticular soft tissue, followed by the head and neck, the extremities and the genitourinary tract [
16,
17]. ERMS account for only 0,3–1 % of all malignant prostate tumors [
18,
19]. In pediatric patients spindle cell type of ERMS has a good prognosis and thus correct subtyping is of crucial importance for therapy and prognosis. However, the same tumor entity in adults is a very rare and aggressive tumor. In younger men it is crucial to consider this unusual differential diagnosis in order not to delay the appropriate therapy. We report a case of spindle cell embryonal rhabdomyosarcoma in the prostate of an adult patient and discuss clinicopathological features.
Discussion
Spindle cell ERMS of the prostate in adults are very rare. A recently published review of the literature resulted in only 25 cases of confirmed primary ERMS of the prostate in males 18 years of age or older until October 2010 [
20]. Since then, a literature search yielded five more cases of prostatic ERMS [
9,
12,
13,
21,
22], resulting in a total of 30 published and confirmed primary ERMS of the prostate in adults. Of all published cases in adults so far, only three were specifically subtyped as spindle cell type of ERMS [
9,
13,
22], thus, the case we present here is the fourth one published to date.
In sharp contrast to adult rhabdomyosarcoma where prognosis is generally very poor irrespective of histological subtype, in children and adolescents therapy and clinical outcome is highly dependent on histological subtype of rhabdomyosarcoma. Especially the spindle cell subtype of ERMS heralds a good prognosis and is categorized in the low risk group according to the CWS guidelines in which three risk groups are defined (low risk, standard risk, high risk). Thus, correct subtyping of soft tissue sarcomas is of utmost importance even in adults where the development of new therapy protocols may in the future be dependent on the histological subtype.
The histologic diagnosis of the spindle cell variant of ERMS is usually based on the presence of small, round to spindle-shaped tumor cells with moderate nuclear pleomorphism. Frequent findings are scattered large rhabdomyoblasts with an eccentric nucleus and striated, eosinophilic cytoplasm [
9,
10].
Immunohistochemically, ERMS typically express skeletal muscle markers: Tumor cells usually stain positive for vimentin, desmin, myogenin and myoglobin [
8]. However, desmin negative cases have been reported. Thus, for confirmation of the histological subtype a panel of desmin, myogenin and myoglobin is recommended [
22]. A cytoplasmic staining for CD 99 is present in 15 % of all ERMS [
23], in the spindle cell subtype however the positivity rate for CD 99 was reported to be 100 % [
20], which is significant especially considering peripheral primitive neuroectodermal tumor (PPNET) being an important differential diagnosis.
Besides PPNET, differential diagnosis of spindle cell ERMS includes other sarcomatous tumors such as pleomorphic and alveolar rhabdomyosarcoma, leiomyosarcoma and fibrosarcoma. In addition, malignant peripheral nerve sheath tumors, spindle cell malignant melanoma, lymphomas and phyllodes tumors with focal rhabdomyoblastic differentiation have to be considered [
8,
20]. Immunohistochemistry, cytogenetic and molecular pathological findings are crucial to confirm the diagnosis [
8].
ERMS lack the characteristic translocation t(1;13) and t(2;13) of alveolar rhabdomyosarcoma. In contrast to ERMS, leiomyosarcomas stain negatively for myoglobin and myogenin. Fibrosarcomas do not show scattered rhabdomyoblasts in hematoxylin and eosin (H&E) staining and express neither desmin nor myogenin. In PPNET, immunohistochemical staining with myogenin is mostly negative [
8]. PPNET with divergent skeletal muscle differentiation may show immunohistologic features of skeletal muscles. Here, cytogenetic analysis for translocation t(11;22)(q24;q12) which is found in most cases of PPNET but not in ERMS is of utmost importance [
23]. In contrast to ERMS, malignant peripheral nerve sheath tumors express neural markers such as S-100. Malignant melanomas, unlike ERMS, stain positively with melanocytic markers [
20]. Lymphomas show immunopositivity for common leukocyte antigen CD 45.
Molecular pathological diagnostics to date have not detected any specific mutations in ERMS. In some cases, a loss of heterozygosity has been described in the chromosomal region 11p15.5 [
20].
Clinical symptoms usually include micturition problems like urinary retention, dysuria and seldom hematuria. Typical clinical findings include an enlarged prostate gland and normal serum value of PSA. The disease usually progresses rapidly so that diagnosis is often made at an advanced stage with presence of distant metastases [
7]. Macroscopic findings often show a nodular tumor with grayish-white indurated cut surfaces [
14].
In our case, a 25-year-old adolescent presented with micturition problems and an enlarged prostate gland. PSA levels were within normal range. At this age, ERMS of the prostate is rather seldom as ERMS occur more often in the lower urogenital tract in children. The most common prostate tumor in male adults is adenocarcinoma, however, this diagnosis is very rare in an age below 40 years [
7]. In the age group between 20 and 40 years enlargement of the prostate gland usually is classified as benign prostatic hyperplasia and malignant disease is initially virtually never considered. Clinical differences of both tumor entities are compared in Table
1.
Table 1
Clinical and radiological differences between prostatic rhabdomyosarcoma and carcinoma, modified according to Waring et al. [
7]
Incidence | very rare | common |
Age group | Children, rarely young adults | >40 years |
Symptoms | urinary obstruction | urinary obstruction |
Digital rectal examination | Enlarged, firm, smooth prostate | Hard, fixed, nodular, irregular prostate |
PSA levels | normal | elevated |
Course | rapid | usually slow |
Ultrasound and MRI | often extensive invasion of periprostatic tissues | often localized to the prostate gland |
Treatment of ERMS depends on stage of disease and includes a combination of chemotherapy, radical surgery and radiotherapy [
10]. Our patient was treated according to the recommendations of the CWS-guidance for risk adapted treatment of soft tissue sarcoma and soft tissue tumors in children, adolescents, and young adults. After chemotherapy treatment he showed a good partial response. Local therapy of the tumor is a crucial element in the overall treatment.
If resection of the primary tumor would be mutilating as in our case radiotherapy is a local therapy option. 50 Gy (conventional fractionated) is considered as sufficient for rhabdomyosarcoma with residual disease following induction chemotherapy without an option for secondary resection [
24].
Prognosis of ERMS in adults is generally poor. Most patients with prostatic ERMS die under therapy. Children and adolescents usually have a much better response to multimodal therapy than adults and primary surgical treatment is not standard of therapy [
10,
11]. In a retrospective study Wang et al. analysed outcome of 25 adult patients with prostate sarcoma. Age more than 50 years, metastasis at presentation, and a lack of surgery with curative intent were independently predictive of an unfavorable outcome [
25]. Musser et al. reviewed 38 cases of adult prostate sarcoma treated at the Memorial Sloan Kettering Cancer Center between 1982 and 2012. They found an association between histological tumor subtype and outcome: Rhabdomyosarcoma patients had worse overall and cancer-specific survival compared to leiomyosarcoma patients [
26]. Latz et al. [
9] describe a case of spindle cell rhabdomyosarcoma of the prostate in a 23-year-old patient who died 14 month after diagnosis being treated within the CWS 2002 P study which includes children and adolescents with soft tissue sarcoma. They retrospectively criticize that early radical surgery was not performed in the first place but the patient received radiochemotherapy. Latz et al. [
9] discuss that spindle cell rhabdomyosarcoma in adults is not synonymous with rhabdomyosarcoma in childhood leaving primary radical surgical therapy as the only option for curative therapy in the absence of metastatic spread. Recently, a clinicopathological analysis of spindle cell/scerosing rhabdomyosarcoma suggested an improvement of outcome of spindle cell rhabdomyosarcoma in various locations by localized surgical treatment combined with chemotherapy in such cases with initial localized disease [
22]. In the case we describe here primary radical surgery was not an option as our patient already had pulmonary metastases at the time of diagnosis. Standard therapy of prostatic rhabdomyosarcoma in adults is still to be defined.
Acknowledgements
The authors thank Dr. M. Basche, Institute for Radiology and Nuclear Medicine, Kassel, Germany for providing the MRI-scans.