2Department of Radiation Oncology, Dicle University, Faculty of Medicine, Diyarbakır-Turkey DOI : 10.5505/tjo.2019.1820
Summary
Primary or metastatic dura mater sarcomas are rarely seen, and dural synovial sarcomas are quite rare. Here we report the case of a 60-year-old man who presented with headache, nausea, and vomiting and was found to have a 63×33×40-mm mass with solid and cystic components in parieto-occipital lobe. The mass was resected completely, with no residue detected on postoperative magnetic resonance imagining. On pathological evaluation, a vimentin-, S100-, transducer-like enhancer of split 1-, BCL-2-, and EMApositive and desmin-, PR-, CD99-, PANCK-, and GFAP-negative synovial sarcoma with Ki-67 proliferation index of 12% was detected. Postoperatively, chemotherapy has been started, and it will be followed by radiotherapy. Primary meningeal-derived sarcomas are rare, and differential diagnosis with other meningeal mesenchymal tumors is based on the findings of morphological and immunohistochemical analyses.Introduction
Dura mater-originated neoplasms comprise a wide range of primary and metastatic tumors based on their clinical, radiological, morphological, and immunophenotypical features. Treatment decision is based on tumor origin, morphologic type, and degree. Primary and metastatic dura mater tumors are rarely seen, and dural synovial sarcomas are quite rare.[1] There have been few reports on dura mater-originated synovial sarcoma; here we report the case of a patient with primary dural synovial sarcoma.Case Presentation
A 60-year-old woman presented to us with nausea, headache, and vomiting. No abnormalities were detected on neurological examination, and her biochemical parameters were within normal range. Contrastenhanced magnetic resonance imagining revealed a parieto-occipital mass 63×33×40-mm in diameter with a cystic and solid component and peripheral vasogenic edema that had caused right lateral ventricle compression (Fig. 1). The mass was resected completely, and no residue was detected on postoperative MRI.;){kind=link}
Differential diagnosis of dural-origin fusiform and epitheloid tumors comprises hemangiopericytoma, fibrous meningioma, and synovial sarcoma. In the present case, on immunohistochemical examination, the tumor was found to be positive for vimentin, S100, NSE, transducer-like enhancer of split (TLE)-1, BCL-2, EMA, FactorXIIIa, and CD34 and negative for CD30, LCA, desmin, PR, STAT-6, CD99, pancytoceratine, GFAP, and HMB-45. Ki-67 proliferation index was 12%. Based on these findings, the tumor was classified as poorly differentiated dural synovial sarcoma (Fig. 2). Positron emission tomography computed tomography (PET CT) was performed for detecting metastasis; besides the primary lesion, no other lesion was detected. The patient was treated with adjuvant chemotherapy comprising ifosfamide, 2500 mg/m²; mesna, 2500 mg/ m²; and doxorubicin 60 mg/m² for 3 consecutive days every 21 days. Cranial radiotherapy has been planned for the patient after chemotherapy.
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Discussion
Synovial sarcomas comprise 5%-10% of soft tissue sarcomas.[2] The occurrence of head and neck synovial sarcomas is even less, and they comprise 3%-5% of total sarcomas. Slight female predominance is seen, with the woman to man ratio being 1,6:1.[3,4] These tumors are mostly observed in individuals aged 15-35 years; however, their occurrence may range from being present at birth until the age of 89 years.[2]Synovial sarcomas are not derived from synovium; they originate from primitive mesenchymal stem cells and can be seen in regions without synovium. [5] Synovial sarcomas are mostly seen on extremities; however, they may be distributed widely across the head and neck, mediastinum, abdomen, lung, pleura, kidney, and gastrointestinal tract.[6] These tumors have been reported to exist intracranially in the dura mater and base of the skull, indicating that they may be present anywhere in the body.[7]
Clinical presentation of meningothelial mesenchymal tumors includes their anatomic location and diameter. The affected patients mostly present with nausea, vomiting, headache, paresthesia, memory impairment, convulsions, disequilibrium, aphasia, and hearing loss. Neuroradiological examination has reportedly revealed meningeal-originated tumor and a range of dissemination.[8]
The appearance of these tumors is related to differentiation and resembles extracranial soft tissue sarcomas. Rapidly progressive tumors are poorly demarcated, fragile, hemorrhagic, necrotic, and cystic. [9] Histologically, synovial sarcomas are differentiated into four subtypes: monophasic, monophasic epithelial, biphasic, and poorly differentiated types. [10,11] The present case was classified as poorly differentiated synovial sarcoma because cystic, solid component and intratumoral hematoma were observed.
Based on the location and morphological features,
the tumor in the present case was histopathologically
different from meningioma, solitary fibrous
tumor, and others sarcomas.[12] In addition to 100%
immunoreactivity for EMA, 86%-90% nuclear positivity
PgR is observed in meningiomas.[13,14] In the
present case, contrary to EMA positivity, PgR was
negative. Solitary fibrous tumors may also be located
in central nervous system. They are negative for cytokeratin
and EMA, while diffuse positivity is observed
with CD34.[2] Although the present case was
positive for CD34 and negative for cytokeratin, positive
immunoreaction for EMA was inconsistent with
the solitary fibrous tumor. Approximately 10%-20% of synovial sarcomas have the same pattern as hemangiopericytomas.[1] Like peripheral nerve sheath
tumors, 30% of monophasic and poorly differentiated
synovial sarcomas show nuclear and cytoplasmic S-
100-positive immunoreaction.[15] The immune reaction
to EMA and cytokeratin is negative in malign
peripheral nerve sheath tumors; thus, these tests may
be used in differential diagnosis.[16] In the present
case, similar to malign peripheral nerve sheath tumors,
S-100 was immunoreactive, but unlikely EMA
was immunoreactive either. Recently, high expression
of TLE-1 has been observed in synovial sarcomas.
In the present case, TLE immunoreactivity was positive;
this feature is specific and sensitive for synovial
sarcomas.[17] Furthermore, in this case, Ki-67 proliferation
index was 12%. However, because synovial
sarcoma-specific chromosomal translocation (X; 18)
(p11; q11) was seen, diagnosis was made based on the
findings of histological and immunohistochemical
tests in the present case.[
Conclusion
In conclusion, primary meningeal synovial sarcomas have been seldom diagnosed, and case-based presentations are present. They can be differentiated from mesenchymal meningeal tumors on the basis of morphological and immunohistochemical features.Acknowledgements: The research was not financially supported by grants or any other kind of funding from any pharmaceutical company or other possible sources. All the authors had an active involvement in data collection and analysis, as well as writing, preparing and reviewing the manuscript.
Informed consent: Written informed consent was obtained from the patient for the publication of the case report and the accompanying images.
Peer-review: Externally peer-reviewed.
Conflict of Interest: The authors have no conflict of interests
to declare.
Financial Disclosure: The authors declared that this study
has received no financial support.
Authorship contributions: Concept - M.K.; Design -
H.Y.; Supervision - Z.U.; Materials - M.K.; Data collection &/or processing - N.A., F.T.; Analysis and/or interpretation
- N.A., M.A.K.; Literature search - N.A., O.K.; Writing -
N.A., O.K.; Critical review - A.I.
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