Small Blue Cell Research Articles

Abstract 2716: Overexpression of p16INK4a in Merkel cell carcinoma

Abstract Merkel cell polyomavirus (MCV) is a recently discovered human oncogenic virus. The majority of Merkel cell carcinomas (MCC) have been found to be infected with MCV. The MCV large T antigen (LTA) consists of an Rb binding motif that is functionally analogous to the E7 protein of high-risk human papillomavirus (HPV) types (eg. 16 and 18). It has been well documented that inactivation of Rb leads to overexpression of p16INK4a. Clinically, immunohistochemistry for p16INK4a has proven useful in the diagnosis of HPV driven epithelial malignancies including cervical as well as head and neck cancers. The present study explores the relationship between MCV infection and p16INK4a expression using an in vitro cell culture system and 10 clinical specimens of MCC that have been diagnosed at the San Diego VA Hospital over a 21 year period. First, IMR-90 cells were transfected with MCV LTA plasmids, which carry either wild-type or mutant Rb binding motif for immunofluorescence analysis. Only cells transfected with wild-type, but not mutant LTA, were associated with p16INK4a up-regulation. Furthermore, a strong positive correlation was established between MCV LTA and p16INK4a expression in formalin-fixed, paraffin-embedded MCC samples by immunohistochemical staining using p16INK4a and MCV LTA specific monoclonal antibodies, and real-time PCR to detect MCV with two pairs of primers. In conclusion, strong association between p16INK4a expression and MCC suggests that the MCV and HPV related carcinomas share some common oncogenic pathways. In addition, p16INK4a positivity can be a useful diagnostic tool in differentiating MCC from other small blue cell tumors. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 102nd Annual Meeting of the American Association for Cancer Research; 2011 Apr 2-6; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2011;71(8 Suppl):Abstract nr 2716. doi:10.1158/1538-7445.AM2011-2716

Spectrum of orbital and ocular adnexal lesions: An analysis of 389 cases diagnosed by fine needle aspiration cytology

The aim of the present study was to evaluate the scope and the limitations of fine needle aspiration cytology (FNAC) in orbital and ocular adnexal lesions. This study was a retrospective audit of 389 cases of orbital and ocular adnexal lesions subjected to FNAC over a period of 12 years (1998-2009). The cyto-smears were reviewed and the lesions were categorized under different diagnostic categories in adult and pediatric population. Three hundred and one adult patients (age ≥15 years) and 88 pediatric patients (age ≤14 years) constituted the study group. In the adult population, there were 23.3% cases of infectious and lymphoproliferative lesions and 12.6% of benign cysts. In the pediatric population, 18.2% cases had infectious and lymphoproliferative lesions and 8% had benign cysts. Various benign tumors (9.6% in adults) included pleomorphic adenoma, meningioma, and schwannoma. Benign vascular tumors predominated in the pediatric population. A majority of malignant tumors in adults were lymphoreticular malignancies (12.6%); non-Hodgkin's lymphoma being the most common followed by malignant epithelial tumors (10.3%). Nearly 3.6% cases of soft tissue/bone sarcomas and 6.3% of metastatic tumors were seen in adult population. However, most of the orbital tumors in the pediatric population were malignant small blue round cell tumors (33%). FNAC is a cost-effective technique with good diagnostic value in the assessment of ophthalmic lesions, especially when sampling and interpretation are performed by experienced personnel in the light of clinico-radiological information.

Extraosseous Ewing's sarcoma arising from the pterygomandibular space

Extraosseous Ewing’s sarcoma (EES) arising in head and neck is extremely rare. We report on a rare case of EES originating from the pterygomandibular space. A 15-year-old boy was seen with a rapidly growing mass in the right upper neck, difficulty in opening mouth, dysphagia, numbness in the right lower lip and buccal skin. Clinical and radiological examinations indicated that a soft tissue mass origi-nated from the pterygomandibular space with the submandibular space and mouth floor extension. Histological and immunohistochemical evaluations of the biopsy specimen revealed poorly differentiated small blue round cells with positive stains for CD99 and neuron-specific enolase. According to the clinical manifestation, CT and MRI findings, histological pattern and the results of the immunohistochemical studies, the final diagnosis was EES. Our patient was treated with chemotherapy and radiotherapy. The lesion recurred locally after 10 months and he died of multiple distant metastases 22 months later. Early and confident diagnosis coupled with combined surgical excision and modern chemotherapy/radiotherapy appears to be the most effective treatment plan.

In situ hybridisation: background and applications

<i>In situ</i> hybridisation (ISH) offers molecular diagnosis in a morphological context. Over the last 20 years the technique has moved from research tool to mainstream pathology test with the advent of chromogenic assays, an increasing variety of commercially available probes, and automated hybridisation platforms. The technique can be used to detect DNA or RNA depending on the hybridisation protocol, and can be applied at both light microscopy (LM) and electron microscopy (EM) levels. Troubleshooting problems requires a basic understanding of the technique including probe design and stringency. ISH offers the possibility of simultaneous detection of multiple molecular targets, and/or co-detection of gene and protein targets (via IHC), allowing phenotyping of a cell containing a molecular target, or co-analysis of a target gene and its expression. Current clinical applications include detection of virus (EBV, HPV), analysis of chromosomal translocations or losses (haematological malignancies, sarcomas, small blue cell tumours, gliomas), identification of gene amplification (HER2, EGFR), and tracking of host vs donor cells in sex-mismatched transplant patients (Y chromosome).

Nonmelanoma Skin Cancer

Nonmelanoma Skin Cancer

Report on Norrie’s cytology

Report on Norrie’s cytology

Diffuse Anterior Retinoblastoma without Retinal Involvement

To present a unique case of an 8.5-year-old child with unilateral, anterior, pseudouveitis. He was found to have unilateral, invasive, small blue cell tumor of the anterior segment that was diagnosed as diffuse infiltrating retinoblastoma despite lack of retinal involvement on fundus examination or histopathologic analysis. Interventional case report. One patient. The patient was treated with topical prednisolone acetate 1% and oral prednisone with no improvement in anterior chamber reaction. The patient underwent fine-needle aspiration biopsy (FNAB) of anterior chamber fluid, the results of which were consistent with a primitive neuroectodermal neoplasm, either retinoblastoma or medulloepithelioma. Retinoblastoma was favored strongly, and the patient underwent enucleation followed by chemotherapy with vincristine, carboplatin, and etoposide, and radiation to the eye socket of 4140 cGy total was performed. The patient is alive and tumor free with follow-up of 5 years. Microscopic examination demonstrated cells similar to those seen on the FNAB infiltrating the iris stroma, trabecular meshwork, Schlemm's canal, and the inner portion of sclera in the region of the angle. No calcifications were identified. Serial sections of the entire globe were performed to determine the origin of the tumor. No retinal involvement was identified, and tumor was not seen to arise from the ciliary epithelium. Immunohistochemistry demonstrated positive staining with synaptophysin and negative staining with leukocyte common antigen and CD34. This patient represents a case of diffuse anterior retinoblastoma with lack of obvious retinal involvement. Morphologic features typical of medulloepithelioma were not found on pathologic analysis. Although the patient lacked a retinal focus, he is alive at 5 years without evidence of recurrence of tumor.

Small blue round cell tumor of the interosseous membrane bearing a t(2;22)(q34;q12)/EWS-CREB1 translocation: a case report

BackgroundThe group of small blue round cell tumors encompasses a heterogeneous group of neoplasms characterized by primitive appearing round cells with few distinguishing histologic features.ResultsWe report the case of a small blue round cell tumor with an EWS gene rearrangement detected by fluorescent in situ hybridization (FISH) analysis that mimicked Ewing sarcoma, but with unusual histology and immunohistochemical features. Multi-color karyotyping identified the presence of a t(2;22)(q34;q12) that was initially expected to represent a variant EWSR1-FEV translocation. After an extensive workup, the lesion is considered to represent a clear cell sarcoma harboring an EWSR1-CREB1 fusion transcript.ConclusionsThis case appears to represent a rare variant of clear cell sarcoma arising in peripheral soft tissues with unusual histology and unique immunophenotype. In this circumstance, FISH for all EWSR1 translocation partners or RT- PCR for a spectrum of possible transcript variants is critically important for diagnosis, since cytogenetic analysis or clinical FISH assay using only commercial EWSR1 probes will be misleading.

Childhood rhabdomyosarcoma metastatic to bone marrow presenting with disseminated intravascular coagulation and acute tumour lysis syndrome: review of the literature apropos of two cases

The paper presents diagnostic and therapeutic difficulties in two adolescents with widespread rhabdomyosarcoma (RMS) presenting with severe haemorrhages resulting from disseminated intravascular coagulation (DIC) and with laboratory features of acute tumour lysis syndrome (ATLS). Other published cases of childhood RMS with DIC at admission have been listed and reviewed. It has been concluded that the clinical picture of a widespread RMS in children may resemble acute hematologic malignancy and pose a big diagnostic problem. That is why the presence of small blue round cells morphologically similar to lymphoblasts and/or myeloblasts in bone marrow (BM), lacking hematopoietic makers, should prompt the pathologist to consider possible diagnosis of RMS. Inclusion of desmin, MyoD1 and myogenin Myf4 to the immunohistochemical panel is obligatory in such cases. When the representative histopathological tumour specimens are difficult to obtain, the flow cytometric immunophenotyping of BM metastases could help the standard morphological/immunohistological diagnostic procedures and advance the diagnosis. Recently, the flow cytometric CD45− CD56+ immunophenotype together with Myf4 transcript has been assigned to RMS cells infiltrating BM. In children with disseminated RMS complicated with DIC rapid polychemotherapy aimed at diminishing the malignancy-triggered procoagulant activity should be initiated. However, in cases with concomitant ATLS the initial doses of chemotherapy should be reduced and the metabolic disorders and renal function monitored. The prognosis in children with RMS metastatic to BM with signs of DIC or ATLS at admission depends on the response to chemotherapy, however generally it is highly disappointing.

Reverse Transcriptase–Polymerase Chain Reaction as an Ancillary Molecular Technique in the Diagnosis of Small Blue Round Cell Tumors by Fine-Needle Aspiration Cytology

We evaluated the feasibility and usefulness of reverse transcriptase-polymerase chain reaction (RT-PCR) on fine-needle aspirates for categorization of small blue round cell tumors (SBRCTs). A total of 51 cases, including 25 Ewing sarcoma/peripheral primitive neuroectodermal tumors (PNETs), 11 rhabdomyosarcomas, 13 neuroblastomas, and 2 desmoplastic small round cell tumors (DSRCTs) were analyzed. The detection of the EWS-FLI1 (20/25) and EWS-ERG (4/25) fusion transcripts resolved 24 of 25 cases of Ewing sarcoma/PNET. The PAX3/7-FKHR fusion transcript was detected in 2 of 4 cases of alveolar rhabdomyosarcoma and the EWS-WT1 transcript in both cases of DSRCT. Tyrosine hydroxylase and 3,4-dihydroxyphenylalanine (dopa) decarboxylase transcripts were demonstrated in 10 of 13 cases of neuroblastoma. In comparison, immunocytochemical analysis resolved 19 (76%) of 25 Ewing sarcomas, 9 (82%) of 11 rhabdomyosarcomas, 6 (46%) of 13 neuroblastomas, and 1 (50%) of 2 DSRCTs. Overall, RT-PCR resolved 38 (86%) of 44 vs 35 (69%) of 51 cases by immunocytochemical analysis. RT-PCR is easily applied to fine-needle aspirates of SBRCT and greatly facilitates accurate tumor typing.

Primary cutaneous Ewing’s sarcoma/primitive neuroectodermal tumor manifesting numerous small and huge ulcerated masses: its complete remission by chemotherapy and magnetic resonance imaging findings

Extraskeletal Ewing's sarcoma (ES) and primitive neuroectodermal tumor (PNET) are widely regarded as clinically and histologically identical tumors which consist of small blue round cells. Extraskeletal ESs/PNETs usually occur in the deep soft tissues of the paraspinal region, chest wall, or lower extremities. However, superficially located cases, so-called cutaneous ESs/PNETs, are exceedingly rare, and the vast majority of the reported cases present as a single small mass. We present magnetic resonance imaging (MRI) findings and clinical course of a unique case of primary cutaneous ES/PNET presenting as numerous huge masses with severe ulceration on them.

Tumor desmoplásico de pequenas células redondas abdominal da infância: relato de caso

O tumor desmoplásico de pequenas células redondas (TDPCR) é uma neoplasia rara e altamente agressiva, que afeta predominantemente jovens do sexo masculino. Relata-se um caso de TDPCR em um paciente do sexo masculino, de 11 anos, com acometimento intra-abdominal marcado por volumosa massa retroperitoneal em hipocôndrio esquerdo. O estudo histológico da massa revelou presença de blocos de pequenas células tumorais redondas e azuis, envoltas por estroma desmoplásico; a análise imuno-histoquímica evidenciou positividade para desmina, WT-1 e citoceratinas. Após o diagnóstico, o paciente foi submetido a tratamento quimiorradioterápico, tendo evoluído a óbito durante o 24º mês de acompanhamento.

Molecular pathology of sarcomas: concepts and clinical implications

The molecular genetic changes that have been described in sarcomas over the past era have aided our understanding of their pathogenesis. The majority of sarcomas carry nonspecific genetic changes within a background of a complex karyotype. These constitute the challenges in sarcoma research for unraveling a putative multistep genetic model, such as for chondrosarcoma, and finding targets for therapeutic strategies. Approximately 15–20% of mesenchymal tumors carry a specific translocation within a relatively simple karyotype. The resulting fusion products act either as transcription factors upregulating genes responsible for tumor growth, as for instance in Ewing sarcoma, or translocate a highly active promoter in front of an oncogene driving tumor formation, as for instance in aneurysmal bone cyst. In addition, a small subset of mesenchymal tumors have specific somatic mutations driving oncogenesis. The specific genetic changes unraveled so far had great impact on the classification of bone and soft tissue tumors. In addition, these changes can assist the pathologist in the differential diagnosis of some of these entities, especially within the groups of small blue round cell tumors and spindle cell tumors, if performed in specialized centers. While a putative association between certain fusion products and outcome is still under debate, the role of predicting response of targeted therapy has been well established for KIT and PDGFRA mutations in gastrointestinal stromal tumors.

Primary cutaneous Ewing sarcoma/primitive neuroectodermal tumour: a clinicopathological analysis of seven cases highlighting diagnostic pitfalls and the role of FISH testing in diagnosis

Aims:To perform a clinicopathological analysis of a series of primary cutaneous Ewing sarcomas/primitive neuroectodermal tumours (ES/PNET) to highlight the pathological features, discuss the differential diagnosis, emphasise the role of molecular...

Small blue cells mimicking small cell carcinoma in spermatocele and hydrocele specimens: a report of 5 cases

We identified 5 cases of hydrocele and spermatocele resections containing detached small cellular "blue" clusters, raising questions of small cell carcinoma by contributors to our consult service. Patients were 37, 39, 52, 67, and 70 years old. None of the 4 patients with follow-up developed small cell carcinoma. On routine stained sections, there were multiple clusters of detached hypercellular cells with focal streaming, high nuclear-to-cytoplasmic ratios, and hyperchromatic nuclei without prominent nuclei. There were no mitotic figures, apoptotic bodies, or necrosis. In 4 of 5 cases, there was sufficient tissue to perform immunohistochemistry along with 10 cases each of normal rete testis and epididymis. CD56 was positive in 4 of 4 cases of the "blue cells" and in 9 of 10 of normal rete testis; yet, it was positive in only 2 of 10 normal epididymis. Synaptophysin and chromogranin were negative in all cases of "blue cells." PAX2 was negative in all cases of "blue cells" similar to the 1 of 9 positive staining in rete testis and in contrast to the positivity seen in 9 of 9 cases of normal epididymis. Ki-67 was negative or showed only rare positive cells in all of the cases of the "blue cells." Clusters of blue cells suggestive of sloughed rete testis cells can mimic small cell carcinoma in hydrocele and spermatocele specimens based on their low power appearance and positive CD56 staining. Closer examination of the cells' bland morphology, low expression of Ki-67, and lack of chromogranin and synaptophysin, along with recognition of this entity, can prevent a misdiagnosis of malignancy.

MYCN Promotes the Expansion of Phox2B-Positive Neuronal Progenitors to Drive Neuroblastoma Development

Amplification of the oncogene MYCN is a tumorigenic event in the development of a subset of neuroblastomas that commonly consist of undifferentiated or poorly differentiated neuroblasts with unfavorable clinical outcome. The cellular origin of these neuroblasts is unknown. Additionally, the cellular functions and target cells of MYCN in neuroblastoma development remain undefined. Here we examine the cell types that drive neuroblastoma development in TH-MYCN transgenic mice, an animal model of the human disease. Neuroblastoma development in these mice begins with hyperplastic lesions in early postnatal sympathetic ganglia. We show that both hyperplasia and primary tumors are composed predominantly of highly proliferative Phox2B(+) neuronal progenitors. MYCN induces the expansion of these progenitors by both promoting their proliferation and preventing their differentiation. We further identify a minor population of undifferentiated nestin(+) cells in both hyperplastic lesions and primary tumors that may serve as precursors of Phox2B(+) neuronal progenitors. These findings establish the identity of neuroblasts that characterize the tumor phenotype and suggest a cellular pathway by which MYCN can promote neuroblastoma development.

Unusual histological variant of Ewing's sarcoma of mandible

Ewing family of tumors (EFTs) comprise highly malignant, nearly undifferentiated neoplasms including Ewing's sarcoma (ES), primitive neuroectodermal tumor (PNET) and a spectrum of other unusual variants. In general, EFTs are included among small blue cell tumors. Establishing histological diagnosis can be difficult; CD99 and FLI1 immunohistochemical staining has improved diagnosis, but these markers are not specific for EFTs. The diagnosis of EFTs is confirmed by molecular diagnostic testing showing the presence of established rearrangements of the EWS gene. The use of this molecular signature in EFTs revealed rare variants in the histomorphologic spectrum of these tumors. The authors report an unusual variant of EFT in the mandible of a 17-year-old patient, which was confirmed by translocation rearrangement in EWR1 gene at 22q12 by fluorescence in situ hybridization. The unusual histologic features, with prominent spindling of tumor cells and deviation from the classic features of Ewing's sarcoma posed a diagnostic challenge for the medical centers involved in the diagnosis and treatment of this patient. This highlights the importance of the genetic study of undifferentiated sarcomas to identify rare morphologic variants of ES, in view of the chemosensitivity of EFTs and how this affects patient management.

Marginal zone variant of mantle cell lymphoma: CD5‐negative cyclin D1‐positive variant posing a diagnostic dilemma

Described herein is an unusual case of mantle cell lymphoma (MCL) histologically mimicking marginal zone lymphoma (MZL). An 83-year-old man presented with multiple adenopathies and a hilar mass encroaching on the right lung. A transbronchial biopsy showed small blue cells suspicious for small cell carcinoma. On further analysis the cells were predominantly small cleaved and CD20 positive, suggesting follicular lymphoma, grade 2. An axillary lymph node biopsy showed germinal centers surrounded by monocytoid B cells. Flow cytometry was negative for CD5 and CD23 and the diagnosis of MZL was considered. Because of the aggressive clinical behavior, including extensive necrosis on imaging studies, immunohistochemistry for cyclin D-1 was performed and was positive. Bone marrow was extensively involved and it showed t(11;14), in addition to other complex cytogenetic abnormalities. Differentiating MCL from MZL has prognostic and therapeutic implications, particularly when considering the potential role of targeted therapy and cell cycle modulators.

Cytologic features of metanephric adenoma of the kidney

To the Editor, Metanephric adenoma (MA) is a rare, benign renal neoplasm that consists of a proliferation of small epithelial cells, which form acinar, tubular, papillary and glomeruloid structures. The first large series describing the tumor were reported in 1995.[1,2] In many cases, the benign behavior, well-defined limits and small size of the tumors, make them candidates of conservative surgical management. That only a few cytological descriptions are available[3–9] is a reflection on the rarity of the tumor [Table 1]. We describe a case evaluated intraoperatively and in which cytology allowed a precise recognition. Table 1 Reported cytologic cases of metanephric adenoma A 56-year-old woman, presented with a 3 cm renal tumor. Tumorectomy with intraoperative evaluation was performed. The renal mass was well defined, solid and had a grey to white color. Air-dried and alcohol-fixed cytologic samples were obtained after scraping the tumor surface. The smears showed a monomorphous cellular population in a clean background. Most cells presented as naked nuclei, with oval to round morphology. They distributed as clusters and single cells. A minimum amount of deeply stained cytoplasm was evident only in a few aggregates. Many clusters showed an evident tubular arrangement [Figure 1a]. Small, three-dimensional, tightly packed morules were present with a smooth outer surface [Figure 1b]. Ribbons, glandular [Figure 2a] and pseudo-papillary structures were also present. The nuclei were slightly oval and monomorphic [Figure 2b]. Chromatin was regularly distributed and the nuclear membrane was smooth; no nucleolus was seen. The smears showed no atypia, mitotic figures, necrosis or crushing chromatin artefact. Histology revealed an un-encapsulated neoplasm, with a predominant acinar and tubular growth, with pseudo-papillary and solid areas and inconspicuous stroma [Figures. ​[Figures.3a3a and ​andb].b]. Glomeruloid structures were also seen. The cells were small, oval, and uniform with scanty cytoplasm. No nuclear atypia, mitotic figures or apoptosis were seen. Tumoral stroma was inconspicuous, with no necrosis. Immunohistochemistry revealed expression of vimentin, CD57 and WT1. There was no expression of cytokeratin 7 or epithelial membrane antigen. Figure 1 Single cells and clusters with tubular configuration (A) and morules (B) (Papanicolaou). Figure 2 Glandular structures were also evident. Chromatin is regularly distributed and there are no relevant nucleoli (A, Papanicolaou). Cells have inconspicuous cytoplasm and predominantly oval, monomorphic nuclei (B, Diff Quik). Figure 3 Histologically, the limit with normal parenchyma is clear cut, with no capsule (A). Cells are small, with a variable growth pattern in which tubular and pseudo papillary structures predominate (B) (Hematoxylin and eosin). In our opinion, the histopathologic features of MA are well reflected on cytology, allowing its recognition. The present case, as well as previously published ones, reveal a similar cytologic pattern that can be summarized as a small blue cell, epithelial tumor, with oval cells and no atypia. It shows different epithelial structures with tubules, glands, pseudopapillae and morules. In our case, the presence of numerous single cells is probably related to the scraping of the tumor, since fine needle aspirate samples show a marked predominance of clusters.[2,3,5–9] This cytologic image differs considerably from that of other adult renal tumors. The extensive use of image studies has resulted in the detection of many small renal masses. Therapeutic decisions partially depend on the histologic nature of the tumor, but obtaining this information preoperatively may be difficult. Fine needle aspiration and intraoperative studies are often requested for aiding in decision making. The present case illustrates the utility of cytologic evaluation of intraoperative tissue samples. Frozen sections raised the possibility of papillary renal cell carcinoma. This is an obvious consideration in the differential diagnosis of MA, since both neoplasms may share histologic features.[1,2] In our case, papillary renal cell carcinoma was not considered after cytologic evaluation. Instead, the small cell size and epithelial nature raised the possibilities of nephroblastoma and MA. Cellular monomorphism, absence of stromal component, extensive epithelial differentiation, oval morphology, absence of necrosis and apoptosis, as well as the patient's age, favored the possibility of MA. Epithelial-predominant nephroblastoma may resemble MA more closely. In fact, there are also immunohistochemical similarities, and, for some authors, MA represents a hyperdifferentiated, mature form of nephroblastoma.[10] Papillary carcinoma and MA may share architectural features. Tubular, pseudo-papillary structures and spherules of tumoral cells can be present in both neoplasms.[1] However, the neoplastic cells differ. Those from papillary carcinoma are larger and show moderate amounts of cytoplasms, sometimes vacuolated or containing hemosiderin. The macrophagic cell population so frequently present in papillary carcinoma is rare in MA. In conclusion, cytology, either as fine needle aspirates or during intraoperative procedures, may be of great value in the recognition of MA.

Desmoplastic small round cell tumor of the central nervous system: report of two cases and review of the literature

Desmoplastic small round cell tumor (DSRCT) is a malignant tumor often involving the abdominal and/or pelvic peritoneum. Only one fully documented example has arisen in the central nervous system (CNS). Herein, we describe two additional examples, fulfilling the morphologic, immunohistochemical, and molecular criteria (EWS/WT1 translocation) of DSRCT. Both arose in the cerebellopontine angle (CPA) and underwent spinal dissemination. Patient 1, a 37-year-old male, underwent a subtotal resection, and 2 years later died of recurrent disease with spinal dissemination. Patient 2, a 39-year-old man, presented with cerebellar and CPA lesions as well as spinal leptomeningeal deposits. After 27 months of adjuvant therapy, he is alive with progressive disease. In conclusion, CNS DSRCT follows a similar aggressive course as do peritoneal examples. Although rare, DSRCT warrants consideration in the differential diagnosis of "malignant small blue cell tumors" of the CNS.