Peripheral Primitive Neuroectodermal Tumor- Imaging Appearance

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1 ISPUB.COM The Internet Journal of Radiology Volume 9 Number 1 Peripheral Primitive Neuroectodermal Tumor- Imaging Appearance S Agarwal, S Magu, S Kumar Citation S Agarwal, S Magu, S Kumar.. The Internet Journal of Radiology Volume 9 Number 1. Abstract Peripheral primitive neuroectodermal tumors (PPNET) are rare but highly aggressive tumor of the peripheral non-central nervous system tissue. Thoracopulmonary region is the most common site, however they have been described in other sites as well. We present imaging appearance of three such tumors located in the chest, abdomen and mandible. INTRODUCTION Peripheral primitive neuroectodermal tumor (PPNET) is uncommon, and the overall incidence is 1% of all sarcomas. 1 These typically arise outside the central and sympathetic nervous system. The most common locations of PPNETs have been the thoraco-pulmonary region, the retroperitoneal paravertebral soft tissues, the soft tissues of the head and neck, and the intraabdominal and intrapelvic soft tissues and extremities. 2 The diagnosis is based on any hint of neural differentiation at light or electron microscopic level. The rarity of this tumor resulted from diagnosing the most of the PNETs as Ewing's Sarcoma in the past. 3 mass lesion isointense to muscle on T1-weighted images (Fig 1c) and heterogeneously hyperintense on T2-weighted images (Fig 1d).There were areas suggestive of hemorrhage within the mass lesion. T2-weighted images also revealed areas suggestive of necrosis. There was associated right sided pleural effusion. Mediastinal structures were displaced with no obvious evidence of infiltration. Biopsy revealed small round cell tumor consistent with primitive neuroectodermal tumor. Figure 1 Figure 1a: Radiograph chest postero-anterior view revealing right sided pleural effusion with raised right hemidiaphragm CASE REPORT CASE No. 1: A 20-year old male patient was admitted to the hospital after a two-month history of cough and a 6 kg weight loss. The patient's initial X-Ray film showed a small pleural effusion. He was treated for pneumonia. Two weeks later a repeat chest X-Ray film revealed a much larger right pleural effusion and the right hemidiaphragm was raised. (Fig 1a) Thoracocentesis revealed an exudative effusion with 100 percent lymphocytes. This effusion recurred in 48 hours. A pleural biopsy was subsequently performed which revealed chronic inflammation. CT scan was performed at this stage which revealed a large, well defined, poorly enhancing mass lesion occupying the left hemithorax inferiorly measuring approximately 12 x 14 cm. There was associated minimal pleural effusion. There was no calcification within the mass. Also no definite areas of necrosis could be demonstrated within the mass lesion. Adjacent bony structures were normal with no evidence of erosion. (Fig 1b) MRI revealed a similarly well-defined 1 of 6

2 Figure 2 Figure 4 Figure 1b: Sagittal reconstruction of CT images revealing a well-defined heterogeneously enhancing mass lesion involving left hemithorax inferiorly measuring approximately 12 x 14 cm.. In addition minimal pleural effusion is seen. There was no calcification within the mass. Also no definite areas of necrosis could be demonstrated within the mass lesion. Adjacent bony structures were normal with no evidence of erosion Figure 1d: Axial T2-weighted images of the same patient revealing heterogeneously hyperintense on T2-weighted images with areas suggestive of necrosis. Figure 3 Figure 1c: Axial T1-weighted image revealing a welldefined mass lesion isointense to muscle on T1-weighted images. There are hyperintense foci within the mass lesion suggestive of hemorrhage.there was associated right sided pleural effusion. Mediastinal structures are displaced with no obvious evidence of infiltration. 2 of 6 CASE No. 2: An 11 year old female child presented history of painless progressively enlarging mass lesion of approximately 2 months duration. On examination the mass was huge, firm, non tender and fixed originating from mandibular symphysis.the overlying buccal mucosa and neck were normal. CT scan revealed a large 10 x 12 cm mass lesion destroying the body of mandible on left side and invading the roots of the lower teeth. (Fig 2) Incisional biopsy revealed a small round cell tumor consistent with PNET. Figure 5 Figure 2: Reconstructed Panoramic view of CT scan images revealing a large 10 x 12 cm mass lesion destroying the body of mandible on left side and invading the roots of the lower teeth.

3 CASE No. 3: A 16 year old female patient who presented with vague abdominal pain of 1-2 months duration. On Xray examination of the abdomen in the supine position there was a large soft tissue density mass lesion overlapping the left iliac bone obscuring the outline of left psoas muscle inferiorly. Ultrasound of the abdomen was performed and it revealed a large hypoechoic left paravertebral mass. On Computed Tomogram (CT) it was seen as a large heterogeneously enhancing hypodense mass measuring 7x 8 cm, in left paravertebral region displacing the psoas anteriorly and partially infiltrating it. (Fig3a) While on Magnetic Resonance Imaging (MRI) it revealed hypointensity on T1-weighted images (Fig 3b) and hyperintensity on T2-weighted images. (Fig 3c). Left psoas was displaced anteriorly with no evidence of infiltration. No evidence of calcification was noted and there was no erosion of adjacent bony structures. FNAC was performed which revealed scattered nests of small tumor cells with round to oval nuclei. The nuclear-cytoplasmic ratio was high, with occasional mitotic figures. There were focal areas of necrosis without rosette formation. The PAS reaction was negative. Figure 6 Figure 7 Figure 3b: Axial T1-weighted image of the same patient revealing hypointensity on T1-weighted images displacing the Psoas anteriorly. No intraspinal extension was seen. Figure 8 Figure 3c: Axial T2-weighted image revealing that the tumor is hyperintense on T2-weighted images Figure 3a: Axial CT scan image below the level of aortic bifurcation reveals a large heterogeneously enhancing hypodense mass measuring 7x 8 cm, in left paravertebral region displacing the psoas anteriorly and partially infiltrating it. No evidence of calcification was seen within the lesion. Adjacent vertebra is normal. DISCUSSION PNETs were first reported by Stout in Initially they were believed to arise from major nerves. Later reports described these tumours in other anatomic locations as well. Today, the tumor is considered to be a neoplasm of non neural soft tissues that primarily affect the children and adolescents without an apparent gender predilection. 4 These belong to the family of small round cell blue tumors 3 of 6

4 commonly found in the pediatric population. These include neuroblastoma, malignant lymphoma, rhabdomyosarcoma, Ewing's sarcoma, Wilms' tumor and desmoplastic small round cell tumors in addition to PNETs. 5 Central and peripheral primitive neuroectodermal tumors (PNETs) exhibit characteristic immunophenotypical and genetic features that distinguish them from other small round cell tumors. 6 Peripheral PNETs typically express high amounts of the MIC2 antigen (CD99) 7 and exhibit highly characteristic chromosomal translocation between chromosome 11 and They possess neuronal features with neurosecretory granules on electron microscopy and immunohistochemical characteristics, such as positive staining with neuron specific enolase, which make them a distinct pathologic entity and differentiated them from other round cell tumors such as Ewing's sarcoma and neuroblastoma This tumor can occur at any age, although the peak age incidence is adolescence and young adulthood. There is no sex predilection 1213 In their series of 33 patients Dick etal 14 found the age range to be 0-16 years. Various reports have described these tumors as large masses with areas of necrosis or hemorrhage, reflecting the aggressive nature of these tumors Dick et al 14 found that the tumors were typically of soft tissue density on CT with larger tumors (>5 cm) masses tending to be more heterogenous in character. On MRI they were of slightly higher signal than muscles on T1-weighted sequence and all masses were heterogenous on T2W sequences. Calcification was uncommom and generally sparse. These tend to displace adjacent soft tissues structures rather than invade or encase them. These rarely cross the midline. Local or bony invasion at diagnosis was seen. While Kim MS et al 12 found these tumors to be large and aggressive with non-specific imaging appearance. Majority showed heterogenous enhancement with areas of necrosis and hemorrhagic foci. Few of these patients revealed vascular involvement, invasion of adjacent organs and intratumoral cyst and septations. Foci of calcifications were seen in 1 of 10 of their cases. Metastasis was seen to lungs, supraclavicular lymph nodes, mediastinal lymphnodes and pleural fluid in 3 of their series. However, metastasis was seen to lung, pleura, brain, bone, lymphnodes, liver, subcutaneous tissues, kidney and peritoneum in the series reported by Dick et al. 14 Askin's tumor is a relatively rare, highly aggressive neoplasm of the thorax which typically occurs in young 4 of 6 women, with median survival of eight months. 19 The incidence of peripheral PNET in the abdomen and pelvis, including the retroperitoneum, is about 14% of all peripheral PNETs. 2 Peripheral PNETs of the retroperitoneum have been described in a few publications; it is sporadically reported in the kidney, adrenal gland, and pelvis Although head and neck region is a rare site of origin for these malignant neoplasms, they have been reported in the skull, orbit, masseter muscle, and maxilla. To the best of our knowledge only 05 other cases of mandibular PNET have been described in the literature so far. Extraosseous Ewing's sarcoma (EOES) is an important differential diagnosis of PPNET. The distinction between PPNET and extraosseous Ewing's sarcoma (EOES) is important because disease free survival is poorer for patients with PPNET than for those with EOES. Both tumors occur most commonly in truncal & paravertebral soft tissues (50% to 60% of cases) and in extremities (25% of cases), although PPNET occurs less commonly in extremities than does EOES, and patients with EOES are generally younger. 20 CONCLUSION We present our experience with peripheral PNETs over a period of 05 years. These are rare but highly aggressive tumors which do not have any typical imaging features. Their diagnosis depends on histopathology, immunohistochemistry and electron microscopy. Early recognition is important for proper treatment of these tumors. CORRESPONDENCE TO Dr. Shalini Agarwal C/O Dr. Sarita Magu 22/8 FM, Medical Campus Rohtak. Haryana India. Tele: Mobile: agar_shalini@yahoo.com nkmagu@rediffmail.com References 1. Maccioni F, Della Rocca C, Salvi PF, et al. Malignant peripheral neuroectodermal tumor (MPNET) of the kidney. Abdom imaging 2000;25: Jurgens H, Bier V, Harms D, et al. Malignant peripheral neuroectodermal tumors: a retrospective analysis of 42 patients. Cancer 1988;61: Ozer E, Kanlikama M, Karakurum G, et al. Primitive neuroectodermal tumor of the mandible. Int J Pediatr Otorhininolaryngol 2002;65: Alrawi SJ, Tan D, Sullivan M, et al. Peripheral Primitive neuroectodermal Tumor of the Mandible with Cytogenetic and Molecular Biology Aberrations. J Oral Maxillofac Surg. 2005;63: Bellah R, Suzuki-Bardalo L, Brecher E, et al. Desmoplastic Small Round Cell Tumor in the abdomen and Pelvis: Report of CT Findings in 11 affected children and

5 young adults. Am J Radiol 2005;184: Schmidt D. Malignant peripheral neuroectodermal tumor. Curr Top Pathol 1995;89: Ambros IM, Ambros PF, Strehl S, et al. MIC2 is a specific marker for Ewing's sarcoma and peripheral neuroectodermal tumors: evidence for a common histogenesis of Ewing's sarcoma and peripheral primitive neurroectodermal tumors from MIC2 expression and specific chromosome aberration. Cancer 1991;67: Whang-Peng J, Triche TJ, Knutsen T, et al. Chromosome translocation in peripheral neuroepithelia. N Engl J Med 1984; 311: Dedeurwaerdere F, Giannini C, Sciot R, et al. Primary peripheral PNET/ Ewing's sarcoma of the dura: a clinicopathologic entity distinct from central PNET. Mod Pathol 2002;15: Askin FB, Rosai J, Sibley RK, et al. Malignant thoracopulmonary egion in childhood: a distinctive clinicopathologic entity of uncertain histogenesis. Cancer 1979;43: Winer- Muran HT, Kauffman WM, Gronemeyer SA, et al. Primitive neuroectodermal tumor of the chest wall (Askins tumors): CT and MRI findings. Am J Radiol. 1993;161: Kim MS, Kim B, Park CS, et al. Radiologic findings of Peripheral Primitive Neuroectodermal Tumor arising in the retroperitoneum. Am J Radiol 2006;186: of Fletcher JA, Kozakewich HP, Hoffer FA, et al. Diagnostic relevance of clonal cytogenetic aberrations in malignant soft tissue tumors. N Engl J Med 1991;324: Dick EA, Hugh KML, Kimber C, et al. Imaging of noncentral nerous System primitive Neuroectodermal Tumors: Diagnostic features and correlation with outcome. Clin Radiol 2001; 56: Ibarburen C, Haberman JJ, Zerhouni EA. Peripheral primitive neuroectodermal tumors: CT and MRI evaluation. Eur J Radiol 1996;21: Taieb S, Cabaret V, Bonodeau F, et al. MRI of primitive neuroectodermal tumor of the uterus. J Comput Assist Tomogr 1998;22: Parlorio E, Arrazola J, Pedrosa I, et al. Primitive neuroectodermal tumor of the kidney. Am J Radiol 1998;171: Pirani JF, Woolums CS, Dishop MK, et al. Primitive neuroectodermal tumor of the adrenal gland. J Urol 2000;163: Askins FB, Rosai J, Sibley RK, et al. Malignant small cell tumor of the thoracopulmonary region in childhood. Cancer 1979;43: Meyer JS, Fletcher BD. Soft tissue neoplasms. In: Slovis TL Caffey's Pediatric Diagnostic Imaging. 11th ed. Mosby USA 2008; 2514.

6 Author Information Shalini Agarwal, MD Department of Radiodiagnosis and Pathology, Pt. B.D. Sharma, PGIMS Sarita Magu, MD Department of Radiodiagnosis and Pathology, Pt. B.D. Sharma, PGIMS Sanjay Kumar, MD Department of Radiodiagnosis and Pathology, Pt. B.D. Sharma, PGIMS 6 of 6

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