Multi-Disciplinary Treatment of a Rare Pelvic Cavity Ependymoma
- Affiliations
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- 1Department of Internal Medicine, Yonsei University College of Medicine, Seoul, Korea. oncosohn@yuhs.ac
- 2Department of Pathology, Yonsei University College of Medicine, Seoul, Korea.
- 3Department of Pathology, Catholic University College of Medicine, Seoul, Korea.
- KMID: 2158182
- DOI: http://doi.org/10.3349/ymj.2007.48.4.719
Abstract
- Ependymomas usually develop from neuroectodermal organs. Here, we present an ependymoma arising from the pelvic cavity. A 27-year-old Korean female was admitted to the hospital with a sensation of abdominal fullness. Imaging studies revealed a huge heterogeneous nodular mass in the pelvis and lower abdomen. Laparotomy showed that two large masses with multiple nodules were located between the uterus and rectum and uterus and bladder, respectively. Histologically, the tumor was characterized by compact columnar neoplastic cells divided by fibrovascular septae. The neoplastic cells formed true ependymal rosettes and perivascular pseudorosettes. Immunohistochemical staining showed a strong positive reaction for glial fibrillary acidic protein (GFAP) and vimentin and a partial positive reaction for S100 and EMA. The tumor was thus diagnosed as an ependymoma arising from the pelvic cavity. The patient was treated with a debulking operation and chemotherapy based upon the in vitro chemosensitivity test results. The patient was free of cancer for 4 years following surgery. This is a rare case of extraneural ependymoma for which an in vitro chemosensitivity test was critical in determining the multidisciplinary approach for treatment.
MeSH Terms
Figure
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Fig. 1 Two 20 × 20cm and 8 × 8cm-sized large masses with clear cut margins were located between the uterus and rectum and the uterus and bladder, respectively (A and B). Carcinomatosis and seeding metastasis on Rt. subhepatic space were also observed (A and B). On gross pathology, the cut surface of one of the masses shows a pale brown fish flesh solid and partly white pale brown friable appearance with several hemorrhagic foci (C).
Fig. 2 Tumor cells are arranged in true perivascular pseudorosettes (A) and ependymal rosettes (B). Tumor cells show positive immunoreactivity for GFAP (C). Ultrastructural examination revealed compact arrangement of the tumor cells interlacing with the cytoplasmic process and abundant intermediate filaments in the cytoplasmic process. The presence of cilia in the cyst and intracytoplasmic lumen and intercellular junctions; Original magnification (D): × 12,000, right upper: × 30,000.
Reference
-
1. Grody WW, Nieberg RK, Bhuta S. Ependymoma-like tumor of the mesovarium. Arch Pathol Lab Med. 1985. 109:291–293.2. Bell DA, Woodruff JM, Scully RE. Ependymoma of the broad ligament. A report of the two cases. Am J Surg Pathol. 1984. 8:203–209.3. Duggan MA, Hugh J, Nation JG, Robertson DI, Stuart GC. Ependymoma of the uterosacral ligament. Cancer. 1989. 64:2565–2571.
Article4. Hofman V, Isnard V, Chevallier A, Motamedi JP, Michiels JF, Hassoun J, et al. Pelvic ependymoma arising from the small bowel. Pathology. 2001. 33:26–29.
Article5. Dekmezian RH, Sneige N, Ordonez NG. Ovarian and omental ependymomas in peritoneal washings: cytologic and immunocytochemical features. Diagn Cytopathol. 1986. 2:62–68.
Article6. Crotty TB, Hooker RP, Swensen SJ, Scheithauer BW, Myers JL. Primary malignant ependymoma of the lung. Mayo Clin Proc. 1992. 67:373–378.
Article7. Wiendl H, Feiden W, Scherieble H, Renz T, Dichgans J, Weller M. March 2003: a 41-year-old female with a solitary lesion in the liver. Brain Pathol. 2003. 13:421–423.8. Kleinman GM, Young RH, Scully RE. Ependymoma of the ovary: report of three cases. Hum Pathol. 1984. 15:632–638.
Article9. Von Hoff DD, Kronmal R, Salmon SE, Turner J, Green JB, Bonorris JS, et al. A Southwest Oncology Group study on the use of a human tumor cloning assay for predicting response in patients with ovarian cancer. Cancer. 1991. 67:20–27.
Article10. Samson DJ, Seidenfeld J, Ziegler K, Aronson N. Chemotherapy sensitivity and resistance assays: a systematic review. J Clin Oncol. 2004. 22:3618–3630.
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