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2009 ENORMOUS MIXED GERM CELL TUMOR OF THE TESTIS WITH FOUR DIFFERENT TYPES OF TUMORS: TERATOMA, SEMINOMA, EMBRYONAL CANCER AND YOLK SAC TUMOR M. Tzvetkov*, G. Venkov*, A. Vlahova**, T. Dikov** *Clinic of Urology, ** Department of Pathology, Medical University, Sofia Keywords: testicular cancer, teratoma testis, yolk sac tumоr, embryonal carcinoma, seminoma Address for correspondence: G. Venkov, Medical University, Clinic of Urology, 1, St. Georgi Sofiiski Street, 1431 Sofia, Bulgaria, Tel.: +359 877626588, e-mail: [email protected] Abstract: Objective: We report a case of enormous mixed germ cell tumor of the testis with four different types of tumors: teratoma, seminoma, embryonal cancer and yolk sac tumor with a clearly defined histology pattern. Materials and methods: A rare case of a 15-year-old boy with giant tumor of the left testis is presented. At the time of presentation the tumor measured 18x10x9cm. The tumor markers were increased, serum alpha-fetoprotein was over 350.00 ng/ml and human chorionic gonadotropin (beta-HCG) in serum was 125.96mlU/ml. The patient was treated with left inguinal orchiectomy. The tumor was histologically and immunohistochemically verified. Histologically, four different types of tumors were found: teratoma, seminoma, embryonal cancer and yolk sac tumor. The treatment was continuеd with chemotherapy courses. Other cases from world literature are reviewed. Case report We report a rare case of a 15-year-old boy with complaints of swelling and pain in the left testicle detected on self examination. The symptoms had begun two years before and had gradually increased. For this period of time the swelling of the testicle had enlarged and the organ had reached the size of a melon. For unknown reasons, probably religious, the boy hadn’t reached for medical help. The general condition of the boy was good. No pathological finding was found in the lungs and other organs. Local status: the examination detected a giant growth of the left testis sized 18x10x9cm. The skin of the testis was blush, at places livid. Venous blood vessels were wide and could be seen through the 36 skin. When palpated, the consistence of the testicle was hard elastic. Fig.1 The surface groin lymphatic nodes were not palpably enlarged. Laboratory tests were in normal values. The tumor markers were highly elevated. His alphafetoprotein (AFP) in serum was over 350.00ng/ml and human chorionic gonadotropin (beta-HCG) in serum was 125.96mlU/ml. The computer tomography (CT) of scrotum and pelvis showed an enormous tumor mass which originated from the left testicle. The tumor was with infiltrate growth and heterogeneous structure and calcificates. Fig.2 2009 Enormous Mixed Germ Cell Tumor of the Testis Fig.1 Tumor of the testicle – outside look of the formation By moving right arteria illiaca comunis enlarged lymphatic nodes were found in the pelvis. Fig.3 Fig.2 Computer tomography of the scrotal tumor. CT of the chest showed no sign of metastatic disease. Left inguinal orchiectomy was performed. During the operation liquid tumor materials leaked from the lower pole of the testis. At this place the skin of the scrotum was very thin and the tumor extended through tunica albuginea involving tunica vaginalis. The tumor had invaded the spermatic cord. Fig.4 Fig.3 CT scan of pelvis. Enlarged lymphatic nodes. Morphological research proved there were four different types of tumor cells. Fig.4 Extraction of the tumor from scrotum. Pathology report: Macroscopical outlook: A testis filled with tumor formation with versicoloured cut surface. Gross examination revealed an enlarged testis measuring 18х10х9cm due to extensive involvement by tumor with variegated cut surface: confluent greyish– white, yellowish-brown and hemorrhagic zones, 37 2009 Enormous Mixed Germ Cell Tumor of the Testis variably sized cysts, necrotic zones, calcifications, no detectable engagement of the coverings. Fig.5 Fig.6 Histological look of the first component immature teratoma Fig.5 Macroscopical outlook and tumor formation Histological finding of a mixed germ-cells tumor. Histology slides disclose diffent types of tumour tissue, determining the diagnosis mixed germ cell tumor. The largest area is occupied by i m m ature teratoma, composed of immature tissue and organoid components derived from all three germinal layers. Endo- and ecto-dermal structures are abundantly represented: hair follicules, keratinous cysts, epithelial-like glandular formations, islands of primitive neuroepithelium; all these are unproportionally admixed with immature-appearing mesenchyme and cartilage of mesodermal origin. Fig.6 Roughly quantified, second in size to the teratoma, is a tumor tissue composed of monomorphic cells with abundant clear cytoplsms and centrally placed nuclei; nesting pattern is discernible by tiny fibrous, lymphocyte-rich, septae. Part of these nests contain single moderately pleomorphic, multinucleated tumor cells, and the immunohistochemistry (IHC) assay verified their syncytiotrophoblastic origin (hCGT; code N1534, Dako). The finding is consistent with seminoma with syncytiothrophoblast cells. Fig.7 The histology picture is further varied by the presence of yolk sac tumor - relatively minor areas with papillary-reticular and microcystic appearance; 38 with interspersed single, ill-formed, pathognomic Schiller-Duvall bodies. Fig.8 Fig.7 Histology of the second component seminoma with syncytiothrophoblast cells Totaling less than 5% of the whole tumor tissue is the embryonal carcinoma – solid and glandular areas are noted composed of highly pleomorphic cells, exhibiting vesicular nuclei with prominent nucleoli; necrotic parts and calcium depositions are encountered. Fig.9 2009 Enormous Mixed Germ Cell Tumor of the Testis The patient was diagnosed with Stage IIA pT3N1M0S1 mixed-germ cell tumor of the left testis. The treatment was continued with primary chemotherapy courses. Retroperitoneal lymph node dissection was not performed. A new staging was planned after primary chemotherapy. Fig.8 Histology of the third component – yolk sac tumor Post-operative period went without complications and the wound healed completely. To stage correctly the disease, a second examination was performed with spiral computer tomography (SCT). Two paraaortal enlarged lymphatic nodes were found under the left renal vena. Fig.10 In the pelvis two more enlarged lymphatic nodes were found over the inguinal ligament, one on each side. Fig.11 Fig.9 Histology of the forth component - embryonal carcinoma Fig.10 SCT scan shows two enlarged paraaortal lymphatic nodes in the left side under left vena renalis. Дискус ия Fig.11 SCT scan enlarged lymphatic nodes in pelvis 39 2009 Enormous Mixed Germ Cell Tumor of the Testis Discussion Approximately 95% of all testicular neoplasms are of germ cell origin. For unclear reasons, there has been a world-wide increase in the incidence of these tumors1. Testicular germ cell tumors are the most common solid malignancies in men between the 20 and 45 years of age2. Testicular neoplasms account for 1-2% of all malignancies in male population3. According to regional cancer registries in Europe, about 90% of the patients are with low-stage disease (TNM stages I-IIB)4. Most of the patients with testis cancer (61-78%) have clinical stage I disease confined to the testis with normalized markers after orchiectomy5,6. More than half of the germ cell tumors are a mixture of two or more of the basic germ cell tumor types, with the exception of spermatocytic seminoma. The mixed types that contain seminoma occur at a later age compared to those without seminomatous components. Histologically, 59% of mixed germ cell tumors contain seminoma, 41% contain yolk sac tumor, and 47% contain embryonal carcinoma and teratoma. Syncytiotrophoblastic cells are present in 42%7. The most well documented risk factor for the development of germ cell tumors is cryptorchidism. The most consistent chromosomal abnormality is an isochromosome of the short arm of chromosome 12, i(12p), which is present in 56% of seminomas and in 83% of nonseminomatous tumors8,9. The most common mixed germ cell tumor is the combination of teratoma, embryonal carcinoma, yolk sac tumor, and syncytiotrophoblastic cells with or without seminoma10-12. The strongest associations of histological subtypes in mixed germ cell tumors are seen between yolk sac tumor and teratoma13. Patients with germ cell tumor (GCT) in one testicle have a 500-1000-fold greater chance of developing a contralateral testicular carcinoma. 0.5-7% of patients will develop a contralateral testicular tumor. 80-85% of bilateral tumors occur metachronously, at a mean of 65.1 months after the first tumor14. Review of the literature shows several reports of enormous testicular tumors. The majority of these reports came from Japan where the incidence of these tumors is low. The largest tumor was reported 32x28x28 cm in size with a calculated weight of 7 kg 40 in a 38-year-old patient with serum levels of LDH, AFP and ß-HCG of 2.040 U/l, 240ng/ml and 5.6 ng/ml, respectively15. These authors’ review of 42 cases in the Japanese literature reported that patient was treated initially with 3 cycles of VIP chemotherapy, followed by high orchiectomy and retroperitoneal lymph node dissection. The histologic examination of resected specimens revealed only necrosis and fibrosis. The authors believed that initial chemotherapy followed by surgery was the management approach of choice for the condition. Some other case reports have described enlarged teratomas, seminomas and a malignant fibrous hystiocytoma16-21. Approximately 70% of testicular GCTs tend to metastasize through the lymphatics, with paraaortic nodes the first to be involved. Hematogenous spread goes often to the lungs and liver22. Total tumor size was not significantly related to the development of metastasis or to the presence of vascular or lymphatic invasion23. The histology of the metastasis may be different from that of the primary tumor. Nonseminomatous germ cell tumors, including mature and immature teratomas, have a variegated appearance and often display hemorrhage and necrosis. These tumors are biologically more aggressive and radioresistant24. The histologic subtype does not influence prognosis. In patients younger than 15 years of age, approximately 90% of testicular germ cell cancers are yolk sac tumors. In these types of patients, the AFP is elevated at diagnosis and is an excellent indicator of response to therapy and of disease status25. Treatment with surgical excision and cisplatin-based chemotherapy provides cures in >90% of the cases. Radical inguinal orchiectomy with initial high ligation of the spermatic cord is the procedure of choice in treating a malignant testicular mass26. Tumors that have a mixture of seminoma and nonseminoma components should be managed as nonseminomas27. Evaluation of the retroperitoneal lymph nodes, usually by CT scanning, is an important aspect of treatment planning in adults with testicular cancer. Patients with a negative result however, have a 25% to 30% chance of having microscopic involvement of the lymph nodes28. A meta-analysis review of the histology of surgical specimens from 24 publications 2009 Enormous Mixed Germ Cell Tumor of the Testis (996 patients) found that residual teratoma was present after chemotherapy in 36% of cases29. Biologic markers, including AFP, HCG, PLAP, and lactate dehydrogenase (LD) are valuable in continued follow up of the patient30. In our case we completed a radical inguinal orchiectomy. In this case surgical treatment was complicated because of the size of the tumor. The patient was diagnosed with Stage IIA pT3N1M0S1 mixed germ cell tumor of the left testis. The treatment was continued with primary chemotherapy courses with PEB. Retroperitoneal lymph node dissection was not performed. A new staging was planned after primary chemotherapy according to the algorithm for patients with advanced disease, according to the International Germ Cell Cancer Consensus Group (IGCCCG)31. References: 1. Cotran, R S. The Male Genital Tract: in Robbins Pathologic Basis of Disease, 6th edition. W.B. Saunders Co, Phil. 1999. 2. Jemal A, Siegel R, Ward E. Cancer statistics 2006. CA Cancer J Clin. 2006; 56:106–30. 3. Berndt H, Berndt R. Inzidenz und Mortalitet an bosartigen Neubildungen der Harnorgane und mannlichen Geschlechtsorgane in der DDr. Urologe A. 1982; 21: 185-189. Albers, P., Albrecht, W., Aigaba, F. Guidelines on testicular 4. cancer. Eur Urol. 2005; 28: 885-894. 5. 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