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Seminomas. Seminomas tend to grow and spread more slowly than non-seminomas. The 2 main sub-types of these tumors are classical (or typical) seminomas and spermatocytic seminomas. Classical seminoma: More than 95% of seminomas are classical. These usually occur in men between 25 and 45. Seminoma by definition must be pure seminoma on histology and not associated with an elevated serum alpha-fetoprotein (AFP).
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Uppföljning. Trots adekvat behandling visar det sig ibland efter en tid att Non-seminom drabbar män i åldrarna 20-40 år. Den här typen av cancer växer snabbt och bildar då metastaser i kroppen. Istället för att spridas till lymfkörtlarna av JE Damber — Vid behandling av testikelcancer hos vuxna patienter skiljer man på de två huvudtyperna seminom och icke-seminom. Alla tumörer med förhöjt Stadium I: Seminom - surveillance för alla. Nonseminom utan kärlinväxt- surveillance för alla.
Se hela listan på radiopaedia.org Interpreting the international trends in testicular seminoma and nonseminoma incidence.
Read me A B 1 Case Inconsistent CC-MCC grading 2 NCC ID
suspecta. 11, IN, No, P, A231, A23, A2310, Brucellosis due to Brucella abortus, Add CC Primary syphilis of other sites, Add CC - A513 has CC - Primär vs sekundär? 1370, C629A, C629A, C62, 9A, C629A, 0, Testicular seminoma, 11/09/1999, 0, 0 Seminom är mycket känsliga för strålbehandling. Nonseminoma: Denna vanligaste typ av testikelcancer tenderar att växa snabbare än seminom.
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Non-seminoma. The cancer has spread to an organ other than the lungs or the serum tumor marker levels are poor, which means: AFP is 10,000 ng/mL or higher. B-hCG is 50,000 iU/L or higher. LDH is 10 x ULN or higher. Seminoma.
Only seminoma vs. non-seminoma is used to determine prognostic groupings Predominant seminoma with focal non-seminoma is managed as non-seminoma Metastatic GCT Prognostic groupings Prognostic Group Tumour type 5 Year Progression Free Survival (%) 5 Year Survival (%) Good Seminoma (90%) 82 86 Non-seminoma (56%) 89 92 Intermediate
Request PDF | On Feb 1, 2003, S. Hautmann and others published New markers for testicular non-seminoma and seminoma: HA and HAS-1 | Find, read and cite all the research you need on ResearchGate
Non-Seminoma: Stage II Overview. Patients with stage II non-seminoma have cancer that involves the testicle and the retroperitoneal lymph nodes and is curable in over 90% of cases. A variety of factors ultimately influence a patient’s decision to receive treatment of cancer. 4596 Background: Controversy exists regarding the optimal management of stage I seminoma. This analysis defines the Kaiser experience over a 20-year period.
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A xenograft line, HX 53, has been established in immune-suppressed mice from a specimen of a lymph node metastasis in a patient with a histological diagnosis of seminoma but with markedly raised circulating levels of alpha-fetoprotein. Histological, immunocytochemical, Non-Seminoma: Stage II Overview.
Most tumors are a mix of different types (sometimes with seminoma cells too), but this doesn’t change the treatment of most non-seminoma cancers. Embryonal carcinoma: These cells are found in about 40% of testicular tumors, but pure embryonal carcinomas occur only 3% to 4% of the time.
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These tumors generally occur between the teen years and early 40s. They also tend to grow and spread more quickly than seminomas. Non-seminoma Seminoma Good prognosis Testis/retroperitoneal primary Any primary site and no non-pulmonary No pulmonary, visceral metastases visceral metastases and normal αFP, and and good markers – all of: hCG, any LDH αFP <1000 ng/ml hCG <5000 IU/l and LDH <1.5×upper limit of normal 56% of non-seminoma 90% of seminoma A seminoma is a germ cell tumor of the testicle or, more rarely, the mediastinum or other extra-gonadal locations. It is a malignant neoplasm and is one of the most treatable and curable cancers, with a survival rate above 95% if discovered in early stages. Testicular seminoma originates in the germinal epithelium of the seminiferous tubules.