Literature DB >> 15386301

Establishing a germ cell origin for metastatic tumors using OCT4 immunohistochemistry.

Liang Cheng1.   

Abstract

BACKGROUND: There are diverse morphologic manifestations of metastatic tumors. The determination of tumor origin is critical for patient management, and it is especially important when the differential diagnosis includes metastatic germ cell tumor, which is a highly treatable condition. OCT4 is a nuclear transcription factor that is expressed in pluripotent embryonic germ cells. In this study, the author sought to determine the usefulness of OCT4 immunohistochemistry in the diagnosis of metastatic germ cell tumors.
METHODS: Sixty-two retroperitoneal lymph node dissection specimens from patients with histories of testicular germ cell tumors were stained using the antibodies against OCT4. In addition, 84 metastatic, nongerm cell lesions from men with known primary tumors were studied in parallel for OCT4 immunohistochemistry.
RESULTS: All embryonal carcinoma components (n = 29 specimens) and seminoma components (n = 18 specimens) from retroperitoneal lymph node dissection specimens showed strong, intense, diffuse nuclear staining for OCT4. Yolk sac tumors (n = 12 tumors), choriocarcinomas (n = 4 tumors), mature teratomas (n = 16 tumors), and primitive neuroectodermal tumors (n = 5 tumors) were negative for OCT4 staining. Metastatic, nonsmall cell carcinomas from the lung (n = 14 tumors), colon (n = 12 tumors), stomach (n = 5 tumors), pancreas (n = 7 tumors), prostate (n = 12 tumors), kidney (n = 3 tumors), and urinary bladder (n = 15 tumors) all were found to be negative immunohistochemically for OCT4, as were metastatic small cell carcinomas (n = 4 tumors) and metastatic melanomas (n = 7 tumors). In addition, malignant lymphomas (n = 5 tumors) also were negative for OCT4.
CONCLUSIONS: Immunohistochemical detection of OCT4 is highly sensitive and specific for the diagnosis of seminoma and embryonal carcinoma metastatic from the testis. Establishing germ cell origin for metastatic tumors has important implications for assessing patient prognosis and treatment options.

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Year:  2004        PMID: 15386301     DOI: 10.1002/cncr.20566

Source DB:  PubMed          Journal:  Cancer        ISSN: 0008-543X            Impact factor:   6.860


  33 in total

1.  Histological evidence for the existence of germ cell tumor cells showing embryonal carcinoma morphology but lacking OCT4 expression and cisplatin sensitivity.

Authors:  Thomas Mueller; Lutz Peter Mueller; Hans-Juergen Holzhausen; Ralf Witthuhn; Peter Albers; Hans-Joachim Schmoll
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2.  Pure nongestational uterine choriocarcinoma in postmenopausal women: a case report with literature review.

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Review 3.  Cellular and molecular mechanisms underlying oxygen-dependent radiosensitivity.

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5.  Spontaneous metastasis in mouse models of testicular germ-cell tumours.

Authors:  J L Zechel; G T MacLennan; J D Heaney; J H Nadeau
Journal:  Int J Androl       Date:  2011-06-09

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Authors:  J Javanbakht; B Pedram; M R Taheriyan; F Khadivar; S H Hosseini; F S Abdi; E Hosseini; M Moloudizargari; S H Aghajanshakeri; S Javaherypour; R Shafiee; R Emrani Bidi
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8.  Mixed germ cell sex cord-stromal tumors of the testis and ovary. Morphological, immunohistochemical, and molecular genetic study of seven cases.

Authors:  Michal Michal; Tomas Vanecek; Radek Sima; Petr Mukensnabl; Ondrej Hes; Dmitry V Kazakov; Jozef Matoska; Anna Zuntova; Vladimir Dvorak; Alexander Talerman
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9.  POU4F1 is associated with t(8;21) acute myeloid leukemia and contributes directly to its unique transcriptional signature.

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10.  Comparative immunohistochemical characterization of canine seminomas and Sertoli cell tumors.

Authors:  Chi-Ho Yu; Du-Na Hwang; Ji-Young Yhee; Jong-Hyuk Kim; Keum-Soon Im; Whan-Gook Nho; Young-Soo Lyoo; Jung-Hyang Sur
Journal:  J Vet Sci       Date:  2009-03       Impact factor: 1.672

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