1 / 30

Modern Pathology (2007) 20, 320–325 Sean K Lau, Lawrence M Weiss and Peiguo G Chu

D2-40 immunohistochemistry in the differential diagnosis of seminoma and embryonal carcinoma: a comparative immunohistochemical study with KIT (CD117) and CD30. Modern Pathology (2007) 20, 320–325 Sean K Lau, Lawrence M Weiss and Peiguo G Chu

kylia
Download Presentation

Modern Pathology (2007) 20, 320–325 Sean K Lau, Lawrence M Weiss and Peiguo G Chu

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript

  1. D2-40immunohistochemistry in thedifferential diagnosis of seminoma andembryonal carcinoma: a comparativeimmunohistochemical study with KIT(CD117) and CD30 Modern Pathology (2007) 20, 320–325 Sean K Lau, Lawrence M Weiss and Peiguo G Chu Department of Pathology, City of Hope National Medical Center, Duarte, CA, USA Intern 鄭詩燕

  2. Testis: Germ Cell Tumors • Seminoma • Nonseminomatous Embryonal carcinoma Yolk sac (endodermal sinus)tumor Choriocarcinoma Teratoma

  3. Germ Cell Tumors

  4. Seminoma • Age: 15-35y/o • 50% of germ cell tumor • Painless swelling • Dysgerminoma in ovary

  5. Seminoma • Bulky masses, sometimes 10 times> the normal testis. • Homogeneous, gray-white, lobulated cut surface, usually devoid of hemorrhage or necrosis • Mostly the entire testis is replaced. • Occasionally, extension to the epididymis, spermatic cord, or scrotal sac

  6. Seminoma

  7. Seminoma • Seminoma Cell: large and round to polyhedral and has a distinct cell membrane • A clear or watery-appearing cytoplasm • A large, central nucleus with one or two prominent nucleoli • The cytoplasm contains varying amounts of glycogen. • AFP(-) or HCG(-), placental alkaline phosphatase(+), 15%HCG(+)

  8. Seminoma

  9. Embryonal carcinoma • 20- to 30-year age group. • Grow faster than seminoma • Painful • More aggressive than seminomas

  10. Embryonal carcinoma • Size: smaller than seminoma • Usually does not replace the entire testis. • The mass is often variegated, poorly demarcated at the margins • Punctuated by foci of hemorrhage or necrosis • Extension through the tunica albuginea into the epididymis or cord is not infrequent.

  11. Embryonal carcinoma

  12. Embryonal carcinoma • The cells: alveolar or tubular patterns, sometimes with papillary convolutions • Undifferentiated cells, epithelial appearance • Hyperchromatic nuclei with prominent nucleoli. • Indistinct cell border, variation in cell and nuclear size and shape, mitotic figures • HCG(+), AFP (+)

  13. Embryonal carcinoma

  14. Introduction • Some seminomas : increased nuclear pleomorphism, cell crowding, and lack a lymphocytic infiltrate -> confusion with embryonal carcinoma. • Limited biopsy specimen or poor tissue fixation.

  15. Introduction Immunohistochemistry • CD 30: Embryonal carcinoma(+), Seminoma(-), Mixed germ cell tumors(+/-) • KIT(CD117): Seminoma(+), Embryonal carcinoma(-) Mixed germ cell tumors(+/-)

  16. Introduction • D2-40 Monoclonal antibody reacts with an oncofetal membrane antigen (M2A) which present in testis fetal germ cells Intratubular germ cell neoplasia, seminoma(+), Embryonal carcinoma(-)

  17. Materials and methods • 40 cases of testicular germ cell tumor • Age 18-41, mean age: 30 • Pure germ cell tumor (26 cases) 19 seminomas, 3 embryonal carcinomas,3 teratomas, 1 yolk sac tumor • Mixed germ cell tumors(14 cases) 7 seminomas, 11 embryonal carcinomas, 10 teratomas, 2 yolk sac tumors, and 1 choriocarcinoma.

  18. Materials and methods • Immunohistochemical staining: D2-40, KIT, CD30 • Xylene (deparaffinized) and ethanol (dehydrated) • Slide heating in EDTA buffer(pH8) in pressure cooker • Automated immunostainer -> antibody detection, counterstained with hematoxylin and coverslipped.

  19. Result 26 14

  20. Result • D2-40 antibody Seminoma -- strong membranous Embryonic carcinoma -- weak, focal, distributed along the apical or luminal surfaces of the cells.

  21. Result (seminoma)

  22. Result (embryonal ca)

  23. Discussion • D2-40 recognizes M2A antigen which present in fetal germ cells, lymphatic endothelium, and mesothelial cells. • M2A antigen expression in all seminomas and seminomatous components of mixed germ cell tumors

  24. Discussion • Present study: -- D2-40 in pure or mixed seminoma: 100% (26/26), (mixed) embryonal carcinoma 29% (4/14) -- Seminoma: diffuse membrane staining -- Embryonal carcinomas: focal and confined to the apical or luminal surfaces. • Marks et al study -- D2-40 in seminomas 98%, embryonal carcinomas 69%.

  25. Discussion • Distinction between seminoma and embryonal carcinoma can be madeon a morphologic basis using conventional histologicmethods. • Studies addressing theimpact of central histopathologic review of previouslydiagnosed testicular tumors have demonstratedmajor discrepancy rates of 4–11%

  26. Discussion • Immunohistochemical markers: keratins, KIT, and CD30. • Antikeratin antibodies -- Embryonal carcinoma : keratin intermediate filaments -- Seminomas lacked • Recent study -- Keratin positive in seminomas 4 to 45% • KIT and CD30: more effective immunohistochemical markers

  27. Discussion • Previous study KIT expression in seminoma: 100% • Present study KIT expression in seminoma: 92% none in embryonal carcinomas or non seminomatous germ cell tumors

  28. Discussion • CD30: as a sensitive as well as a specific maker for embryonal carcinoma (93%) • Focal CD30 expression has been described in a subset of seminomas • Leroy et al CD30 in combination with KIT -- seminoma: KIT(-), CD30(+) impossible -- embryonal carcinoma: KIT(+), CD30(-) impossible

  29. Discussion • Present study Sensitivity: D2-40 > KIT in seminomas Specific: D2-40 < KIT in seminomas (4/11 embryonal carcinomas +) • D2-40 in seminomas: diffuse and membranous • D2-40 in embryonal carcinomas: focal and limited to the apical or luminal surface of the cells.

  30. Summary • KIT and CD30: a useful markers that allows for seminoma to be distinguished from embryonal carcinoma. • Although a highly sensitive marker of seminomas, focal D2-40 immunoreactivity can be seen in a subset of embryonal carcinomas, thus limiting the practical value of this marker for discriminating between these particular malignancies.

More Related