Phenotypic characterization of Ewing sarcoma cell lines with monoclonal antibodies
✍ Scribed by Marc Lipinski; Karim Braham; Irène Philip; Joëlle Wiels; Thierry Philip; Koussay Dellagi; Christo Goridis; Gilbert M. Lenoir; Thomas Tursz
- Publisher
- John Wiley and Sons
- Year
- 1986
- Tongue
- English
- Weight
- 487 KB
- Volume
- 31
- Category
- Article
- ISSN
- 0730-2312
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✦ Synopsis
The histogenesis of Ewing sarcoma, the second most frequent bone tumor in humans, remains controversial. Four Ewing cell lines were analyzed by immunological methods. A panel of antibodies directed to T, B, and myelomonocytic markers gave negative results. Surface antigens recognized on Ewing cells were found to be related to the neuroectoderm lineage. Ganglioside GD2, a marker of neuroectodermal tissues and tumors, was present on all lines. These were also stained by the mouse monoclonal antibody HNK-1, which detects a carbohydrate epitope present on several glycoconjugates of the nervous system, including two glycoproteins, the myelin-associated glycoprotein and the neural cell-adhesion molecule (N-CAM), and an acidic glycolipid of the peripheral nervous system. The P61 monoclonal antibody, which reacts with a peptide moiety of N-CAM, and a rabbit antiserum, raised to purified mouse N-CAM and not recognizing the HNK-1-defined epitope, were also reactive. By contrast, all antibodies specific for hematopoietic cell surface antigens were totally negative. Besides these antigenic features, Ewing sarcomacellsarecharacterized by aspecific t(11;22)(q24;q12) translocation also observed in neuroepithelioma, a neuroectoderrnal tumor, suggesting a possible evolutionary related origin. The recent finding that the human N-CAM gene is located at the vicinity of the breakpoint on chromosome 11 indicates that it might be involved in genetic rearrangements occurring in this region.
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