| Abstract: |
Antisera reactive with the ganglioside GM2 were raised by immunizing C57BL/6 mice with the C57BL/6 melanoma JB-RH. Fusion with NS-1 was performed using splenic mononuclear cells from a mouse with high antibody titer. An immunoglobulin M monoclonal antibody (monoclonal antibody 5–3) was identified which was reactive with an antigen that was resistant to heat, trypsin, and Pronase. A panel of purified glycolipids was used to determine the specificity of monoclonal antibody 5–3. Reactivity was restricted to N-acetyl- and N-glycolyl-GM2. No reactivity was detected with asialo-GM2 or other gangliosides. Monoclonal antibody 5–3 was used to define the expression of GM2 on the cell surface of cultured human normal and malignant cells. Reactivity was seen with cell lines derived from 8 of 8 astrocytomas, 5 of 5 neuroblastomas, 7 of 9 sarcomas, 4 of 18 human melanomas, 2 of 4 murine melanomas, 4 of 37 epithelial cancers and with 0 of 6 skin fibroblast and 0 of 2 brain fibroblast lines. GM2, like GD2 and GD3, appears to be a differentiation antigen largely restricted to cells of neuroectodermal origin. copyright. © 1986, American Association for Cancer Research. All rights reserved. |
| Keywords: |
human cell; animal cell; mouse; animals; mice; cells, cultured; melanoma; tumor antigen; mice, inbred c57bl; monoclonal antibody; antibodies, monoclonal; neuroblastoma; tumor cell; enzyme-linked immunosorbent assay; astrocytoma; antigens, surface; nervous system; cell surface; gangliosides; ganglioside; g(m2) ganglioside; chromatography, thin layer; human; priority journal
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