V-ABL does not abolish IL-6 requirement by murine plasmacytoma cells
Autor: | Tadamitsu Kishimoto, Toshio Hirano, Francis Wiener, Santiago Silva, Hiroyuki Sugiyama, George Klein, Magda Babonits |
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Rok vydání: | 1991 |
Předmět: |
Cancer Research
Ratón medicine.medical_treatment Abelson murine leukemia virus Chromosomal translocation Genes abl Translocation Genetic Mice Tumor Cells Cultured medicine Animals Growth Substances ABL biology Oncogene Interleukin-6 Terpenes Macrophages medicine.disease Molecular biology Recombinant Proteins In vitro Cytokine Oncology Immunology biology.protein Plasmacytoma Antibody Cell Division |
Zdroj: | International Journal of Cancer. 48:234-238 |
ISSN: | 1097-0215 0020-7136 |
DOI: | 10.1002/ijc.2910480214 |
Popis: | Activation of c-myc by juxtaposition to an immunoglobulin locus and introduction of the v-abl oncogene act synergistically in generating a mouse plasmacytoma (PC). The question arose whether the effect of v-abl could be attributed to a deregulation of interleukin-6 (IL-6) production or responsiveness, in view of the fact that IL-6 exerts potent growth-stimulatory activity on PC cells. We studied the effect of IL-6 on the in vitro growth of primary PCs induced by pristane alone (TEPCs) or by pristane + A-MuLV (ABPCs). Five of 13 TEPCs and 3 of 7 ABPCs responded to IL-6. Macrophage supernatants prepared from both TEPCs and ABPCs had similar stimulatory effects on PC cells. From 30 primary PCs (including both TEPCs and ABPCs), we established 9 in vitro lines, 2 of which expressed v-abl. All were able to grow on macrophage feeder layers. Three types of behavior could be distinguished on the basis of growth in feeder-free cultures in the presence and absence of IL-6. Group I contained 4 IL-6-dependent lines. Group II contained 2 IL-6-independent lines (one v-abl expressor) that grew faster in the presence of IL-6. Group III consisted of 3 feeder-dependent lines (one v-abl expressor) that were not significantly stimulated by IL-6. These findings indicate that v-abl expression does not influence IL-6 dependence or responsiveness by itself. The supernatant of one line in group II was able to stimulate PC cells. All 6 lines of Groups I and II carried a typical (12;15) translocation, while all 3 lines in group III had a variant (6;15) or (15;16) translocation. |
Databáze: | OpenAIRE |
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