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首页> 外文期刊>Journal of Virology >Effect of tunicamycin on cell fusion induced by Mason-Pfizer monkey virus.
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Effect of tunicamycin on cell fusion induced by Mason-Pfizer monkey virus.

机译:少腺素对梅森 - 辉瑞猴病毒诱导细胞融合的影响。

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摘要

Mason-Pfizer monkey virus, a D-type retrovirus, has been shown to induce multinucleate cell (syncytium) formation or cell fusion in several normal primate cells. A series of experiments has been carried out to examine whether a glycosylated "fusion-inducing" product is responsible for this biological property of Mason-Pfizer monkey virus. Treatment of rhesus monkey fetal lung cells with different concentrations of tunicamycin, a potent inhibitor of glycosylation, during infection with Mason-Pfizer monkey virus had no effect on cell fusion even though up to 5 micrograms of the drug per ml was tested. Furthermore, no significant effect on the extent of syncytium formation in rhesus monkey fetal lung cells was observed when the time of addition or duration of treatment with this inhibitor was varied. Nevertheless, tunicamycin was very effective in blocking glycosylation in rhesus cells since virions produced in the presence of this drug completely lacked gp70 and gp20, the two structural glycoproteins of Mason-Pfizer monkey virus. These non-glycosylated virus particles produced in the presence of tunicamycin were noninfectious as determined by a protein A binding assay and were unable to induce syncytium formation when assayed on rhesus cells. These results indicate that glycosylation of the fusion-inducing product is not required for multinucleate cell formation induced by Mason Pfizer monkey virus.
机译:已显示Mason-Pufizer猴病毒,D型逆转录病毒,诱导若干正常灵长类细胞中的多核细胞(Syncytium)形成或细胞融合。已经进行了一系列实验,以检查糖基化的“融合诱导”产品是否负责梅森 - 辉瑞猴病毒的这种生物特性。治疗恒河猴胎儿肺细胞具有不同浓度的葡萄糖霉素,在用梅森 - 辉瑞猴病毒感染期间对糖基化的有效抑制剂对细胞融合的影响虽然最多5微克的药物测试了每mL。此外,当随这种抑制剂治疗的时间或变化时,观察到对恒河猴胎儿肺细胞中的合胞间形成的程度没有显着影响。然而,由于在该药物存在下在该药物存在下完全缺乏GP70和GP20,因此,唐氏霉素在恒毛细胞中阻断糖基化的糖基化非常有效,这是Mason-Pfizer猴病毒的两个结构糖蛋白。这些非糖基化病毒颗粒在存在的宫霉素存在下是非染色的,如通过蛋白质A结合测定法测定,并且在测定恒河细胞上时不能诱导合胞形成。这些结果表明,由梅森辉瑞制品猴病毒诱导的多核细胞形成不需要融合诱导产物的糖基化。

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