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白屈菜红碱、阿霉素和阿克拉霉素对K562细胞自然杀伤细胞介导的细胞溶解敏感性的比较效应。转铁蛋白受体和CD15抗原表达的改变与对自然杀伤细胞抗性诱导之间缺乏一致性。

Comparative effects of fagaronine, adriamycin and aclacinomycin on K562 cell sensitivity to natural-killer-mediated lysis. Lack of agreement between alteration of transferrin receptor and CD15 antigen expressions and induction of resistance to natural killer.

作者信息

Benoist H, Comoe L, Joly P, Carpentier Y, Desplaces A, Dufer J

机构信息

Laboratoire d'Immunologie, UFR de Pharmacie, Toulouse, France.

出版信息

Cancer Immunol Immunother. 1989;30(5):289-94. doi: 10.1007/BF01744896.

Abstract

Little is known about membrane target antigens for natural killer (NK) cells. Transferrin receptor and CD15 antigen might be two of these target structures. A novel antileukemic alkaloid, fagaronine, is able to induce hemoglobin synthesis in the K562 cell line. Numerous reports suggest relations between the expression of natural killer target structures and the differentiation stage of malignant cells. Effects of fagaronine on the expression of glycophorin A, transferrin receptor and CD15 antigen and susceptibility to NK-mediated lysis have been investigated in K562 cells and compared to those of two anthracyclines (Adriamycin and aclacinomycin A) known to be erythroid-differentiation inducers. When comparing the balance of differentiating effect and toxicity, the dose and time-dependent effects of the drugs, fagaronine and aclacinomycin, are equivalent on K562 cells. In experimental conditions where fagaronine (3500 nM), Adriamycin (40 nM) and aclacinomycin (15 nM) recruit the same percentage of hemoglobin-containing cells (40%-50%), glycophorin A expression increases and transferrin receptor expression decreases. Only Adriamycin treatment decreases CD15 antigen expression. In addition, Adriamycin and aclacinomycin, but not fagaronine, induce resistance to NK-mediated lysis. These data suggest that (a) it is unlikely that CD15 antigen and transferrin receptor, separately considered, can be unique target structures for NK cells; and (b) fagaronine is a potent erythroid inducer which, in our system, has similar effects to aclacinomycin without induced resistance to NK attack.

摘要

关于自然杀伤(NK)细胞的膜靶抗原,人们了解甚少。转铁蛋白受体和CD15抗原可能是其中的两种靶结构。一种新型抗白血病生物碱法格任宁,能够在K562细胞系中诱导血红蛋白合成。众多报告表明自然杀伤靶结构的表达与恶性细胞的分化阶段之间存在关联。在K562细胞中研究了法格任宁对血型糖蛋白A、转铁蛋白受体和CD15抗原表达以及对NK介导裂解的敏感性的影响,并与两种已知为红系分化诱导剂的蒽环类药物(阿霉素和阿克拉霉素A)进行了比较。在比较分化效应和毒性的平衡时,法格任宁和阿克拉霉素这两种药物对K562细胞的剂量和时间依赖性效应相当。在法格任宁(3500 nM)、阿霉素(40 nM)和阿克拉霉素(15 nM)使含血红蛋白细胞的百分比相同(40%-50%)的实验条件下,血型糖蛋白A表达增加,转铁蛋白受体表达减少。只有阿霉素处理会降低CD15抗原表达。此外,阿霉素和阿克拉霉素,但不是法格任宁,会诱导对NK介导裂解的抗性。这些数据表明:(a)单独考虑时,CD15抗原和转铁蛋白受体不太可能是NK细胞唯一的靶结构;(b)法格任宁是一种有效的红系诱导剂,在我们的系统中,其效果与阿克拉霉素相似,但不会诱导对NK攻击的抗性。

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