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米色小鼠中多形核白细胞的肿瘤细胞毒性:高反应性与线性β-1,3-D-葡聚糖及米色基因的关联。

Tumor cytotoxicity of polymorphonuclear leukocytes in beige mice: linkage of high responsiveness to linear beta-1,3-D-glucan with the beige gene.

作者信息

Fukase S, Inoue T, Arai S, Sendo F

出版信息

Cancer Res. 1987 Sep 15;47(18):4842-7.

PMID:3621179
Abstract

Beige mice (bg/bg) have many functional defects in their leukocytes and these phenotypes are inherited autosomal recessively. We studied the tumor cytotoxicity of polymorphonuclear leukocytes (PMN) obtained from bg/bg. The intensity of tumor cytotoxicity of PMN induced by linear beta-1,3-D-glucan was significantly higher in bg/bg PMN than in PMN of heterozygous control mice (bg/+). To analyze this phenomenon more precisely from the genetic viewpoint, we determined the tumor cytotoxicity of PMN from mice obtained by several mating experiments. (a) The intensity of linear beta-1,3-D-glucan-induced PMN cytotoxicity was found to be genetically defined and linked completely with the beige gene. In litter mates obtained from bg/+(female) X bg/bg(male), bg/bg(female) X bg/+(male), and bg/+(female) X bg/+(male) mating, PMN from only bg/bg showed significantly higher tumor cytotoxicity than those from bg/+ or mice that do not possess the beige gene (+/+). (b) The tumor cytotoxicity induced by other stimulants (phorbol myristate acetate and cytokines) was not significantly higher in bg/bg than bg/+ or +/+ PMN. It was concluded that the high responsiveness to linear beta-1,3-D-glucan in terms of tumor cytotoxicity of PMN was determined by the locus that is linked to the beige gene and is expressed autosomal recessively.

摘要

米色小鼠(bg/bg)的白细胞存在多种功能缺陷,这些表型呈常染色体隐性遗传。我们研究了从bg/bg小鼠获得的多形核白细胞(PMN)的肿瘤细胞毒性。线性β-1,3-D-葡聚糖诱导的bg/bg小鼠PMN的肿瘤细胞毒性强度显著高于杂合对照小鼠(bg/+)的PMN。为了从遗传学角度更精确地分析这一现象,我们测定了通过多次交配实验获得的小鼠PMN的肿瘤细胞毒性。(a)发现线性β-1,3-D-葡聚糖诱导的PMN细胞毒性强度是由基因决定的,并且与米色基因完全连锁。在从bg/ +(雌性)×bg/bg(雄性)、bg/bg(雌性)×bg/ +(雄性)和bg/ +(雌性)×bg/ +(雄性)交配获得的同窝小鼠中,只有bg/bg小鼠的PMN表现出比bg/+或不携带米色基因(+/+)的小鼠更高的肿瘤细胞毒性。(b)其他刺激物(佛波酯肉豆蔻酸酯和细胞因子)诱导的肿瘤细胞毒性在bg/bg小鼠中并不显著高于bg/+或+/+小鼠的PMN。得出的结论是,PMN在肿瘤细胞毒性方面对线性β-1,3-D-葡聚糖的高反应性是由与米色基因连锁且呈常染色体隐性表达的基因座决定的。

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