首页> 外文期刊>European Journal of Pharmacology: An International Journal >Involvement of resident macrophages and mast cells in the writhing nociceptive response induced by zymosan and acetic acid in mice.
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Involvement of resident macrophages and mast cells in the writhing nociceptive response induced by zymosan and acetic acid in mice.

机译:驻留巨噬细胞和肥大细胞参与小鼠中由酵母聚糖和乙酸诱导的扭曲的伤害感受性反应。

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Intraperitoneal administration of zymosan and acetic acid induced a dose-dependent nociceptive writhing response in mice. Lavage of the peritoneal cavities with saline reduced the number of total resident peritoneal cells and caused a proportional decrease in the nociceptive responses induced by these stimuli. Furthermore, the specific reduction of the peritoneal mast cell population by intraperitoneal administration of compound 48/80 also reduced the nociceptive responses induced by zymosan and acetic acid. In contrast, enhancement of the peritoneal macrophage population by pretreatment of the cavities with thioglycollate caused an increase in the number of writhes induced by both stimuli. These data suggest that the nociceptive responses induced by zymosan and acetic acid are dependent upon the peritoneal resident macrophages and mast cells. These cells modulate the nociceptive response induced by zymosan and acetic acid via release of tumour necrosis factor alpha (TNF-alpha), interleukin 1beta and interleukin 8. This suggestion is supported by the following observations: (a) pretreatment of the peritoneal cavities with antisera against these cytokines reduced the nociceptive responses induced by these stimuli; (b) peritoneal cells harvested from cavities injected with zymosan or acetic acid released both interleukin 1beta and TNF-alpha; (c) although individual injection of TNF-alpha, interleukin 1beta or interleukin 8 did not induce the nociceptive effect, intraperitoneal injection of a mixture of these three recombinant cytokines caused a significant nociceptive writhing response. In conclusion, our results suggest that the nociceptive activity of zymosan and acetic acid in the writhing model is due to the release of TNF-alpha, interleukin 1beta and interleukin 8 by resident peritoneal macrophages and mast cells.
机译:腹膜内给予酵母聚糖和乙酸可引起小鼠剂量依赖性伤害性扭体反应。用盐水冲洗腹膜腔可减少总驻留腹膜细胞的数量,并导致这些刺激引起的伤害感受反应成比例下降。此外,通过腹膜内施用化合物48/80来特异性减少腹膜肥大细胞群也减少了由酵母聚糖和乙酸诱导的伤害感受性反应。相反,通过用巯基乙酸盐对腔体进行预处理来增强腹膜巨噬细胞群会导致两种刺激引起的扭曲次数增加。这些数据表明,由酵母聚糖和乙酸诱导的伤害反应取决于腹膜常驻巨噬细胞和肥大细胞。这些细胞通过释放肿瘤坏死因子α(TNF-alpha),白介素1beta和白介素8来调节酵母聚糖和乙酸诱导的伤害感受反应。以下观察结果支持这一建议:(a)用抗血清预处理腹膜腔针对这些细胞因子减少了由这些刺激诱导的伤害性反应; (b)从注入酵母聚糖或乙酸的腔中收获的腹膜细胞释放白介素1β和TNF-α; (c)尽管单独注射TNF-α,白介素1β或白介素8不会诱导伤害感受,但腹膜内注射这三种重组细胞因子的混合物会引起明显的伤害扭曲反应。总之,我们的结果表明,在扭曲模型中,酵母聚糖和乙酸的伤害感受活性是由于常驻腹膜巨噬细胞和肥大细胞释放TNF-α,白介素1β和白介素8所致。

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