EVIDENCE THAT ENDOGENOUS INTERLEUKIN-1 IS INVOLVED IN LEUKOCYTE MIGRATION IN ACUTE EXPERIMENTAL INFLAMMATION IN RATS AND MICE

被引:51
作者
PERRETTI, M [1 ]
SOLITO, E [1 ]
PARENTE, L [1 ]
机构
[1] SCLAVO RES CTR,PHARMACOL LAB,VIA FIORENTINA 1,I-53100 SIENNA,ITALY
来源
AGENTS AND ACTIONS | 1992年 / 35卷 / 1-2期
关键词
D O I
10.1007/BF01990954
中图分类号
O6 [化学];
学科分类号
0703 ;
摘要
As a putative mediator of inflammation interleukin-1 has been implicated in the recruitment of leukocytes during the early stages of the inflammatory reaction. In the present report we have investigated the release of endogenous IL-1 in the rat zymosan pleurisy and in the mouse zymosan peritonitis. In both cases the release of the cytokine was maximal 4 hours after zymosan injection and appeared to be time-related to neutrophil migration into the inflammatory site. The effect of in vivo treatment with dexamethasone in rat pleurisy and with polyclonal anti-murine IL-1-beta antibody in mouse peritonitis was also assessed. The steroid reduced both cell migration and the release of IL-1-like activity as well as the formation of exudate and the release of eicosanoids. The anti-IL-1-beta serum inhibited selectively the number of neutrophil that migrated to the inflamed site (approximately 40%) and the IL-1 activity recovered in (approximately 70%) the exudate. In vitro incubation of the inflammatory exudate with polyclonal anti-murine IL-1-alpha or anti-murine IL-1-beta sera allowed the identification of the IL-1 species present. In the rat pleurisy IL-1 biological activity was mainly due to the a species, whereas IL-1-beta was the only species apparently present in the mouse peritoneal exudate.
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页码:71 / 78
页数:8
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