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抗性和易感大鼠小肠结肠炎中组织白细胞介素1及白细胞介素-1受体拮抗剂的表达

Tissue interleukin 1 and interleukin-1 receptor antagonist expression in enterocolitis in resistant and susceptible rats.

作者信息

McCall R D, Haskill S, Zimmermann E M, Lund P K, Thompson R C, Sartor R B

机构信息

Department of Internal Medicine, University of North Carolina at Chapel Hill.

出版信息

Gastroenterology. 1994 Apr;106(4):960-72. doi: 10.1016/0016-5085(94)90755-2.

Abstract

BACKGROUND/AIMS: Subserosal injection of purified group A streptococcal peptidoglycan-polysaccharide (PG-APS) induces chronic relapsing granulomatous enterocolitis and systemic inflammation in susceptible inbred Lewis rats but only transient intestinal injury in Buffalo and Fischer rats. Cecal interleukin 1 (IL-1) and IL-1 receptor antagonist (IL-1ra) expression was measured in inbred rats displaying differential susceptibility to experimental enterocolitis.

METHODS

The ileum and cecum of Lewis, Buffalo, and Fischer rats were subserosally injected with purified PG-APS or albumin. IL-1 and IL-1ra messenger RNA (mRNA) and protein (IL-1 only) were measured 1 or 27 days later. PG-APS-injected Lewis rats were treated with recombinant human IL-1ra. Kinetics of IL-1 and IL-1ra mRNA expression were studied in peritoneal cells.

RESULTS

All rats strains developed acute inflammation with increased cecal concentrations of IL-1 beta and IL-1ra mRNA. Lewis rats developed chronic enterocolitis and had higher IL-1 and IL-1ra mRNA tissue levels than Buffalo or Fischer rats, which displayed no chronic inflammation. IL-1 beta and IL-1ra were produced by submucosal granulomas and correlated with inflammation. IL-1 alpha protein levels paralleled IL-1 beta mRNA expression. IL-1ra treatment attenuated acute and chronic enterocolitis, adhesions, and arthritis. PG-APS induced IL-1 and IL-1ra expression in peritoneal cells from Lewis and Fischer rats.

CONCLUSIONS

Bacterial cell wall polymers stimulate IL-1 and IL-1ra expression in vivo and in vitro. These counterbalancing cytokines are increased in experimental enterocolitis and have important immunoregulatory roles in intestinal inflammation.

摘要

背景/目的:在易感性近交系Lewis大鼠中,浆膜下注射纯化的A组链球菌肽聚糖-多糖(PG-APS)可诱发慢性复发性肉芽肿性小肠结肠炎和全身炎症,但在布法罗大鼠和Fischer大鼠中仅引起短暂性肠道损伤。对实验性小肠结肠炎易感性不同的近交系大鼠的盲肠白细胞介素1(IL-1)和IL-1受体拮抗剂(IL-1ra)表达进行了检测。

方法

对Lewis大鼠、布法罗大鼠和Fischer大鼠的回肠和盲肠进行浆膜下注射纯化的PG-APS或白蛋白。在1天或27天后检测IL-1和IL-1ra信使核糖核酸(mRNA)及蛋白质(仅检测IL-1)。对注射PG-APS的Lewis大鼠用重组人IL-1ra进行治疗。研究了腹膜细胞中IL-1和IL-1ra mRNA表达的动力学。

结果

所有大鼠品系均发生急性炎症,盲肠中IL-1β和IL-1ra mRNA浓度升高。Lewis大鼠发生慢性小肠结肠炎,其IL-1和IL-1ra mRNA组织水平高于未出现慢性炎症的布法罗大鼠或Fischer大鼠。IL-1β和IL-1ra由黏膜下肉芽肿产生,并与炎症相关。IL-1α蛋白水平与IL-1β mRNA表达平行。IL-1ra治疗减轻了急性和慢性小肠结肠炎、粘连及关节炎。PG-APS可诱导Lewis大鼠和Fischer大鼠腹膜细胞中IL-1和IL-1ra表达。

结论

细菌细胞壁聚合物在体内和体外均可刺激IL-1和IL-1ra表达。在实验性小肠结肠炎中,这些相互平衡的细胞因子增加,在肠道炎症中具有重要的免疫调节作用。

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