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巴西日圆线虫致敏大鼠过敏反应期间白三烯的肠内和全身释放

Enteral and systemic release of leukotrienes during anaphylaxis of Nippostrongylus brasiliensis-primed rats.

作者信息

Moqbel R, King S J, MacDonald A J, Miller H R, Cromwell O, Shaw R J, Kay A B

出版信息

J Immunol. 1986 Jul 1;137(1):296-301.

PMID:3011907
Abstract

Rats with acquired immunity to the intestinal nematode Nippostrongylus brasiliensis develop anaphylaxis after i.v. challenge with an extract of worm antigen, with the small intestine being the primary shock organ. In the present study we have shown that these events were associated with significant elevations in intestinal and plasma concentrations of leukotrienes LTB4 and LTC4. The changes were observed in immune rats over 10-, 30-, and 60-min intervals after antigen challenge but were absent in control animals. These lipid mediators were identified both in the perfusate of the gut lumen, which contained large quantities of mucus, and in homogenates of intestinal tissue. In addition, significant elevations in the concentrations of plasma LTB4 and LTC4 were detected in immune challenged rats but not in controls. Leukotrienes were identified by radioimmunoassay and validated by reverse-phase high-performance liquid chromatography (RP-HPLC). RP-HPLC analysis of SRS-A leukotrienes in immune challenged rats indicated that LTC4 was the predominant sulfidopeptide leukotriene at 10 min, with almost complete biodegradation to LTD4 and LTE4 within 30 min. Infected rats also had significant increases in the numbers of intestinal mucosal mast cells (MMC) and eosinophils. Evidence of MMC activation during anaphylaxis was obtained by showing significant elevations of intestinal and systemic concentrations of their exclusive serine enzyme, rat mast cell proteinase II (RMCPII). Thus, the release of substantial amounts of leukotrienes in the gut and plasma of N. brasiliensis-primed rats after interaction with worm antigens suggests that these potent mediators may play an important role in allergic-type hypersensitivity known to occur during immune reactions against parasitic helminths.

摘要

对巴西日圆线虫具有获得性免疫力的大鼠,在静脉注射蠕虫抗原提取物后会发生过敏反应,小肠是主要的休克器官。在本研究中,我们发现这些事件与肠道和血浆中白三烯LTB4和LTC4浓度的显著升高有关。在抗原攻击后的10分钟、30分钟和60分钟间隔内,在免疫大鼠中观察到了这些变化,但在对照动物中未观察到。这些脂质介质在含有大量黏液的肠腔灌流液和肠组织匀浆中均被鉴定出来。此外,在免疫攻击的大鼠中检测到血浆LTB4和LTC4浓度显著升高,而在对照大鼠中未检测到。通过放射免疫测定法鉴定白三烯,并通过反相高效液相色谱法(RP-HPLC)进行验证。对免疫攻击大鼠中SRS-A白三烯的RP-HPLC分析表明,LTC4在10分钟时是主要的硫醚肽白三烯,在30分钟内几乎完全生物降解为LTD4和LTE4。感染大鼠的肠道黏膜肥大细胞(MMC)和嗜酸性粒细胞数量也显著增加。通过显示其唯一的丝氨酸酶大鼠肥大细胞蛋白酶II(RMCPII)在肠道和全身的浓度显著升高,获得了过敏反应期间MMC激活的证据。因此,与蠕虫抗原相互作用后,巴西日圆线虫致敏大鼠的肠道和血浆中释放大量白三烯,这表明这些强效介质可能在针对寄生蠕虫的免疫反应中已知发生的过敏型超敏反应中起重要作用。

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