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兔肠道中肽反应性类花生酸产生的组织起源。

Tissue origin of peptide-responsive eicosanoid production in rabbit intestine.

作者信息

Leduc L E, Zipser R D

机构信息

Division of Gastroenterology/Department of Medicine, Harbor-University of California, Los Angeles, Torrance 90509.

出版信息

Am J Physiol. 1989 Dec;257(6 Pt 1):G879-86. doi: 10.1152/ajpgi.1989.257.6.G879.

DOI:10.1152/ajpgi.1989.257.6.G879
PMID:2610259
Abstract

Different layers of rabbit large and small intestine display different peptide sensitivity and different profiles of eicosanoid release. Isolated perfused mesenteric pedicle alone, with muscularis/submucosa or with muscularis and mucosa from normal small bowel, normal colon, or inflamed colon were stimulated with bradykinin (BK) or n-formyl-methionyl-leucyl-phenylalanine (fMLP). Released prostaglandin (PG)E2, thromboxane (Tx)B2, and leukotriene (LT)B4 were assayed using extensively validated radioimmunoassays. In rabbit colon, PGE2 arises primarily from the mesentery, while in small intestine the muscularis/mucosa releases 70-80% of the total PGE2. BK releases no significant thromboxane from healthy colon, although both muscularis/submucosa and mucosa respond in inflamed colon. In contrast, fMLP stimulates thromboxane from muscularis/submucosa and mucosa of even healthy colon, while release is greatly potentiated in inflammation. Lipoxygenase in the colon is regulated differently than cyclooxygenase; it is not stimulated by BK in either healthy or inflamed colon. fMLP releases equal amounts of LTB4 from healthy and inflamed colon, but release was primarily from healthy colonic mucosa, whereas it was distributed throughout mesenteric pedicle, muscularis, and mucosa in inflamed colon. The ability of normal colonic mucosa to release proinflammatory LTB4 in response to a chemotactic factor (fMLP) produced by enteric bacteria suggests a possible role for these compounds as a stimulus for inflammation in some patients with inflammatory bowel disease.

摘要

兔大肠和小肠的不同层次表现出不同的肽敏感性和类花生酸释放谱。单独分离灌注的肠系膜蒂、带有肌层/黏膜下层或带有正常小肠、正常结肠或炎症结肠的肌层和黏膜,用缓激肽(BK)或N-甲酰甲硫氨酰-亮氨酰-苯丙氨酸(fMLP)进行刺激。使用经过广泛验证的放射免疫分析法测定释放的前列腺素(PG)E2、血栓素(Tx)B2和白三烯(LT)B4。在兔结肠中,PGE2主要来自肠系膜,而在小肠中,肌层/黏膜释放的PGE2占总量的70-80%。健康结肠中的BK不会释放大量血栓素,尽管肌层/黏膜下层和黏膜在炎症结肠中会产生反应。相比之下,fMLP会刺激即使是健康结肠的肌层/黏膜下层和黏膜释放血栓素,而在炎症状态下释放会大大增强。结肠中的脂氧合酶与环氧化酶的调节方式不同;在健康或炎症结肠中,它都不会被BK刺激。fMLP从健康和炎症结肠中释放等量的LTB4,但释放主要来自健康结肠黏膜,而在炎症结肠中,它分布在整个肠系膜蒂、肌层和黏膜中。正常结肠黏膜对肠道细菌产生的趋化因子(fMLP)做出反应释放促炎LTB4的能力表明,这些化合物可能在一些炎症性肠病患者的炎症刺激中发挥作用。

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