首页> 外文期刊>American Journal of Physiology >Early weaning stress impairs development of mucosal barrier function in the porcine intestine.
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Early weaning stress impairs development of mucosal barrier function in the porcine intestine.

机译:早期断奶胁迫损害猪肠中粘膜屏障功能的发展。

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摘要

Early life stress is a predisposing factor for the development of chronic intestinal disorders in adult life. Here, we show that stress associated with early weaning in pigs leads to impaired mucosal barrier function. Early weaning (15- to 21-day weaning age) resulted in sustained impairment in intestinal barrier function, as indicated by reductions in jejunal transepithelial electrical resistance and elevations in mucosal-to-serosal flux of paracellular probes [(3)H]mannitol and [(14)C]inulin measured at 5 and 9 wk of age, compared with that shown in late-weaned pigs (23- to 28-day weaning age). Elevated baseline short-circuit current was observed in jejunum from early-weaned pigs and was shown to be mediated via enhanced Cl(-) secretion. Jejunal barrier dysfunction in early-weaned pigs coincided with increased lamina propria immune cell density particularly mucosal mast cells. The mast cell stabilizer drug sodium cromoglycolate ameliorated barrier dysfunction and hypersecretion in early-weaned pigs, demonstrating an important role of mast cells. Furthermore, activation of mast cells ex vivo with c48/80 and corticotrophin-releasing factor (CRF) in pig jejunum mounted in Ussing chambers induced barrier dysfunction and elevations in short-circuit current that were inhibited with mast cell protease inhibitors. Experiments in which selective CRF receptor antagonists were administered to early-weaned pigs revealed that CRF receptor 1 (CRFr1) activation mediates barrier dysfunction and hypersecretion, whereas CRFr2 activation may be responsible for novel protective properties in the porcine intestine in response to early life stress.
机译:早期生命压力是成年生命中慢性肠障碍发育的概述因素。在这里,我们表明与猪早期断奶相关的压力导致粘膜屏障功能受损。早期断奶(15至21天的断奶年龄)导致肠道屏障功能持续损害,如在静脉曲张探针的粘膜探针粘膜腹水通量的粘膜静脉渗透下降[(3)H]甘露醇和[(14)C]菊粉在5和9周龄测量,与晚断奶猪(23-28天断奶年龄)显示。从早期断奶猪的Jejunum观察到基线短路电流升高,并显示通过增强的Cl( - )分泌介导。早期猪的Jejunal屏障功能障碍与薄膜丙蛋白免疫细胞密度较高,特别是粘膜肥大细胞。肥大细胞稳定剂药物氧化钠,早期猪中的有效屏障功能障碍和过度折叠,展示了肥大细胞的重要作用。此外,用C48 / 80和皮质萎缩蛋白释放因子(CRF)在猪Jejunum中的肥大细胞释放因子(CRF)活化,安装在USSing腔室中的屏障功能障碍和升高的短路电流升高,其被抑制肥大细胞蛋白酶抑制剂。将选择性CRF受体拮抗剂施用于早期断奶猪的实验表明,CRF受体1(CRFR1)活化介导屏障功能障碍和Hypersecretion,而CRFR2活化可能负责猪肠中的新型保护性能响应于早期生命应激。

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