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腔内 FeSO4 诱导的豚鼠空肠运动变化。

Motility changes induced by intraluminal FeSO4 in guinea pig jejunum.

机构信息

Department of Physiology, School of Medical Sciences, University of New South Wales, Sydney, New South Wales, Australia.

出版信息

Neurogastroenterol Motil. 2014 Mar;26(3):385-96. doi: 10.1111/nmo.12276. Epub 2013 Dec 15.

Abstract

BACKGROUND

Dietary iron supplementation is associated with gastrointestinal (GI) side effects including vomiting, nausea, and diarrhea. Although inorganic iron in high concentrations may be damaging to the intestinal mucosa, we hypothesize that there are physiological effects on the GI tract that occur at concentrations achieved by supplementation. Thus, our aim was to investigate the effect of intraluminal ferrous sulfate (FeSO4 ) on jejunal motility.

METHODS

Segments of guinea pig jejunum were cannulated and the intraluminal pressure recorded with a transducer, while movements were recorded with a video camera. Peristaltic threshold was the oral pressure that evoked four consecutive propulsive contractions. The nutrients decanoic acid (1 mM), l-phenylalanine (50 mM), or the micronutrient FeSO4 (1 mM) were infused intraluminally. We also tested the effect of FeSO4 on electrochemically detected serotonin (5-HT, 5-hydroxytryptamine) released from in vitro tissues, both at rest and following mechanical stimulation.

KEY RESULTS

The jejuna peristaltic threshold was significantly decreased by all three nutrients: FeSO4 : 31 ± 2-23 ± 3 mmH2 O; decanoic acid: 27 ± 2-14 ± 2 mmH2 O; and l-phenylalanine: 30 ± 3-14 ± 3mmH2 O. Of the three, only decanoic acid induced segmentation, while FeSO4 inhibited decanoic acid-induced segmentation. Resting 5-HT release was increased by FeSO4 (128% of control), but mechanically evoked 5-HT release was reduced (70% of control).

CONCLUSIONS & INFERENCES: These data suggest that some luminal effects of inorganic iron on jejunal motility could be mediated through a pathway involving altered release of 5-HT. A better understanding of the interaction between luminal iron and 5-HT containing enterochromaffin cells could improve iron supplementation strategies, thus reducing side effects.

摘要

背景

膳食铁补充与胃肠道(GI)副作用相关,包括呕吐、恶心和腹泻。虽然高浓度的无机铁可能对肠黏膜造成损害,但我们假设在补充剂达到的浓度下,胃肠道会发生生理效应。因此,我们的目的是研究肠腔内硫酸亚铁(FeSO4)对空肠运动的影响。

方法

将豚鼠空肠段进行套管,并通过换能器记录腔内压力,同时使用摄像机记录运动。蠕动阈值是引起连续 4 次推进性收缩的口腔压力。将营养物癸酸(1mM)、L-苯丙氨酸(50mM)或微量营养素 FeSO4(1mM)经腔内输注。我们还测试了 FeSO4 对电检测到的来自体外组织的 5-羟色胺(5-HT,5-羟色胺)释放的影响,包括在休息时和机械刺激后。

主要结果

三种营养素均显著降低空肠蠕动阈值:FeSO4:31±2-23±3mmH2O;癸酸:27±2-14±2mmH2O;L-苯丙氨酸:30±3-14±3mmH2O。在这三种营养素中,只有癸酸诱导了分段,而 FeSO4 抑制了癸酸诱导的分段。FeSO4 增加了静止状态下 5-HT 的释放(对照的 128%),但机械刺激引起的 5-HT 释放减少(对照的 70%)。

结论和推论

这些数据表明,无机铁对空肠运动的一些腔内效应可能通过涉及改变 5-HT 释放的途径介导。更好地理解腔内铁与含有 5-HT 的肠嗜铬细胞之间的相互作用,可以改善铁补充策略,从而减少副作用。

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