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伊立替康化疗引起的肠道氧化应激:黏膜水和电解质转运紊乱的潜在原因。

Irinotecan chemotherapy-induced intestinal oxidative stress: Underlying causes of disturbed mucosal water and electrolyte transport.

作者信息

Rtibi Kaïs, Selmi Slimen, Grami Dhekra, Sebai Hichem, Amri Mohamed, Marzouki Lamjed

机构信息

Laboratoire de Physiologie Fonctionnelle et Valorisation des Bioressources-Institut Supérieur de Biotechnologie de Béja, B.P. 382, 09000 Béja, Tunisia; Laboratoire de Neurophysiologie Fonctionnelle et Pathologies, Département des Sciences Biologiques, Faculté des Sciences de Tunis, 2092 Tunis, Tunisia.

Laboratoire de Physiologie Fonctionnelle et Valorisation des Bioressources-Institut Supérieur de Biotechnologie de Béja, B.P. 382, 09000 Béja, Tunisia.

出版信息

Pathophysiology. 2017 Dec;24(4):275-279. doi: 10.1016/j.pathophys.2017.07.002. Epub 2017 Jul 23.

Abstract

Irinotecan, a chemotherapy drug, can cause acute diarrhea immediately after administration. Hence, the present study was designed to investigate the gastrointestinal (GI) disturbances after an intraperitoneal (IP) administration of irinotecan in rats.Twenty Wistar rats were separated into two groups of ten. Group A was considered as a control group (NaCl, 0.9%). Group B was treated with irinotecan at a single dose of 200mgkg. The rats were observed for defecation. For the enteropooling test, the animals were sacrificed by decapitation 1h post-treatment. The small intestine was excised and the fluid was milked into a graduated tube and the volume was measured. After centrifugation of intraluminal liquid, the electrolyte concentrations in the supernatants were measured by flame photometry. Oxidative stress parameters and intracellular mediators as well as the MPO activity were determined in intestinal mucosa by colorimetric methods Our result indicated that irinotecan produces an intestinal fluid accumulation and electrolyte transport disorders. These effects were associated with augmented intestinal MPO activity and oxidative damage such as an elevation of MDA production and a depletion of enzymatic and non-enzymatic antioxidants. More than that, drug administration provoked intracellular mediator disturbances such as a free iron, HO and calcium levels. In conclusion, the data suggest that irinotecan caused a gastrointestinal stress via oxidative stress-induced disturbances in water and electrolyte transport in the intestinal mucosa in rats.

摘要

伊立替康是一种化疗药物,给药后可立即引起急性腹泻。因此,本研究旨在探讨腹腔注射伊立替康后大鼠的胃肠道紊乱情况。将20只Wistar大鼠分为两组,每组10只。A组作为对照组(0.9%氯化钠)。B组用200mg/kg的单剂量伊立替康治疗。观察大鼠排便情况。在肠内积液试验中,治疗后1小时将动物断头处死。取出小肠,将肠液挤入刻度管中并测量体积。腔内液体离心后,通过火焰光度法测量上清液中的电解质浓度。采用比色法测定肠黏膜中的氧化应激参数、细胞内介质以及MPO活性。我们的结果表明,伊立替康会导致肠液积聚和电解质转运紊乱。这些影响与肠MPO活性增强和氧化损伤有关,如MDA生成增加以及酶促和非酶促抗氧化剂耗竭。此外,给药引发了细胞内介质紊乱,如游离铁、HO和钙水平的变化。总之,数据表明伊立替康通过氧化应激诱导大鼠肠黏膜水和电解质转运紊乱,从而导致胃肠道应激。

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