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首页> 外文期刊>Life sciences >Methylamine dichloramine may play a role in the process of colorectal disease through architectural and oxidative changes in crypts in mice.
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Methylamine dichloramine may play a role in the process of colorectal disease through architectural and oxidative changes in crypts in mice.

机译:甲胺二氯胺可能通过小鼠隐窝的结构和氧化变化在结直肠疾病的过程中发挥作用。

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摘要

AIMS: Methylamine dichloramine (CH(3)NCl(2)) produced by neutrophils may promote colon tumors and colitis via architectural and oxidative changes in crypts, which are secretory granulae composed of goblet cells located in the colorectal mucosal layer. We investigated whether CH(3)NCl(2), in comparison with the other reactive oxygen species (ROS) such as H(2)O(2) and HOCl, derived from primed neutrophils in inflammatory sites in the large intestine, is a biogenic factor for the induction of colorectal disease in mice. MAIN METHODS: Male ICR-strain mice were administered each oxidant (0.5-0.7 micromol/mouse) by enema under anesthesia. The colorectal tissues were evaluated by histopathological and immunohistochemical analyses. Hemolysis and hemoglobin oxidation by the methylamine chloramines and HOCl were examined by adding them (50-400 microM) to a sheep erythrocyte suspension (1x10(8) cells/ml) and its lysate at pH 7 and 37 degrees C. KEY FINDINGS: CH(3)NCl(2) oxidized erythrocyte hemoglobin more effectively than HOCl, indicating it has high cell permeability and selective oxidation ability. CH(3)NCl(2) mainly induced atrophy of crypts at 6 h after administration, while the other ROS tested did not. Furthermore, 4-hydroxy-2-nonenal (4-HNE) showed positive immunostains throughout the mucosal layer, including around the basal regions of atrophied crypts, only with CH(3)NCl(2), while positive immunostains were observed for 3-nitrotyrosine (3-NT) in the atrophied crypts and their surrounding lamina propria in the mucosal layer. SIGNIFICANCE: The results suggest that CH(3)NCl(2)derived from primed neutrophils may play the most important role in promoting the development of colon tumor formation and colitis by oxidative stress through its high degree of cell permeability.
机译:目的:中性粒细胞产生的甲胺二氯胺(CH(3)NCl(2))可能通过隐窝的结构和氧化变化促进结肠肿瘤和结肠炎,隐窝是位于结肠直肠粘膜层的杯状细胞组成的分泌性颗粒。我们调查了CH(3)NCl(2),与其他活性氧(ROS),例如H(2)O(2)和HOCl,是否是大肠炎性部位中的中性粒细胞衍生的相比,是否是一种诱导大肠疾病的生物成因。主要方法:在麻醉下,通过灌肠对雄性ICR品系小鼠进行每种氧化剂(0.5-0.7微摩尔/小鼠)的给药。通过组织病理学和免疫组织化学分析评估结直肠组织。通过将它们(50-400 microM)添加到绵羊红细胞悬液(1x10(8)细胞/ ml)及其裂解液中的pH为7和37摄氏度下,检测了甲胺氯胺和HOCl的溶血和血红蛋白氧化。主要发现:CH (3)NCl(2)比HOCl更有效地氧化了红细胞血红蛋白,表明它具有较高的细胞渗透性和选择性氧化能力。 CH(3)NCl(2)主要在给药后6小时引起隐窝萎缩,而其他经测试的ROS则没有。此外,4-羟基-2-壬烯醛(4-HNE)在整个粘膜层,包括萎缩性隐窝的基底区域周围,均显示阳性免疫染色,仅使用CH(3)NCl(2),而对于3-则观察到阳性免疫染色萎缩性隐窝中的硝基酪氨酸(3-NT)及其黏膜层周围的固有层。意义:结果表明,源自中性粒细胞的CH(3)NCl(2)可能通过其高度的细胞渗透性,通过氧化应激促进结肠肿瘤形成和结肠炎的发展。

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