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甲磺酸伊马替尼可缓解肠道过敏小鼠模型的腹泻。

Imatinib mesylate alleviates diarrhea in a mouse model of intestinal allergy.

机构信息

Institute of Medicine, University of Bergen, Norway.

出版信息

Neurogastroenterol Motil. 2012 Jul;24(7):e325-35. doi: 10.1111/j.1365-2982.2012.01941.x.

DOI:10.1111/j.1365-2982.2012.01941.x
PMID:22709239
Abstract

BACKGROUND

When sensitized epicutaneously and challenged orally with ovalbumin, Balb/c mice develop allergen-induced diarrhea. As mast cells play important roles in diarrhea, we studied whether allergic diarrhea could be alleviated with imatinib mesylate.

METHODS

Balb/c mice were sensitized and challenged with ovalbumin and treated orally with imatinib. Cytokine mRNA expressions were determined with quantitative RT-PCR and numbers of small intestinal mast cells determined by staining for chloroacetate esterase and mucosal mast cell protease-1. Immunofluorescence staining was used to assess the intestinal CCL1 expression.

KEY RESULTS

Ovalbumin-sensitized and challenged Balb/c mice developed diarrhea, which was associated with increased number of mast cells and expression of interleukin (IL)-4 and -13, and chemokines CCL1 and CCL17 in the small intestine. Treatment with imatinib reduced the incidence of diarrhea, inhibited the development of mastocytosis and jejunal mRNA expression of IL-13, CCL1, CCL17 and CCL22. Mast cell-deficient W/W(-V) mice, and surprisingly, also their mast cell-competent control (+/+) littermates failed to develop diarrhea as a response to ovalbumin. This strain-dependent difference was associated with the inability of +/+ and W/W(-V) mice to increase the number of intestinal mast cells and expression of IL-4, IL-13, CCL1 and CCL17 after ovalbumin challenge.

CONCLUSIONS & INFERENCES: Development of allergic diarrhea is associated with the ability of mice to develop intestinal mastocytosis. Imatinib inhibited the development of intestinal mastocytosis, reduced the incidence of diarrhea, and reduced the expression of IL-13, CCL1, and CCL17. Targeting intestinal mast cells could be a feasible approach to treat allergic diarrhea.

摘要

背景

当 Balb/c 小鼠经皮致敏并用卵清蛋白进行口服挑战时,会发展为变应原诱导性腹泻。由于肥大细胞在腹泻中发挥重要作用,我们研究了甲磺酸伊马替尼是否可以缓解变应性腹泻。

方法

用卵清蛋白对 Balb/c 小鼠进行致敏和挑战,并口服给予伊马替尼进行治疗。通过定量 RT-PCR 测定细胞因子 mRNA 的表达,并通过氯乙酸酯酶染色和黏膜肥大细胞蛋白酶-1 测定来确定小肠肥大细胞的数量。采用免疫荧光染色来评估肠道 CCL1 的表达。

主要结果

卵清蛋白致敏和挑战的 Balb/c 小鼠发生腹泻,其与小肠肥大细胞数量增加以及白细胞介素 (IL)-4 和 -13 和趋化因子 CCL1 和 CCL17 的表达有关。伊马替尼治疗可降低腹泻的发生率,抑制肥大细胞增生以及空肠 IL-13、CCL1、CCL17 和 CCL22 的 mRNA 表达。肥大细胞缺陷型 W/W(-V) 小鼠,以及令人惊讶的是它们的肥大细胞功能正常的对照 (+/+) 同窝仔鼠,在卵清蛋白刺激后也未能发展为腹泻。这种与应变相关的差异与 +/+ 和 W/W(-V) 小鼠在卵清蛋白刺激后无法增加肠道肥大细胞数量和 IL-4、IL-13、CCL1 和 CCL17 的表达有关。

结论

变应性腹泻的发展与小鼠发展肠道肥大细胞的能力有关。伊马替尼抑制了肠道肥大细胞的发展,降低了腹泻的发生率,并降低了 IL-13、CCL1 和 CCL17 的表达。靶向肠道肥大细胞可能是治疗变应性腹泻的可行方法。

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