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基于急性炎症反应性选择的小鼠品系中结肠癌与肺癌发生的反向遗传易感性。

Inverse genetic predisposition to colon versus lung carcinogenesis in mouse lines selected based on acute inflammatory responsiveness.

作者信息

Di Pace Roberto Francisco, Massa Solange, Ribeiro Orlando Garcia, Cabrera Wafa Hanna Koury, De Franco Marcelo, Starobinas Nancy, Seman Michel, Ibañez Olga Célia Martinez

机构信息

Laboratório de Imunogenética, Instituto Butantan, São Paulo, SP, Brazil.

出版信息

Carcinogenesis. 2006 Aug;27(8):1517-25. doi: 10.1093/carcin/bgl080. Epub 2006 Jun 13.

Abstract

Mouse lines produced by bidirectional selection on the basis of maximum (AIRmax) or minimum (AIRmin) acute inflammatory reactions were examined for the development of chemically induced acute colitis and colon tumors and the development of lung tumors. AIRmax mice were more susceptible than AIRmin to acute colitis induced by ingestion of dextran sodium sulfate showing a 3-fold higher disease activity index and presenting an intense inflammatory infiltrate in the base of colon crypts as well as elevated expression of IL-1beta, TNFalpha, IFNgamma and IL-6 mRNA in colon tissue. AIRmax were also more susceptible than AIRmin to colon cancer induced by 2 or 7 weekly doses of 1,2-dimethylhydrazine (DMH), showing significantly higher numbers of colonic aberrant crypt foci (ACF) at 150 days after DMH treatment (P = 0.01) and significantly higher numbers of tumors affecting larger intestinal areas at 300-475 days. At the latter time point, however, multiple lung adenomas and large adenocarcinomas were found in AIRmin but not in AIRmax mice. Treatment of mice with nimesulide for 60 days beginning 24 h before the first of two DMH doses almost completely inhibited the appearance of ACF in both lines. Furthermore, ACF numbers and the degree of acute inflammation directly co-segregated in an F2 (AIRmax x AIRmin) intercross population. The results demonstrate that genetic determinants of the inflammatory response differentially influence susceptibility to colon and lung carcinogenesis in the AIRmax and AIRmin mouse model.

摘要

对基于最大(AIRmax)或最小(AIRmin)急性炎症反应通过双向选择产生的小鼠品系,检测其化学诱导的急性结肠炎和结肠肿瘤的发生情况以及肺肿瘤的发生情况。与AIRmin小鼠相比,AIRmax小鼠对葡聚糖硫酸钠诱导的急性结肠炎更易感,疾病活动指数高出3倍,结肠隐窝底部有强烈的炎性浸润,结肠组织中IL-1β、TNFα、IFNγ和IL-6 mRNA的表达也升高。与AIRmin小鼠相比,AIRmax小鼠对每周2次或7次给予1,2 - 二甲基肼(DMH)诱导的结肠癌也更易感,在DMH治疗后150天,结肠异常隐窝灶(ACF)数量显著更多(P = 0.01),在300 - 475天影响大肠区域的肿瘤数量也显著更多。然而,在后者这个时间点,在AIRmin小鼠中发现了多个肺腺瘤和大腺癌,而AIRmax小鼠中未发现。在两次DMH剂量中的第一次之前24小时开始,用尼美舒利治疗小鼠60天,几乎完全抑制了两个品系中ACF的出现。此外,在F2(AIRmax×AIRmin)杂交群体中,ACF数量和急性炎症程度直接共分离。结果表明,在AIRmax和AIRmin小鼠模型中,炎症反应的遗传决定因素对结肠癌和肺癌发生的易感性有不同影响。

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