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首页> 外文期刊>Veterinary Immunology and Immunopathology >Increased type 1 chemokine expression in experimental Chagas disease correlates with cardiac pathology in Beagle dogs
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Increased type 1 chemokine expression in experimental Chagas disease correlates with cardiac pathology in Beagle dogs

机译:实验性Chagas病中1型趋化因子表达增加与Beagle犬的心脏病理相关

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Chemokines and chemokine receptors interaction have presented important role in leukocyte migration to specific immune reaction sites. Recently, it has been reported that chemokine receptors CXC (CXCR3) and CC (CCR5) were preferentially expressed on Th1 cells while CCR3 and CCR4 were preferentially expressed on Th2 cells. This study evaluated the mRNA expression of type 1 and type 2 chemokine and chemokine receptors in the cardiac tissue of Beagle dogs infected with distinct genetic groups of Trypanosoma cruzi (Y, Berenice-78 and ABC strains) during acute and chronic phases. To analyze the correlation between chemokine and chemokine receptors expression and the development of heart pathology, the chronic infected animals were divided into groups, according to the parasite strain and based on the degree of heart damage: cardiac and indeterminate form of Chagas disease. Our results indicated that cardiac type1/2 chemokines and their receptors were partially dependent on the genetic diversity of parasites as well as the polarization of clinical forms. Also, dogs presenting cardiac form showed lower heart tissue mRNA expression of CCL24 (type 2) and higher expression of CCL5, CCL4 and CXCR3 (type 1) when compared with those with indeterminate form of disease. Together, these data reinforce a close-relation between T. cruzi genetic population and the host specific type 1 immune response and, for the first time, we show the distribution of type 1/2 chemokines associated with the development of cardiac pathology using dogs, a well similar model to study human Chagas disease.
机译:趋化因子和趋化因子受体的相互作用在白细胞向特定免疫反应部位的迁移中已经发挥了重要作用。最近,有报道称趋化因子受体CXC(CXCR3)和CC(CCR5)在Th1细胞上优先表达,而CCR3和CCR4在Th2细胞上优先表达。这项研究评估了在急性和慢性期感染了克鲁斯锥虫不同基因组(Y,Berenice-78和ABC株)的比格犬心脏组织中1型和2型趋化因子及趋化因子受体的mRNA表达。为了分析趋化因子和趋化因子受体表达与心脏病理学发展之间的相关性,根据寄生虫品系并根据心脏损害的程度将慢性感染的动物分为几类:恰加斯病和心脏病。我们的结果表明,心脏1/2型趋化因子及其受体部分取决于寄生虫的遗传多样性以及临床形式的分化。同样,与不确定形式的犬相比,呈心脏形式的犬显示出较低的心脏组织mRNA表达,CCL24(2型)和较高的CCL5,CCL4和CXCR3(1型)表达。这些数据共同加强了克鲁氏锥虫遗传种群与宿主特异性1型免疫反应之间的密切关系,并且首次显示了使用狗导致心脏病理发展的1/2型趋化因子的分布,研究人类恰加斯病的模型非常相似。

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