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A role for an animal model in determining the immune mechanisms involved in the pathogenesis of rheumatic heart disease

机译:动物模型在确定涉及风湿性心脏病发病机制的免疫机制方面的作用

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Rheumatic heart disease (RHD) is an autoimmune disease mediated by group A streptococcal (GAS) infection. To study the immune mechanisms underlying RHD, a robust animal model with immunopathology similar to that seen in humans is essential. A Lewis rat model of autoimmune valvulitis has been shown to have potential in investigating the immunopathogenesis of RHD. In our studies, rats immunized with M protein C-region peptides developed cardiac lesions reflective of those seen in RHD patients, including mononuclear cell infiltration, granuloma formation and valvulitis. Furthermore, mononuclear cells sensitized to cardiac myosin extracted from rat heart lesions were shown to be cross-reactive with streptococcal M protein. These data add further support for using the Lewis rat model for investigating the cell-mediated responses involved in RHD and for testing the safety of GAS peptide-based vaccine candidates.
机译:风湿性心脏病(RHD)是由组链球菌(气体)感染介导的自身免疫性疾病。为了研究RHD的免疫机制,具有类似于人类免疫病理学的强大动物模型至关重要。已经显示出自身免疫胰腺炎的Lewis大鼠模型具有调查RHD免疫病理学的潜力。在我们的研究中,用M蛋白C区肽免疫的大鼠发生了反射RHD患者中的那些的心脏病变,包括单核细胞浸润,肉芽肿形成和valvulitis。此外,向从大鼠心脏病变中提取的心脏肌蛋白致敏的单核细胞被显示为与链球菌M蛋白的交叉反应。这些数据增加了使用Lewis大鼠模型来研究RHD中涉及的细胞介导的响应以及用于测试基于气体肽的疫苗候选物的安全性。

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