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实验性自身免疫性心肌炎大鼠心脏浸润T细胞的特征。它们与小鼠胸腺外T细胞的相似性及增殖部位。

Characterization of T cells infiltrating the heart in rats with experimental autoimmune myocarditis. Their similarity to extrathymic T cells in mice and the site of proliferation.

作者信息

Hanawa H, Tsuchida M, Matsumoto Y, Watanabe H, Abo T, Sekikawa H, Kodama M, Zhang S, Izumi T, Shibata A

机构信息

Department of Immunology, Niigata University School of Medicine, Japan.

出版信息

J Immunol. 1993 Jun 15;150(12):5682-95.

PMID:8515083
Abstract

A model of experimental autoimmune myocarditis, which resembles fatal giant cell myocarditis in humans, was previously established in rats immunized by s.c. injection of human cardiac myosin. We characterized herein the surface phenotype of lymphocytes infiltrating the heart and pericardial cavity as well as of mononuclear cells in various organs by using mAb in conjunction with immunofluorescence tests. Since profound thymic atrophy always accompanied the diseased states, attention was focused on characterization of T cells with properties similar to those of extrathymic T cells. In mice, extrathymic T cells were activated in association with thymic atrophy, expressed high levels of LFA-1 and IL-2R beta-chains, and contained a significant proportion of double negative CD4-CD8- T cells. In diseased rats, a large proportion of activated T cells that expressed high levels of LFA-1 and IL-2R was demonstrated in the pericardial effusion and heart tissue. Such T cells were rare in the other organs. Light scatter and microscopic observation revealed that activated lymphoblasts were most abundant in the pericardial effusion. Moreover, one-fourth of such T cells in the pericardial effusion displayed double negative phenotype. These cells in rats might correspond to the extrathymic T cells in mice. However, only a limited population of such activated T cells infiltrated the heart tissue. Concerning the location of such T cells mainly in the outer layer of the heart, it raised the possibility that extrathymic T cell differentiation in these autoimmune rats might occur in the pericardial cavity, and the differentiated cells then migrated to the sites of the cardiac lesion.

摘要

一种实验性自身免疫性心肌炎模型,其类似于人类的致命性巨细胞心肌炎,先前已在通过皮下注射人心脏肌凝蛋白免疫的大鼠中建立。我们在此通过使用单克隆抗体结合免疫荧光试验,对浸润心脏和心包腔的淋巴细胞以及各器官中的单核细胞的表面表型进行了表征。由于严重的胸腺萎缩总是伴随着疾病状态,因此注意力集中在对具有与胸腺外T细胞相似特性的T细胞的表征上。在小鼠中,胸腺外T细胞与胸腺萎缩相关被激活,表达高水平的淋巴细胞功能相关抗原-1(LFA-1)和白细胞介素-2受体β链(IL-2Rβ链),并且含有相当比例的双阴性CD4-CD8-T细胞。在患病大鼠中,在心包积液和心脏组织中证实了很大比例的表达高水平LFA-1和IL-2R的活化T细胞。此类T细胞在其他器官中很少见。光散射和显微镜观察显示,活化的成淋巴细胞在心包积液中最为丰富。此外,心包积液中四分之一的此类T细胞表现出双阴性表型。大鼠中的这些细胞可能与小鼠中的胸腺外T细胞相对应。然而,只有有限数量的此类活化T细胞浸润心脏组织。关于此类T细胞主要位于心脏外层的位置,这增加了这些自身免疫性大鼠中胸腺外T细胞分化可能发生在心包腔中,然后分化细胞迁移至心脏病变部位的可能性。

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