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实验性恰加斯病的免疫病理学:T 细胞与克氏锥虫感染的心脏组织的结合。

Immunopathology of experimental Chagas' disease: binding of T cells to Trypanosoma cruzi-infected heart tissue.

作者信息

Mortatti R C, Maia L C, de Oliveira A V, Munk M E

机构信息

Department of Immunology, Federal University Rio de Janeiro, Brazil.

出版信息

Infect Immun. 1990 Nov;58(11):3588-93. doi: 10.1128/iai.58.11.3588-3593.1990.

Abstract

The immunopathology of Chagas' disease was studied in the experimental model of chronic infection in C57BL/10JT or mice. Sublethal infection with Trypanosoma cruzi, Y strain, induced specific antibodies and a delayed hypersensitivity response to parasite antigens. Mice developed chronic chagasic myocarditis but not skeletal muscle myositis. Binding of T cells to infected heart tissue was investigated during short-term cocultivation of lymphocytes with heart cryostat sections. T cells from infected mice and from normal controls bound equally to myocardium and liver sections from both infected and normal mice. A search in depth was attempted with cells heavily tagged with 99mTc. Labeled T cells from chagasic mice bound to both normal and infected myocardium slices. 99mTc-labeled T cells from controls gave the same binding values. Glass-adherent spleen cells behaved identically to T cells. Prior treatment of the tissue with serum from chronically infected mice did not increase the number of binding cells. Peritoneal macrophages tagged with 99mTc-sulfur colloid also bound to infected myocardium slices. The binding of macrophages was not changed by pretreatment of infected tissue with anti-T, cruzi antibodies. In short, this work did not detect any population of T cells or macrophages which could bind specifically to infected heart tissue to initiate an autoreactive process.

摘要

在C57BL/10JT小鼠慢性感染的实验模型中研究了恰加斯病的免疫病理学。用克氏锥虫Y株进行亚致死感染可诱导特异性抗体以及对寄生虫抗原的迟发型超敏反应。小鼠会发展为慢性恰加斯性心肌炎,但不会出现骨骼肌肌炎。在淋巴细胞与心脏低温切片短期共培养期间,研究了T细胞与受感染心脏组织的结合情况。来自受感染小鼠和正常对照的T细胞与受感染和正常小鼠的心肌和肝脏切片的结合情况相同。尝试用大量标记有99mTc的细胞进行深入研究。来自恰加斯病小鼠的标记T细胞与正常和受感染的心肌切片均有结合。来自对照的99mTc标记T细胞的结合值相同。玻璃黏附的脾细胞表现与T细胞相同。用慢性感染小鼠的血清对组织进行预处理不会增加结合细胞的数量。用99mTc硫胶体标记的腹腔巨噬细胞也与受感染的心肌切片结合。用抗克氏锥虫抗体对受感染组织进行预处理不会改变巨噬细胞的结合情况。简而言之,这项研究未检测到任何能够特异性结合受感染心脏组织以启动自身反应过程的T细胞或巨噬细胞群体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1f57/313702/b3bff0c64f8f/iai00059-0133-a.jpg

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