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人源日本血吸虫卵抗原特异性T细胞系和克隆的产生及功能特性分析

Generation and functional characterization of T cell lines and clones specific for Schistosoma japonicum egg antigen in humans.

作者信息

Ohta N, Edahiro T, Tohgi N, Ishii A, Minai M, Hosaka Y

机构信息

Department of Parasitology, Okayama University Medical School, Japan.

出版信息

J Immunol. 1988 Oct 1;141(7):2445-50.

PMID:2459210
Abstract

T cell lines specific for Schistosoma japonicum egg Ag were established in vitro from patients with chronic schistosomiasis japonica, and investigated their possible immunopathologic roles by testing lymphokines production and in vitro granuloma formation assay. All lines tested had surface phenotypes of CD3+ CD4+ CD8-, and showed S. japonicum soluble egg Ag (SEA)-specific proliferation requiring HLA-DR-restricted Ag presentation. Of these fractions of SEA separated by gel filtration, Fraction II (m.w. 7,000 to 18,000) and III (m.w. 7,000) induced strong proliferation of T cell lines, whereas fraction I (m.w. 18,000+) failed to induce detectable proliferation to any T cell lines tested. One of the T cell lines was cloned by micromanipulation: two of eight clones responded only to fraction II, and six to both fractions II and III. We observed that four of eight clones tested produced IL-2 in response to SEA, and three of them were able to transfer S. japonicum egg-specific granulomatous hypersensitivity in vitro to an HLA haplo-identical individual without previous schistosome infection. These immunopathologic functions of T cell clones seemed to be activated by at least two distinct epitopes of SEA. Our present observations suggest that at least two distinct CD4+ human T cells, both of which recognize epitopes expressed on SEA molecules of less than 18 kDa, might have critical roles in granulomatous hypersensitivity to eggs of S. japonicum in humans.

摘要

从慢性日本血吸虫病患者体内体外建立了针对日本血吸虫虫卵抗原的T细胞系,并通过检测细胞因子产生和体外肉芽肿形成试验研究了它们可能的免疫病理作用。所有检测的细胞系均具有CD3 + CD4 + CD8 - 的表面表型,并显示出日本血吸虫可溶性虫卵抗原(SEA)特异性增殖,这需要HLA - DR限制的抗原呈递。在通过凝胶过滤分离的SEA这些组分中,组分II(分子量7,000至18,000)和III(分子量7,000)诱导T细胞系强烈增殖,而组分I(分子量18,000 +)未能诱导对任何测试的T细胞系产生可检测到的增殖。其中一个T细胞系通过显微操作进行克隆:八个克隆中有两个仅对组分II有反应,六个对组分II和III都有反应。我们观察到,测试的八个克隆中有四个在接触SEA后产生IL - 2,其中三个能够在体外将日本血吸虫虫卵特异性肉芽肿超敏反应转移给一个没有血吸虫感染史的HLA单倍型相同的个体。T细胞克隆的这些免疫病理功能似乎被SEA的至少两个不同表位激活。我们目前的观察结果表明,至少两种不同的CD4 + 人T细胞,它们都识别分子量小于18 kDa的SEA分子上表达的表位,可能在人类对日本血吸虫虫卵的肉芽肿超敏反应中起关键作用。

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