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对疟疾有反应的“天然”T细胞:有证据表明免疫交叉反应在维持未接触过疟疾的供体的TCRαβ+疟疾特异性反应中起作用。

'Natural' T cells responsive to malaria: evidence implicating immunological cross-reactivity in the maintenance of TCR alpha beta+ malaria-specific responses from non-exposed donors.

作者信息

Currier J, Sattabongkot J, Good M F

机构信息

Queensland Institute of Medical Research, Bancroft Centre, Brisbane, Australia.

出版信息

Int Immunol. 1992 Sep;4(9):985-94. doi: 10.1093/intimm/4.9.985.

Abstract

It is now generally accepted that peripheral blood of humans not exposed previously to malaria contains T cells which proliferate vigorously in response to malaria parasites and antigens. Although it has been claimed that these cells express a memory phenotype, their origin is uncertain. We have examined the phenotype and immunological responses of such cells. We confirm that these cells do express the 'memory phenotype', CD45Ro, in that depletion of such cells, but not of CD45Ra (virgin) cells, abrogates the immune response to malaria parasites. In an effort to define the genesis of these responses, numerous malaria-specific T cell clones have been generated from non-exposed individuals. These were tested for reactivity to a large panel of common bacterial, viral, and fungal pathogenic and non-pathogenic organisms. Most clones proliferated vigorously in response to one or more such organisms, while many clones demonstrated smaller but significant degrees of proliferation in response to many different organisms. Our data offers insights into the maintenance of immunological memory. All clones examined were CD3+, CD4+, CD8-, TCR alpha beta+, and TCR delta-. The ratio of TCR alpha beta+ to TCR delta+ cells among peripheral blood lymphocytes increased during polyclonal culture in the presence of parasite. The high frequency of such cells in peripheral blood (1/800-1/9000), and their response to a wide range of geographically different Plasmodium falciparum isolates and clones by both proliferation and lymphokine secretion (predominantly IFN-gamma) with a high degree of sensitivity (less than 1 parasite/microliters blood in some cases) suggests that these cells must be quickly activated following malaria infection. Their contribution to the outcome of the disease (protection/immunopathology) may be significant.

摘要

目前普遍认为,未曾接触过疟疾的人类外周血中含有T细胞,这些T细胞会对疟原虫和抗原产生强烈增殖反应。尽管有人声称这些细胞表达记忆表型,但其来源尚不确定。我们已经研究了此类细胞的表型和免疫反应。我们证实这些细胞确实表达“记忆表型”CD45Ro,因为去除此类细胞而非CD45Ra(初始)细胞会消除对疟原虫的免疫反应。为了确定这些反应的起源,已从未接触过疟疾的个体中产生了许多疟疾特异性T细胞克隆。对这些克隆进行了测试,以检测它们对大量常见细菌、病毒和真菌病原体及非病原体的反应性。大多数克隆对一种或多种此类生物体产生强烈增殖反应,而许多克隆对许多不同生物体表现出较小但显著的增殖程度。我们的数据为免疫记忆的维持提供了见解。所有检测的克隆均为CD3+、CD4+、CD8-、TCRαβ+和TCRδ-。在存在寄生虫的情况下进行多克隆培养期间,外周血淋巴细胞中TCRαβ+与TCRδ+细胞的比例增加。外周血中此类细胞的高频率(1/800 - 1/9000),以及它们通过增殖和淋巴因子分泌(主要是IFN-γ)对广泛地理区域不同的恶性疟原虫分离株和克隆作出反应,且具有高度敏感性(在某些情况下每微升血液中寄生虫少于1个),这表明这些细胞在疟疾感染后必须迅速被激活。它们对疾病结局(保护/免疫病理)的贡献可能很大。

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