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疟疾外抗原诱导非T细胞依赖性抗体,该抗体可阻断其诱导肿瘤坏死因子的能力。

Malaria exoantigens induce T-independent antibody that blocks their ability to induce TNF.

作者信息

Bate C A, Taverne J, Davé A, Playfair J H

机构信息

Department of Immunology, University College & Middlesex School of Medicine, London.

出版信息

Immunology. 1990 Jul;70(3):315-20.

Abstract

Much of the pathology of malaria may be due to the interactions of cytokines, especially tumour necrosis factor (TNF), with various cell types, including endothelial cells, with consequent widespread systemic effects. It has been shown previously that heat-stable exoantigens in the supernatants of blood-stage parasite cultures induced the release of TNF in vitro from activated macrophages and behaved like toxins in vivo, that mice immunized with the antigens are protected from the toxic effect and that their serum specifically blocks the ability of the antigens to stimulate the production of TNF. It is reported here that the inhibitory antibody is mainly IgM and that it appears to be T-independent, as the titres of antisera from T-deficient and immunologically intact mice were similar. Antisera raised against exoantigens from two species of rodent parasite inhibited TNF production by those of the human parasite Plasmodium falciparum, and vice versa, indicating that the TNF-inducing moieties of the exoantigens cross-react and therefore presumably contain common epitopes. Thus vaccination with these exoantigens might provide a means of protection against the clinical effects of malaria and of generating anti-disease immunity by reducing cytokine production. However, these findings imply that it will be necessary to confer on these antigens the ability to stimulate T cells and generate memory before they can provide a useful basis for an anti-disease vaccine. The results obtained are discussed in relation to some of the epidemiological features of malaria.

摘要

疟疾的许多病理变化可能归因于细胞因子,尤其是肿瘤坏死因子(TNF)与包括内皮细胞在内的各种细胞类型的相互作用,从而产生广泛的全身效应。先前已表明,血液阶段寄生虫培养上清液中的热稳定外抗原在体外可诱导活化巨噬细胞释放TNF,且在体内表现得像毒素,用这些抗原免疫的小鼠可免受毒性作用,并且它们的血清能特异性阻断抗原刺激TNF产生的能力。本文报道,抑制性抗体主要是IgM,并且它似乎是不依赖T细胞的,因为来自T细胞缺陷小鼠和免疫功能正常小鼠的抗血清效价相似。针对两种啮齿动物寄生虫外抗原产生的抗血清可抑制人类寄生虫恶性疟原虫外抗原诱导的TNF产生,反之亦然,这表明外抗原中诱导TNF产生的部分会发生交叉反应,因此推测含有共同表位。因此,用这些外抗原进行疫苗接种可能提供一种预防疟疾临床效应的方法,并通过减少细胞因子的产生来产生抗疾病免疫力。然而,这些发现意味着在这些抗原能够为抗疾病疫苗提供有用基础之前,有必要赋予它们刺激T细胞并产生记忆的能力。结合疟疾的一些流行病学特征对所得结果进行了讨论。

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