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人类T细胞对疟原虫环子孢子蛋白多态性表位的识别。

Human T cell recognition of polymorphic epitopes from malaria circumsporozoite protein.

作者信息

de Groot A S, Johnson A H, Maloy W L, Quakyi I A, Riley E M, Menon A, Banks S M, Berzofsky J A, Good M F

机构信息

Laboratory of Parasitic Diseases, National Institutes of Allergy and Infectious Disease, Bethesda, MD 20892.

出版信息

J Immunol. 1989 Jun 1;142(11):4000-5.

PMID:2469729
Abstract

Lymphocytes obtained from forty individuals living in a malaria endemic area of West Africa were tested for in vitro proliferative responses to peptides representing variant regions of the immunodominant T cell domain of the circumsporozoite protein (amino acids 326 to 345, referred to as Th2R, and 361 to 380, referred to as Th3R) from three distinct strains of Plasmodium falciparum. A total of 83% of the individuals responded to at least one of the six peptides tested, confirming that these epitopes are immunodominant. A much greater number of individuals than expected by chance (32% of the responders to Th2R and 27% of the responders to Th3R) reacted to all three of the variant peptides for that epitope, indicating interdependency of the T cell responses, suggestive of cross-reactivity. Nevertheless, some subjects' T cells were clearly able to distinguish each variant peptide from the others. Using EBV transformed B cells, lymphocytes from 10 of the individuals were HLA typed. In this small group, HLA DRw13 was associated with a positive response to any of the peptides, whereas there was a negative association between DQw3 and response to any of the peptides. These results, although limited by the small sample size, suggest that recognition of T epitopes may be Ir gene linked. Our findings suggest that it may be possible to broaden the immunogenicity of an anti-sporozoite malaria vaccine.

摘要

从生活在西非疟疾流行地区的40个人身上获取淋巴细胞,检测其对来自三种不同恶性疟原虫菌株的环子孢子蛋白免疫显性T细胞结构域变异区(氨基酸326至345,称为Th2R,以及361至380,称为Th3R)肽段的体外增殖反应。共有83%的个体对所检测的六种肽段中的至少一种有反应,证实这些表位具有免疫显性。对该表位的所有三种变异肽有反应的个体数量比随机预期的要多得多(对Th2R有反应的个体中32%,对Th3R有反应的个体中27%),表明T细胞反应存在相互依赖性,提示存在交叉反应性。然而,一些受试者的T细胞显然能够区分每种变异肽。使用EBV转化的B细胞,对其中10个人的淋巴细胞进行了HLA分型。在这个小群体中,HLA DRw13与对任何肽段的阳性反应相关,而DQw3与对任何肽段的反应之间存在负相关。这些结果虽然受样本量小的限制,但表明T表位的识别可能与Ir基因相关。我们的发现表明,有可能扩大抗子孢子疟疾疫苗的免疫原性。

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