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细菌脂蛋白通过 Toll 样受体 2 调节人原发性和记忆性 CD4+T 和 B 细胞对肺炎球菌蛋白抗原的反应。

Bacterial lipoproteins differentially regulate human primary and memory CD4+ T and B cell responses to pneumococcal protein antigens through Toll-like receptor 2.

机构信息

Department of Cellular and Molecular Medicine, University of Bristol, Bristol, UK.

出版信息

J Infect Dis. 2010 Jun 1;201(11):1753-63. doi: 10.1086/652495.

Abstract

BACKGROUND

Bacterial lipoproteins (BLPs) are expressed across a range of bacteria and are able to activate Toll-like receptor 2 (TLR-2). BLPs enhance immune responses in naive individuals and have therefore been tested as candidate vaccine adjuvants. It is not known whether BLPs affect any preexisting immunity (eg, memory cell response in primed individuals). Colonization with pneumococcus (PNC), which primes for memory cell response, is common in young children.

METHODS

We studied effects of BLPs on memory and primary B and CD4+ T cell responses to pneumococcal proteins using adenoidal cells from children.

RESULTS

Although BLPs enhanced the primary antibody responses seen in some children with no detectable nasal PNC, BLPs unexpectedly reduced the memory antibody responses in children with positive nasal culture results. Likewise, BLPs augmented the naive but inhibited the memory antigen-driven CD4+ T cell response. The downregulation of the memory responses was associated with increases in interleukin 10 and inducible costimulatory molecule expression, as well as a decrease in CD28 expression in memory CD4+ T cells; all were blocked by anti-TLR2 and anti-B7h antibodies. Augmentation of naive CD4+ T cell proliferation was blocked by anti-B7.2.

CONCLUSION

Differential regulation of primary and memory responses by BLPs through TLR2 may have important implications for therapeutic and vaccination strategies against bacterial infection.

摘要

背景

细菌脂蛋白 (BLPs) 在多种细菌中表达,能够激活 Toll 样受体 2 (TLR-2)。BLPs 增强了未致敏个体的免疫反应,因此已被测试作为候选疫苗佐剂。目前尚不清楚 BLPs 是否会影响任何预先存在的免疫(例如,已致敏个体的记忆细胞反应)。肺炎球菌(PNC)定植,可诱导记忆细胞反应,在幼儿中很常见。

方法

我们使用儿童的腺样体细胞研究了 BLPs 对肺炎球菌蛋白的记忆和原发性 B 和 CD4+T 细胞反应的影响。

结果

尽管 BLPs 增强了一些未检测到鼻 PNC 的儿童的初级抗体反应,但 BLPs 出人意料地降低了鼻培养阳性儿童的记忆抗体反应。同样,BLPs 增强了幼稚但抑制了记忆抗原驱动的 CD4+T 细胞反应。记忆反应的下调与白细胞介素 10 和诱导型共刺激分子表达的增加以及记忆 CD4+T 细胞中 CD28 表达的降低有关;所有这些都被 TLR2 和 B7h 抗体阻断。幼稚 CD4+T 细胞增殖的增强被抗 B7.2 阻断。

结论

BLPs 通过 TLR2 对原发性和记忆反应的差异调节可能对针对细菌感染的治疗和疫苗接种策略具有重要意义。

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