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沙门氏菌诱导一种无生发中心的转换抗体反应,这种反应会阻碍感染在细胞外的传播。

Salmonella induces a switched antibody response without germinal centers that impedes the extracellular spread of infection.

作者信息

Cunningham Adam F, Gaspal Fabrina, Serre Karine, Mohr Elodie, Henderson Ian R, Scott-Tucker Anthony, Kenny Sinead M, Khan Mahmood, Toellner Kai-Michael, Lane Peter J L, MacLennan Ian C M

机构信息

Medical Research Council Centre for Immune Regulation, University of Birmingham, Birmingham, United Kingdom.

出版信息

J Immunol. 2007 May 15;178(10):6200-7. doi: 10.4049/jimmunol.178.10.6200.

Abstract

T-dependent Ab responses are characterized by parallel extrafollicular plasmablast growth and germinal center (GC) formation. This study identifies that, in mice, the Ab response against Salmonella is novel in its kinetics and its regulation. It demonstrates that viable, attenuated Salmonella induce a massive early T-dependent extrafollicular response, whereas GC formation is delayed until 1 mo after infection. The extrafollicular Ab response with switching to IgG2c, the IgG2a equivalent in C57BL/6 mice, is well established by day 3 and persists through 5 wk. Switching is strongly T dependent, and the outer membrane proteins are shown to be major targets of the early switched IgG2c response, whereas flagellin and LPS are not. GC responses are associated with affinity maturation of IgG2c, and their induction is associated with bacterial burden because GC could be induced earlier by treating with antibiotics. Clearance of these bacteria is not a consequence of high-affinity Ab production, for clearance occurs equally in CD154-deficient mice, which do not develop GC, and wild-type mice. Nevertheless, transferred low- and high-affinity IgG2c and less efficiently IgM were shown to impede Salmonella colonization of splenic macrophages. Furthermore, Ab induced during the infection markedly reduces bacteremia. Thus, although Ab does not prevent the progress of established splenic infection, it can prevent primary infection and impedes secondary hemogenous spread of the disease. These results may explain why attenuated Salmonella-induced B cell responses are protective in secondary, but not primary infections.

摘要

T 细胞依赖性抗体反应的特征是滤泡外浆母细胞平行生长和生发中心(GC)形成。本研究发现,在小鼠中,针对沙门氏菌的抗体反应在动力学和调节方面具有新颖性。研究表明,活的减毒沙门氏菌诱导大量早期 T 细胞依赖性滤泡外反应,而生发中心形成则延迟至感染后 1 个月。到第 3 天时,向 IgG2c(C57BL/6 小鼠中的 IgG2a 等效物)转换的滤泡外抗体反应已充分建立,并持续 5 周。转换强烈依赖 T 细胞,外膜蛋白被证明是早期转换的 IgG2c 反应的主要靶标,而鞭毛蛋白和脂多糖则不是。生发中心反应与 IgG2c 的亲和力成熟相关,其诱导与细菌负荷有关,因为用抗生素治疗可更早诱导生发中心。这些细菌的清除不是高亲和力抗体产生的结果,因为在不形成生发中心的 CD154 缺陷小鼠和野生型小鼠中清除情况相同。然而,转移的低亲和力和高亲和力 IgG2c 以及效率较低的 IgM 被证明可阻碍沙门氏菌在脾巨噬细胞中的定植。此外,感染期间诱导的抗体可显著降低菌血症。因此,尽管抗体不能阻止已建立的脾脏感染的进展,但它可以预防原发性感染并阻碍疾病的继发性血行播散。这些结果可能解释了为什么减毒沙门氏菌诱导的 B 细胞反应在继发性感染中具有保护作用,但在原发性感染中则不然。

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