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人体口服霍乱疫苗一年后血液中循环的霍乱抗毒素记忆细胞。

Circulating cholera antitoxin memory cells in the blood one year after oral cholera vaccination in humans.

作者信息

Lycke N, Hellström U, Holmgren J

出版信息

Scand J Immunol. 1987 Aug;26(2):207-11. doi: 10.1111/j.1365-3083.1987.tb02253.x.

Abstract

Oral vaccination with the combined B subunit/whole cell cholera vaccine generates antitoxin memory cells that could be isolated from peripheral blood for at least 1 year after immunization. These memory cells were triggered by antigen in vitro to produce antitoxin in the presence of autologous T cells and monocytes. Antitoxin-producing peripheral blood lymphocytes (PBL) were found in 4 out of 5 previously vaccinated subjects. IgA and IgM isotypes dominated the memory response. The antigen-dose dependency and requirements for a specific ratio of T to B cells for activation of the memory cells in vitro implies T-cell control of antitoxin responses. These antitoxin memory cells in peripheral blood (and corresponding antibacterial memory cells) might represent a pool of circulating cells that on renewed exposure to cholera rapidly produce protective antibody in the gut and thus might have a central role in the long-term protection against reinfection and disease seen in convalescents from cholera.

摘要

口服B亚单位/全细胞霍乱联合疫苗可产生抗毒素记忆细胞,免疫后至少1年内可从外周血中分离到这些细胞。这些记忆细胞在体外被抗原触发,在自体T细胞和单核细胞存在的情况下产生抗毒素。在5名先前接种过疫苗的受试者中,有4名发现了产生抗毒素的外周血淋巴细胞(PBL)。IgA和IgM同种型在记忆反应中占主导地位。体外激活记忆细胞对抗原剂量的依赖性以及对T细胞与B细胞特定比例的要求意味着抗毒素反应受T细胞控制。外周血中的这些抗毒素记忆细胞(以及相应的抗菌记忆细胞)可能代表了一组循环细胞,再次接触霍乱时它们会在肠道中迅速产生保护性抗体,因此可能在长期预防霍乱康复者再次感染和发病方面发挥核心作用。

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