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血清免疫球蛋白A对黏膜疾病作出反应,对细菌肠毒素进行选择性中和。

Selective neutralization of a bacterial enterotoxin by serum immunoglobulin A in response to mucosal disease.

作者信息

Johnson S, Sypura W D, Gerding D N, Ewing S L, Janoff E N

机构信息

Department of Medicine, Veterans Affairs Medical Center, Minneapolis, Minnesota 55417, USA.

出版信息

Infect Immun. 1995 Aug;63(8):3166-73. doi: 10.1128/iai.63.8.3166-3173.1995.

Abstract

One-third of convalescent-phase serum samples (6 of 18) from patients with Clostridium difficle-associated diarrhea demonstrated neutralization of the clostridial enterotoxin, toxin A. Although appreciable amounts of toxin A-specific immunoglobulin G (IgG) and IgA were present in these sera, the ability to neutralize the cytotoxic activity of toxin A on OTF9-63 cells in vitro was confined to the IgA fraction and the IgA1 subclass in serum samples from all six patients. In contrast to the patients with C. difficile diarrhea, this activity was present in both the IgA and IgG fractions in sera from two C. difficile-infected patients without diarrhea, one of whom presented with a splenic abscess. Sera and purified IgA which neutralized the cytotoxicity of toxin A on OTF9-63 cell cultures in vitro also neutralized the enterotoxicity of toxin A in rabbit ileal loops in vivo. This activity was not Fc dependent, since IgA retained neutralizing activity after pepsin digestion and F(ab')2 purification. The transition from nonneutralizing toxin A-specific IgA in the acute-phase sera to neutralizing specific IgA in the convalescent-phase sera was accompanied by a shift from a polymeric to a predominantly monomeric form of specific IgA. However, the neutralizing activity in convalescent-phase sera was present as both monomeric and polymeric IgA. Convalescent-phase sera from other patients with C. difficile diarrhea that failed to neutralize toxin A also failed to produce a predominantly monomeric-form specific IgA response. We conclude that serum IgA, not IgG, characteristically neutralizes toxin A in patients with C. difficile diarrhea who develop neutralizing systemic responses. This neutralization of an enteric bacterial toxin is a unique and selective role for serum IgA which provides a novel functional link between the systemic and mucosal immune systems.

摘要

艰难梭菌相关性腹泻患者恢复期血清样本中有三分之一(18份中的6份)表现出对梭菌肠毒素A的中和作用。尽管这些血清中存在大量毒素A特异性免疫球蛋白G(IgG)和IgA,但体外中和毒素A对OTF9 - 63细胞细胞毒性活性的能力仅限于所有6名患者血清样本中的IgA组分和IgA1亚类。与艰难梭菌腹泻患者不同,两名无腹泻的艰难梭菌感染患者血清中的IgA和IgG组分均有此活性,其中一名患者患有脾脓肿。体外中和毒素A对OTF9 - 63细胞培养物细胞毒性的血清和纯化IgA,在体内兔回肠袢中也能中和毒素A的肠毒性。该活性不依赖Fc,因为IgA在胃蛋白酶消化和F(ab')2纯化后仍保留中和活性。急性期血清中无中和作用的毒素A特异性IgA向恢复期血清中中和特异性IgA的转变伴随着特异性IgA从多聚体形式向主要单体形式的转变。然而,恢复期血清中的中和活性以单体和多聚体IgA形式存在。其他未中和毒素A的艰难梭菌腹泻患者的恢复期血清也未能产生主要为单体形式的特异性IgA反应。我们得出结论,在产生中和性全身反应的艰难梭菌腹泻患者中,血清IgA而非IgG具有特征性地中和毒素A的作用。这种对肠道细菌毒素的中和是血清IgA独特且选择性的作用,它在全身和黏膜免疫系统之间提供了一种新的功能联系。

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