Infectious episodes during pregnancy, at particular mucosal sites, increase specific IgA1 or IgA2 subtype levels in human colostrum.

Maternal health, neonatology and perinatology Pub Date : 2019-06-11 eCollection Date: 2019-01-01 DOI:10.1186/s40748-019-0104-x
Erick Sánchez-Salguero, Geovanni Kaleb Mondragón-Ramírez, Julio C Alcántara-Montiel, Arturo Cérbulo-Vázquez, Xóchitl Villegas-Domínguez, Víctor Manuel Contreras-Vargas, María Del Rocío Thompson-Bonilla, Héctor Romero-Ramírez, Leopoldo Santos-Argumedo
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引用次数: 10

Abstract

Background: Colostrum is the primary source of maternal immunoglobulin A (IgA) for the newborn. IgA participates in protection and regulation mechanisms of the immune response at the neonate's mucosa. Several studies have evaluated infectious diseases and vaccine protocols effects during pregnancy on maternal milk IgA levels, with the aim to understand lactation protecting effect on newborn. However, most of their results demonstrated that there were no differences in the total IgA levels. In humans, IgA has two subclasses (IgA1 and IgA2), they have an anatomical distribution among mucosal compartments, their levels vary after antigen stimulation and are also seen to describe differential affinities in colostrum. Although there are differences between IgA subclasses in several compartments, these studies have excluded specific colostrum IgA1 and IgA2 determination.

Methods: We analyzed data from 900 women in Mexico City. With Pearson correlation, we compared the number of infectious episodes during their pregnancy that was associated with mucosal compartments (skin, respiratory and gastrointestinal tracts) and colostrum IgA subclasses.

Results: We show a correlation between increased colostrum IgA1 levels and the number of infectious episodes at respiratory tract and the skin. In contrast, infections at the gastrointestinal tract correlated with increased IgA2 amounts.

Conclusions: Infections present during pregnancy at certain mucosal site increase specific IgA subclasses levels in human colostrum. These results will help in understanding infections and immunizations effects on maternal IgA at the mammary gland, and their impact on the development and protection of the newborn.

Abstract Image

Abstract Image

Abstract Image

妊娠期感染发作,在特定的粘膜部位,增加人类初乳中特异性IgA1或IgA2亚型水平。
背景:初乳是新生儿母体免疫球蛋白A (IgA)的主要来源。IgA参与新生儿黏膜免疫应答的保护和调节机制。一些研究评估了怀孕期间传染性疾病和疫苗方案对母乳IgA水平的影响,目的是了解哺乳对新生儿的保护作用。然而,他们的大多数结果表明,总IgA水平没有差异。在人类中,IgA有两个亚类(IgA1和IgA2),它们在粘膜间室中有解剖分布,它们的水平在抗原刺激后变化,也被认为描述了初乳的不同亲和力。尽管在几个隔室中存在不同的IgA亚类,但这些研究排除了特异性初乳IgA1和IgA2的测定。方法:我们分析了来自墨西哥城的900名妇女的数据。通过Pearson相关性,我们比较了怀孕期间与粘膜室(皮肤、呼吸道和胃肠道)和初乳IgA亚类相关的感染发作次数。结果:我们发现初乳IgA1水平升高与呼吸道和皮肤感染发作次数之间存在相关性。相反,胃肠道感染与IgA2含量增加相关。结论:妊娠期间某些粘膜部位的感染增加了人初乳中特异性IgA亚类的水平。这些结果将有助于了解感染和免疫对母体乳腺IgA的影响,以及它们对新生儿发育和保护的影响。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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