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微生物组与补体激活:早产的一种机制模型。

The Microbiome and Complement Activation: A Mechanistic Model for Preterm Birth.

作者信息

Dunn Alexis B, Dunlop Anne L, Hogue Carol J, Miller Andrew, Corwin Elizabeth J

机构信息

1 Nell Hodgson Woodruff School of Nursing, Emory University, Atlanta, GA, USA.

2 Rollins School of Public Health, Emory University, Atlanta, GA, USA.

出版信息

Biol Res Nurs. 2017 May;19(3):295-307. doi: 10.1177/1099800416687648. Epub 2017 Jan 11.

Abstract

Preterm birth (PTB, <37 completed weeks' gestation) is one of the leading obstetrical problems in the United States, affecting approximately one of every nine births. Even more concerning are the persistent racial disparities in PTB, with particularly high rates among African Americans. There are several recognized pathophysiologic pathways to PTB, including infection and/or exaggerated systemic or local inflammation. Intrauterine infection is a causal factor linked to PTB thought to result most commonly from inflammatory processes triggered by microbial invasion of bacteria ascending from the vaginal microbiome. Trials to treat various infections have shown limited efficacy in reducing PTB risk, suggesting that other complex mechanisms, including those associated with inflammation, may be involved in the relationship between microbes, infection, and PTB. The complement system, a key mediator of the inflammatory response, is an innate defense mechanism involved in both normal physiologic processes that occur during pregnancy implantation and processes that promote the elimination of pathogenic microbes. Recent research has demonstrated an association between this system and PTB. The purpose of this article is to present a mechanistic model of inflammation-associated PTB, which hypothesizes a relationship between the microbiome and dysregulation of the complement system. Exploring the relationships between the microbial environment and complement biomarkers may elucidate a potentially modifiable biological pathway to PTB.

摘要

早产(PTB,妊娠<37 足周)是美国主要的产科问题之一,约每九例分娩中就有一例受其影响。更令人担忧的是早产方面持续存在的种族差异,非裔美国人的早产率尤其高。早产有几种公认的病理生理途径,包括感染和/或全身性或局部炎症反应过度。宫内感染是与早产相关的一个致病因素,一般认为其最常见的起因是阴道微生物群中的细菌上行引发的炎症过程。治疗各种感染的试验在降低早产风险方面显示出有限的疗效,这表明包括与炎症相关的机制在内的其他复杂机制可能参与了微生物、感染与早产之间的关系。补体系统是炎症反应的关键介质,是一种先天性防御机制,参与妊娠着床期间发生的正常生理过程以及促进清除致病微生物的过程。最近的研究表明该系统与早产之间存在关联。本文旨在提出一种与炎症相关的早产的机制模型,该模型假设微生物群与补体系统失调之间存在关联。探索微生物环境与补体生物标志物之间的关系可能会阐明一条潜在的、可改变的早产生物学途径。

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Diversity of the vaginal microbiome correlates with preterm birth.阴道微生物组的多样性与早产相关。
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A critical role of interleukin-1 in preterm labor.白细胞介素-1 在早产中的关键作用。
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The relationship of circulating proteins in early pregnancy with preterm birth.孕早期循环蛋白与早产的关系。
Am J Obstet Gynecol. 2016 Apr;214(4):517.e1-517.e8. doi: 10.1016/j.ajog.2015.11.001. Epub 2015 Nov 11.
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Temporal and spatial variation of the human microbiota during pregnancy.孕期人类微生物群的时空变化
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Is preterm birth a human-specific syndrome?早产是人类特有的综合征吗?
Evol Med Public Health. 2015 Jun 14;2015(1):136-48. doi: 10.1093/emph/eov010.
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The complement system and adverse pregnancy outcomes.补体系统与不良妊娠结局
Mol Immunol. 2015 Sep;67(1):56-70. doi: 10.1016/j.molimm.2015.02.030. Epub 2015 Mar 21.
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Births: final data for 2013.出生情况:2013年最终数据。
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