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妊娠期急性病毒感染的固有免疫应答。

Innate Immune Responses to Acute Viral Infection During Pregnancy.

机构信息

Elizabeth Garrett Anderson Institute for Women's Health, University College London, London, United Kingdom.

Center for Infectious Medicine, Department of Medicine Huddinge, Karolinska Institute, Stockholm, Sweden.

出版信息

Front Immunol. 2020 Sep 30;11:572567. doi: 10.3389/fimmu.2020.572567. eCollection 2020.

Abstract

Immunological adaptations in pregnancy allow maternal tolerance of the semi-allogeneic fetus but also increase maternal susceptibility to infection. At implantation, the endometrial stroma, glands, arteries and immune cells undergo anatomical and functional transformation to create the decidua, the specialized secretory endometrium of pregnancy. The maternal decidua and the invading fetal trophoblast constitute a dynamic junction that facilitates a complex immunological dialogue between the two. The decidual and peripheral immune systems together assume a pivotal role in regulating the critical balance between tolerance and defense against infection. Throughout pregnancy, this equilibrium is repeatedly subjected to microbial challenge. Acute viral infection in pregnancy is associated with a wide spectrum of adverse consequences for both mother and fetus. Vertical transmission from mother to fetus can cause developmental anomalies, growth restriction, preterm birth and stillbirth, while the mother is predisposed to heightened morbidity and maternal death. A rapid, effective response to invasive pathogens is therefore essential in order to avoid overwhelming maternal infection and consequent fetal compromise. This sentinel response is mediated by the innate immune system: a heritable, highly evolutionarily conserved system comprising physical barriers, antimicrobial peptides (AMP) and a variety of immune cells-principally neutrophils, macrophages, dendritic cells, and natural killer cells-which express pattern-receptors that detect invariant molecular signatures unique to pathogenic micro-organisms. Recognition of these signatures during acute infection triggers signaling cascades that enhance antimicrobial properties such as phagocytosis, secretion of pro-inflammatory cytokines and activation of the complement system. As well as coordinating the initial immune response, macrophages and dendritic cells present microbial antigens to lymphocytes, initiating and influencing the development of specific, long-lasting adaptive immunity. Despite extensive progress in unraveling the immunological adaptations of pregnancy, pregnant women remain particularly susceptible to certain acute viral infections and continue to experience mortality rates equivalent to those observed in pandemics several decades ago. Here, we focus specifically on the pregnancy-induced vulnerabilities in innate immunity that contribute to the disproportionately high maternal mortality observed in the following acute viral infections: Lassa fever, Ebola virus disease (EVD), dengue fever, hepatitis E, influenza, and novel coronavirus infections.

摘要

妊娠期间的免疫适应性使母体能够耐受半同种异体胎儿,但也增加了母体易感染的风险。在着床时,子宫内膜基质、腺体、动脉和免疫细胞经历解剖和功能转化,形成蜕膜,即妊娠的特化分泌子宫内膜。母体蜕膜和入侵的胎儿滋养层构成了一个动态的连接,促进了两者之间复杂的免疫对话。蜕膜和外周免疫系统共同承担着调节耐受和防御感染之间关键平衡的关键作用。整个妊娠期间,这种平衡反复受到微生物的挑战。妊娠期间的急性病毒感染会给母亲和胎儿带来广泛的不良后果。母婴垂直传播可导致胎儿发育异常、生长受限、早产和死产,而母亲则易患更高的发病率和孕产妇死亡。因此,迅速、有效地应对入侵病原体对于避免母体感染和胎儿受损至关重要。这种哨兵反应是由固有免疫系统介导的:一种遗传的、高度进化保守的系统,包括物理屏障、抗菌肽 (AMP) 和多种免疫细胞——主要是中性粒细胞、巨噬细胞、树突状细胞和自然杀伤细胞——它们表达模式受体,可识别独特的致病微生物的不变分子特征。在急性感染期间,这些特征的识别会触发信号级联反应,增强吞噬作用、促炎细胞因子的分泌和补体系统的激活等抗菌特性。除了协调初始免疫反应外,巨噬细胞和树突状细胞还向淋巴细胞呈递微生物抗原,启动并影响特定的、持久的适应性免疫的发展。尽管在揭示妊娠期间的免疫适应性方面取得了广泛进展,但孕妇仍然特别容易受到某些急性病毒感染的影响,并且仍然经历着与几十年前大流行时相当的死亡率。在这里,我们专门关注妊娠引起的固有免疫脆弱性,这些脆弱性导致以下急性病毒感染中孕产妇死亡率异常高:拉沙热、埃博拉病毒病 (EVD)、登革热、戊型肝炎、流感和新型冠状病毒感染。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1d41/7556209/42b89ef3a5b4/fimmu-11-572567-g0001.jpg

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