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吡喹酮通过增强抗蠕虫免疫反应降低母婴死亡率和后代发病率。

Praziquantel Reduces Maternal Mortality and Offspring Morbidity by Enhancing Anti-Helminthic Immune Responses.

机构信息

Technical University of Munich (TUM), School of Medicine, Institute for Med. Microbiology, Immunology and Hygiene, Munich, Germany.

Department of Biosciences, University of Salzburg, Salzburg, Austria.

出版信息

Front Immunol. 2022 Jun 27;13:878029. doi: 10.3389/fimmu.2022.878029. eCollection 2022.

Abstract

Alongside the wide distribution throughout sub Saharan Africa of schistosomiasis, the morbidity associated with this chronic parasitic disease in endemic regions is often coupled with infection-driven immunomodulatory processes which modify inflammatory responses. Early life parasite exposure is theorized to drive immune tolerance towards cognate infection as well as bystander immune responses, beginning with exposure to maternal infection. Considering that 40 million women of childbearing-age are at risk of infection worldwide, treatment with Praziquantel during pregnancy as currently recommended by WHO could have significant impact on disease outcomes in these populations. Here, we describe the effects of anthelminthic treatment on parasite-induced changes to fetomaternal cross talk in a murine model of maternal schistosomiasis. Praziquantel administration immediately prior to mating lead to clear re-awakening of maternal anti-parasite immune responses, with persistent maternal immune activation that included enhanced anti-schistosome cytokine responses. Clearance of parasites also improved capacity of dams to endure the additional pressure of pregnancy during infection. Maternal treatment also drove lasting functional alterations to immune system development of exposed offspring. Prenatal anthelminthic treatment skewed offspring immune responses towards parasite clearance and reduced morbidity during cognate infection. Maternal treatment also restored offspring protective IgE antibody responses directed against schistosome antigens, which were otherwise suppressed following exposure to untreated maternal infection. This was further associated with enhanced anti-schistosome cytokine responses from treatment-exposed offspring during infection. In the absence of cognate infection, exposed offspring further demonstrated imprinting across cellular populations. We provide further evidence that maternal treatment can restore a more normalized immune profile to such offspring exposed to parasite infection, particularly in B cell populations, which may underlie improved responsiveness to cognate infection, and support the WHO recommendation of anthelminthic treatment during pregnancy.

摘要

在撒哈拉以南非洲广泛分布的同时,这种慢性寄生虫病在流行地区与这种疾病相关的发病率常常伴随着感染驱动的免疫调节过程,改变炎症反应。理论上,早期寄生虫暴露会导致对同源感染和旁观者免疫反应的免疫耐受,从暴露于母体感染开始。考虑到全世界有 4000 万育龄妇女面临感染的风险,目前世卫组织建议在怀孕期间用吡喹酮治疗可能会对这些人群的疾病结局产生重大影响。在这里,我们描述了驱虫治疗对母体血吸虫病小鼠模型中胎儿-母体交叉对话中寄生虫诱导的变化的影响。在交配前立即给予吡喹酮治疗,导致母体抗寄生虫免疫反应明显重新激活,持续的母体免疫激活包括增强抗血吸虫细胞因子反应。寄生虫的清除也提高了母体在感染期间耐受怀孕额外压力的能力。母体治疗还导致暴露后代免疫系统发育的持久功能改变。产前驱虫治疗使后代的免疫反应偏向于清除寄生虫,并减少同源感染时的发病率。母体治疗还恢复了针对血吸虫抗原的后代保护性 IgE 抗体反应,否则在接触未经治疗的母体感染后,这种反应会受到抑制。这与治疗暴露的后代在感染期间产生更强的抗血吸虫细胞因子反应进一步相关。在没有同源感染的情况下,暴露的后代在细胞群中进一步表现出印记。我们提供了进一步的证据表明,母体治疗可以使接触寄生虫感染的后代恢复更正常的免疫特征,特别是在 B 细胞群体中,这可能是对同源感染的反应性提高的基础,并支持世卫组织在怀孕期间进行驱虫治疗的建议。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/54a1/9272909/4aa4492ad134/fimmu-13-878029-g001.jpg

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