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血液干扰素特征可能将RTS,S重组疟疾疫苗缺乏保护作用与抗原特异性IgE反应联系起来。

Blood Interferon Signatures Putatively Link Lack of Protection Conferred by the RTS,S Recombinant Malaria Vaccine to an Antigen-specific IgE Response.

作者信息

Rinchai Darawan, Presnell Scott, Vidal Marta, Dutta Sheetij, Chauhan Virander, Cavanagh David, Moncunill Gemma, Dobaño Carlota, Chaussabel Damien

机构信息

Sidra Medical and Research Center, Doha, Qatar.

Benaroya Research Institute, Seattle, WA, USA.

出版信息

F1000Res. 2015 Sep 29;4:919. doi: 10.12688/f1000research.7093.2. eCollection 2015.

Abstract

Malaria remains a major cause of mortality and morbidity worldwide. Progress has been made in recent years with the development of vaccines that could pave the way towards protection of hundreds of millions of exposed individuals. Here we used a modular repertoire approach to re-analyze a publically available microarray blood transcriptome dataset monitoring the response to malaria vaccination. We report the seminal identification of interferon signatures in the blood of subjects on days 1, 3 and 14 following administration of the third dose of the RTS,S recombinant malaria vaccine. These signatures at day 1 correlate with protection, and at days 3 and 14 to susceptibility to subsequent challenge of study subjects with live parasites. In addition we putatively link the decreased abundance of interferon-inducible transcripts observed at days 3 and 14 post-vaccination with the elicitation of an antigen-specific IgE response in a subset of vaccine recipients that failed to be protected by the RTS,S vaccine. Furthermore, profiling of antigen-specific levels of IgE in a Mozambican cohort of malaria-exposed children vaccinated with RTS,S identified an association between elevated baseline IgE levels and subsequent development of naturally acquired malaria infection during follow up. Taken together these findings warrant further investigation of the role of antigen-specific IgE in conferring susceptibility to malaria infection.

摘要

疟疾仍然是全球范围内导致死亡和发病的主要原因。近年来,随着疫苗的研发取得进展,有望为数亿易感人群提供保护。在这里,我们采用模块化方法重新分析了一个公开可用的微阵列血液转录组数据集,该数据集监测了对疟疾疫苗接种的反应。我们报告了在接种第三剂RTS,S重组疟疾疫苗后第1天、第3天和第14天,受试者血液中干扰素特征的开创性鉴定。第1天的这些特征与保护相关,而第3天和第14天的特征与研究对象随后受到活寄生虫攻击时的易感性相关。此外,我们推测接种疫苗后第3天和第14天观察到的干扰素诱导转录本丰度降低,与一部分未受到RTS,S疫苗保护的疫苗接种者中抗原特异性IgE反应的激发有关。此外,对莫桑比克一组接种RTS,S疫苗的疟疾暴露儿童的抗原特异性IgE水平进行分析发现,基线IgE水平升高与随访期间自然获得性疟疾感染的后续发生之间存在关联。综上所述,这些发现值得进一步研究抗原特异性IgE在导致疟疾感染易感性方面的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1a93/5580412/104b4d52ae81/f1000research-4-13000-g0000.jpg

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