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在疟疾攻击临床试验中通过转录组预测RTS,S疫苗介导的保护作用。

Predicting RTS,S Vaccine-Mediated Protection from Transcriptomes in a Malaria-Challenge Clinical Trial.

作者信息

van den Berg Robert A, Coccia Margherita, Ballou W Ripley, Kester Kent E, Ockenhouse Christian F, Vekemans Johan, Jongert Erik, Didierlaurent Arnaud M, van der Most Robbert G

机构信息

GSK Vaccines, Rue de l'Institut, Rixensart, Belgium.

Walter Reed Army Institute of Research, Silver Spring, MD, USA.

出版信息

Front Immunol. 2017 May 23;8:557. doi: 10.3389/fimmu.2017.00557. eCollection 2017.

Abstract

The RTS,S candidate malaria vaccine can protect against controlled human malaria infection (CHMI), but how protection is achieved remains unclear. Here, we have analyzed longitudinal peripheral blood transcriptome and immunogenicity data from a clinical efficacy trial in which healthy adults received three RTS,S doses 4 weeks apart followed by CHMI 2 weeks later. Multiway partial least squares discriminant analysis (N-PLS-DA) of transcriptome data identified 110 genes that could be used in predictive models of protection. Among the 110 genes, 42 had known immune-related functions, including 29 that were related to the NF-κB-signaling pathway and 14 to the IFN-γ-signaling pathway. Post-dose 3 serum IFN-γ concentrations were also correlated with protection; and N-PLS-DA of IFN-γ-signaling pathway transcriptome data selected almost all (44/45) of the representative genes for predictive models of protection. Hence, the identification of the NF-κB and IFN-γ pathways provides further insight into how vaccine-mediated protection may be achieved.

摘要

RTS,S候选疟疾疫苗可预防人体可控疟疾感染(CHMI),但其保护机制尚不清楚。在此,我们分析了一项临床疗效试验中的纵向外周血转录组和免疫原性数据,该试验中健康成年人每隔4周接种3剂RTS,S,2周后进行CHMI。对转录组数据进行多向偏最小二乘判别分析(N-PLS-DA),确定了110个可用于保护预测模型的基因。在这110个基因中,42个具有已知的免疫相关功能,其中29个与NF-κB信号通路相关,14个与IFN-γ信号通路相关。第3剂接种后血清IFN-γ浓度也与保护作用相关;对IFN-γ信号通路转录组数据进行N-PLS-DA,几乎选择了所有(44/45)代表性基因用于保护预测模型。因此,对NF-κB和IFN-γ通路的鉴定为疫苗介导的保护作用实现方式提供了进一步的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b272/5440508/eb67158ead90/fimmu-08-00557-g001.jpg

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