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利用计算机器学习工具来理解 CD8 T 细胞介导的 HIV 反应背景下的免疫广度。

Utilizing Computational Machine Learning Tools to Understand Immunogenic Breadth in the Context of a CD8 T-Cell Mediated HIV Response.

机构信息

IAVI Human Immunology Laboratory, Imperial College, London, United Kingdom.

Cancer Evolution and Genome Instability Laboratory, Francis Crick Institute, London, United Kingdom.

出版信息

Front Immunol. 2021 Feb 18;12:609884. doi: 10.3389/fimmu.2021.609884. eCollection 2021.

Abstract

Predictive models are becoming more and more commonplace as tools for candidate antigen discovery to meet the challenges of enabling epitope mapping of cohorts with diverse HLA properties. Here we build on the concept of using two key parameters, diversity metric of the HLA profile of individuals within a population and consideration of sequence diversity in the context of an individual's CD8 T-cell immune repertoire to assess the HIV proteome for defined regions of immunogenicity. Using this approach, analysis of HLA adaptation and functional immunogenicity data enabled the identification of regions within the proteome that offer significant conservation, HLA recognition within a population, low prevalence of HLA adaptation and demonstrated immunogenicity. We believe this unique and novel approach to vaccine design as a supplement to vitro functional assays, offers a bespoke pipeline for expedited and rational CD8 T-cell vaccine design for HIV and potentially other pathogens with the potential for both global and local coverage.

摘要

预测模型作为候选抗原发现的工具越来越普遍,以应对使具有不同 HLA 特性的队列进行表位作图的挑战。在这里,我们基于使用两个关键参数的概念,即人群中个体 HLA 特征的多样性指标和个体 CD8 T 细胞免疫受体中序列多样性的考虑,来评估 HIV 蛋白质组中定义的免疫原性区域。使用这种方法,对 HLA 适应性和功能免疫原性数据的分析使我们能够识别蛋白质组中具有显著保守性、人群中 HLA 识别、HLA 适应性低流行率和已证明的免疫原性的区域。我们相信,这种将疫苗设计作为体外功能测定的补充的独特新颖方法,为 HIV 及其他潜在病原体的 CD8 T 细胞疫苗设计提供了一个定制的流水线,具有全球和局部覆盖的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b3f8/7930081/35693b3abbc0/fimmu-12-609884-g0001.jpg

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