利用多任务学习法学习 HIV-1 抗广泛中和抗体的模式,减少亚型偏差。

IF 3.8 2区 生物学 Q1 BIOCHEMICAL RESEARCH METHODS PLoS Computational Biology Pub Date : 2024-11-20 DOI:10.1371/journal.pcbi.1012618
Aime Bienfait Igiraneza, Panagiota Zacharopoulou, Robert Hinch, Chris Wymant, Lucie Abeler-Dörner, John Frater, Christophe Fraser
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引用次数: 0

摘要

预测 HIV-1 对广谱中和抗体(bnAbs)耐药性的能力将提高 bnAb 的治疗效果。机器学习是进行此类预测的有力方法。面临的挑战之一是目前可用的训练数据集中某些 HIV-1 亚型的代表性不足,这可能会影响模型在不同亚型之间的通用性。第二个挑战是需要 bnAbs 组合来避免对单一 bnAb 产生不可避免的抗药性,而通过计算确定 bnAbs 的最佳组合是一个尚未解决的问题。最近,使用多种抗体的耐药性结果同时训练的机器学习模型(一种称为多任务学习(MTL)的策略)已被证明能提高预测效果。我们开发了一个新模型,并证明除了性能提升外,MTL 还有助于解决前两个难题。具体来说,我们通过实证证明 MTL 可以减轻代表性不足的亚型带来的偏差,而且 MTL 允许模型学习对抗体组合的共同抗性模式,从而为预测抗体表位和潜在选择最佳 bnAb 组合提供工具。我们的分析结果可在 https://github.com/iaime/LBUM 网站上公开,也可适用于采用抗体疗法治疗的其他传染病。
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Learning patterns of HIV-1 resistance to broadly neutralizing antibodies with reduced subtype bias using multi-task learning.

The ability to predict HIV-1 resistance to broadly neutralizing antibodies (bnAbs) will increase bnAb therapeutic benefits. Machine learning is a powerful approach for such prediction. One challenge is that some HIV-1 subtypes in currently available training datasets are underrepresented, which likely affects models' generalizability across subtypes. A second challenge is that combinations of bnAbs are required to avoid the inevitable resistance to a single bnAb, and computationally determining optimal combinations of bnAbs is an unsolved problem. Recently, machine learning models trained using resistance outcomes for multiple antibodies at once, a strategy called multi-task learning (MTL), have been shown to improve predictions. We develop a new model and show that, beyond the boost in performance, MTL also helps address the previous two challenges. Specifically, we demonstrate empirically that MTL can mitigate bias from underrepresented subtypes, and that MTL allows the model to learn patterns of co-resistance to combinations of antibodies, thus providing tools to predict antibodies' epitopes and to potentially select optimal bnAb combinations. Our analyses, publicly available at https://github.com/iaime/LBUM, can be adapted to other infectious diseases that are treated with antibody therapy.

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来源期刊
PLoS Computational Biology
PLoS Computational Biology BIOCHEMICAL RESEARCH METHODS-MATHEMATICAL & COMPUTATIONAL BIOLOGY
CiteScore
7.10
自引率
4.70%
发文量
820
审稿时长
2.5 months
期刊介绍: PLOS Computational Biology features works of exceptional significance that further our understanding of living systems at all scales—from molecules and cells, to patient populations and ecosystems—through the application of computational methods. Readers include life and computational scientists, who can take the important findings presented here to the next level of discovery. Research articles must be declared as belonging to a relevant section. More information about the sections can be found in the submission guidelines. Research articles should model aspects of biological systems, demonstrate both methodological and scientific novelty, and provide profound new biological insights. Generally, reliability and significance of biological discovery through computation should be validated and enriched by experimental studies. Inclusion of experimental validation is not required for publication, but should be referenced where possible. Inclusion of experimental validation of a modest biological discovery through computation does not render a manuscript suitable for PLOS Computational Biology. Research articles specifically designated as Methods papers should describe outstanding methods of exceptional importance that have been shown, or have the promise to provide new biological insights. The method must already be widely adopted, or have the promise of wide adoption by a broad community of users. Enhancements to existing published methods will only be considered if those enhancements bring exceptional new capabilities.
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