Litcius/Paper detail

Machine learning identifies T cell receptor repertoire signatures associated with COVID-19 severity

Jonathan J. Park, Kyoung A Lee, Stanley Z. Lam, Katherine S. Moon, Zhenhao Fang, Sidi Chen

2023Communications Biology44 citationsDOIOpen Access PDF

Abstract

T cell receptor (TCR) repertoires are critical for antiviral immunity. Determining the TCR repertoire composition, diversity, and dynamics and how they change during viral infection can inform the molecular specificity of host responses to viruses such as SARS-CoV-2. To determine signatures associated with COVID-19 disease severity, here we perform a large-scale analysis of over 4.7 billion sequences across 2130 TCR repertoires from COVID-19 patients and healthy donors. TCR repertoire analyses from these data identify and characterize convergent COVID-19-associated CDR3 gene usages, specificity groups, and sequence patterns. Here we show that T cell clonal expansion is associated with the upregulation of T cell effector function, TCR signaling, NF-kB signaling, and interferon-gamma signaling pathways. We also demonstrate that machine learning approaches accurately predict COVID-19 infection based on TCR sequence features, with certain high-power models reaching near-perfect AUROC scores. These analyses provide a systems immunology view of T cell adaptive immune responses to COVID-19.

Topics & Concepts

T-cell receptorRepertoireBiologyComputational biologyImmune systemCoronavirus disease 2019 (COVID-19)EffectorT cellImmunityImmunologyAcquired immune systemSignal transductionGeneticsDiseaseMedicineInfectious disease (medical specialty)PhysicsAcousticsPathologySARS-CoV-2 and COVID-19 Researchvaccines and immunoinformatics approachesCOVID-19 Clinical Research Studies