Divergent trajectories of antiviral memory after SARS-Cov-2 infection

Adriana Tomic*,Donal T. Skelly*,Ane Ogbe*,Daniel O'Connor*,Matthew Pace,Emily Adland,Frances Alexander,Mohammad Ali, Kirk Allott,M. Azim Ansari, Sandra Belij-Rammerstorfer,Sagida Bibi,Luke Blackwell,Anthony Brown,Helen Brown,Breeze Cavell,Elizabeth A. Clutterbuck,Thushan I de Silva,David Eyre, Amy Flaxman,James Grist,Carl-Philipp Hackstein, Rachel Halkerston,Adam C. Harding,Jennifer Hill,Tim James, Cecilia Jay,Síle A. Johnson,Barbara Kronsteiner,Yolanda Lie,Aline Linder,Stephanie Longet,Spyridoula Marinou,Philippa C. Matthews,Jack Mellors,Christos Petropoulos,Patpong Rongkard, Cynthia Sedik,Laura Silva-Reyes,Holly Smith, Lisa Stockdale,Stephen Taylor,Stephen Thomas,Timothy Tipoe,Lance Turtle,Vinicius Adriano Vieira, Terri Wrin,OPTIC Clinical Group,PITCH Study Group, C-MORE Group,Andrew J. Pollard,Teresa Lambe, Christopher P. Conlon,Katie Jeffery,Simon Travis,Philip J. Goulder,John Frater,Alexander J. Mentzer,Lizzie Stafford,Miles W. Carroll,William S. James,Paul Klenerman#,Eleanor Barnes#,Christina Dold#,Susanna J. Dunachie#

Research Square (Research Square)（2021）

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Abstract

Abstract Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection is normally controlled by effective host immunity including innate, humoral and cellular responses. However, the trajectories and correlates of acquired immunity, and the capacity of memory responses months after infection to neutralise variants of concern - which has important public health implications - is not fully understood. To address this, we studied a cohort of 78 UK healthcare workers who presented in April to June 2020 with symptomatic PCR-confirmed infection or who tested positive during an asymptomatic screening programme and tracked virus-specific B and T cell responses longitudinally at 5-6 time points each over 6 months, prior to vaccination. We observed a highly variable range of responses, some of which - T cell interferon-gamma (IFN-γ) ELISpot, N-specific antibody waned over time across the cohort, while others (spike-specific antibody, B cell memory ELISpot) were stable. In such cohorts, antiviral antibody has been linked to protection against re-infection. We used integrative analysis and a machine-learning approach (SIMON - Sequential Iterative Modeling Over Night) to explore this heterogeneity and to identify predictors of sustained immune responses. Hierarchical clustering defined a group of high and low antibody responders, which showed stability over time regardless of clinical presentation. These antibody responses correlated with IFN-γ ELISpot measures of T cell immunity and represent a subgroup of patients with a robust trajectory for longer term immunity. Importantly, this immune-phenotype associates with higher levels of neutralising antibodies not only against the infecting (Victoria) strain but also against variants B.1.1.7 (alpha) and B.1.351 (beta). Overall memory responses to SARS-CoV-2 show distinct trajectories following early priming, that may define subsequent protection against infection and severe disease from novel variants.* These authors contributed equally.# These authors jointly supervised this work and contributed equally.Corresponding authors: Eleanor Barnes, email: ellie.barnes@ndm.ox.ac.ukand Adriana Tomic, email: 19info@adrianatomic.com

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Key words

antiviral memory,infection,sars-cov

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