Pre-existing polymerase-specific T cells expand in abortive seronegative SARS-CoV-2
Author:
Swadling LeoORCID, Diniz Mariana O., Schmidt Nathalie M.ORCID, Amin Oliver E., Chandran Aneesh, Shaw Emily, Pade Corinna, Gibbons Joseph M.ORCID, Le Bert NinaORCID, Tan Anthony T., Jeffery-Smith Anna, Tan Cedric C. S., Tham Christine Y. L.ORCID, Kucykowicz StephanieORCID, Aidoo-Micah Gloryanne, Rosenheim JoshuaORCID, Davies Jessica, Johnson Marina, Jensen Melanie P., Joy George, McCoy Laura E.ORCID, Valdes Ana M.ORCID, Chain Benjamin M.ORCID, Goldblatt DavidORCID, Altmann Daniel M., Boyton Rosemary J.ORCID, Manisty Charlotte, Treibel Thomas A., Moon James C., Abbass Hakam, Abiodun Aderonke, Alfarih Mashael, Alldis Zoe, Andiapen Mervyn, Artico Jessica, Augusto João B., Baca Georgina L., Bailey Sasha N. L., Bhuva Anish N., Boulter Alex, Bowles Ruth, Boyton Rosemary J., Bracken Olivia V., O’Brien Ben, Brooks Tim, Bullock Natalie, Butler David K., Captur Gabriella, Champion Nicola, Chan Carmen, Collier David, de Sousa Jorge Couto, Couto-Parada Xose, Cutino-Mogue Teresa, Davies Rhodri H., Douglas Brooke, Di Genova Cecilia, Dieobi-Anene Keenan, Ellis Anaya, Feehan Karen, Finlay Malcolm, Fontana Marianna, Forooghi Nasim, Gaier Celia, Gilroy Derek, Hamblin Matt, Harker Gabrielle, Hewson Jacqueline, Hickling Lauren M., Hingorani Aroon D., Howes Lee, Hughes Alun, Hughes Gemma, Hughes Rebecca, Itua Ivie, Jardim Victor, Lee Wing-Yiu Jason, Jensen Melanie Petra, Jones Jessica, Jones Meleri, Joy George, Kapil Vikas, Kurdi Hibba, Lambourne Jonathan, Lin Kai-Min, Louth Sarah, Mandadapu Vineela, McKnight Áine, Menacho Katia, Mfuko Celina, Mitchelmore Oliver, Moon Christopher, Munoz-Sandoval Diana, Murray Sam M., Noursadeghi Mahdad, Otter Ashley, Palma Susana, Parker Ruth, Patel Kush, Pawarova Babita, Petersen Steffen E., Piniera Brian, Pieper Franziska P., Pope Daniel, Prossora Mary, Rannigan Lisa, Rapala Alicja, Reynolds Catherine J., Richards Amy, Robathan Matthew, Sambile Genine, Semper Amanda, Seraphim Andreas, Simion Mihaela, Smit Angelique, Sugimoto Michelle, Taylor Stephen, Temperton Nigel, Thomas Stephen, Thornton George D., Tucker Art, Veerapen Jessry, Vijayakumar Mohit, Welch Sophie, Wodehouse Theresa, Wynne Lucinda, Zahedi Dan, van Dorp LucyORCID, Balloux FrancoisORCID, McKnight Áine, Noursadeghi MahdadORCID, Bertoletti AntonioORCID, Maini Mala K.ORCID,
Abstract
AbstractIndividuals with potential exposure to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) do not necessarily develop PCR or antibody positivity, suggesting that some individuals may clear subclinical infection before seroconversion. T cells can contribute to the rapid clearance of SARS-CoV-2 and other coronavirus infections1–3. Here we hypothesize that pre-existing memory T cell responses, with cross-protective potential against SARS-CoV-2 (refs. 4–11), would expand in vivo to support rapid viral control, aborting infection. We measured SARS-CoV-2-reactive T cells, including those against the early transcribed replication–transcription complex (RTC)12,13, in intensively monitored healthcare workers (HCWs) who tested repeatedly negative according to PCR, antibody binding and neutralization assays (seronegative HCWs (SN-HCWs)). SN-HCWs had stronger, more multispecific memory T cells compared with a cohort of unexposed individuals from before the pandemic (prepandemic cohort), and these cells were more frequently directed against the RTC than the structural-protein-dominated responses observed after detectable infection (matched concurrent cohort). SN-HCWs with the strongest RTC-specific T cells had an increase in IFI27, a robust early innate signature of SARS-CoV-2 (ref. 14), suggesting abortive infection. RNA polymerase within RTC was the largest region of high sequence conservation across human seasonal coronaviruses (HCoV) and SARS-CoV-2 clades. RNA polymerase was preferentially targeted (among the regions tested) by T cells from prepandemic cohorts and SN-HCWs. RTC-epitope-specific T cells that cross-recognized HCoV variants were identified in SN-HCWs. Enriched pre-existing RNA-polymerase-specific T cells expanded in vivo to preferentially accumulate in the memory response after putative abortive compared to overt SARS-CoV-2 infection. Our data highlight RTC-specific T cells as targets for vaccines against endemic and emerging Coronaviridae.
Publisher
Springer Science and Business Media LLC
Subject
Multidisciplinary
Reference57 articles.
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