Humoral and cellular responses to SARS-CoV-2 vaccination in patients with lymphoid malignancies

  1. Sean H. Lim
  2. Nicola Campbell
  3. Beth Stuart
  4. Marina Johnson
  5. Debora Joseph-Pietras
  6. Adam Kelly
  7. Danielle Jeffrey
  8. Anna H. Turaj
  9. Kate Rolfvondenbaumen
  10. Celine Galloway
  11. Thomas Wynn
  12. Adam R. Coleman
  13. Benjamin Ward
  14. Karen Long
  15. Andrew T. Bates
  16. Diana Ayres
  17. Robert Lown
  18. Janlyn Falconer
  19. Oliver Brake
  20. James Batchelor
  21. Victoria Willimott
  22. Anna Bowzyk Al-Naeeb
  23. Lisa Robinson
  24. Ann O’Callaghan
  25. Graham P. Collins
  26. Tobias Menne
  27. Saul N. Faust
  28. Christopher P. Fox
  29. Matthew Ahearne
  30. Peter W.M. Johnson
  31. Andrew J. Davies
  32. David Goldblatt
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Abstract

SARS-CoV-2 vaccination protects against COVID-19. Antibodies and antigen-specific T-cell responses against the spike domain can be used to measure vaccine immune response. Individuals with lymphoma have defects in humoral and cellular immunity that may compromise vaccine response. In this prospective observational study of 457 participants with lymphoma, 52% of participants vaccinated on treatment had undetectable anti-spike IgG antibodies compared to 9% who were not on treatment. Marked impairment was observed in those receiving anti- CD20 antibody within 12 months where 60% had undetectable antibodies compared to 11% on chemotherapy, which persisted despite three vaccine doses. Overall, 63% had positive T-cell responses irrespective of treatment. Individuals with indolent B-cell lymphoma have impaired antibody and cellular responses that were independent of treatment. The significant reduction and heterogeneity in immune responses in these individuals emphasise the urgent need for immune response monitoring and alternative prophylactic strategies to protect against COVID- 19.

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