Vaccines (Oct 2023)

Immune Profile Determines Response to Vaccination against COVID-19 in Kidney Transplant Recipients

  • Stamatia Stai,
  • Asimina Fylaktou,
  • Efstratios Kasimatis,
  • Aliki Xochelli,
  • Georgios Lioulios,
  • Vasiliki Nikolaidou,
  • Anastasia Papadopoulou,
  • Grigorios Myserlis,
  • Artemis Maria Iosifidou,
  • Myrto Aikaterini Iosifidou,
  • Aikaterini Papagianni,
  • Evangelia Yannaki,
  • Georgios Tsoulfas,
  • Maria Stangou

DOI
https://doi.org/10.3390/vaccines11101583
Journal volume & issue
Vol. 11, no. 10
p. 1583

Abstract

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Background and Aim: Immune status profile can predict response to vaccination, while lymphocyte phenotypic alterations represent its effectiveness. We prospectively evaluated these parameters in kidney transplant recipients (KTRs) regarding Tozinameran (BNT162b2) vaccination. Method: In this prospective monocenter observational study, 39 adult KTRs, on stable immunosuppression, naïve to COVID-19, with no protective humoral response after two Tozinameran doses, received the third vaccination dose, and, based on their immunity activation, they were classified as responders or non-responders. Humoral and cellular immunities were assessed at predefined time points (T0: 48 h before the first, T1: 48 h prior to the third and T2: three weeks after the third dose). Results: Responders, compared to non-responders, had a higher total and transitional B-lymphocyte count at baseline (96.5 (93) vs. 51 (52)cells/μL, p: 0.045 and 9 (17) vs. 1 (2)cells/μL, p: 0.031, respectively). In the responder group, there was a significant increase, from T0 to T1, in the concentrations of activated CD4+ (from 6.5 (4) to 10.08 (11)cells/μL, p: 0.001) and CD8+ (from 8 (19) to 14.76 (16)cells/μL, p: 0.004) and a drop in CD3+PD1+ T-cells (from 130 (121) to 30.44 (25)cells/μL, p: 0.001), while naïve and transitional B-cells increased from T1 to T2 (from 57.55 (66) to 1149.3 (680)cells/μL, p p: 0.003). The percentages of memory and marginal zone B-lymphocytes, and activated CD4+, CD8+ and natural killer (NK) T-cells significantly increased, while those of naïve B-cells and CD3+PD1+ T-cells reduced from T0 to T1. Conclusions: Responders and non-responders to the third BNT162b2 dose demonstrated distinct initial immune cell profiles and changes in cellular subpopulation composition following vaccination.

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