A third SARS-CoV-2 mRNA vaccine dose in people receiving hemodialysis overcomes B cell defects but elicits a skewed CD4+ T cell profile
Author:
Sannier Gérémy, Nicolas Alexandre, Dubé Mathieu, Marchitto Lorie, Nayrac Manon, Tastet Olivier, Tauzin Alexandra, Lima-Barbosa Raphaël, Laporte Mélanie, Cloutier Rose, Flores Alina Sreng, Boutin Marianne, Gong Shang Yu, Benlarbi Mehdi, Ding Shilei, Bourassa Catherine, Gendron-Lepage Gabrielle, Medjahed Halima, Goyette Guillaume, Brassard Nathalie, Ortega-Delgado Gloria-Gabrielle, Niessl Julia, Gokool Laurie, Morrisseau Chantal, Arlotto Pascale, Rios Norka, Tremblay Cécile, Martel-Laferrière Valérie, Prat Alexandre, Bélair Justin, Beaubien-Souligny William, Goupil Rémi, Nadeau-Fredette Annie-Claire, Lamarche Caroline, Finzi Andrés, Suri Rita S., Kaufmann Daniel E.ORCID
Abstract
ABSTRACTCellular immune defects associated with suboptimal responses to SARS-CoV-2 mRNA vaccination in people receiving hemodialysis (HD) are poorly understood. We longitudinally analyzed antibody, B cell, CD4+ and CD8+ T cell vaccine responses in 27 HD patients and 26 low-risk control individuals (CI). The first two doses elicit weaker B cell and CD8+ T cell responses in HD than in CI, while CD4+ T cell responses are quantitatively similar. In HD, a third dose robustly boosts B cell responses, leads to convergent CD8+ T cell responses and enhances comparatively more Thelper (TH) immunity. Unsupervised clustering of single-cell features reveals phenotypic and functional shifts over time and between cohorts. The third dose attenuates some features of TH cells in HD (TNFα/IL-2 skewing), while others (CCR6, CXCR6, PD-1 and HLA-DR overexpression) persist. Therefore, a third vaccine dose is critical to achieve robust multifaceted immunity in hemodialysis patients, although some distinct TH characteristics endure.
Publisher
Cold Spring Harbor Laboratory
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