Abstract Background Chronic kidney disease (CKD) contributes to global mortality and morbidity, also due to infectious complications resulting from immune system dysregulation. Recently, respiratory syncytial virus (RSV) vaccines based on the prefusion F (preF) glycoprotein have been licensed for prevention of severe disease in elderly and in patients with comorbidities, but data on immunogenicity in patients with CKD is scarce. Methods We characterized humoral and cellular immunogenicity of 75 patients with CKD stages G3a to G5d both before and 14 (IQR 2) days after vaccination with an adjuvanted protein-based RSVpreF3-vaccine using ELISA and flow cytometry. Data on adverse events were collected through a self-reported questionnaire. Results Vaccination led to a significant induction of RSV-specific CD4 T-cells (P 0.0001) and the increase did not differ between the CKD stages. CD8 T-cells were not specifically induced. Despite high seroprevalence prior to vaccination, quantitative levels of RSV-specific immunoglobulins IgG and F protein-specific IgG were significantly induced upon vaccination (both P 0.0001), with a less pronounced increase in patients with advanced CKD. Urinary albumin-creatinine-ratio (UACR) was shown to be predictive of vaccine response in a multivariate regression model using age, serum creatinine and urea as covariates (P = 0.035). The vaccine was well tolerated with mostly transient adverse events at the injection site. Conclusions RSV-vaccination led to a robust CD4 T-cell and humoral response in patients with CKD with less pronounced effects in those with high-grade proteinuria. Long-term data on immunogenicity and correlation with clinical outcomes are warranted to define optimal vaccination strategies.
Radun et al. (Tue,) studied this question.