Author:
Gonzalez-Perez Maria,Montes-Casado Maria,Conde Patricia,Cervera Isabel,Baranda Jana,Berges-Buxeda Marcos J.,Perez-Olmeda Mayte,Sanchez-Tarjuelo Rodrigo,Utrero-Rico Alberto,Lozano-Ojalvo Daniel,Torre Denis,Schwarz Megan,Guccione Ernesto,Camara Carmen,Llópez-Carratalá M Rosario,Gonzalez-Parra Emilio,Portoles Pilar,Ortiz Alberto,Portoles Jose,Ochando Jordi
Abstract
Long-term hemodialysis (HD) patients are considered vulnerable and at high-risk of developing severe acute respiratory syndrome coronavirus type 2 (SARS-CoV-2) infection due to their immunocompromised condition. Since COVID-19 associated mortality rates are higher in HD patients, vaccination is critical to protect them. The response towards vaccination against COVID-19 in HD patients is still uncertain and, in particular the cellular immune response is not fully understood. We monitored the humoral and cellular immune responses by analysis of the serological responses and Spike-specific cellular immunity in COVID-19-recovered and naïve HD patients in a longitudinal study shortly after vaccination to determine the protective effects of 1273-mRNA vaccination against SARS-CoV-2 in these high-risk patients. In naïve HD patients, the cellular immune response measured by IL-2 and IFN-ɣ secretion needed a second vaccine dose to significantly increase, with a similar pattern for the humoral response. In contrast, COVID-19 recovered HD patients developed a potent and rapid cellular and humoral immune response after the first vaccine dose. Interestingly, when comparing COVID-19 recovered healthy volunteers (HV), previously vaccinated with BNT162b2 vaccine to HD patients vaccinated with 1273-mRNA, these exhibited a more robust immune response that is maintained longitudinally. Our results indicate that HD patients develop strong cellular and humoral immune responses to 1273-mRNA vaccination and argue in favor of personalized immune monitoring studies in HD patients, especially if COVID-19 pre-exposed, to adapt COVID-19 vaccination protocols for this immunocompromised population.
Subject
Immunology,Immunology and Allergy
Cited by
8 articles.
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