Primary and booster COVID-19 vaccination in patients with Sjögren's disease: data from the longitudinal SAFER cohort study
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Introduction: The COVID-19 pandemic posed additional challenges for this vulnerable
population, such as Sjögren’s disease (SjD), underscoring the need for effective and safe
vaccination strategies. Objective: To evaluate the immunogenicity and safety of COVID-19
vaccines in patients with SjD. Methods: This prospective, observational, longitudinal study
included SjD patients from the SAFER cohort. Immunogenicity was assessed via antispike
IgG (IgG-S) titers using chemiluminescence reported as geometric mean titers (GMT)
and fold increase in GMT (FI-GMT). Disease activity was evaluated using the ESSDAI
score. Adverse events and COVID-19 infections were also monitored. Assessments were
conducted at four time points: pre-first dose (T1), pre-second dose (T2), pre-booster (T3),
and four weeks post-booster (T4). Primary vaccination involved ChAdOx1 nCoV-19 or
inactivated vaccine (CoronaVac), and boosters were either homologous (ChAdOx1 nCoV-
19) or heterologous (BNT162b2). Results: Among 51 participants (mean age 46 years; 90%
female), 41% had comorbidities and 27% (n = 14/51) were highly immunosuppressed.
Among those 73% (n = 37/51) under low immunosuppression, n = 8/51 (13%) were
not using any medication. At baseline, 11% (n = 4/35) showed moderate/high disease
activity, which decreased to 6.5% (n = 2/31) at T4. Primary vaccination was ChAdOx1 in
94% (n = 48/51) and CoronaVac in 6% (n = 3/51); 73% (n = 37/51) received heterologous
and 27% (n = 14/51) homologous boosters. COVID-19 infection post-booster occurred
in 20% (n = 10/51). Seroconversion rates reached nearly 100% across all medication
subgroups except for biologic users, who showed delayed but stable seroconversion by T4. IgG-S titers increased progressively through T4. Primary immunization induced an
ascending GMT in both vaccine types. At T4, the GMT was significantly higher in the
BNT162b2 group (2148.03 [1452.05–3155.84]; p < 0.001; 95% CI) than in the ChAdOx1 group
(324.29 [107.92–974.48]; p < 0.001; 95% CI); the fold-increase in immune response was six
times greater with BNT162b2 (5.98 [2.97–12.03]; p = 0.001; 95% CI). Seroconversion was
100% in the heterologous group versus 83% in the homologous group (p > 0.01). Those with
prior infection showed significantly higher titers, particularly at T2 and T3 (p < 0.001 for
T1–T3). Adverse events were mild and not statistically significant. Multivariate regression
confirmed BNT162b2 as an independent factor for higher antibody titers. Conclusion:
COVID-19 vaccination in patients with SjD was safe and induced high anti-spike antibody
titers and seropositivity. Heterologous boosting, particularly with BNT162b2, demonstrated
superior immunogenicity. No association was found between vaccination and SjD disease
flares or worsening activity.
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LIRIO, Maressa Barbosa Beloni et.al. Primary and booster COVID-19 vaccination in patients with Sjögren's disease: data from the longitudinal SAFER cohort study. Vaccines, Basel, v. 13, n. 11, p. 1152-1160, 2025. DOI: 10.3390/vaccines13111152. Disponível em: https://www.mdpi.com/2076-393X/13/11/1152. Acesso em: 12 jun. 2026.