SARS-CoV-2 mRNA vaccinations fail to elicit humoral and cellular immune responses in patients with multiple sclerosis receiving fingolimod.
Lil Meyer-ArndtJulian BraunFlorent FauchereKanika VanshyllaLucie LoyalLarissa HenzeBeate KruseManuela DingeldeyKarsten JürchottMaike MangoldArdit MarajAndre BraginetsChotima BöttcherAndreas NitscheKathrin de la RosaChristoph RatswohlBirgit SawitzkiPavlo HolenyaUlf ReimerLeif E SanderFlorian KleinFriedemann PaulJudith Bellmann-StroblAndreas ThielClaudia Giesecke-ThielPublished in: Journal of neurology, neurosurgery, and psychiatry (2022)
The lack of immunogenicity under long-term fingolimod treatment demonstrates that functional immune responses require not only immune cells themselves, but also access of these cells to the site of inoculation and their unimpeded movement. The absence of humoral and T cell responses suggests that fingolimod-treated patients with MS are at risk for severe SARS-CoV-2 infections despite booster vaccinations, which is highly relevant for clinical decision-making and adapted protective measures, particularly considering additional recently approved sphingosine-1-phosphate receptor antagonists for MS treatment.