Abstract
Childhood vaccines have been the cornerstone tool of public health over the past century. A major barrier to neonatal vaccination is the “immaturity” of the infant immune system and the inefficiency of conventional vaccine approaches at inducing immunity at birth. While much of the literature on fetal and neonatal immunity has focused on the early life propensity toward immune tolerance, recent studies indicate that the fetus is more immunologically capable than previously thought, and can, in some circumstances, mount adaptive B and T cell responses to perinatal pathogens in utero. Although significant hurdles remain before these findings can be translated into vaccines and other protective strategies, they should lend optimism to the prospect that neonatal and even fetal vaccination is achievable. Next steps toward this goal should include efforts to define the conditions for optimal stimulation of infant immune responses, including antigen timing, dose, and route of delivery, as well as antigen presentation pathways and co-stimulatory requirements. A better understanding of these factors will enable optimal deployment of vaccines against malaria and other pathogens to protect infants during their period of greatest vulnerability.
Highlights
Reviewed by: Stephen Rogerson, The University of Melbourne, Australia Celia Dechavanne, Institut de Recherche Pour le Développement (IRD) UMR216 Mère et Enfant Face Aux Infections Tropicales (MERIT), France
In light of recent studies demonstrating an association between NK cell antibody dependent cellular cytotoxicity (ADCC) and malaria outcomes in children and adults [53], these findings raise the possibility that NK cells could play an important antimalarial role in utero and in the newborn through engagement of transplacentally acquired malaria-specific antibodies
The fetal immune system gradually evolves from one that is skewed toward tolerance to one that is poised to fight foreign pathogens
Summary
Reviewed by: Stephen Rogerson, The University of Melbourne, Australia Celia Dechavanne, IRD UMR216 Mère et Enfant Face Aux Infections Tropicales (MERIT), France. While much of the literature on fetal and neonatal immunity has focused on the early life propensity toward immune tolerance, recent studies indicate that the fetus is more immunologically capable than previously thought, and can, in some circumstances, mount adaptive B and T cell responses to perinatal pathogens in utero.
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