Abstract
Background. It has been recognized that microbiota plays a key role in shaping immune system maturation and activity. Since probiotic administration influences the microbiota composition and acts as a biological response modifier, the efficacy of an adjuvant for boosting vaccine-specific immunity is investigated. Methods. A review of the literature was performed, starting from the mechanisms to laboratory and clinical evidence. Results. The mechanisms, and in vitro and animal models provide biological plausibility for microbiota use. Probiotics have been investigated as adjuvants in farm conditions and as models to understand their potential in human vaccinations with promising results. In human studies, although probiotics were effective in ameliorating seroconversion to vaccines for influenza, rotavirus and other micro-organisms, the results for clinical use are still controversial, especially in particular settings, such as during the last trimester of pregnancy. Conclusion. Although this topic remains controversial, the use of probiotics as adjuvant factors in vaccination represents a strategic key for different applications. The available data are deeply influenced by heterogeneity among studies in terms of strains, timing and duration of administration, and patients. Although these do not allow us to draw definitive conclusions, probiotics as adjuvants in vaccination should be considered in future studies, especially in the elderly and in children, where vaccine effectiveness and duration of immunization really matter.
Highlights
It has been recognized that microbiota plays a key role in shaping immune system maturation and activity
Probiotic bacteria have been investigated in animal models both as adjuvants for vaccination in farm conditions and as models to understand the adjuvant potential in human vaccinations
As a matter of fact, very recently, it has been shown that a range of probiotic bacteria increases the efficacy of vaccinations in chickens treated with a vaccine specific for Newcastle disease [26] or avian influenza H9N2 [27,28]
Summary
There is consensus that all Gram-positive bacteria may release LTA, wall teichoic acid, peptidoglycan (PG) and other wall components into the surrounding environment All of these components are able to interact with the gut-associated lymphoid tissue (GALT) cells and with the systemic immune system of the subject [22]. These substances released by or produced through the metabolic activity of the microorganism may exert beneficial effects on the host, directly or indirectly, including an interaction with the immune system. The above-cited data may provide the molecular bases for the observed in vivo adjuvant effects discussed here below in animal models
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