Abstract
There have been few in vivo studies on the effect of aluminum hydroxide adjuvant and its influence on the immune response to vaccination. In this study, lambs received a parallel subcutaneous treatment with either commercial vaccines containing aluminum hydroxide or an equivalent dose of this compound only with the aim of identifying the activated molecular signature. Blood samples were taken from each animal at the beginning and at the end of the experiment and PBMCs isolated. Total RNA and miRNA libraries were prepared and sequenced. After alignment to the Oar3.1 reference genome and differential expression with 3 programs, gene enrichment modeling was performed. For miRNAs, miRBase and RNAcentral databases were used for detection and characterization. Three expression comparisons were made: vaccinated animals at the beginning and at the end of the treatment, adjuvanted animals at the same times, and animals of both treatments at the end of the experiment. After exposure to both treatments, a total of 2,473; 2,980 and 429 differentially expressed genes were identified in vaccinated animals, adjuvanted animals and animals at the end of both treatments, respectively. In both adjuvant and vaccine treated animals the NF-κB signaling pathway was enriched. On the other hand, it can be observed a downregulation of cytokines and cytokine receptors in the adjuvanted group compared to the vaccinated group at the final time, suggesting a milder induction of the immune response when the adjuvant is alone. As for the miRNA analysis, 95 miRNAs were detected: 64 previously annotated in Ovis aries, 11 annotated in Bos taurus and 20 newly described. Interestingly, 6 miRNAs were differentially expressed in adjuvant treated animals, and 3 and 1 in the other two comparisons. Lastly, an integrated miRNA-mRNA expression profile was developed, in which a miRNA-mediated regulation of genes related to DNA damage stimulus was observed. In brief, it seems that aluminum-containing adjuvants are not simple delivery vehicles for antigens, but also induce endogenous danger signals that can stimulate the immune system. Whether this contributes to long-lasting immune activation or to the overstimulation of the immune system remains to be elucidated.
Highlights
Aluminum compounds have been used as adjuvants for nearly 90 years in veterinary and human vaccines
The 12 miRNA-seq libraries were sequenced, giving a mean value of 17.2 million raw paired-end reads per library
Alignment of the filtered reads to the Ovis aries reference genome (Oar3.1), allowing a maximum of 20 multiple mappings per read, yielded a mean value of 12.9 million read pairs (91.40% of the filtered reads) mapping to different loci per library
Summary
Aluminum compounds have been used as adjuvants for nearly 90 years in veterinary and human vaccines. The mechanism of how aluminum-based adjuvants exert their beneficial effects is still not fully understood. They occasionally can cause adverse reactions [1]. A form of the autoimmune/autoinflammatory syndrome induced by adjuvants (ASIA) [5] has been described as linked to repetitive inoculation with aluminum-containing vaccines. This syndrome was extensively observed after compulsory vaccination against the bluetongue virus of ruminants in 2008 [6]
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