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Article Abstract

Anthrax is an acute zoonotic disease caused by infection with Bacillus anthracis. B. anthracis spores are highly resistant to environmental degradation and are used as a biological weapon. In this study, we investigated the adjuvant activity of CIA07 to anthrax protective antigen (PA). A/J mice were immunized intraperitoneally once, or twice with a 4-week interval, with recombinant PA alone or combined with alum, CpG1826, or CIA07 as adjuvant, and serum anti-PA IgG antibody responses were measured 4 weeks after each immunization. All three adjuvants significantly enhanced anti-PA IgG antibody titer 4 weeks after the priming and boosting immunizations, and alum gave the highest titer. In order to evaluate the adjuvant activity of CIA07 in the presence of alum, Balb/c mice were immunized 3 times at 1-week intervals with PA in combination with alum, CIA07 or alum plus CIA07, and the immune responses were assessed 2 weeks after the third immunization. The serum anti-PA IgG antibody titer of the CIA07-treated group was 14-fold higher than the group given PA alone, and the coadministration of CIA07 with alum further increased the titer 3.5-fold (P < 0.05). The toxin neutralizing activity of the sera from the mice given the combination of CIA07 and alum was 109-times higher than the animals given PA alone. The mice given CIA07 plus alum also showed a marked increase in the number of IFN-gamma-, IL-2-, and IL-4-producing CD4(+) T cells among their splenocytes. These data suggest the potential of CIA07 in combination with alum as an adjuvant for the development of a potent anthrax vaccine.

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http://dx.doi.org/10.1007/s12272-001-2121-2DOI Listing

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Anthrax is an acute zoonotic disease caused by infection with Bacillus anthracis. B. anthracis spores are highly resistant to environmental degradation and are used as a biological weapon.

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Article Synopsis
  • CIA07 is an immunostimulatory agent made of bacterial DNA fragments and modified lipopolysaccharide, showing promise against bladder cancer and enhancing immune responses against hepatitis B virus.
  • In a study, mice immunized with CIA07 alongside hepatitis B virus surface antigen (HBsAg) exhibited significantly higher levels of specific IgG antibodies compared to those receiving HBsAg alone or with other adjuvants, with effects lasting up to 8 weeks.
  • CIA07 not only increased serum antibody responses but also boosted the levels of CD8(+) T cells and induced Th1-type immune responses, highlighting its potential as an effective adjuvant for hepatitis B therapeutic vaccines.
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