Vaccines (May 2024)

An Adjuvanted Vaccine-Induced Pathogenesis Following Influenza Virus Infection

  • Shiou-Chih Hsu,
  • Kun-Hsien Lin,
  • Yung-Chieh Tseng,
  • Yang-Yu Cheng,
  • Hsiu-Hua Ma,
  • Ying-Chun Chen,
  • Jia-Tsrong Jan,
  • Chung-Yi Wu,
  • Che Ma

DOI
https://doi.org/10.3390/vaccines12060569
Journal volume & issue
Vol. 12, no. 6
p. 569

Abstract

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An incomplete Freund’s adjuvant elicited an overt pathogenesis in vaccinated mice following the intranasal challenge of A/California/07/2009 (H1N1) virus despite the induction of a higher specific antibody titer than other adjuvanted formulations. Aluminum hydroxide adjuvants have not induced any pathogenic signs in a variety of formulations with glycolipids. A glycolipid, α-galactosyl ceramide, improved a stimulatory effect of distinct adjuvanted formulations on an anti-influenza A antibody response. In contrast to α-galactosyl ceramide, its synthetic analogue C34 was antagonistic toward a stimulatory effect of an aluminum hydroxide adjuvant on a specific antibody response. The aluminum hydroxide adjuvant alone could confer complete vaccine-induced protection against mortality as well as morbidity caused by a lethal challenge of the same strain of an influenza A virus. The research results indicated that adjuvants could reshape immune responses either to improve vaccine-induced immunity or to provoke an unexpected pathogenic consequence. On the basis of these observations, this research connotes the prominence to develop a precision adjuvant for innocuous vaccination aimed at generating a protective immunity without aberrant responses.

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