Recombinant Shiga toxin B subunit elicits protection against Shiga toxin via mixed Th type immune response in mice.

Vaccine

Biotechnology Division, Defence Research and Development Establishment, Gwalior 474002, MP, India.

Published: October 2011

AI Article Synopsis

  • Shigella dysenteriae is a major cause of childhood diarrhoea, leading to millions of deaths annually and producing a dangerous toxin called Shiga toxin, classified as a potential biological weapon.
  • Previous research developed a recombinant version of the Shiga toxin B subunit (rStxB) that neutralizes its toxicity in cell cultures.
  • The study demonstrated that rStxB triggers significant immune responses in mice, leading to the production of antibodies and differing cytokine levels, indicating its potential as a promising vaccine candidate against Shiga toxin-related infections.

Article Abstract

Shigella dysenteriae is the causative agent of the third commonest bacterial disease for childhood diarrhoea and responsible for millions of deaths per year. It produces potent toxin termed Shiga toxin which is listed in category B biological warfare agent of CDC, USA. Earlier we have reported production of recombinant Shiga toxin B subunit that produced antibodies which neutralized Shiga toxin toxicity in HeLa cells. In the present study, we have evaluated the immunomodulatory potential of rStxB protein in Balb/c mice using Freunds adjuvants. Animal protection with recombinant StxB was conferred through both humoral and cellular immune responses as indicated by an increased antibody titre with predominance of IgG2a and IgG2b isotypes along with elevated levels of IgG1 subtype. Cytokine profile of the mice antiserum and splenocyte also indicates Th2 and Th1 type of immune responses where former dominates in early stage of immunization. Histopathology study of kidneys of vaccinated mice showed remarkable differences when compared to the animals infected with Shigella dysenteriae type1. The present study indicates that recombinant StxB is a promising vaccine candidate and can be used for production of therapeutic antibodies to counter Shiga intoxication.

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Source
http://dx.doi.org/10.1016/j.vaccine.2011.08.040DOI Listing

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