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Immune response and protection against Streptococcus pyogenes after vaccination with Lactococcus lactis that expresses conserved region of M6 protein

Most pathogens gain access to their host through mucosal surfaces. It is
therefore desirable to develop mucosal vaccines that elicit an immune response
to prevent this crucial first step in infection. Current mucosal vaccines are live
attenuated strains of pathogens. More recent efforts have focused on the use of
recombinant non-pathogenic gram-positive bacteria as live vaccine delivery
vectors. Here I have tested the potential of Lactococcus lactis to be used as a
vaccine vector. A recombinant strain of L. lactis has been constructed which
expresses and displays on its surface the C repeat region (CRR) of the M6
protein of Streptococcus pyogenes. I show that nasal vaccination of mice with
this strain elicited strong salivary IgA and serum lgG response. These responses
protected mice against a nasal challenge with S. pyogenes. Subcutaneous
vaccination with the same strain of L. lactis produced a strong serum lgG
response, but no salivary lgA response. Subcutaneous vaccination did not
protect the mice against nasal infections when the mice were challenged with
S. pyogenes. The immune response and protection afforded by concomitant
vaccination by both nasal and subcutaneous routes were better that that seen in
nasal vaccination alone. This study shows that an effective vaccine against
S. pyogenes is possible using L. lactis as a vaccine vector. It also opens up the
potential of L. lactis to be used in the development of vaccines to other mucosal
infections. / Graduation date: 2004

Identiferoai:union.ndltd.org:ORGSU/oai:ir.library.oregonstate.edu:1957/30816
Date04 June 2003
CreatorsMannam, Praveen
ContributorsGeller, Bruce L.
Source SetsOregon State University
Languageen_US
Detected LanguageEnglish
TypeThesis/Dissertation

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