Fraction 1 capsular antigen (F1) purification from Yersinia pestis CO92 and from an Escherichia coli recombinant strain and efficacy against lethal plague challenge

Author:

Andrews G P1,Heath D G1,Anderson G W1,Welkos S L1,Friedlander A M1

Affiliation:

1. Bacteriology Division, U.S. Army Medical Research Institute of Infectious Diseases, Fort Detrick, Frederick, Maryland 21702, USA.

Abstract

As a first step in formulating an improved plague vaccine, we developed a simple purification strategy that produced high yields of pure cell-associated and culture supernatant-derived fraction 1 capsular antigen (F1) from both avirulent Yersinia pestis C092 (Pgm- Lcr-) and an Escherichia coli F1-producing recombinant strain. Cell-associated F1 was partially purified by sequential ammonium sulfate precipitations of a sodium chloride extract of acetone-dried bacteria harvested from broth cultures. Cell-free F1 was precipitated directly from culture supernatants with a single application of 30% ammonium sulfate. By exploiting the aggregative property of F1, large quantities of purified high-molecular-weight F1 species from both cell extracts and supernatants were isolated in the void volume of a preparative gel filtration column. Highly purified, endotoxin-free F1, combined with two different adjuvants, induced very high F1 titers in mice and protected them against either subcutaneous (70 to 100% survival) or aerosol (65 to 84% survival) challenge with virulent organisms. This protection was independent of the source of the antigen and the adjuvant used. F1-induced protection against both subcutaneous and aerosol challenge was also significantly better than that conferred by immunization with the licensed killed whole-cell vaccine. Our results indicate that F1 antigen represents a major protective component of previously studied crude capsule preparations, and immunity to F1 antigen provides a primary means for the host to overcome plague infection by either the subcutaneous or respiratory route.

Publisher

American Society for Microbiology

Subject

Infectious Diseases,Immunology,Microbiology,Parasitology

Reference42 articles.

1. Anderson G. W. Jr. P. L. Worsham G. P. Andrews C. R. Bolt S. L. Welkos A. M. Friedlander and J. P. Burans. 1995. Passive immunization with monoclonal antibodies against the F1 antigen of Yersinia pestis protects mice from fatal bubonic and pneumonic plague abstr. 211. In Abstracts from the 44th Annual Meeting of the American Society of Tropical Medicine and Hygiene.

2. Andrews G. P. Unpublished observations.

3. Atlas R. M. A. E. Brown K. W. Dobra and L. Miller (ed.). 1984. Experimental microbiology: fundamentals and applications p. 54. Macmillan Publishing Company New York.

4. Studies on immunization against plague. I. The isolation and characterization of the soluble antigen of Pasteurella pestis;Baker E. E.;J. Immunol.,1952

5. Characterization of the antigenic subunits of the envelope protein of Yersinia pestis;Bennett L. G.;J. Bacteriol.,1974

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