Determination of the Virulenec of the Pigmentation-Deficient and Pigmentation-/Plasminogen Activator-Deficient Strains of Yersinia pestis in Non-Human Primate and Mouse Models of Pneumonic Plague

Abstract

The current human plague vaccine, a killed Yersinia pestis whole-cell preparation, does not protect against aerosol challenge and is reactogenic and antigenically undefined. Live attenuated Y. pestis, such as pigmentation-deficient (Pgm-) strains, have been used frequently as vaccines and are efficacious. They are used widely in plague research and assumed to be safe. However, they can cause serious adverse reactions, and their aerosol infectivity is not known. We tested the virulence of a defined Pgm- variant of the C092 strain of Y. pestis in mouse and non-human primate models of pneumonic plague. The ten-fold lower median lethal dose by the aerosol compared to the subcutaneous (s.c.) routes of the Pgm -strain in mice suggested that the Pgm -strain might be less attenuated by the former than by the latter route. After exposure of 16 African green monkeys to inhaled doses ranging from 1.1 x 10e4 to 8.1 X 1Oe7 cfu, eight died and eight survived. The terminal cultures collected from five of the non-survivors were all positive for Y. pestis. Two of the remaining three non-survivors were culture-negative but had pathologic and immunologic evidence of infection with Y. pestis, specimens could not be obtained nor the cause of death determined for the third one. The deaths were not dose-related, and there were some differences in the pathology associated with infection by the Pgm- strain compared to the wild-type (wt) strain. However, the Pgm- derivative was clearly virulent for monkeys by the aerosol route. A mutant of the Pgm- strain, which has a deletion m the plasminogen activator (Pla) virulence locus (Pla), appeared to be more attenuated than was either the Pgm- single mutant (in NHPs and mice) or the Pla- single mutant strain (in mice) and has potential as a live vaccine.

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Document Details

Document Type
Technical Report
Publication Date
Jan 01, 2002
Accession Number
ADA407896

Entities

People

  • A. Friedlander
  • M. Chow-Martínez
  • M. L. Pitt
  • Peter Vogel
  • S. Welkos

Organizations

  • United States Army Medical Research Institute of Infectious Diseases

Tags

DTIC Thesaurus Topics

  • Animals
  • Biomedical Research
  • Blood
  • Cells
  • Diseases And Disorders
  • Health Services
  • Infection
  • Infectious Diseases
  • Lethal Dosage
  • Lymphatic System
  • Macrophages
  • Pathology
  • Plasminogen
  • Rodents
  • Vaccines
  • Virulence
  • Wound Infections

Fields of Study

  • Biology

Readers

  • Immunology
  • Toxicology/Environmental Toxicology

Technology Areas

  • Biotechnology