GuaA and GuaB Are Essential for B orrelia burgdorferi Survival in the Tick-Mouse Infection Cycle

Author:

Jewett Mollie W.1,Lawrence Kevin A.1,Bestor Aaron1,Byram Rebecca12,Gherardini Frank1,Rosa Patricia A.1

Affiliation:

1. Laboratory of Zoonotic Pathogens, Rocky Mountain Laboratories, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Hamilton, Montana 59840

2. Department of Molecular Biology, University of Wyoming, Laramie, Wyoming 82701

Abstract

ABSTRACT Pathogens lacking the enzymatic pathways for de novo purine biosynthesis are required to salvage purines and pyrimidines from the host environment for synthesis of DNA and RNA. Two key enzymes in purine salvage pathways are IMP dehydrogenase (GuaB) and GMP synthase (GuaA), encoded by the guaB and guaA genes, respectively. While these genes are typically found on the chromosome in most bacterial pathogens, the guaAB operon of B orrelia burgdorferi is present on plasmid cp26, which also harbors a number of genes critical for B. burgdorferi viability. Using molecular genetics and an experimental model of the tick-mouse infection cycle, we demonstrate that the enzymatic activities encoded by the guaAB operon are essential for B. burgdorferi mouse infectivity and provide a growth advantage to spirochetes in the tick. These data indicate that the GuaA and GuaB proteins are critical for the survival of B. burgdorferi in the infection cycle and highlight a potential difference in the requirements for purine salvage in the disparate mammalian and tick environments.

Publisher

American Society for Microbiology

Subject

Molecular Biology,Microbiology

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