Affiliation:
1. Department of Medical Microbiology & Immunology and Department of Biochemistry, University of Wisconsin, Madison, Wisconsin, USA
2. University of Wisconsin School of Medicine and Public Health, Madison, Wisconsin, USA
Abstract
ABSTRACT
d
-Cycloserine (DCS) is a broad-spectrum antibiotic that inhibits
d
-alanine ligase and alanine racemase activity. When
Escherichia coli
K-12 or CFT073 is grown in minimal glucose or glycerol medium, CycA transports DCS into the cell.
E. coli
K-12
cycA
and CFT073
cycA
mutant strains display increased DCS resistance when grown in minimal medium. However, the
cycA
mutants exhibit no change in DCS sensitivity compared to their parental strains when grown in LB (CFT073 and K-12) or human urine (CFT073 only). These data suggest that
cycA
does not participate in DCS sensitivity when strains are grown in a non-minimal medium. The small RNA GvcB acts as a negative regulator of
E. coli
K-12
cycA
expression when grown in LB. Three
E. coli
K-12
gcvB
mutant strains failed to demonstrate a change in DCS sensitivity when grown in LB. This further suggests a limited role for
cycA
in DCS sensitivity. To aid in the identification of
E. coli
genes involved in DCS sensitivity when grown on complex media, the Keio K-12 mutant collection was screened for DCS-resistant strains.
dadA
,
pnp
,
ubiE
,
ubiF
,
ubiG
,
ubiH
, and
ubiX
mutant strains showed elevated DCS resistance. The phenotypes associated with these mutants were used to further define three previously characterized
E. coli
DCS-resistant strains (χ316, χ444, and χ453) isolated by Curtiss and colleagues (R. Curtiss, III, L. J. Charamella, C. M. Berg, and P. E. Harris, J. Bacteriol.
90:
1238–1250, 1965). A
dadA
mutation was identified in both χ444 and χ453. In addition, results are presented that indicate for the first time that DCS can antagonize
d
-amino acid dehydrogenase (DadA) activity.
Publisher
American Society for Microbiology
Subject
Molecular Biology,Microbiology
Cited by
35 articles.
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