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Infection and Immunity, September 1998, p. 4389-4396, Vol. 66, No. 9
Department of Medical Microbiology, Faculty
of Medicine and Health Sciences, United Arab Emirates University,
Al Ain, United Arab Emirates
Received 23 March 1998/Returned for modification 8 June
1998/Accepted 1 July 1998
To define cross-reactive epitopes in Salmonella
lipopolysaccharide (LPS), antisera designated anti-S, anti-Ra, and
anti-Re were generated against smooth (S), complete-core (Ra), and
deep-core mutant (Re) strains, respectively, and characterized
immunochemically. The reactivities of anti-Ra and anti-S with rough LPS
(rLPS) chemotypes in enzyme-linked immunosorbent assays (ELISA)
decreased progressively with increasing truncation of the complete-core
oligosaccharide (e.g., Ra > Rb1 >...Re), while
that of anti-Re increased (Ra < Rb1 <...Re).
Anti-Ra was relatively more reactive with nonhomologous smooth LPS
(sLPS) than anti-S, which in turn was more reactive than anti-Re. This
order reflected the relative reactivities of these sera with
outer-core rLPS but not those with inner-core rLPS, which suggests
that the cross-reactivities of all three sera with sLPS were mediated
by antibodies which bind outer-core determinants. Anti-Ra, but not
anti-S or anti-Re, reacted with molecules substituted by O chains in
immunoblots and revealed ladder-like patterns in sLPSs of various
serospecificities. Anti-Ra, however, did not react with
O-antigen-specific neoglycoconjugates in ELISA, thus demonstrating
specificity for core epitopes. Ra and Rb1 but not other
Salmonella core chemotypes inhibited the reactivity of
anti-Ra with sLPS in ELISA, which showed that the terminal outer-core
disaccharide,
0019-9567/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.
-GlcNAc-1
2-
-Glc, the Salmonella
Homologue of a Conserved Lipopolysaccharide Motif in the
Enterobacteriaceae, Elicits Broadly Cross-Reactive
Antibodies
-GlcNAc-1
2-
-Glc (GlcNAc
Glc), was the
major epitope of cross-reactive antibodies in the serum. GlcNAc
Glc represents the conserved motif
-hexose-1
2-
-hexose in cores of the
Enterobacteriaceae, other homologues of which should
likewise be cross-reactive. These results demonstrate that S or Re
strains do not elicit cross-reactive antibodies and indicate that
immunization with Ra strains may represent a general strategy for
eliciting cross-reactive antibodies against LPSs from enteric bacteria.
*
Present address: Department of Microbiology, Molecular
Genetics and Immunology, The University of Kansas Medical Center, 1000 Wahl Hall East, 3901 Rainbow Blvd., Kansas City, KS 66160. Phone: (913)
588-7061. Fax: (913) 588-1388. E-mail: nnnalue{at}kumc.edu.
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