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Journal of Clinical Microbiology, December 1999, p. 3965-3970, Vol. 37, No. 12
0095-1137/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
Genetic Analysis of Borrelia garinii
OspA Serotype 4 Strains Associated with Neuroborreliosis: Evidence for
Extensive Genetic Homogeneity
R. T.
Marconi,1
S.
Hohenberger,2
S.
Jauris-Heipke,2
U.
Schulte-Spechtel,2
C. P.
LaVoie,1
D.
Rößler,2 and
B.
Wilske2,*
Medical College of Virginia at Virginia
Commonwealth University, Richmond, Virginia
23298-0678,1 and Max von Pettenkofer
Institut, Ludwig-Maximilians-Universität München, D-80336
Munich, Germany2
Received 27 May 1999/Returned for modification 22 July
1999/Accepted 19 August 1999
Infection with Borrelia garinii outer surface protein
(Osp) A serotype 4 strains has been correlated with the development of
neuroborreliosis in Lyme borreliosis patients in Europe. OspA serotype
4 isolates have been recovered primarily from human cerebrospinal fluid, suggesting a tropism for this environment. Previous studies with
monoclonal antibodies directed against OspA and OspC demonstrated that
OspA serotype 4 strains are antigenically closely related. In view of
the pronounced antigenic and genetic variability that has been noted in
the Osps of other Borrelia isolates, we sought to determine
if OspA serotype 4 strains represent a recently emerged clonal lineage
of B. garinii. Toward this goal, a representative group of
OspA serotype 4 strains was analyzed for traits that typically exhibit
hypervariability among isolates that cause Lyme borreliosis. The
following criteria were assessed: (i) ospC sequences, (ii)
plasmid composition, (iii) genomic restriction fragment length polymorphism (RFLP) patterns, and (iv) the RFLP patterns of the upstream homology box (UHB) element which flanks members of the UHB
gene family at their 5' end. Collectively, these analyses demonstrate
genetic homogeneity, suggesting that OspA serotype 4 strains are a
recently emerged clonal lineage with an apparent tropism for the
central nervous system.
*
Corresponding author. Mailing address: Max von
Pettenkofer Institut, Ludwig-Maximilians-Universität
München, Pettenkoferstrasse 9 a, D-80336, Munich, Germany.
Phone: 49-89-51605225. Fax: 49-89-51604757. E-mail:
Bettina.Wilske{at}mvp-bak.med.uni-muenchen.de.
Journal of Clinical Microbiology, December 1999, p. 3965-3970, Vol. 37, No. 12
0095-1137/99/$04.00+0
Copyright © 1999, American Society for Microbiology. All rights reserved.
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