Direct demonstration of antigenic substitution of Borrelia burgdorferi ex vivo: exploration of the paradox of the early immune response to outer surface proteins A and C in Lyme disease.

The outer surface proteins (Osps) of Borrelia burgdorferi, the etiologic agent of Lyme disease, are principle targets of protective immune responses against this organism. Whereas most North American strains of B. burgdorferi in culture express an abundant amount of Osp A, antibodies to this protein are either absent or only weakly detected in the sera of naturally infected patients or experimentally infected mice. In contrast, Osp C, which has variable expression on cultured organisms; elicits an early, strong humoral response. To examine this paradox, we have studied the in vivo adaptation of a cloned population of B. burgdorferi strain N40 during the early course of experimental murine borreliosis. As in human disease, antibodies to Osp A were only weakly present in the early immune repertoire after murine inoculation with low dose (10(3)) spirochetes. In contrast, antibodies to Osp C were prominent, even though on cultured spirochetes Osp C mRNA and protein expression could not be detected by reverse transcription polymerase chain reaction (RT-PCR) or indirect immunofluorescence, respectively. These observations led us to investigate the expression of Osp A and Osp C in vivo. By direct fluorescent staining of uncultured spirochetes ex vivo and by PCR amplification of spirochetal mRNA, we show that Osp C is indeed expressed by some spirochetes after infection in the mouse. Spirochetes expressing Osp A could also be detected within the first 2 wk of infection, but not at 30 d. Osp A mRNA, although present at day 14 of infection, could not be amplified by RT-PCR at day 30, suggesting that the expression of this Osp is transient. This further implies that the late burst in Osp A antibodies in both mice and humans may be anamnestic. These results indicate that either Osp C is upregulated on spirochetes after infection, or Osp C-expressing spirochetes expand preferentially over those expressing Osp A during infection. These results have important implications for vaccine design and offer one explanation for the failure of Osp A antibodies to eradicate spirochetes from the infected host.

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Temporal regulation of outer surface proteins of the Lyme-disease spirochaete Borrelia burgdorferi

Biochemical Society Transactions ◽

10.1042/bst0310108 ◽

2003 ◽

Vol 31 (1) ◽

pp. 108-112 ◽

Cited By ~ 58

Author(s):

T.G. Schwan

Keyword(s):

Life Cycle ◽

Lyme Disease ◽

Borrelia Burgdorferi ◽

Outer Surface ◽

Surface Proteins ◽

Temporal Regulation ◽

Outer Surface Proteins ◽

Vertebrate Hosts

In the 20 years since the first agent of Lyme disease was discovered, much interest has focused on the possible biological roles of a few outer surface proteins (Osps) in the alternating life cycle that includes ticks and vertebrate hosts. Two major proteins, OspA and OspC, are differentially regulated by the spirochaete Borrelia burgdorferi during the several days when ticks feed. The reciprocal decrease in OspA with the rapid up-regulation of OspC by the spirochaetes when ticks are feeding suggests that OspA aids in spirochaete attachment while OspC assists in the dissemination of spirochaetes from tick to vertebrate. Future experiments in ticks with mutant spirochaetes that lack these proteins should clarify the speculative functions currently given to these proteins.

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Structural analysis of the outer surface proteins from Borrelia burgdorferi paralogous gene family 54 that are thought to be the key players in the pathogenesis of Lyme disease

Journal of Structural Biology ◽

10.1016/j.jsb.2020.107490 ◽

2020 ◽

Vol 210 (2) ◽

pp. 107490 ◽

Cited By ~ 1

Author(s):

Kalvis Brangulis ◽

Inara Akopjana ◽

Ivars Petrovskis ◽

Andris Kazaks ◽

Kaspars Tars

Keyword(s):

Structural Analysis ◽

Lyme Disease ◽

Borrelia Burgdorferi ◽

Gene Family ◽

Outer Surface ◽

Surface Proteins ◽

Paralogous Gene ◽

Outer Surface Proteins ◽

Key Players ◽

Paralogous Gene Family

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Outer surface proteins E and F of Borrelia burgdorferi, the agent of Lyme disease.

Infection and Immunity ◽

10.1128/iai.62.1.290-298.1994 ◽

1994 ◽

Vol 62 (1) ◽

pp. 290-298 ◽

Cited By ~ 101

Author(s):

T T Lam ◽

T P Nguyen ◽

R R Montgomery ◽

F S Kantor ◽

E Fikrig ◽

...

Keyword(s):

Lyme Disease ◽

Borrelia Burgdorferi ◽

Outer Surface ◽

Surface Proteins ◽

Outer Surface Proteins

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Identification of Borrelia burgdorferi Outer Surface Proteins

Infection and Immunity ◽

10.1128/iai.74.1.296-304.2006 ◽

2006 ◽

Vol 74 (1) ◽

pp. 296-304 ◽

Cited By ~ 70

Author(s):

Chad S. Brooks ◽

Santosh R. Vuppala ◽

Amy M. Jett ◽

Darrin R. Akins

Keyword(s):

Lyme Disease ◽

Borrelia Burgdorferi ◽

Outer Surface ◽

Natural Infection ◽

Infection Process ◽

Surface Proteins ◽

Enzyme Linked Immunosorbent Assay ◽

Mammalian Host ◽

Outer Surface Proteins ◽

Genes Encoding

ABSTRACT Several Borrelia burgdorferi outer surface proteins have been identified over the past decade that are up-regulated by temperature- and/or mammalian host-specific signals as this spirochete is transmitted from ticks to mammals. Given the potential role(s) that these differentially up-regulated proteins may play in B. burgdorferi transmission and Lyme disease pathogenesis, much attention has recently been placed on identifying additional borrelial outer surface proteins. To identify uncharacterized B. burgdorferi outer surface proteins, we previously performed a comprehensive gene expression profiling analysis of temperature-shifted and mammalian host-adapted B. burgdorferi. The combined microarray analyses revealed that many genes encoding known and putative outer surface proteins are down-regulated in mammalian host-adapted B. burgdorferi. At the same time, however, several different genes encoding putative outer surface proteins were found to be up-regulated during the transmission and infection process. Among the putative outer surface proteins identified, biochemical and surface localization analyses confirmed that seven (Bb0405, Bb0689, BbA36, BbA64, BbA66, BbA69, and BbI42) are localized to the surface of B. burgdorferi. Furthermore, enzyme-linked immunosorbent assay analysis using serum from tick-infested baboons indicated that all seven outer surface proteins identified are immunogenic and that antibodies are generated against all seven during a natural infection. Specific antibodies generated against all seven of these surface proteins were found to be bactericidal against B. burgdorferi, indicating that these newly identified outer surface proteins are prime candidates for analysis as second-generation Lyme disease vaccinogens.

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Fibroblast Protection of Borrelia burgdorferi from Doxycycline, Cefuroxime and Daptomycin Combination is Eliminated by Oregano or Carvacrol Essential Oil

10.1101/861575 ◽

2019 ◽

Author(s):

Chunxiang Bai ◽

Hua Yang ◽

Peng Cui ◽

Rong Quan ◽

Ying Zhang

Keyword(s):

Lyme Disease ◽

Essential Oil ◽

Borrelia Burgdorferi ◽

Drug Combination ◽

Defense Mechanisms ◽

Ex Vivo ◽

Fibroblast Cells ◽

Murine Fibroblast ◽

Drug Regimens

AbstractBorrelia burgdorferi could be occasionally recovered from patients after antibiotic treatment, which indicates it may resist eradication by antibiotic and host defense mechanisms. Skin fibroblast cells have previously been shown to protect the killing of B. burgdorferi by ceftriaxone, a powerful antibiotic commonly used to treat Lyme disease. In this study, we evaluated if fibroblast cells could also protect against the doxycycline+ cefuroxime+ daptomycin drug combination which has previously been shown to completely eradicate highly persistent biofilm-like microcolonies of B. burgdorferi. To do so, we utilized a GFP-labeled B. burgdorferi for infection of murine fibroblast cells and assessed the effect of the drug combination on killing the bacteria in the presence or absence of the fibroblast cells. Surprisingly, we found that fibroblasts could protect B. burgdorferi from being completely killed by the drug combination doxycycline, cefuroxime and daptomycin, which eradicated B. burgdorferi completely in the absence of fibroblast cells. Interestingly, addition of essential oil carvacrol or oregano at 0.1% could enhance the activity of the doxycycline+ cefuroxime+ daptomycin drug combination and led to complete eradication of B. burgdorferi even in the presence of fibroblast cells. Further studies are needed to determine if the essential oil drug combinations could eradicate persistent B. burgdorferi infection in vivo in animal models. Our study provides a useful and convenient ex vivo model for evaluating different drug regimens needed for developing more effective treatment of persistent Lyme disease in the future.

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