Decorin‐binding adhesins from <i>Borrelia burgdorferi</i>

Guo, Betty P.; Brown, Eric L.; Dorward, David W.; Rosenberg, Lawrence; Höök, Magnus

doi:10.1046/j.1365-2958.1998.01103.x

Cited by 248 publications

(265 citation statements)

References 39 publications

(44 reference statements)

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“…6D) and DbpA (Fig. 6E), which are well-characterized adhesins mediating adherence of B. burgdorferi to fibronectin (64,75) and decorin (39), respectively. In addition, there was increased expression of BBA64 in ES25 while there was little or no expression of this lp54-encoded protein in both the parental control strain and MSK5 when these strains are propagated in BSK-II medium at pH 7.6 and 32°C.…”

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confidence: 99%

“…Differential gene expression plays a critical role in the transmission, colonization, and dissemination of B. burgdorferi in mammalian hosts. Several of these open reading frames (ORFs) include mediators that provide a selective advantage to B. burgdorferi by enhancing its ability to adhere to host matrices (24,39,64) and to evade the mediators of innate and adaptive immunity (16,26,48,89), as well as other deleterious physiological processes encountered in its hosts (27). A number of studies have determined the significance of alterations of surface lipoproteins in response to these signals, and the molecular mechanisms responsible for these changes are beginning to be understood (41,86).…”

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confidence: 99%

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Overexpression of CsrA (BB0184) Alters the Morphology and Antigen Profiles ofBorrelia burgdorferi

et al. 2009

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Section: Downloaded Frommentioning

confidence: 99%

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confidence: 99%

Overexpression of CsrA (BB0184) Alters the Morphology and Antigen Profiles ofBorrelia burgdorferi

et al. 2009

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“…The recombinant proteins rEfb (17), rEfb104, rEfb120, and rEfb165 were expressed as recombinant N-terminal His-tagged proteins that allowed for purification using metal ion-chelating chromatography as described previously (12,59). Proteins were expressed and purified as previously described (59,60).…”

Section: Cloning Of and Expression Of The Efb Truncations From S Aureusmentioning

confidence: 99%

Identification and Characterization of the C3 Binding Domain of the Staphylococcus aureus Extracellular Fibrinogen-binding Protein (Efb)

Lee

Liang

Höök

et al. 2004

Journal of Biological Chemistry

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115

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The secreted Staphylococcus aureus extracellular fibrinogen-binding protein (Efb) is a virulence factor that binds to both the complement component C3b and fibrinogen. Our laboratory previously reported that by binding to C3b, Efb inhibited complement activation and blocked opsonophagocytosis. We have now located the Efb binding domain in C3b to the C3d fragment and determined a disassociation constant (K d ) of 0.24 M for the Efb-C3d binding using intrinsic fluorescence quenching assays. Using truncated, recombinant forms of Efb, we also demonstrate that the C3b binding region of Efb is located within the C terminus, in contrast to the fibrinogen binding domains that are located at the N-terminal end of the protein. Enzyme-linked immunosorbent assay-type binding assays demonstrated that recombinant Efb could bind to both C3b and fibrinogen simultaneously, forming a trimolecular complex and that the C-terminal region of Efb could inhibit complement activity in vitro. In addition, secondary structure analysis using circular dichroism spectroscopy revealed that the C-terminal, C3b binding region of Efb is composed primarily of ␣-helices, suggesting that this domain of Efb represents a novel type of C3b-binding protein.

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“…Among the B. burgdorferi proteins that bind ECM components are DbpA and DbpB, which bind decorin [145], BBK32, which binds fibronectin [146], Bgp, which binds proteoglycans [147], and P66, which binds integrins [148]. These proteins may help B. burgdorferi migrate through mammalian tissue and persist in joints and skin, where the spirochetes may be inaccessible to circulating antibodies.…”

Section: B Burgdorferi Products Required For Mammalian Infectionmentioning

confidence: 99%

Biology of Infection with Borrelia burgdorferi

Tilly

Rosa

Stewart

2008

Infectious Disease Clinics of North America

177

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The spirochete Borrelia burgdorferi is a tick-borne obligate parasite whose normal reservoir is a variety of small mammals [1]. Whereas infection of these natural hosts does not lead to disease, infection of humans can result in Lyme disease, as a consequence of the human immunopathological response to B. burgdorferi [2,3]. Consistent with the pathogenesis of Lyme disease, bacterial products that allow B. burgdorferi to replicate and survive, rather than true "virulence factors," appear to be primarily what is required for the bacterium to cause disease in a susceptible host. In support of this idea, the genome sequence of B31, the type strain of B. burgdorferi sensu stricto [4,5], revealed that the bacterium lacks factors common to many bacterial pathogens, such as lipopolysaccharide, toxins, and specialized secretion systems. In this chapter, we will describe the basic biology of B. burgdorferi, and some of the bacterial components required to infect and survive in the mammalian and tick hosts.

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Decorin‐binding adhesins from Borrelia burgdorferi

Cited by 248 publications

References 39 publications

Overexpression of CsrA (BB0184) Alters the Morphology and Antigen Profiles ofBorrelia burgdorferi

Overexpression of CsrA (BB0184) Alters the Morphology and Antigen Profiles ofBorrelia burgdorferi

Identification and Characterization of the C3 Binding Domain of the Staphylococcus aureus Extracellular Fibrinogen-binding Protein (Efb)

Biology of Infection with Borrelia burgdorferi

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