Hypothetical Protein BB0569 Is Essential for Chemotaxis of the Lyme Disease Spirochete Borrelia burgdorferi

Zhang, Kai; Li, Jun; Charon, Nyles W.; Li, Chunhao

doi:10.1128/jb.00877-15

Cited by 11 publications

(7 citation statements)

References 56 publications

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“…The current evidence has revealed that all of the chemotaxis genes in the cheA 2 cluster are required for chemotaxis [11][12][13]. In contrast, the genes in the cheW 2 cluster that have been studied (with the exception of bb0569, which encodes for an atypical MCP [14]) are not involved in chemotaxis in vitro. For instance, cheW 2 and cheY 2 mutants have a similar in vitro phenotype as the wild type with no apparent defect in chemotactic function [11,13,15,16].…”

Section: Introductionmentioning

confidence: 82%

A chemosensory-like histidine kinase is dispensable for chemotaxis in vitro but regulates the virulence of Borrelia burgdorferi through modulating the stability of RpoS

Sze,

Zhang,

Lynch

et al. 2023

PLoS Pathog

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As an enzootic pathogen, the Lyme disease bacterium Borrelia burgdorferi possesses multiple copies of chemotaxis proteins, including two chemotaxis histidine kinases (CHK), CheA1 and CheA2. Our previous study showed that CheA2 is a genuine CHK that is required for chemotaxis; however, the role of CheA1 remains mysterious. This report first compares the structural features that differentiate CheA1 and CheA2 and then provides evidence to show that CheA1 is an atypical CHK that controls the virulence of B. burgdorferi through modulating the stability of RpoS, a key transcriptional regulator of the spirochete. First, microscopic analyses using green-fluorescence-protein (GFP) tags reveal that CheA1 has a unique and dynamic cellular localization. Second, loss-of-function studies indicate that CheA1 is not required for chemotaxis in vitro despite sharing a high sequence and structural similarity to its counterparts from other bacteria. Third, mouse infection studies using needle inoculations show that a deletion mutant of CheA1 (cheA1mut) is able to establish systemic infection in immune-deficient mice but fails to do so in immune-competent mice albeit the mutant can survive at the inoculation site for up to 28 days. Tick and mouse infection studies further demonstrate that CheA1 is dispensable for tick colonization and acquisition but essential for tick transmission. Lastly, mechanistic studies combining immunoblotting, protein turnover, mutagenesis, and RNA-seq analyses reveal that depletion of CheA1 affects RpoS stability, leading to reduced expression of several RpoS-regulated virulence factors (i.e., OspC, BBK32, and DbpA), likely due to dysregulated clpX and lon protease expression. Bulk RNA-seq analysis of infected mouse skin tissues further show that cheA1mut fails to elicit mouse tnf-α, il-10, il-1β, and ccl2 expression, four important cytokines for Lyme disease development and B. burgdorferi transmigration. Collectively, these results reveal a unique role and regulatory mechanism of CheA1 in modulating virulence factor expression and add new insights into understanding the regulatory network of B. burgdorferi.

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Section: Introductionmentioning

confidence: 82%

A chemosensory-like histidine kinase is dispensable for chemotaxis in vitro but regulates the virulence of Borrelia burgdorferi through modulating the stability of RpoS

Sze,

Zhang,

Lynch

et al. 2023

PLoS Pathog

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“…The number of chemotaxis homologs encoded in the B. burgdorferi genome is greater and far more complex than other motile pathogens, such as E. coli or S. enterica ( 13 , 14 ). Additional genes, csrA and bb0569 , influence the motility regulation of B. burgdorferi ( 58 , 59 ). Carbon storage regulator, CsrA, is involved in posttranscriptional regulation of flagellar genes and contributes to cell morphology ( 59 , 60 ).…”

Section: Morphology Motility and Chemotaxis Regulationmentioning

confidence: 99%

“…Carbon storage regulator, CsrA, is involved in posttranscriptional regulation of flagellar genes and contributes to cell morphology ( 59 , 60 ). BB0569, annotated as a hypothetical protein, has sequence similarity to MCPs and was found to localize to the poles of the borrelial cell and important for motility and chemotaxis ( 58 ). B. burgdorferi motility is regulated throughout the enzootic cycle with the distinct behavior of intermittent swimming in the tick vector that includes periods of a non-motile state relative to the persistent swimming observed in the murine host ( 44 , 61 ).…”

Section: Morphology Motility and Chemotaxis Regulationmentioning

confidence: 99%

Borrelia burgdorferi Keeps Moving and Carries on: A Review of Borrelial Dissemination and Invasion

Hyde

2017

Front. Immunol.

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Borrelia burgdorferi is the etiological agent of Lyme disease, a multisystemic, multistage, inflammatory infection resulting in patients experiencing cardiac, neurological, and arthritic complications when not treated with antibiotics shortly after exposure. The spirochetal bacterium transmits through the Ixodes vector colonizing the dermis of a mammalian host prior to hematogenous dissemination and invasion of distal tissues all the while combating the immune response as it traverses through its pathogenic lifecycle. The innate immune response controls the borrelial burden in the dermis, but is unable to clear the infection and thereby prevent progression of disease. Dissemination in the mammalian host requires temporal regulation of virulence determinants to allow for vascular interactions, invasion, and colonization of distal tissues. Virulence determinants and/or adhesins are highly heterogenetic among environmental B. burgdorferi strains with particular genotypes being associated with the ability to disseminate to specific tissues and the severity of disease, but fail to generate cross-protective immunity between borrelial strains. The unique motility of B. burgdorferi rendered by the endoflagella serves a vital function for dissemination and protection from immune recognition. Progress has been made toward understanding the chemotactic regulation coordinating the activity of the two polar localized flagellar motors and their role in borrelial virulence, but this regulation is not yet fully understood. Distinct states of motility allow for dynamic interactions between several B. burgdorferi adhesins and host targets that play roles in transendothelial migration. Transmigration across endothelial and blood–brain barriers allows for the invasion of tissues and elicits localized immune responses. The invasive nature of B. burgdorferi is lacking in proactive mechanisms to modulate disease, such as secretion systems and toxins, but recent work has shown degradation of host extracellular matrices by B. burgdorferi contributes to the invasive capabilities of the pathogen. Additionally, B. burgdorferi may use invasion of eukaryotic cells for immune evasion and protection against environmental stresses. This review provides an overview of B. burgdorferi mechanisms for dissemination and invasion in the mammalian host, which are essential for pathogenesis and the development of persistent infection.

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“…Constitutive gene expression is mostly limited to the use of very strong promoters. Moreover, apart from a few exceptions ( 14 – 19 ), fluorescent protein reporters have primarily been used as gene expression reporters or as cellular stains for in vivo localization of the spirochete ( 13 ). Yet, fluorescent proteins have many more uses which have transformed the field of cell biology ( 20 ).…”

Section: Introductionmentioning

confidence: 99%

Fluorescent Proteins, Promoters, and Selectable Markers for Applications in the Lyme Disease Spirochete Borrelia burgdorferi

Takacs

Kloos

Scott

et al. 2018

Appl Environ Microbiol

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Genetic manipulation of the Lyme disease spirochete B. burgdorferi remains cumbersome, despite significant progress in the field. The scarcity of molecular reagents available for use in this pathogen has slowed research efforts to study its unusual biology. Of interest, B. burgdorferi displays complex cellular organization features that have yet to be understood. These include an unusual morphology and a highly fragmented genome, both of which are likely to play important roles in the bacterium’s transmission, infectivity, and persistence. Here, we complement and expand the array of molecular tools available for use in B. burgdorferi by generating and characterizing multiple fluorescent proteins, antibiotic selection markers, and promoters of varied strengths. These tools will facilitate investigations in this important human pathogen, as exemplified by the polar and midcell localization of the cell envelope regulator BB0323, which we uncovered using these reagents.

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Hypothetical Protein BB0569 Is Essential for Chemotaxis of the Lyme Disease Spirochete Borrelia burgdorferi

Cited by 11 publications

References 56 publications

A chemosensory-like histidine kinase is dispensable for chemotaxis in vitro but regulates the virulence of Borrelia burgdorferi through modulating the stability of RpoS

A chemosensory-like histidine kinase is dispensable for chemotaxis in vitro but regulates the virulence of Borrelia burgdorferi through modulating the stability of RpoS

Borrelia burgdorferi Keeps Moving and Carries on: A Review of Borrelial Dissemination and Invasion

Fluorescent Proteins, Promoters, and Selectable Markers for Applications in the Lyme Disease Spirochete Borrelia burgdorferi

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