Chlamydia trachomatis Polymorphic Membrane Protein D Is a Virulence Factor Involved in Early Host-Cell Interactions

Kari, László; Southern, Timothy R.; Downey, Carey J.; Watkins, Heather; Randall, Linnell B.; Taylor, Lacey D.; Sturdevant, Gail L.; Whitmire, William M.

doi:10.1128/iai.01686-14

Cited by 37 publications

(34 citation statements)

References 33 publications

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“…Interestingly, at later time points (2 weeks post-infection), there were no differences in terms of ocular bacterial burden. 65 These data suggest that PmpD plays a critical role in chlamydial pathogenesis at the early stages of infection.…”

Section: Functional Properties As Adhesinsmentioning

confidence: 87%

Chlamydial polymorphic membrane proteins: regulation, function and potential vaccine candidates

et al. 2015

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Section: Functional Properties As Adhesinsmentioning

confidence: 87%

Chlamydial polymorphic membrane proteins: regulation, function and potential vaccine candidates

et al. 2015

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“…Limitations of this method include extensive hands-on work to both create the library and identify mutants along with back-end whole-genome sequencing to confirm the clonal isolate contains a mutation only in the gene of interest. This reverse genetic approach has been used to study the function of trpB and pmpD in C. trachomatis and has been adapted for use with C. muridarum (28,67,68).…”

Section: Targeting the Chromosomementioning

confidence: 99%

A Coming of Age Story: Chlamydia in the Post-Genetic Era

Hooppaw

Fisher

2016

Infect Immun

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Chlamydia spp. are ubiquitous, obligate, intracellular Gram-negative bacterial pathogens that undergo a unique biphasic developmental cycle transitioning between the infectious, extracellular elementary body and the replicative, intracellular reticulate body. The primary Chlamydia species associated with human disease are C. trachomatis, which is the leading cause of both reportable bacterial sexually transmitted infections and preventable blindness, and C. pneumoniae, which infects the respiratory tract and is associated with cardiovascular disease. Collectively, these pathogens are a significant source of morbidity and pose a substantial financial burden on the global economy. Past efforts to elucidate virulence mechanisms of these unique and important pathogens were largely hindered by an absence of genetic methods. Watershed studies in 2011 and 2012 demonstrated that forward and reverse genetic approaches were feasible with Chlamydia and that shuttle vectors could be selected and maintained within the bacterium. While these breakthroughs have led to a steady expansion of the chlamydial genetic tool kit, there are still roads left to be traveled. This minireview provides a synopsis of the currently available genetic methods for Chlamydia along with a comparison to the methods used in other obligate intracellular bacteria. Limitations and advantages of these techniques will be discussed with an eye toward the methods still needed, and how the current state of the art for genetics in obligate intracellular bacteria could direct future technological advances for Chlamydia.

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“…140,141 An important addition around the same time was the use of chemical mutagens, such as ethyl methanesulfonate, to generate libraries of chlamydial mutants. [142][143][144] Unfortunately, these mutants tend to have multiple mutations, but nevertheless, it is possible to screen such libraries to identify clones with your gene of interest disrupted, and subsequently to evaluate such mutants in vitro. 144 By complementing the mutated gene with an intact gene on the plasmid shuttle vector, it is now possible to more definitively test the role of key virulence targets.…”

Section: The Choice Of Immunogenic Target Antigens Is Rapidly Expandingmentioning

confidence: 99%

“…[142][143][144] Unfortunately, these mutants tend to have multiple mutations, but nevertheless, it is possible to screen such libraries to identify clones with your gene of interest disrupted, and subsequently to evaluate such mutants in vitro. 144 By complementing the mutated gene with an intact gene on the plasmid shuttle vector, it is now possible to more definitively test the role of key virulence targets. Several of these newly characterized virulence targets are being evaluated as potential vaccine candidates.…”

Section: The Choice Of Immunogenic Target Antigens Is Rapidly Expandingmentioning

confidence: 99%

Development of a vaccine for Chlamydia trachomatis: challenges and current progress

Hafner¹

2015

VDT

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Abstract:Chlamydia trachomatis remains an enigmatic bacterial pathogen with no vaccine yet available to treat human ocular and genital tract infections caused by tissue-tropic serovars of the organism. Globally, it is the leading cause of preventable blindness as well as the leading cause of bacterial sexually transmitted infections. The pathogen has a range of virulence factors that enable it to successfully evade both the innate and adaptive immune system of the host. The host immune system, although protective, paradoxically is also associated closely with the pathologies of trachoma and pelvic inflammatory disease -disease sequelae of some chlamydial infections and reinfections in some genetically susceptible hosts. In this review, we focus on what is known currently about the pathogenesis of ocular and genital infections caused by this mucosal pathogen. We also discuss novel insights into the pathogenesis of infections caused by the genital and ocular serovars of C. trachomatis, including a discussion of both pathogen and host factors, such as the human microbiota at these mucosal sites as well as the current immunological challenges facing vaccine development. Finally, we discuss the current progress toward development of a vaccine against C. trachomatis. A wide range of recombinant protein antigens are being identified and, hence, are available for vaccine trials. A plasmid-free live strain has recently been produced and evaluated in the mouse (Chlamydia muridarum) and monkey (C. trachomatis) models. The data for ocular infections in the monkey model was particularly encouraging, although the path to regulatory approval of a live vaccine is still uncertain. While still a major challenge, vaccines for ocular and genital C. trachomatis infections are looking more promising.

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Chlamydia trachomatis Polymorphic Membrane Protein D Is a Virulence Factor Involved in Early Host-Cell Interactions

Cited by 37 publications

References 33 publications

Chlamydial polymorphic membrane proteins: regulation, function and potential vaccine candidates

Chlamydial polymorphic membrane proteins: regulation, function and potential vaccine candidates

A Coming of Age Story: Chlamydia in the Post-Genetic Era

Development of a vaccine for Chlamydia trachomatis: challenges and current progress

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