Multinucleation during C. trachomatis Infections Is Caused by the Contribution of Two Effector Pathways

Brown, Heather M.; Knowlton, Andrea E.; Snavely, Emily; Nguyen, Bidong D.; Richards, Theresa S.; Grieshaber, Scott S.

doi:10.1371/journal.pone.0100763

Cited by 20 publications

(40 citation statements)

References 38 publications

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“…Indeed, mutants from this collection have been recently characterized (Chen et al, 2014; Snavely and Kokes et al, 2014; Brown et al, 2014), underscoring its utility in reverse genetic applications. Mutant strains were sequenced in pools of 20 to lower the overall DNA sequencing costs (~$15/genome).…”

Section: Discussionmentioning

confidence: 99%

Integrating Chemical Mutagenesis and Whole-Genome Sequencing as a Platform for Forward and Reverse Genetic Analysis of Chlamydia

Kokes

Dunn

Granek

et al. 2015

Cell Host & Microbe

117

185

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SUMMARY Gene inactivation by transposon insertion or allelic exchange is a powerful approach to probe gene function. Unfortunately, many microbes, including Chlamydia, are not amenable to routine molecular genetic manipulations. Here we describe an arrayed library of chemically-induced mutants of the genetically-intransigent pathogen Chlamydia trachomatis, in which all mutations have been identified by whole genome sequencing, providing a platform for reverse genetic applications. An analysis of possible loss-of-function mutations in the collection uncovered plasticity in the central metabolic properties of this obligate intracellular pathogen. We also describe the use of the library in a forward genetic screen that identified InaC as a bacterial factor that binds host ARF and 14-3-3 proteins to modulate F-actin assembly and Golgi redistribution around the pathogenic vacuole. This work provides a robust platform for reverse and forward genetic approaches in Chlamydia and should serve as a valuable resource to the community.

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Section: Discussionmentioning

confidence: 99%

Integrating Chemical Mutagenesis and Whole-Genome Sequencing as a Platform for Forward and Reverse Genetic Analysis of Chlamydia

Kokes

Dunn

Granek

et al. 2015

Cell Host & Microbe

117

185

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“…Chlamydia spp. induce early mitotic exit by bypassing the spindle assembly checkpoint 111 . C. pneumoniae may mediate the arrest of the cell cycle through the T3SS effector, CopN, which has been reported to bind to microtubules and perturb their assembly in vitro ; however, whether this occurs during infection is unclear 112,113 .…”

Section: Modifying the Host Responsementioning

confidence: 99%

“…CPAF is required for the induction of centrosome amplification, potentially through the degradation of one or more proteins that control centrosome duplication 111 . C. trachomatis also prevents centrosome clustering during mitosis in a CPAF-independent manner, presumably through the Inc-mediated tethering of centrosomes to the inclusion 51,111,115,116 . The cumulative effect of centro some amplification, early mitotic exit and errors in centrosome-positioning, halts cytokinesis, which results in multinucleated cells 111,114 .…”

Section: Modifying the Host Responsementioning

confidence: 99%

Chlamydia cell biology and pathogenesis

2016

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Chlamydia spp. are important causes of human disease for which no effective vaccine exists. These obligate intracellular pathogens replicate in a specialized membrane compartment and use a large arsenal of secreted effectors to survive in the hostile intracellular environment of the host. In this Review, we summarize the progress in decoding the interactions between Chlamydia spp. and their hosts that has been made possible by recent technological advances in chlamydial proteomics and genetics. The field is now poised to decipher the molecular mechanisms that underlie the intimate interactions between Chlamydia spp. and their hosts, which will open up many exciting avenues of research for these medically important pathogens.

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“…5). This collection of mutants also serves as a platform for reverse genetics and has facilitated the identification of several strains carrying recently characterized mutations of interest (160)(161)(162). Furthermore, the remaining point mutations offer a comprehensive source of point mutations that can be screened for suppressors, adaptive mutations, conditional alleles, and partial loss-and gain-of-function mutations.…”

Section: Resources For Genome-wide Genetic Analysismentioning

confidence: 99%

Emancipating Chlamydia: Advances in the Genetic Manipulation of a Recalcitrant Intracellular Pathogen

Bastidas

Valdivia

2016

Microbiol Mol Biol Rev

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SUMMARYChlamydiaspecies infect millions of individuals worldwide and are important etiological agents of sexually transmitted disease, infertility, and blinding trachoma. Historically, the genetic intractability of this intracellular pathogen has hindered the molecular dissection of virulence factors contributing to its pathogenesis. The obligate intracellular life cycle ofChlamydiaand restrictions on the use of antibiotics as selectable markers have impeded the development of molecular tools to genetically manipulate these pathogens. However, recent developments in the field have resulted in significant gains in our ability to alter the genome ofChlamydia, which will expedite the elucidation of virulence mechanisms. In this review, we discuss the challenges affecting the development of molecular genetic tools forChlamydiaand the work that laid the foundation for recent advancements in the genetic analysis of this recalcitrant pathogen.

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Multinucleation during C. trachomatis Infections Is Caused by the Contribution of Two Effector Pathways

Cited by 20 publications

References 38 publications

Integrating Chemical Mutagenesis and Whole-Genome Sequencing as a Platform for Forward and Reverse Genetic Analysis of Chlamydia

Integrating Chemical Mutagenesis and Whole-Genome Sequencing as a Platform for Forward and Reverse Genetic Analysis of Chlamydia

Chlamydia cell biology and pathogenesis

Emancipating Chlamydia: Advances in the Genetic Manipulation of a Recalcitrant Intracellular Pathogen

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