Plasmid-Encoded Pgp5 Is a Significant Contributor to Chlamydia muridarum Induction of Hydrosalpinx

Huang, Yumeng; Zhang, Qi; Yang, Zhangsheng; Conrad, Turner; Liu, Yuanjun; Zhong, Guangming

doi:10.1371/journal.pone.0124840

Cited by 31 publications

(48 citation statements)

References 34 publications

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“…The success in transforming C. muridarum [19] further enabled the evaluation of the plasmid-encoded pGPs in a female mouse hydrosalpinx/infertility induction model [79–81]. C. muridarum deficient in pGP3 either by deletion of the pgp3 gene or installation of a premature stop codon in the start region of the gene largely phenocopied the plasmid-free C. muridarum [20] although deficiency in pGP5 also reduced C. muridarum pathogenicity [82]. The failure of the pGP3-deficient C. muridarum to induce hydrosalpinx correlates with its reduced ascension to, decreased survival and attenuated induction of inflammatory infiltration in the oviduct [20].…”

Section: Pgp3 Is a Key Virulence Factor Encoded By The Plasmidmentioning

confidence: 99%

“…The C. trachomatis pgp5 was as competent as C. muridarum pgp5 in suppressing the expression of the plasmid-dependent genes during C. muridarum infection, demonstrating that inhibition of the plasmid-dependent chromosomal genes is a common property of Pgp5 protein from different chlamydial species. More importantly, when pGP5-deficient C. muridarum was evaluated in mice, it displayed a partial but significant attenuation in inducing hydrosalpinx [82], suggesting that pGP5 also contributes to chlamydial pathogenicity in the mouse upper genital tract although not as robust as Pgp3 [20]. The challenge questions are how pGP5 regulates its target gene expression in chlamydial chromosome and whether the attenuated pathogenicity is caused by the increased expression of the chromosomal genes.…”

Section: The Roles Of Pgp5 and Pgp8 And Their Antisense Rnas In Chlammentioning

confidence: 99%

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Chlamydial Plasmid-Dependent Pathogenicity

Zhong

2017

Trends in Microbiology

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Most Chlamydia species carry a 7.5kb plasmid encoding 8 open reading frames conventionally called plasmid glycoproteins 1–8 or pGP1–8. Although the plasmid is not critical for chlamydial growth in vitro, its role in chlamydial pathogenesis is clearly demonstrated in the genital tracts of mice infected with Chlamydia muridarum, a model for investigating the human pathogen Chlamydia trachomatis. Plasmid-free C. trachomatis is also attenuated in both the mouse genital tract and nonhuman primate ocular tissue. Deficiency in pGP3 alone, which is regulated by pGP4, largely reproduced the in vivo but not in vitro phenotypes of the plasmid-free organisms, suggesting that pGP3 is a key in vivo virulence factor. The positive and negative regulations of some chromosomal genes by pGP4 and pGP5 respectively may allow the plasmid to promote chlamydial adaptation to varied animal tissue environments. The focus of this review is to summarize the progress on the pathogenic functions of the plasmid-encoded open reading frames, which may motivate further investigation of the molecular mechanisms of chlamydial pathogenicity and development of medical utility of the chlamydial plasmid system.

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Section: Pgp3 Is a Key Virulence Factor Encoded By The Plasmidmentioning

confidence: 99%

Section: The Roles Of Pgp5 and Pgp8 And Their Antisense Rnas In Chlammentioning

confidence: 99%

Chlamydial Plasmid-Dependent Pathogenicity

Zhong

2017

Trends in Microbiology

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“…We have previously demonstrated that C. muridarum clones carrying mutations in the chromosomal gene tc0237 and/or tc0668 or plasmid gene pgp3 are significantly attenuated in inducing hydrosalpinx in the mouse upper genital tract (26)(27)(28)(29)(30). Thus, the C. muridarum chromosomal gene-encoded TC0237/TC0668 and plasmid-encoded pGP3 have been defined as genital tract virulence factors (23,31).…”

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Distinct Roles of Chromosome- versus Plasmid-Encoded Genital Tract Virulence Factors in Promoting Chlamydia muridarum Colonization in the Gastrointestinal Tract

et al. 2019

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The genital pathogen Chlamydia is known to colonize the gastrointestinal tract. Orally delivered Chlamydia muridarum can reach the colon and maintain a long-lasting colonization there. However, C. muridarum with mutations in chromosomal genes tc0237 and tc0668 (designated a chromosomal mutant) or deficient in plasmid-encoded pGP3 (designated a plasmid mutant) is unable to do so. We now report that the chromosomal mutant is still able to reach the colon while the plasmid mutant fails to do so following an oral delivery, suggesting that lack of colon colonization by different mutants may involve distinct mechanisms. Consistently, a direct intracolonic delivery selectively restored the ability of the plasmid mutant, but not the chromosomal mutant, to colonize the colon. The chromosomal mutant was rescued only in the colon of mice deficient in gamma interferon (IFN-␥). Thus, the chromosomal mutant's deficiency in colonizing colonic mucosal tissue is likely due to its increased susceptibility to IFN-␥-mediated immunity. Furthermore, IFN-␥ deficiency was sufficient for rescuing colon colonization of an orally delivered chromosomal mutant but not plasmid mutant while mice deficient in gastric acid production rescued the plasmid mutant but not the chromosomal mutant. Both mutants are attenuated in inducing genital tract pathology. Thus, we propose that chlamydial chromosomal-gene-encoded genital tract virulence factors may be essential for Chlamydia to maintain long-lasting colonization in the colon while the plasmid may enable Chlamydia to reach the colon by promoting evasion of gastric barriers.

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“…Development of a C. trachomatis plasmid manipulation system and a transformation system for C. muridarum helped to reveal that plasmid-encoded Pgp3 and Pgp5 are crucial for C. muridarum induction of upper genital tract disease (17,18). Deficiency in Pgp3 or Pgp5 results in reduced ascending infection to and chronic inflammatory infiltration in the upper genital tract.…”

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The Chromosome-Encoded Hypothetical Protein TC0668 Is an Upper Genital Tract Pathogenicity Factor of Chlamydia muridarum

et al. 2016

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cWe previously associated a missense mutation of the tc0668 gene of serial in vitro-passaged Chlamydia muridarum, a murine model of human urogenital C. trachomatis, with severely attenuated disease development in the upper genital tract of female mice. Since these mutants also contained a TC0237 Q117E missense mutation that enhances their in vitro infectivity, an effort was made here to isolate and characterize a tc0668 single mutant to determine its individual contribution to urogenital pathogenicity. Detailed genetic analysis of C. muridarum passages revealed a truncated variant with a G216* nonsense mutation of the 408-amino-acid TC0668 protein that does not produce a detectable product. Intracellular growth and infectivity of C. muridarum in vitro remain unaffected in the absence of TC0668. Intravaginal inoculation of the TC0668 null mutant into C3H/HeJ mice results in a typical course of lower genital tract infection but, unlike a pathogenic isogenic control, is unable to elicit significant chronic inflammation of the oviduct and fails to induce hydrosalpinx. Thus, TC0668 is demonstrated as an important chromosome-encoded urogenital pathogenicity factor of C. muridarum and the first with these characteristics to be discovered for a Chlamydia pathogen. Chlamydia muridarum is a Gram-negative obligate intracellular pathogen that was isolated from a steady-state respiratory infection of laboratory mice in the early 1940s (1, 2). Like other chlamydial organisms, C. muridarum has a biphasic life cycle that alternates between infectious elementary body (EB) and replicating reticulate body (RB) morphologies. The genome of C. muridarum is reductively evolved, containing a 1.07-Mb circular chromosome and single 7.5-kb extrachromosomal plasmid (3). In that C. muridarum and other chlamydial pathogens have fewer than 1,000 genes and ϳ900 encoded proteins, roughly half the number encoded by environmental chlamydial organisms that parasitize simple single-celled eukaryotes (4), it is not known which of the many cryptic genetic factors allow them to thrive within and harm complex vertebrates.In the laboratory, C. muridarum is used as a model of urogenital disease resulting from sexually transmitted Chlamydia trachomatis in women. The basic biology and genomes of these two pathogens are highly conserved. The urogenital biovar of C. trachomatis is responsible for the most reported cases of bacterial infection in the United States (5) and is a pervasive global health problem (6). In women, ascending infection from the lower to upper genital tracts, separated by the cervical barrier, can lead to loss of the ciliated epithelium and irreversible fibrotic remodeling of the fallopian tubes after primary infection is resolved (7). If left untreated, often because of asymptomatic infection (8), afflicted women can experience severe chronic sequelae, such as tubal blockage, hydrosalpinx, spontaneous abortion, ectopic pregnancy, and tubal factor infertility (9, 10). Genital inoculation of female mice with C. muridarum results in analo...

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Plasmid-Encoded Pgp5 Is a Significant Contributor to Chlamydia muridarum Induction of Hydrosalpinx

Cited by 31 publications

References 34 publications

Chlamydial Plasmid-Dependent Pathogenicity

Chlamydial Plasmid-Dependent Pathogenicity

Distinct Roles of Chromosome- versus Plasmid-Encoded Genital Tract Virulence Factors in Promoting Chlamydia muridarum Colonization in the Gastrointestinal Tract

The Chromosome-Encoded Hypothetical Protein TC0668 Is an Upper Genital Tract Pathogenicity Factor of Chlamydia muridarum

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