Early MicroRNA expression profile as a prognostic biomarker for the development of pelvic inflammatory disease in a mouse model of chlamydial genital infection

Yeruva, L; Myers, GSA; Spencer, N; Creasy, HH; Adams, NE; Maurelli, AT; McChesney, GR; Cleves, MA; Ravel, J; Bowlin, A; Rank, RG

Early MicroRNA expression profile as a prognostic biomarker for the development of pelvic inflammatory disease in a mouse model of chlamydial genital infection

Yeruva, L Myers, GSA

Spencer, N Creasy, HH Adams, NE Maurelli, AT McChesney, GR Cleves, MA Ravel, J Bowlin, A Rank, RG

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Publication Type:: Journal Article
Citation:: mBio, 2014, 5 (3)
Issue Date:: 2014-06-24

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Field	Value	Language
dc.contributor.author	Yeruva, L	en_US
dc.contributor.author	Myers, GSA https://orcid.org/0000-0002-4756-4810	en_US
dc.contributor.author	Spencer, N	en_US
dc.contributor.author	Creasy, HH	en_US
dc.contributor.author	Adams, NE	en_US
dc.contributor.author	Maurelli, AT	en_US
dc.contributor.author	McChesney, GR	en_US
dc.contributor.author	Cleves, MA	en_US
dc.contributor.author	Ravel, J	en_US
dc.contributor.author	Bowlin, A	en_US
dc.contributor.author	Rank, RG	en_US
dc.date.issued	2014-06-24	en_US
dc.identifier.citation	mBio, 2014, 5 (3)	en_US
dc.identifier.issn	2161-2129	en_US
dc.identifier.uri	http://hdl.handle.net/10453/37149
dc.description.abstract	It is not currently possible to predict the probability of whether a woman with a chlamydial genital infection will develop pelvic inflammatory disease (PID). To determine if specific biomarkers may be associated with distinct chlamydial pathotypes, we utilized two Chlamydia muridarum variants (C. muridarum Var001 [CmVar001] and CmVar004) that differ in their abilities to elicit upper genital tract pathology in a mouse model. CmVar004 has a lower growth rate in vitro and induces pathology in only 20% of C57BL/6 mouse oviducts versus 83.3% of oviducts in CmVar001-infected mice. To determine if chemokine and cytokine production within 24 h of infection is associated with the outcome of pathology, levels of 15 chemokines and cytokines were measured. CmVar004 infection induced significantly lower levels of CXCL1, CXCL2, tumor necrosis factor alpha (TNF-α), and CCL2 in comparison to CmVar001 infection with similar rRNA (rs16) levels for Chlamydiae. A combination of microRNA (miRNA) sequencing and quantitative real-time PCR (qRT-PCR) analysis of 134 inflammation-related miRNAs was performed 24 h postinfection to determine if the chemokine/cytokine responses would also be reflected in miRNA expression profiles. Interestingly, 12 miRNAs (miR-135a-5p, miR298-5p, miR142-3p, miR223-3p, miR299a-3p, miR147-3p, miR105, miR325-3p, miR132-3p, miR142-5p, miR155-5p, and miR-410-3p) were overexpressed during CmVar004 infection compared to CmVar001 infection, inversely correlating with the respective chemokine/cytokine responses. To our knowledge, this is the first report demonstrating that early biomarkers elicited in the host can differentiate between two pathological variants of chlamydiae and be predictive of upper tract disease. © 2014 Yeruva et al.	en_US
dc.relation.ispartof	mBio	en_US
dc.relation.isbasedon	10.1128/mBio.01241-14	en_US
dc.subject.mesh	Animals	en_US
dc.subject.mesh	Mice, Inbred BALB C	en_US
dc.subject.mesh	Mice, Inbred C57BL	en_US
dc.subject.mesh	Humans	en_US
dc.subject.mesh	Mice	en_US
dc.subject.mesh	Chlamydia	en_US
dc.subject.mesh	Chlamydia Infections	en_US
dc.subject.mesh	Pelvic Inflammatory Disease	en_US
dc.subject.mesh	Disease Models, Animal	en_US
dc.subject.mesh	MicroRNAs	en_US
dc.subject.mesh	Chemokines	en_US
dc.subject.mesh	Biomarkers	en_US
dc.subject.mesh	Cytokines	en_US
dc.subject.mesh	Female	en_US
dc.subject.mesh	Molecular Sequence Data	en_US
dc.subject.mesh	Prognosis	en_US
dc.subject.mesh	Transcriptome	en_US
dc.subject.mesh	Virulence	en_US
dc.title	Early MicroRNA expression profile as a prognostic biomarker for the development of pelvic inflammatory disease in a mouse model of chlamydial genital infection	en_US
dc.type	Journal Article
utslib.citation.volume	3	en_US
utslib.citation.volume	5	en_US
utslib.for	0605 Microbiology	en_US
pubs.embargo.period	Not known	en_US
pubs.organisational-group	/University of Technology Sydney
pubs.organisational-group	/University of Technology Sydney/Faculty of Science
pubs.organisational-group	/University of Technology Sydney/Strength - ithree - Institute of Infection, Immunity and Innovation
utslib.copyright.status	open_access
pubs.issue	3	en_US
pubs.publication-status	Published	en_US
pubs.volume	5	en_US

Abstract:

It is not currently possible to predict the probability of whether a woman with a chlamydial genital infection will develop pelvic inflammatory disease (PID). To determine if specific biomarkers may be associated with distinct chlamydial pathotypes, we utilized two Chlamydia muridarum variants (C. muridarum Var001 [CmVar001] and CmVar004) that differ in their abilities to elicit upper genital tract pathology in a mouse model. CmVar004 has a lower growth rate in vitro and induces pathology in only 20% of C57BL/6 mouse oviducts versus 83.3% of oviducts in CmVar001-infected mice. To determine if chemokine and cytokine production within 24 h of infection is associated with the outcome of pathology, levels of 15 chemokines and cytokines were measured. CmVar004 infection induced significantly lower levels of CXCL1, CXCL2, tumor necrosis factor alpha (TNF-α), and CCL2 in comparison to CmVar001 infection with similar rRNA (rs16) levels for Chlamydiae. A combination of microRNA (miRNA) sequencing and quantitative real-time PCR (qRT-PCR) analysis of 134 inflammation-related miRNAs was performed 24 h postinfection to determine if the chemokine/cytokine responses would also be reflected in miRNA expression profiles. Interestingly, 12 miRNAs (miR-135a-5p, miR298-5p, miR142-3p, miR223-3p, miR299a-3p, miR147-3p, miR105, miR325-3p, miR132-3p, miR142-5p, miR155-5p, and miR-410-3p) were overexpressed during CmVar004 infection compared to CmVar001 infection, inversely correlating with the respective chemokine/cytokine responses. To our knowledge, this is the first report demonstrating that early biomarkers elicited in the host can differentiate between two pathological variants of chlamydiae and be predictive of upper tract disease. © 2014 Yeruva et al.

Please use this identifier to cite or link to this item:

http://hdl.handle.net/10453/37149