Koala immunogenetics and chlamydial strain type are more directly involved in chlamydial disease progression in koalas from two south east Queensland koala populations than koala retrovirus subtypes

Robbins, Amy; Hanger, Jon; Jelocnik, Martina; Chaban, Bonnie

doi:10.1038/s41598-020-72050-2

Cited by 18 publications

(26 citation statements)

References 55 publications

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“…The detection of C. psittaci in a wallaby joint in this study is the first detection of C. psittaci in a marsupial. However, the severe impact of C. pecorum infections on Australian koalas, resulting in reproductive, urinary, and ocular disease, is well known [ 8 , 29 ]. Earlier reports of C. psittaci in koalas have since been revised, and to date, there remains no evidence of C. psittaci in koalas, nor any other marsupial.…”

Section: Discussionmentioning

confidence: 99%

Chlamydia Psittaci ST24: Clonal Strains of One Health Importance Dominate in Australian Horse, Bird and Human Infections

et al. 2021

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Chlamydia psittaci is traditionally regarded as a globally distributed avian pathogen that can cause zoonotic spill-over. Molecular research has identified an extended global host range and significant genetic diversity. However, Australia has reported a reduced host range (avian, horse, and human) with a dominance of clonal strains, denoted ST24. To better understand the widespread of this strain type in Australia, multilocus sequence typing (MLST) and ompA genotyping were applied on samples from a range of hosts (avian, equine, marsupial, and bovine) from Australia. MLST confirms that clonal ST24 strains dominate infections of Australian psittacine and equine hosts (82/88; 93.18%). However, this study also found novel hosts (Australian white ibis, King parrots, racing pigeon, bovine, and a wallaby) and demonstrated that strain diversity does exist in Australia. The discovery of a C. psittaci novel strain (ST306) in a novel host, the Western brush wallaby, is the first detection in a marsupial. Analysis of the results of this study applied a multidisciplinary approach regarding Chlamydia infections, equine infectious disease, ecology, and One Health. Recommendations include an update for the descriptive framework of C. psittaci disease and cell biology work to inform pathogenicity and complement molecular epidemiology.

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Section: Discussionmentioning

confidence: 99%

Chlamydia Psittaci ST24: Clonal Strains of One Health Importance Dominate in Australian Horse, Bird and Human Infections

et al. 2021

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“…Previous study has determined that KoRV proviral profiles generated from multiple sample types can be combined for analysis (12), so all samples were DNA extracted, PCR amplified to obtain the KoRV envelope gene receptor binding region from all subtypes simultaneously, deep amplicon sequenced and processed to obtain representative operational taxonomic units (OTUs) or strains present in each koala. This procedure is on February 1, 2021 by guest http://jvi.asm.org/ Downloaded from analogous to several previous KoRV proviral studies (7,11,12,19,20). Study samples generated an average of 188,016 ± 69,301 KoRV proviral reads, with an overall average Good's coverage estimate of 0.999996, meaning that overall, each sample was predicted to have been profiled to 99.9996% completion.…”

Section: Resultsmentioning

confidence: 95%

Koala Retrovirus in Northern Australia Shows a Mixture of Stable Endogenization and Exogenous Lineage Diversification within Fragmented Koala Populations

Chaban

Melzer

Ellis

et al. 2021

J Virol

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The koala population in northern Australia has become increasingly fragmented due to natural and man-made barriers and interventions. This situation has created a unique opportunity to study both endogenous and exogenous koala retrovirus (KoRV). To determine the impact that population isolation has had on KoRV diversity in Queensland, 272 koalas from six fragmented koala populations were profiled for their KoRV provirus across two natural biogeographical barriers (the St Lawrence Gap and the Brisbane Valley Barrier), one man-made geographical barrier (the city of Brisbane) and two translocation events (the single movement of koalas to an island and the repeated movement of koalas into a koala sanctuary). Analysis revealed that all koalas tested were KoRV-A positive, with 90 - 96% of the detected KoRV provirus from each koala representing a single, likely endogenous, KoRV-A strain. The next most abundant proviral sequence was a defective variant of the dominant KoRV-A strain, accounting for 3 – 10% of detected provirus. The remaining KoRV provirus represented expected exogenous strains of KoRV and included geographically localized patterns of KoRV-B, -C, -D, -F, -G, and -I. These results indicate that lineage diversification of exogenous KoRV is actively ongoing. In addition, comparison of KoRV provirus within known dam-sire-joey family groups from the koala sanctuary revealed that joeys consistently had KoRV proviral patterns more similar to their dams than their sires in KoRV-B, -C and -D provirus composition. Collectively, this study highlights both the consistency of endogenous KoRV and the diversity of exogenous KoRV across the fragmented koala populations in northern Australia. IMPORTANCE KoRV infection has become a permanent part of koalas in northern Australia. With KoRV presence and abundance linked to more severe chlamydial disease and neoplasia in these koalas, understanding how KoRV exists throughout an increasingly fragmented koala population is a key first step in designing conservation and management strategies. This survey of KoRV provirus in Queensland koalas indicates that endogenous KoRV provirus is ubiquitous and consistent throughout the state while exogenous KoRV provirus is diverse and distinct in fragmented koala populations. Understanding the prevalence and impact of both endogenous and exogenous KoRV will be needed to ensure a future for all koala populations.

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“…Studies investigating the allelic diversity of class II subunits within DA and DB genes have found that the beta subfamilies (DAB and DBB) contain more allelic diversity than the alpha subfamilies (DAA and DAA), leading to more focus on the beta subfamilies in research studies [ 45 ]. As such, the current collection of sequenced koala MHC class II alleles stands at three DAA, 42 DAB, three DBA, 26 DBB, three DCB, and four DMB alleles, with DCA and DMA alleles yet to be characterised [ 43 , 47 , 48 ].…”

Section: Chlamydial Infection Disease and Vaccine Responses In Kmentioning

confidence: 99%

“…In the same population, koalas possessing the DBB*04 allele had higher levels of Chlamydia heat shock protein 60 (c-hsp60) antibody levels than koalas without DBB*04 [ 47 ]. Moving further north to examine koalas already infected with Chlamydia in southeast Queensland, Australia, DAB*10 and DBB*04 alleles again emerged with significant associations, but to different circumstances [ 48 ]. In these infected koalas, both DAB*10 and UC*01:01 alleles were significantly more prevalent in infected koalas that did not progress to clinical disease, while DBB*04 and DCB*03 alleles were significantly more prevalent in infected koalas that did progress to clinical disease [ 48 ].…”

Section: Chlamydial Infection Disease and Vaccine Responses In Kmentioning

confidence: 99%

“…Moving further north to examine koalas already infected with Chlamydia in southeast Queensland, Australia, DAB*10 and DBB*04 alleles again emerged with significant associations, but to different circumstances [ 48 ]. In these infected koalas, both DAB*10 and UC*01:01 alleles were significantly more prevalent in infected koalas that did not progress to clinical disease, while DBB*04 and DCB*03 alleles were significantly more prevalent in infected koalas that did progress to clinical disease [ 48 ]. Finally, a modelling study that also looked at southeast Queensland koalas found that knowing the MHC class II DAB and DBB profiles of a koala improved the likelihood of predicting a koala’s chlamydial disease status and that koalas without DBB*03 were more likely to have clinical chlamydial disease [ 49 ].…”

Section: Chlamydial Infection Disease and Vaccine Responses In Kmentioning

confidence: 99%

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The Koala Immune Response to Chlamydial Infection and Vaccine Development—Advancing Our Immunological Understanding

Chaban

2021

Animals

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Chlamydia is a significant pathogen for many species, including the much-loved Australian marsupial, the koala (Phascolarctos cinereus). To combat this situation, focused research has gone into the development and refinement of a chlamydial vaccine for koalas. The foundation of this process has involved characterising the immune response of koalas to both natural chlamydial infection as well as vaccination. From parallels in human and mouse research, it is well-established that an effective anti-chlamydial response will involve a balance of cell-mediated Th1 responses involving interferon-gamma (IFN-γ), humoral Th2 responses involving systemic IgG and mucosal IgA, and inflammatory Th17 responses involving interleukin 17 (IL-17) and neutrophils. Characterisation of koalas with chlamydial disease has shown increased expression within all three of these major immunological pathways and monitoring of koalas’ post-vaccination has detected further enhancements to these key pathways. These findings offer optimism that a chlamydial vaccine for wider distribution to koalas is not far off. Recent advances in marsupial genetic knowledge and general nucleic acid assay technology have moved koala immunological research a step closer to other mammalian research systems. However, koala-specific reagents to directly assay cytokine levels and cell-surface markers are still needed to progress our understanding of koala immunology.

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Koala immunogenetics and chlamydial strain type are more directly involved in chlamydial disease progression in koalas from two south east Queensland koala populations than koala retrovirus subtypes

Cited by 18 publications

References 55 publications

Chlamydia Psittaci ST24: Clonal Strains of One Health Importance Dominate in Australian Horse, Bird and Human Infections

Chlamydia Psittaci ST24: Clonal Strains of One Health Importance Dominate in Australian Horse, Bird and Human Infections

Koala Retrovirus in Northern Australia Shows a Mixture of Stable Endogenization and Exogenous Lineage Diversification within Fragmented Koala Populations

The Koala Immune Response to Chlamydial Infection and Vaccine Development—Advancing Our Immunological Understanding

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