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Dive into the research topics where Sonja Metzger is active.

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Featured researches published by Sonja Metzger.


Journal of Virology | 2011

Novel Adenoviruses in Wild Primates: a High Level of Genetic Diversity and Evidence of Zoonotic Transmissions

Diana Wevers; Sonja Metzger; Fred Babweteera; Marc Bieberbach; Christophe Boesch; Kenneth Cameron; Emmanuel Couacy-Hymann; Mike Cranfield; Maryke Gray; Laurie A. Harris; Josephine Head; Kathryn Jane Jeffery; Sascha Knauf; Felix Lankester; Siv Aina J. Leendertz; Elizabeth V. Lonsdorf; Lawrence Mugisha; Andreas Nitsche; Patricia Reed; Martha M. Robbins; Dominic A. Travis; Zinta Zommers; Fabian H. Leendertz; Bernhard Ehlers

ABSTRACT Adenoviruses (AdVs) broadly infect vertebrate hosts, including a variety of nonhuman primates (NHPs). In the present study, we identified AdVs in NHPs living in their natural habitats, and through the combination of phylogenetic analyses and information on the habitats and epidemiological settings, we detected possible horizontal transmission events between NHPs and humans. Wild NHPs were analyzed with a pan-primate AdV-specific PCR using a degenerate nested primer set that targets the highly conserved adenovirus DNA polymerase gene. A plethora of novel AdV sequences were identified, representing at least 45 distinct AdVs. From the AdV-positive individuals, 29 nearly complete hexon genes were amplified and, based on phylogenetic analysis, tentatively allocated to all known human AdV species (Human adenovirus A to Human adenovirus G [HAdV-A to -G]) as well as to the only simian AdV species (Simian adenovirus A [SAdV-A]). Interestingly, five of the AdVs detected in great apes grouped into the HAdV-A, HAdV-D, HAdV-F, or SAdV-A clade. Furthermore, we report the first detection of AdVs in New World monkeys, clustering at the base of the primate AdV evolutionary tree. Most notably, six chimpanzee AdVs of species HAdV-A to HAdV-F revealed a remarkably close relationship to human AdVs, possibly indicating recent interspecies transmission events.


Emerging Infectious Diseases | 2010

Wild Chimpanzees Infected with 5 Plasmodium Species

Marco Kaiser; Anna Löwa; Markus Ulrich; Heinz Ellerbrok; Adeelia S. Goffe; Anja Blasse; Zinta Zommers; Emmanuel Couacy-Hymann; Fred Babweteera; Klaus Zuberbühler; Sonja Metzger; Sebastian Geidel; Christophe Boesch; Thomas R. Gillespie; Fabian H. Leendertz

Data are missing on the diversity of Plasmodium spp. infecting apes that live in their natural habitat, with limited possibility of human-mosquito-ape exchange. We surveyed Plasmodium spp. diversity in wild chimpanzees living in an undisturbed tropical rainforest habitat and found 5 species: P. malariae, P. vivax, P. ovale, P. reichenowi, and P. gaboni.


Emerging Infectious Diseases | 2013

Novel mycobacterium tuberculosis complex isolate from a wild chimpanzee

Mireia Coscolla; Astrid Lewin; Sonja Metzger; Kerstin Maetz-Rennsing; Sébastien Calvignac-Spencer; Andreas Nitsche; Pjotr Wojtek Dabrowski; Aleksandar Radonić; Stefan Niemann; Julian Parkhill; Emmanuel Couacy-Hymann; Julia Feldman; Iñaki Comas; Christophe Boesch; Sebastien Gagneux; Fabian H. Leendertz

Tuberculosis (TB) is caused by gram-positive bacteria known as the Mycobacterium tuberculosis complex (MTBC). MTBC include several human-associated lineages and several variants adapted to domestic and, more rarely, wild animal species. We report an M. tuberculosis strain isolated from a wild chimpanzee in Côte d’Ivoire that was shown by comparative genomic and phylogenomic analyses to belong to a new lineage of MTBC, closer to the human-associated lineage 6 (also known as M. africanum West Africa 2) than to the other classical animal-associated MTBC strains. These results show that the general view of the genetic diversity of MTBC is limited and support the possibility that other MTBC variants exist, particularly in wild mammals in Africa. Exploring this diversity is crucial to the understanding of the biology and evolutionary history of this widespread infectious disease.


Emerging Infectious Diseases | 2014

Fatal monkeypox in wild-living sooty mangabey, Côte d’Ivoire, 2012

Aleksandar Radonić; Sonja Metzger; Piotr Wojtek Dabrowski; Emmanuel Couacy-Hymann; Livia Schuenadel; Andreas Kurth; Kerstin Mätz-Rensing; Christophe Boesch; Fabian H. Leendertz; Andreas Nitsche

We isolated a monkeypox virus from a wild-living monkey, a sooty mangabey, found dead in Taï National Park, Côte d’Ivoire, in March 2012. The whole-genome sequence obtained from this isolate and directly from clinical specimens showed its close relationship to monkeypox viruses from Western Africa.


Journal of Virology | 2013

Absence of Frequent Herpesvirus Transmission in a Nonhuman Primate Predator-Prey System in the Wild

Sripriya Murthy; Emmanuel Couacy-Hymann; Sonja Metzger; Kathrin Nowak; Hélène M. De Nys; Christophe Boesch; Roman M. Wittig; Michael A. Jarvis; Fabian H. Leendertz; Bernhard Ehlers

ABSTRACT Emergence of viruses into the human population by transmission from nonhuman primates (NHPs) represents a serious potential threat to human health that is primarily associated with the increased bushmeat trade. Transmission of RNA viruses across primate species appears to be relatively frequent. In contrast, DNA viruses appear to be largely host specific, suggesting low transmission potential. Herein, we use a primate predator-prey system to study the risk of herpesvirus transmission between different primate species in the wild. The system was comprised of western chimpanzees (Pan troglodytes verus) and their primary (western red colobus, Piliocolobus badius badius) and secondary (black-and-white colobus, Colobus polykomos) prey monkey species. NHP species were frequently observed to be coinfected with multiple beta- and gammaherpesviruses (including new cytomegalo- and rhadinoviruses). However, despite frequent exposure of chimpanzees to blood, organs, and bones of their herpesvirus-infected monkey prey, there was no evidence for cross-species herpesvirus transmission. These findings suggest that interspecies transmission of NHP beta- and gammaherpesviruses is, at most, a rare event in the wild.


Nature | 2017

Persistent anthrax as a major driver of wildlife mortality in a tropical rainforest

Constanze Hoffmann; Fee Zimmermann; Roman Biek; Hjalmar S. Kuehl; Kathrin Nowak; Roger Mundry; Anthony Agbor; Samuel Angedakin; Mimi Arandjelovic; Anja Blankenburg; Gregory Brazolla; Katherine Corogenes; Emmanuel Couacy-Hymann; Tobias Deschner; Paula Dieguez; Karsten Dierks; Ariane Düx; Susann Dupke; Henk Eshuis; Pierre Formenty; Yisa Ginath Yuh; Annemarie Goedmakers; Jan F. Gogarten; Anne-Céline Granjon; Scott William McGraw; Roland Grunow; John Hart; Sorrel Jones; Jessica Junker; John Kiang

Anthrax is a globally important animal disease and zoonosis. Despite this, our current knowledge of anthrax ecology is largely limited to arid ecosystems, where outbreaks are most commonly reported. Here we show that the dynamics of an anthrax-causing agent, Bacillus cereus biovar anthracis, in a tropical rainforest have severe consequences for local wildlife communities. Using data and samples collected over three decades, we show that rainforest anthrax is a persistent and widespread cause of death for a broad range of mammalian hosts. We predict that this pathogen will accelerate the decline and possibly result in the extirpation of local chimpanzee (Pan troglodytes verus) populations. We present the epidemiology of a cryptic pathogen and show that its presence has important implications for conservation.


PLOS ONE | 2014

Low rates of antimicrobial-resistant enterobacteriaceae in wildlife in Taï National Park, Côte d’Ivoire, surrounded by villages with high prevalence of multiresistant ESBL-producing Escherichia coli in people and domestic animals

Katerina Albrechtova; Ivo Papousek; Hélène M. De Nys; Maude Pauly; Etile Anoh; Arsène Mossoun; Monika Dolejska; Martina Masarikova; Sonja Metzger; Emmanuel Couacy-Hymann; Chantal Akoua-Koffi; Roman M. Wittig; Jiri Klimes; Alois Cizek; Fabian H. Leendertz; Ivan Literak

Antimicrobial resistance genes can be found in all ecosystems, including those where antibiotic selective pressure has never been exerted. We investigated resistance genes in a collection of faecal samples of wildlife (non-human primates, mice), people and domestic animals (dogs, cats) in Côte d’Ivoire; in the chimpanzee research area of Taï National Park (TNP) and adjacent villages. Single bacteria isolates were collected from antibiotic-containing agar plates and subjected to molecular analysis to detect Enterobacteriaceae isolates with plasmid-mediated genes of extended-spectrum beta-lactamases (ESBLs) and plasmid-mediated quinolone resistance (PMQR). While the prevalence of ESBL-producing E. coli in the villages was 27% in people (n = 77) and 32% in dogs (n = 38), no ESBL-producer was found in wildlife of TNP (n = 75). PMQR genes, mainly represented by qnrS1, were also present in human- and dog-originating isolates from the villages (36% and 42% in people and dogs, respectively), but no qnrS has been found in the park. In TNP, different variants of qnrB were detected in Citrobacter freundii isolates originating non-human primates and mice. In conclusion, ESBL and PMQR genes frequently found in humans and domestic animals in the villages were rather exceptional in wildlife living in the protected area. Although people enter the park, the strict biosecurity levels they are obliged to follow probably impede transmission of bacteria between them and wildlife.


Scientific Reports | 2017

Evidence for Human Streptococcus pneumoniae in wild and captive chimpanzees: A potential threat to wild populations.

Sophie Köndgen; Sébastien Calvignac-Spencer; Kim S. Grützmacher; Verena Keil; Kerstin Mätz-Rensing; Kathrin Nowak; Sonja Metzger; John Kiyang; Antina Lübke Becker; Tobias Deschner; Roman M. Wittig; Felix Lankester; Fabian H. Leendertz

Habituation of wild great apes for tourism and research has had a significant positive effect on the conservation of these species. However, risks associated with such activities have been identified, specifically the transmission of human respiratory viruses to wild great apes, causing high morbidity and, occasionally, mortality. Here, we investigate the source of bacterial-viral co-infections in wild and captive chimpanzee communities in the course of several respiratory disease outbreaks. Molecular analyses showed that human respiratory syncytial viruses (HRSV) and human metapneumoviruses (HMPV) were involved in the etiology of the disease. In addition our analysis provide evidence for coinfection with Streptococcus (S.) pneumoniae. Characterisation of isolates from wild chimpanzees point towards a human origin of these bacteria. Transmission of these bacteria is of concern because – in contrast to HRSV and HMPV - S. pneumoniae can become part of the nasopharyngeal flora, contributing to the severity of respiratory disease progression. Furthermore these bacteria have the potential to spread to other individuals in the community and ultimately into the population. Targeted vaccination programs could be used to vaccinate habituated great apes but also human populations around great ape habitats, bringing health benefits to both humans and wild great apes.


Emerging Infectious Diseases | 2015

No Evidence of Gouléako and Herbert Virus Infections in Pigs, Côte d'Ivoire and Ghana

Sandra Junglen; Marco Marklewitz; Florian Zirkel; Robert Wollny; Benjamin Meyer; Hanna Heidemann; Sonja Metzger; Augustina Annan; Dickson Dei; Fabian H. Leendertz; Samuel Oppong; Christian Drosten

A recent report suggested that 2 novel bunyaviruses discovered in insects in Côte d’Ivoire caused lethal disease in swine in South Korea. We conducted cell culture studies and tested serum from pigs exposed to mosquitoes in Côte d’Ivoire and Ghana and found no evidence for infection in pigs.


Molecular Ecology | 2013

Carrion fly-derived DNA as a tool for comprehensive and cost-effective assessment of mammalian biodiversity

Sébastien Calvignac-Spencer; Kevin Merkel; Nadine Kutzner; Hjalmar S. Kühl; Christophe Boesch; Peter M. Kappeler; Sonja Metzger; Grit Schubert; Fabian H. Leendertz

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Andreas Nitsche

Humboldt University of Berlin

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