Your search keyword '"Gern, James E"' showing total 4 results

1. Viruses associated with ill health in wild chimpanzees.

Author

Negrey, Jacob D., Mitani, John C., Wrangham, Richard W., Otali, Emily, Reddy, Rachna B., Pappas, Tressa E., Grindle, Kristine A., Gern, James E., Machanda, Zarin P., Muller, Martin N., Langergraber, Kevin E., Emery Thompson, Melissa, and Goldberg, Tony L.

Subjects

CHIMPANZEES, VIRAL variation, METAGENOMICS, VIRUSES, VIRAL load, DISEASE outbreaks, PICORNAVIRUSES, VIRUS diseases

Abstract

Viral infection is a major cause of ill health in wild chimpanzees (Pan troglodytes), but most evidence to date has come from conspicuous disease outbreaks with high morbidity and mortality. To examine the relationship between viral infection and ill health during periods not associated with disease outbreaks, we conducted a longitudinal study of wild eastern chimpanzees (P. t. schweinfurthii) in the Kanyawara and Ngogo communities of Kibale National Park, Uganda. We collected standardized, observational health data for 4 years and then used metagenomics to characterize gastrointestinal viromes (i.e., all viruses recovered from fecal samples) in individual chimpanzees before and during episodes of clinical disease. We restricted our analyses to viruses thought to infect mammals or primarily associated with mammals, discarding viruses associated with nonmammalian hosts. We found 18 viruses (nine of which were previously identified in this population) from at least five viral families. Viral richness (number of viruses per sample) did not vary by health status. By contrast, total viral load (normalized proportion of sequences mapping to viruses) was significantly higher in ill individuals compared with healthy individuals. Furthermore, when ill, Kanyawara chimpanzees exhibited higher viral loads than Ngogo chimpanzees, and males, but not females, exhibited higher infection rates with certain viruses and higher total viral loads as they aged. Post‐hoc analyses, including the use of a machine‐learning classification method, indicated that one virus, salivirus (Picornaviridae), was the main contributor to health‐related and community‐level variation in viral loads. Another virus, chimpanzee stool‐associated virus (chisavirus; unclassified Picornavirales), was associated with ill health at Ngogo but not at Kanyawara. Chisavirus, chimpanzee adenovirus (Adenoviridae), and bufavirus (Parvoviridae) were also associated with increased age in males. Associations with sex and age are consistent with the hypothesis that nonlethal viral infections cumulatively reflect or contribute to senescence in long‐lived species such as chimpanzees. Research Highlights: Some viruses of wild primates are relatively benign but may be useful as biomarkers of physiology and health.We used metagenomic methods to characterize viral communities in feces of wild chimpanzees in two long‐term study communities (Kanyawara and Ngogo) in Kibale National Park, Uganda.Chimpanzees exhibited higher viral loads (normalized abundances of viral genetic sequences) when they were ill than when those same individuals were previously healthy.When ill, Kanyawara chimpanzees exhibited higher viral loads than Ngogo chimpanzees, and males, but not females, exhibited higher viral loads as they aged. [ABSTRACT FROM AUTHOR]

Published

2022

2. Lethal Respiratory Disease Associated with Human Rhinovirus C in Wild Chimpanzees, Uganda, 2013.

Author

Scully, Erik J., Basnet, Sarmi, Wrangham, Richard W., Muller, Martin N., Otali, Emily, Hyeroba, David, Grindle, Kristine A., Pappas, Tressa E., Thompson, Melissa Emery, Machanda, Zarin, Watters, Kelly E., Palmenberg, Ann C., Gern, James E., and Goldberg, Tony L.

Subjects

RESPIRATORY diseases, RHINOVIRUSES, CHIMPANZEES, MOLECULAR epidemiology, EPIDEMIOLOGICAL research, HEALTH

Abstract

We describe a lethal respiratory outbreak among wild chimpanzees in Uganda in 2013 for which molecular and epidemiologic analyses implicate human rhinovirus C as the cause. Postmortem samples from an infant chimpanzee yielded near-complete genome sequences throughout the respiratory tract; other pathogens were absent. Epidemiologic modeling estimated the basic reproductive number (R0) for the epidemic as 1.83, consistent with the common cold in humans. Genotyping of 41 chimpanzees and examination of 24 published chimpanzee genomes from subspecies across Africa showed universal homozygosity for the cadherin-related family member 3 CDHR3-Y529 allele, which increases risk for rhinovirus C infection and asthma in human children. These results indicate that chimpanzees exhibit a species-wide genetic susceptibility to rhinovirus C and that this virus, heretofore considered a uniquely human pathogen, can cross primate species barriers and threatens wild apes. We advocate engineering interventions and prevention strategies for rhinovirus infections for both humans and wild apes. [ABSTRACT FROM AUTHOR]

Published

2018

3. Common cold viruses circulating in children threaten wild chimpanzees through asymptomatic adult carriers.

Author

Weary TE, Pappas T, Tusiime P, Tuhaise S, Otali E, Emery Thompson M, Ross E, Gern JE, and Goldberg TL

Subjects

Animals, Humans, Child, Female, Male, Child, Preschool, Adult, Uganda epidemiology, Prospective Studies, Zoonoses epidemiology, Zoonoses virology, COVID-19 epidemiology, COVID-19 virology, COVID-19 transmission, Ape Diseases epidemiology, Ape Diseases virology, Respiratory Tract Infections epidemiology, Respiratory Tract Infections virology, Respiratory Tract Infections veterinary, Rhinovirus isolation & purification, Rhinovirus genetics, SARS-CoV-2 isolation & purification, Incidence, Pan troglodytes, Common Cold epidemiology, Common Cold virology

Abstract

Reverse zoonotic respiratory diseases threaten great apes across Sub-Saharan Africa. Studies of wild chimpanzees have identified the causative agents of most respiratory disease outbreaks as "common cold" paediatric human pathogens, but reverse zoonotic transmission pathways have remained unclear. Between May 2019 and August 2021, we conducted a prospective cohort study of 234 children aged 3-11 years in communities bordering Kibale National Park, Uganda, and 30 adults who were forest workers and regularly entered the park. We collected 2047 respiratory symptoms surveys to quantify clinical severity and simultaneously collected 1989 nasopharyngeal swabs approximately monthly for multiplex viral diagnostics. Throughout the course of the study, we also collected 445 faecal samples from 55 wild chimpanzees living nearby in Kibale in social groups that have experienced repeated, and sometimes lethal, epidemics of human-origin respiratory viral disease. We characterized respiratory pathogens in each cohort and examined statistical associations between PCR positivity for detected pathogens and potential risk factors. Children exhibited high incidence rates of respiratory infections, whereas incidence rates in adults were far lower. COVID-19 lockdown in 2020-2021 significantly decreased respiratory disease incidence in both people and chimpanzees. Human respiratory infections peaked in June and September, corresponding to when children returned to school. Rhinovirus, which caused a 2013 outbreak that killed 10% of chimpanzees in a Kibale community, was the most prevalent human pathogen throughout the study and the only pathogen present at each monthly sampling, even during COVID-19 lockdown. Rhinovirus was also most likely to be carried asymptomatically by adults. Although we did not detect human respiratory pathogens in the chimpanzees during the cohort study, we detected human metapneumovirus in two chimpanzees from a February 2023 outbreak that were genetically similar to viruses detected in study participants in 2019. Our data suggest that respiratory pathogens circulate in children and that adults become asymptomatically infected during high-transmission times of year. These asymptomatic adults may then unknowingly carry the pathogens into forest and infect chimpanzees. This conclusion, in turn, implies that intervention strategies based on respiratory symptoms in adults are unlikely to be effective for reducing reverse zoonotic transmission of respiratory viruses to chimpanzees., (© 2024. The Author(s).)

Published

2024

4. Simultaneous outbreaks of respiratory disease in wild chimpanzees caused by distinct viruses of human origin.

Author

Negrey JD, Reddy RB, Scully EJ, Phillips-Garcia S, Owens LA, Langergraber KE, Mitani JC, Emery Thompson M, Wrangham RW, Muller MN, Otali E, Machanda Z, Hyeroba D, Grindle KA, Pappas TE, Palmenberg AC, Gern JE, and Goldberg TL

Subjects

Animals, Ape Diseases epidemiology, Feces virology, Female, Humans, Male, Metapneumovirus genetics, Pan troglodytes virology, Parainfluenza Virus 3, Human genetics, Paramyxoviridae Infections diagnosis, Phylogeny, Respiratory Tract Infections virology, Uganda epidemiology, Zoonoses virology, Ape Diseases virology, Disease Outbreaks veterinary, Metapneumovirus isolation & purification, Parainfluenza Virus 3, Human isolation & purification, Paramyxoviridae Infections transmission, Respiratory Tract Infections veterinary

Abstract

Respiratory viruses of human origin infect wild apes across Africa, sometimes lethally. Here we report simultaneous outbreaks of two distinct human respiratory viruses, human metapneumovirus (MPV; Pneumoviridae: Metapneumovirus) and human respirovirus 3 (HRV3; Paramyxoviridae; Respirovirus, formerly known as parainfluenza virus 3), in two chimpanzee (Pan troglodytes schweinfurthii) communities in the same forest in Uganda in December 2016 and January 2017. The viruses were absent before the outbreaks, but each was present in ill chimpanzees from one community during the outbreak period. Clinical signs and gross pathologic changes in affected chimpanzees closely mirrored symptoms and pathology commonly observed in humans for each virus. Epidemiologic modelling showed that MPV and HRV3 were similarly transmissible (R 0 of 1.27 and 1.48, respectively), but MPV caused 12.2% mortality mainly in infants and older chimpanzees, whereas HRV3 caused no direct mortality. These results are consistent with the higher virulence of MPV than HRV3 in humans, although both MPV and HRV3 cause a significant global disease burden. Both viruses clustered phylogenetically within groups of known human variants, with MPV closely related to a lethal 2009 variant from mountain gorillas (Gorilla beringei beringei), suggesting two independent and simultaneous reverse zoonotic origins, either directly from humans or via intermediary hosts. These findings expand our knowledge of human origin viruses threatening wild chimpanzees and suggest that such viruses might be differentiated by their comparative epidemiological dynamics and pathogenicity in wild apes. Our results also caution against assuming common causation in coincident outbreaks.

Published

2019