TY - JOUR
T1 - Viruses associated with ill health in wild chimpanzees
AU - Negrey, Jacob D.
AU - Mitani, John C.
AU - Wrangham, Richard W.
AU - Otali, Emily
AU - Reddy, Rachna B.
AU - Pappas, Tressa E.
AU - Grindle, Kristine A.
AU - Gern, James E.
AU - Machanda, Zarin P.
AU - Muller, Martin N.
AU - Langergraber, Kevin E.
AU - Emery Thompson, Melissa
AU - Goldberg, Tony L.
N1 - Funding Information:
We are grateful to the Uganda Wildlife Authority, Uganda National Council for Science and Technology, and Makerere University Biological Field Station for granting research approval. We thank the field assistants of the Kibale and Ngogo Chimpanzee Projects for help with sample collection. For additional advice and technical assistance, we thank Samuel Angedakin, Christopher Dunn, and Taylor Weary. This study was supported by the National Institutes of Health Award R01AG049395 through the National Institute for Aging and the Office of Research on Women's Health. Further support was provided by the National Science Foundation (Awards BCS-1355014, BCS-1613392, BCS-1613393, DGE-1256260, and NCS-FO 1926653), National Geographic Society (Awards 9742-15 and 9824-15), Leakey Foundation, Wenner-Gren Foundation, Nacey-Maggioncalda Foundation, Boston University, University of Michigan, University of New Mexico, and University of Wisconsin-Madison.
Funding Information:
We are grateful to the Uganda Wildlife Authority, Uganda National Council for Science and Technology, and Makerere University Biological Field Station for granting research approval. We thank the field assistants of the Kibale and Ngogo Chimpanzee Projects for help with sample collection. For additional advice and technical assistance, we thank Samuel Angedakin, Christopher Dunn, and Taylor Weary. This study was supported by the National Institutes of Health Award R01AG049395 through the National Institute for Aging and the Office of Research on Women's Health. Further support was provided by the National Science Foundation (Awards BCS‐1355014, BCS‐1613392, BCS‐1613393, DGE‐1256260, and NCS‐FO 1926653), National Geographic Society (Awards 9742‐15 and 9824‐15), Leakey Foundation, Wenner‐Gren Foundation, Nacey‐Maggioncalda Foundation, Boston University, University of Michigan, University of New Mexico, and University of Wisconsin‐Madison.
Publisher Copyright:
© 2022 Wiley Periodicals LLC
PY - 2022/2
Y1 - 2022/2
N2 - 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.
AB - 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.
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U2 - 10.1002/ajp.23358
DO - 10.1002/ajp.23358
M3 - Article
C2 - 35015311
AN - SCOPUS:85122888445
SN - 0275-2565
VL - 84
JO - American Journal of Primatology
JF - American Journal of Primatology
IS - 2
M1 - e23358
ER -