The influence of body mass index, age and sex on inflammatory disease risk in semi-captive Chimpanzees.

Obesity and ageing are emerging issues in the management of captive primates, including Chimpanzees, Pan troglodytes. Studies on humans show that obesity and old age can independently increase the risk of inflammatory-associated diseases indicated by elevated levels of pro-inflammatory cells and pro...

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Main Authors: Vincent Obanda, George Paul Omondi, Patrick Ilukol Chiyo
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4133249?pdf=render
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spelling doaj-de347d477e5f491188952942777a86302020-11-25T00:20:23ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-0198e10460210.1371/journal.pone.0104602The influence of body mass index, age and sex on inflammatory disease risk in semi-captive Chimpanzees.Vincent ObandaGeorge Paul OmondiPatrick Ilukol ChiyoObesity and ageing are emerging issues in the management of captive primates, including Chimpanzees, Pan troglodytes. Studies on humans show that obesity and old age can independently increase the risk of inflammatory-associated diseases indicated by elevated levels of pro-inflammatory cells and proteins in the blood of older or obese compared to levels in younger or non-obese individuals. In humans, sex can influence the outcomes of these risks. Health management of these problems in chimpanzee populations requires an understanding of similarities and differences of factors influencing inflammatory disease risks in humans and in chimpanzees. We examined the relationship between age, sex and Body Mass Index (BMI) with hematological biomarkers of inflammatory disease risk established for humans which include the neutrophil to lymphocyte ratio (NLR), and neutrophil, white blood cell (WBC), platelet microparticle and platelet counts. We found that higher values of NLR, neutrophil count and platelet microparticle count were associated with higher BMI values and older age indicating increased inflammation risk in these groups; a similar pattern to humans. There was a strong sex by age interaction on inflammation risk, with older males more at risk than older females. In contrast to human studies, total WBC count was not influenced by BMI, but like humans, WBC and platelet counts were lower in older individuals compared to younger individuals. Our findings are similar to those of humans and suggest that further insight on managing chimpanzees can be gained from extensive studies of ageing and obesity in humans. We suggest that managing BMI should be an integral part of health management in captive chimpanzee populations in order to partially reduce the risk of diseases associated with inflammation. These results also highlight parallels in inflammation risk between humans and chimpanzees and have implications for understanding the evolution of inflammation related diseases in apes.http://europepmc.org/articles/PMC4133249?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Vincent Obanda
George Paul Omondi
Patrick Ilukol Chiyo
spellingShingle Vincent Obanda
George Paul Omondi
Patrick Ilukol Chiyo
The influence of body mass index, age and sex on inflammatory disease risk in semi-captive Chimpanzees.
PLoS ONE
author_facet Vincent Obanda
George Paul Omondi
Patrick Ilukol Chiyo
author_sort Vincent Obanda
title The influence of body mass index, age and sex on inflammatory disease risk in semi-captive Chimpanzees.
title_short The influence of body mass index, age and sex on inflammatory disease risk in semi-captive Chimpanzees.
title_full The influence of body mass index, age and sex on inflammatory disease risk in semi-captive Chimpanzees.
title_fullStr The influence of body mass index, age and sex on inflammatory disease risk in semi-captive Chimpanzees.
title_full_unstemmed The influence of body mass index, age and sex on inflammatory disease risk in semi-captive Chimpanzees.
title_sort influence of body mass index, age and sex on inflammatory disease risk in semi-captive chimpanzees.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Obesity and ageing are emerging issues in the management of captive primates, including Chimpanzees, Pan troglodytes. Studies on humans show that obesity and old age can independently increase the risk of inflammatory-associated diseases indicated by elevated levels of pro-inflammatory cells and proteins in the blood of older or obese compared to levels in younger or non-obese individuals. In humans, sex can influence the outcomes of these risks. Health management of these problems in chimpanzee populations requires an understanding of similarities and differences of factors influencing inflammatory disease risks in humans and in chimpanzees. We examined the relationship between age, sex and Body Mass Index (BMI) with hematological biomarkers of inflammatory disease risk established for humans which include the neutrophil to lymphocyte ratio (NLR), and neutrophil, white blood cell (WBC), platelet microparticle and platelet counts. We found that higher values of NLR, neutrophil count and platelet microparticle count were associated with higher BMI values and older age indicating increased inflammation risk in these groups; a similar pattern to humans. There was a strong sex by age interaction on inflammation risk, with older males more at risk than older females. In contrast to human studies, total WBC count was not influenced by BMI, but like humans, WBC and platelet counts were lower in older individuals compared to younger individuals. Our findings are similar to those of humans and suggest that further insight on managing chimpanzees can be gained from extensive studies of ageing and obesity in humans. We suggest that managing BMI should be an integral part of health management in captive chimpanzee populations in order to partially reduce the risk of diseases associated with inflammation. These results also highlight parallels in inflammation risk between humans and chimpanzees and have implications for understanding the evolution of inflammation related diseases in apes.
url http://europepmc.org/articles/PMC4133249?pdf=render
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