| Literature DB >> 26711562 |
Anderson Sá-Nunes1, Bruna Bizzarro2, Flávia Egydio3, Michele S Barros2, Renata Sesti-Costa4, Elyara M Soares5, Adriana Pina2, Momtchilo Russo2, Lúcia H Faccioli5, Sergio Tufik3, Monica L Andersen3.
Abstract
We aimed to evaluate the effect of paradoxical sleep deprivation on the cellular migration during inflammation, the peritoneal macrophage phenotype and the infectious stimulus outcomes. A/J mice were inoculated with thioglycollate and exposed to paradoxical sleep deprivation. Sleep-deprived animals presented decreased cell migration compared to controls. Nitric oxide production was reduced in macrophages from sleep-deprived mice compared to controls. Cell surface analysis showed that sleep deprivation reduced F4/80(+)/CD80(low) peritoneal cell population induced by thioglycollate injection. Sleep-deprived mice were not more susceptible to infection than control mice. Our findings challenge the general perception that sleep loss always increases infection susceptibility.Entities:
Keywords: Histoplasma capsulatum; Immune response; Inflammation; Macrophages; Sleep; Trypanosoma cruzi
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Year: 2015 PMID: 26711562 DOI: 10.1016/j.jneuroim.2015.11.013
Source DB: PubMed Journal: J Neuroimmunol ISSN: 0165-5728 Impact factor: 3.478