Effects of short-term Western diet on cerebral oxidative stress and diabetes related factors in APPPS1 knock-in mice

AbstractA chronic high fat Western diet (WD) promotes a variety of morbidity factors although experimental evidence for short-term WD mediating brain dysfunction remains to be elucidated. The amyloid precursor protein and presenilin-1 (APPPS1) knock-in mouse model has been demonstrated to recapitula...

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Published inJournal of neurochemistry Vol. 108; no. 4; pp. 860 - 866
Main Authors Studzinski, Christa M, Li, Feng, Bruce-Keller, Annadora J, Fernandez-Kim, Sun Ok, Zhang, Le, Weidner, Adam M, Markesbery, William R, Murphy, MPaul, Keller, Jeffrey N
Format Journal Article
LanguageEnglish
Published 01.02.2009
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Abstract AbstractA chronic high fat Western diet (WD) promotes a variety of morbidity factors although experimental evidence for short-term WD mediating brain dysfunction remains to be elucidated. The amyloid precursor protein and presenilin-1 (APPPS1) knock-in mouse model has been demonstrated to recapitulate some key features of Alzheimer's disease pathology, including amyloid- beta (A beta ) pathogenesis. In this study, we placed 1-month-old APPPS1 mice and non-transgenic littermates on a WD for 4weeks. The WD resulted in a significant elevation in protein oxidation and lipid peroxidation in the brain of APPPS1 mice relative to non-transgenic littermates, which occurred in the absence of increased A beta levels. Altered adipokine levels were also observed in APPPS1 mice placed on a short-term WD, relative to non-transgenic littermates. Taken together, these data indicate that short-term WD is sufficient to selectively promote cerebral oxidative stress and metabolic disturbances in APPPS1 knock-in mice, with increased oxidative stress preceding alterations in A beta . These data have important implications for understanding how WD may potentially contribute to brain dysfunction and the development of neurodegenerative disorders such as Alzheimer's disease.
AbstractList AbstractA chronic high fat Western diet (WD) promotes a variety of morbidity factors although experimental evidence for short-term WD mediating brain dysfunction remains to be elucidated. The amyloid precursor protein and presenilin-1 (APPPS1) knock-in mouse model has been demonstrated to recapitulate some key features of Alzheimer's disease pathology, including amyloid- beta (A beta ) pathogenesis. In this study, we placed 1-month-old APPPS1 mice and non-transgenic littermates on a WD for 4weeks. The WD resulted in a significant elevation in protein oxidation and lipid peroxidation in the brain of APPPS1 mice relative to non-transgenic littermates, which occurred in the absence of increased A beta levels. Altered adipokine levels were also observed in APPPS1 mice placed on a short-term WD, relative to non-transgenic littermates. Taken together, these data indicate that short-term WD is sufficient to selectively promote cerebral oxidative stress and metabolic disturbances in APPPS1 knock-in mice, with increased oxidative stress preceding alterations in A beta . These data have important implications for understanding how WD may potentially contribute to brain dysfunction and the development of neurodegenerative disorders such as Alzheimer's disease.
Author Bruce-Keller, Annadora J
Weidner, Adam M
Zhang, Le
Murphy, MPaul
Keller, Jeffrey N
Li, Feng
Studzinski, Christa M
Fernandez-Kim, Sun Ok
Markesbery, William R
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