FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2890198591> ?p ?o ?g. }

• W2890198591 abstract "Alzheimer’s disease (AD) is a highly prevalent neurodegenerative disorder characterized by pathological hallmarks of beta-amyloid plaque deposits, tau pathology, inflammation, and cognitive decline. Treatment remains a clinical obstacle due to lack of effective therapeutics. Agonists targeting nuclear receptors, such as bexarotene, reversed cognitive deficits regardless of treatment duration and age in murine models of AD. While bexarotene demonstrated marked efficacy in decreasing plaque levels following short-term treatment, prolonged treatment did not modulate plaque burden. This suggested that plaques might reform in mice treated chronically with bexarotene and that cessation of bexarotene treatment before plaques reform might alter amyloid pathology, inflammation, and cognition in AD mice. We utilized one-year-old APP/PS1 mice that were divided into two groups. We treated one group of mice for 2 weeks with bexarotene. The other group of mice was treated for 2 weeks with bexarotene followed by withdrawal of drug treatment for an additional 2 weeks. Cognition was evaluated using the novel-object recognition test either at the end of bexarotene treatment or the end of the withdrawal period. We then analyzed amyloid pathology and microgliosis at the conclusion of the study in both groups. Bexarotene treatment enhanced cognition in APP/PS1 mice similar to previous findings. Strikingly, we observed sustained cognitive improvements in mice in which bexarotene treatment was discontinued for 2 weeks. We observed a sustained reduction in microgliosis and plaque burden following drug withdrawal exclusively in the hippocampus. Our findings demonstrate that bexarotene selectively modifies aspects of neuroinflammation in a region-specific manner to reverse hippocampal-dependent cognitive deficits in AD mice and may provide insight to inform future studies with nuclear receptor agonists." @default.
• W2890198591 created "2018-09-27" @default.
• W2890198591 creator A5028641323 @default.
• W2890198591 creator A5073496526 @default.
• W2890198591 creator A5081488726 @default.
• W2890198591 date "2018-02-15" @default.
• W2890198591 modified "2023-09-26" @default.
• W2890198591 title "Nuclear receptor agonist-driven modification of inflammation and amyloid pathology enhances and sustains cognitive improvements in a mouse model of Alzheimer's disease" @default.
• W2890198591 hasPublicationYear "2018" @default.
• W2890198591 type Work @default.
• W2890198591 sameAs 2890198591 @default.
• W2890198591 citedByCount "0" @default.
• W2890198591 crossrefType "journal-article" @default.
• W2890198591 hasAuthorship W2890198591A5028641323 @default.
• W2890198591 hasAuthorship W2890198591A5073496526 @default.
• W2890198591 hasAuthorship W2890198591A5081488726 @default.
• W2890198591 hasConcept C104317684 @default.
• W2890198591 hasConcept C126322002 @default.
• W2890198591 hasConcept C142724271 @default.
• W2890198591 hasConcept C2776914184 @default.
• W2890198591 hasConcept C2778820923 @default.
• W2890198591 hasConcept C2779134260 @default.
• W2890198591 hasConcept C2779483572 @default.
• W2890198591 hasConcept C2984863031 @default.
• W2890198591 hasConcept C55493867 @default.
• W2890198591 hasConcept C63932345 @default.
• W2890198591 hasConcept C71924100 @default.
• W2890198591 hasConcept C86339819 @default.
• W2890198591 hasConcept C86803240 @default.
• W2890198591 hasConcept C87753298 @default.
• W2890198591 hasConcept C98274493 @default.
• W2890198591 hasConceptScore W2890198591C104317684 @default.
• W2890198591 hasConceptScore W2890198591C126322002 @default.
• W2890198591 hasConceptScore W2890198591C142724271 @default.
• W2890198591 hasConceptScore W2890198591C2776914184 @default.
• W2890198591 hasConceptScore W2890198591C2778820923 @default.
• W2890198591 hasConceptScore W2890198591C2779134260 @default.
• W2890198591 hasConceptScore W2890198591C2779483572 @default.
• W2890198591 hasConceptScore W2890198591C2984863031 @default.
• W2890198591 hasConceptScore W2890198591C55493867 @default.
• W2890198591 hasConceptScore W2890198591C63932345 @default.
• W2890198591 hasConceptScore W2890198591C71924100 @default.
• W2890198591 hasConceptScore W2890198591C86339819 @default.
• W2890198591 hasConceptScore W2890198591C86803240 @default.
• W2890198591 hasConceptScore W2890198591C87753298 @default.
• W2890198591 hasConceptScore W2890198591C98274493 @default.
• W2890198591 hasLocation W28901985911 @default.
• W2890198591 hasOpenAccess W2890198591 @default.
• W2890198591 hasPrimaryLocation W28901985911 @default.
• W2890198591 hasRelatedWork W1029387585 @default.
• W2890198591 hasRelatedWork W1187966713 @default.
• W2890198591 hasRelatedWork W1769924399 @default.
• W2890198591 hasRelatedWork W2051067814 @default.
• W2890198591 hasRelatedWork W2069454756 @default.
• W2890198591 hasRelatedWork W2079304341 @default.
• W2890198591 hasRelatedWork W2116608029 @default.
• W2890198591 hasRelatedWork W2228582852 @default.
• W2890198591 hasRelatedWork W2235843597 @default.
• W2890198591 hasRelatedWork W2612927177 @default.
• W2890198591 hasRelatedWork W2750299285 @default.
• W2890198591 hasRelatedWork W2765888687 @default.
• W2890198591 hasRelatedWork W2794459022 @default.
• W2890198591 hasRelatedWork W2796660324 @default.
• W2890198591 hasRelatedWork W2808229106 @default.
• W2890198591 hasRelatedWork W2899087182 @default.
• W2890198591 hasRelatedWork W2998892128 @default.
• W2890198591 hasRelatedWork W3003733049 @default.
• W2890198591 hasRelatedWork W3112537149 @default.
• W2890198591 hasRelatedWork W3153076694 @default.
• W2890198591 isParatext "false" @default.
• W2890198591 isRetracted "false" @default.
• W2890198591 magId "2890198591" @default.
• W2890198591 workType "article" @default.