4.7 Article

Characterization of histamine H3 receptors in Alzheimer's Disease brain and amyloid over-expressing TASTPM mice

Journal

BRITISH JOURNAL OF PHARMACOLOGY
Volume 157, Issue 1, Pages 130-138

Publisher

WILEY-BLACKWELL
DOI: 10.1111/j.1476-5381.2008.00075.x

Keywords

H-3 receptor; Alzheimer's Disease; [H-3]GSK189254; TASTPM mouse; neocortex

Funding

  1. Department Clinical Research, Singapore General Hospital [DCR/P06/2006]

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Histamine H-3 receptor antagonists are currently being evaluated for their potential use in a number of central nervous system disorders including Alzheimer's Disease (AD). To date, little is known about the state of H-3 receptors in AD. In the present study we used the radiolabelled H-3 receptor antagonist [H-3]GSK189254 to investigate H-3 receptor binding in the amyloid over-expressing double mutant APPswe x PSI.MI46V (TASTPM) transgenic mouse model of AD and in post-mortem human AD brain samples. No significant differences in specific H-3 receptor binding were observed between wild type and TASTPM mice in the cortex, hippocampus or hypothalamus. Specific [H-3]GSK189254 binding was detected in sections of human medial frontal cortex from AD brains of varying disease severity (Braak stages I-VI). With more quantitative analysis in a larger cohort, we observed that H-3 receptor densities were not significantly different between AD and age-matched control brains in both frontal and temporal cortical regions. However, within the AD group, [H-3]GSK189254 binding density in frontal cortex was higher in individuals with more severe dementia prior to death. The maintenance of H-3 receptor integrity observed in the various stages of AD in this study is important, given the potential use of H-3 antagonists as a novel therapeutic approach for the symptomatic treatment of AD.

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