Literature DB >> 22884549

CREB-binding protein levels in the rat hippocampus fail to predict chronological or cognitive aging.

Inês Tomás Pereira1, Christopher E Coletta, Evelyn V Perez, David H Kim, Michela Gallagher, Ilya G Goldberg, Peter R Rapp.   

Abstract

Normal cognitive aging is associated with deficits in memory processes dependent on the hippocampus, along with large-scale changes in the hippocampal expression of many genes. Histone acetylation can broadly influence gene expression and has been recently linked to learning and memory. We hypothesized that CREB-binding protein (CBP), a key histone acetyltransferase, may contribute to memory decline in normal aging. Here, we quantified CBP protein levels in the hippocampus of young, aged unimpaired, and aged impaired rats, classified on the basis of spatial memory capacity documented in the Morris water maze. First, CBP-immunofluorescence was quantified across the principal cell layers of the hippocampus using both low and high resolution laser scanning imaging approaches. Second, digital images of CBP immunostaining were analyzed by a multipurpose classifier algorithm with validated sensitivity across many types of input materials. Finally, CBP protein levels in the principal subfields of the hippocampus were quantified by quantitative Western blotting. CBP levels were equivalent as a function of age and cognitive status in all analyses. The sensitivity of the techniques used was substantial, sufficient to reveal differences across the principal cell fields of the hippocampus, and to correctly classify images from young and aged animals independent of CBP immunoreactivity. The results are discussed in the context of recent evidence suggesting that CBP decreases may be most relevant in conditions of aging that, unlike normal cognitive aging, involve significant neuron loss. Published by Elsevier Inc.

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Year:  2012        PMID: 22884549      PMCID: PMC3518677          DOI: 10.1016/j.neurobiolaging.2012.07.010

Source DB:  PubMed          Journal:  Neurobiol Aging        ISSN: 0197-4580            Impact factor:   4.673


  54 in total

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Authors:  Edward Korzus; Michael G Rosenfeld; Mark Mayford
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Review 8.  Melatonin regulates aging and neurodegeneration through energy metabolism, epigenetics, autophagy and circadian rhythm pathways.

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9.  The CBP KIX domain regulates long-term memory and circadian activity.

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