Abstract

Our previous work has demonstrated that aged monkeys show cognitive loss and accumulation of amyloid and senile plaques in the cerebral cortex similar to changes observed in normal human aging. However monkeys do not show neurofibrillary tangles and there is no major loss of cortical projection neurons in areas so far examined (primary visual and motor cortex, the subiculum of the hippocampal formation). There is cell loss in subcortical sites, including the cholinergic nucleus basalis, and, based upon other studies, there is likely to be cell loss in other subcortical nuclei that provide neurochemically specific afferent input to the cerebral cortex. In addition, we have observed degeneration in intracortical and subcortical white matter and in cortical neuropil that may reflect loss of synaptic input, while other data suggest changes in levels of neurotransmitters and their processing enzymes as well as related receptors. Finally the amyloid proteins in monkey brain are identical to those in human brain. It is not known whether they are the result of direct age-related pathogenic factors or a result of changes in free radical metabolism. The similarity of these behavioral and neurobiological changes with those observed in humans form a basis for our proposed investigation of age-related changes in rhesus monkeys. The overall hypothesis of this project is that cortical pathology underlines the cognitive decline seen in aging monkeys to man. To investigate this hypothesis we propose the following specific aims. We will behaviorally test monkeys that range in age from young adults (5 yrs) to the very elderly (25+ yrs) to assess memory and executive function, and since it is likely that these two cognitive domains are localized primarily in frontal lobe association cortex and the temporal lobe system, respectively, we will examine these areas in detain in a number of ways. We will look for changes in the neuronal population, and especially in the inhibitory neuronal types, and also for loss of synapses, and alteration in glial cells and changes in neurotransmitter levels, metabolism and receptors and the maturation states and distribution of plaques. We will also correlate the changes in neurochemically specific nuclei with cognitive changes of individual monkeys and their cortical pathology since these nuclei provide inputs to the cerebral cortex. To identify pathogenic factors we also assess free radical metabolism and its relationship to alterations in mechanisms of amyloid accumulation. These data will allow us to identify the time of onset and the sequence of structural and metabolic alterations that underlie age-related cognitive decline. We expect these data to provide the basis for a suitable primate model of normal human aging that can eventually be used for evaluation of potential therapeutic intervention.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG000001-19
Application #
3090484
Study Section
Aging Review Committee (AGE)
Project Start
1975-06-01
Project End
1996-01-31
Budget Start
1993-02-01
Budget End
1994-01-31
Support Year
19
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Boston University
Department
Type
Schools of Medicine
DUNS #
604483045
City
Boston
State
MA
Country
United States
Zip Code
02118

  Publications

Robinson, Amy A; Abraham, Carmela R; Rosene, Douglas L (2018) Candidate molecular pathways of white matter vulnerability in the brain of normal aging rhesus monkeys. Geroscience 40:31-47
Ragan, I K; Davis, A S; McVey, D S et al. (2018) Evaluation of Fluorescence Microsphere Immunoassay for Detection of Antibodies to Rift Valley Fever Virus Nucleocapsid Protein and Glycoproteins. J Clin Microbiol 56:
Moore, Tara L; Bowley, Bethany G E; Shultz, Penny L et al. (2018) Oral curcumin supplementation improves fine motor function in the middle-aged rhesus monkey. Somatosens Mot Res 35:1-10
Hsu, Alexander; Luebke, Jennifer I; Medalla, Maria (2017) Comparative ultrastructural features of excitatory synapses in the visual and frontal cortices of the adult mouse and monkey. J Comp Neurol 525:2175-2191
Shobin, Eli; Bowley, Michael P; Estrada, Larissa I et al. (2017) Microglia activation and phagocytosis: relationship with aging and cognitive impairment in the rhesus monkey. Geroscience 39:199-220
Estrada, Larissa I; Robinson, Amy A; Amaral, Ana C et al. (2017) Evaluation of Long-Term Cryostorage of Brain Tissue Sections for Quantitative Histochemistry. J Histochem Cytochem 65:153-171
Medalla, Maria; Gilman, Joshua P; Wang, Jing-Yi et al. (2017) Strength and Diversity of Inhibitory Signaling Differentiates Primate Anterior Cingulate from Lateral Prefrontal Cortex. J Neurosci 37:4717-4734
Rumbell, Timothy H; Dragulji?, Danel; Yadav, Aniruddha et al. (2016) Automated evolutionary optimization of ion channel conductances and kinetics in models of young and aged rhesus monkey pyramidal neurons. J Comput Neurosci 41:65-90
Wilson, William C; Davis, A Sally; Gaudreault, Natasha N et al. (2016) Experimental Infection of Calves by Two Genetically-Distinct Strains of Rift Valley Fever Virus. Viruses 8:
Shivanna, Vinay; McDowell, Chester; Wilson, William C et al. (2016) Complete Genome Sequence of Two Rift Valley Fever Virus Strains Isolated from Outbreaks in Saudi Arabia (2000) and Kenya (2006 to 2007). Genome Announc 4:

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