Abstract

Immunocytochemical and pharmacological studies have provided evidence that calcium activated thiol proteases (calpains) plays am important role in neuropathology. Partial digestion of an endogenous substrate for these enzymes occurs in several pathogenic circumstances, in some cases days before the onset of overt signs of cellular degeneration, and a drug that inhibits calpain blocks the development of a=pathology in two paradigms in which it has been tested. In light of these results, it is now reasonable to begin exploring the possibility that calpain, acting in concert with other factors, also contributes to age-related changes in the brain. Four projects of this type constitute the present proposal. Experiment 1 will test if the concentration of a breakdown product that results from the digestion of spectrin by calpain increases in the aged mouse brain. Pilot data point to this conclusion; if confirmed, this would provide indirect evidence for greater calpain activity, with aging. Experiment 2 will use pharmacological stimulation of NMDA receptors and hypoxia to determine if the aged brain is more vulnerable to pathogenic conditions and if this is associated with an enhanced activation of calpain. Preliminary work suggests that episodes of hypoxia too short to cause aged slices. The proposed studies will extend this project and test if the aged slices are also more vulnerable to NMDA receptor stimulation. Assays of spectrin breakdown and physiological tests of the protective effects of calpain inhibitors will be used to assess the likelihood that excessive stimulation of the protease contributes to pathological responses in the aged brain. These studies will include recently introduced calpain inhibitors that appear to be more potent and selective. Experiment 3 will examine the possibility that the increased degradation of calpain substrates found in pathogenesis and possibly aging is due in part to a facilitation of the interactions between substrates and protease. Membranes will be isolated from the brain of gerbils after transient ischemia and from different regions of the aged rat brain and proteolysis assessed following an incubation with exogenous calpain. Experiment 4 will determine if various components of the amyloid precursor protein are substrates for calpain and if pathogenic manipulations trigger the partial digestion of the protein. These experiments should provide evidence needed to evaluate the possibility that excessive activation of calpain contributes to amyloid formation in aging.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG000538-17
Application #
3767825
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
17
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
University of California Irvine
Department
Type
DUNS #
161202122
City
Irvine
State
CA
Country
United States
Zip Code
92697

  Publications

Sosna, Justyna; Philipp, Stephan; Albay 3rd, Ricardo et al. (2018) Early long-term administration of the CSF1R inhibitor PLX3397 ablates microglia and reduces accumulation of intraneuronal amyloid, neuritic plaque deposition and pre-fibrillar oligomers in 5XFAD mouse model of Alzheimer's disease. Mol Neurodegener 13:11
Tong, Liqi; Prieto, G Aleph; Cotman, Carl W (2018) IL-1? suppresses cLTP-induced surface expression of GluA1 and actin polymerization via ceramide-mediated Src activation. J Neuroinflammation 15:127
Hainsworth, A H; Lee, S; Foot, P et al. (2018) Super-resolution imaging of subcortical white matter using stochastic optical reconstruction microscopy (STORM) and super-resolution optical fluctuation imaging (SOFI). Neuropathol Appl Neurobiol 44:417-426
Krotee, Pascal; Griner, Sarah L; Sawaya, Michael R et al. (2018) Common fibrillar spines of amyloid-? and human islet amyloid polypeptide revealed by microelectron diffraction and structure-based inhibitors. J Biol Chem 293:2888-2902
Prieto, G Aleph; Tong, Liqi; Smith, Erica D et al. (2018) TNF? and IL-1? but not IL-18 Suppresses Hippocampal Long-Term Potentiation Directly at the Synapse. Neurochem Res :
Hernandez, Michael X; Namiranian, Pouya; Nguyen, Eric et al. (2017) C5a Increases the Injury to Primary Neurons Elicited by Fibrillar Amyloid Beta. ASN Neuro 9:1759091416687871
Hatami, Asa; Monjazeb, Sanaz; Milton, Saskia et al. (2017) Familial Alzheimer's Disease Mutations within the Amyloid Precursor Protein Alter the Aggregation and Conformation of the Amyloid-? Peptide. J Biol Chem 292:3172-3185
Love, Julia E; Day, Ryan J; Gause, Justin W et al. (2017) Nuclear uptake of an amino-terminal fragment of apolipoprotein E4 promotes cell death and localizes within microglia of the Alzheimer's disease brain. Int J Physiol Pathophysiol Pharmacol 9:40-57
Marsh, Samuel E; Yeung, Stephen T; Torres, Maria et al. (2017) HuCNS-SC Human NSCs Fail to Differentiate, Form Ectopic Clusters, and Provide No Cognitive Benefits in a Transgenic Model of Alzheimer's Disease. Stem Cell Reports 8:235-248
Krotee, Pascal; Rodriguez, Jose A; Sawaya, Michael R et al. (2017) Atomic structures of fibrillar segments of hIAPP suggest tightly mated ?-sheets are important for cytotoxicity. Elife 6:

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