Abstract

Our overall aim is to determine the molecular mechanisms of _-amyloid (A_)-induced synaptic loss and neuronal death. Deposition of insoluble A_, together with tangle formation, loss of synapses and neurons, are hallmarks of Alzheimer's disease. More recently soluble A_ oligomeric species have been found in AD and these may correlate with synaptic loss. While the debate continues about the role of each of these in the disease it is important to develop model systems where these processes can be studied. Studies show that increased A_ induces synaptotoxicity, a parameter which correlates with cognitive decline in AD. Evidence from our work and from other laboratories shows that aggregated and oligomeric A_ induce apoptosis in cultured neurons and that sublethal concentrations of A_ induce changes in synapse morphology in primary neurons and brain slices. Our work shows that A_ induces activation of caspase-2 and - 3 but that only caspase-2 executes death. Caspase-2, and its downstream target Bim, and caspase-3 are increased in AD brains. We are proposing that, in neurons exposed to A_, the main function of caspase-3 is the regulation of synaptic plasticity, not the execution of cell death;caspase-2 executes death. We propose the hypothesis that there is dose-dependent activation of different caspases by A_ leading to synaptic remodeling, synaptic loss and neuronal death. Sublethal doses of A_ activate caspase- 3;caspase-3 in this setting does not execute death but is responsible for remodeling synapses as a protective mechanism in response to A_;the activity of caspase-3 is modulated by IAPs. With increasing time of exposure or increasing levels of A_, synapse pruning becomes excessive, leading to synaptotoxicity which in turn induces trophic factor deprivation leading to further synaptic loss and eventually to activation of caspase-2 and neuronal death. Lethal doses of A_ activate caspase-2 and caspase-3;caspase-2 induces Bim and executes the neuron, caspase-3 activity is inhibited from executing death by cIAP1. Different complexes serve to regulate caspase-2 activity in neurons. Caspase-2 activation requires RAIDD;PIDD complexes with RAIDD in healthy neurons to prevent caspase-2 activation. We will examine these hypotheses using primary hippocampal neuron cultures and mouse models of neurodegeneration with the following specific aims: To determine if caspase-3 and IAPs mediate spine changes induced by A_. 2: To determine how caspase-2 is regulated and activated by A_ and TFD. 3: To determine how caspase-2 induces of Bim expression.

Public Health Relevance

Alzheimer's Diseaes is an increasingly prevalent untreatable neurodegenerative disease. Without appropriate therapeutic interventions patients with AD will require increasing amounts of healthcare dollars to address their medical needs, as this is a chronic progressive disease. Our work aims to determine the molecular mechanisms underlying the neuronal dysfunction and death that are the hallmarks of this disease;such studies will identify targets for therapeutic intervention.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS043089-05A2
Application #
7533204
Study Section
Special Emphasis Panel (ZRG1-MDCN-L (02))
Program Officer
Sieber, Beth-Anne
Project Start
2000-12-01
Project End
2011-07-31
Budget Start
2009-08-01
Budget End
2010-07-31
Support Year
5
Fiscal Year
2009
Total Cost
$438,844
Indirect Cost

  Institution

Name
Columbia University (N.Y.)
Department
Pathology
Type
Schools of Medicine
DUNS #
621889815
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Vigneswara, Vasanthy; Akpan, Nsikan; Berry, Martin et al. (2014) Combined suppression of CASP2 and CASP6 protects retinal ganglion cells from apoptosis and promotes axon regeneration through CNTF-mediated JAK/STAT signalling. Brain 137:1656-75
Jean, Ying Y; Ribe, Elena M; Pero, Maria Elena et al. (2013) Caspase-2 is essential for c-Jun transcriptional activation and Bim induction in neuron death. Biochem J 455:15-25
Pozueta, Julio; Lefort, Roger; Ribe, Elena M et al. (2013) Caspase-2 is required for dendritic spine and behavioural alterations in J20 APP transgenic mice. Nat Commun 4:1939
Tamayev, Robert; Akpan, Nsikan; Arancio, Ottavio et al. (2012) Caspase-9 mediates synaptic plasticity and memory deficits of Danish dementia knock-in mice: caspase-9 inhibition provides therapeutic protection. Mol Neurodegener 7:60
Ribe, Elena M; Jean, Ying Y; Goldstein, Rebecca L et al. (2012) Neuronal caspase 2 activity and function requires RAIDD, but not PIDD. Biochem J 444:591-9
Puzzo, Daniela; Privitera, Lucia; Fa', Mauro et al. (2011) Endogenous amyloid-? is necessary for hippocampal synaptic plasticity and memory. Ann Neurol 69:819-30
Akpan, Nsikan; Serrano-Saiz, Esther; Zacharia, Brad E et al. (2011) Intranasal delivery of caspase-9 inhibitor reduces caspase-6-dependent axon/neuron loss and improves neurological function after stroke. J Neurosci 31:8894-904
Tizon, Belen; Ribe, Elena M; Mi, Weiqian et al. (2009) Cystatin C Protects Neuronal Cells from Amyloid-beta-induced Toxicity. J Alzheimers Dis :
Siddiq, Ambreena; Aminova, Leila R; Troy, Carol M et al. (2009) Selective inhibition of hypoxia-inducible factor (HIF) prolyl-hydroxylase 1 mediates neuroprotection against normoxic oxidative death via HIF- and CREB-independent pathways. J Neurosci 29:8828-38