Synaptic activity becomes excitotoxic in neurons exposed to elevated levels of platelet-activating factor
Matthew J. Bellizzi, Shao-Ming Lu, Eliezer Masliah, Harris A. Gelbard
Matthew J. Bellizzi, Shao-Ming Lu, Eliezer Masliah, Harris A. Gelbard
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Research Article Neuroscience

Synaptic activity becomes excitotoxic in neurons exposed to elevated levels of platelet-activating factor

Abstract

Neurologic impairment in HIV-1–associated dementia (HAD) and other neuroinflammatory diseases correlates with injury to dendrites and synapses, but how such injury occurs is not known. We hypothesized that neuroinflammation makes dendrites susceptible to excitotoxic injury following synaptic activity. We report that platelet-activating factor, an inflammatory phospholipid that mediates synaptic plasticity and neurotoxicity and is dramatically elevated in the brain during HAD, promotes dendrite injury following elevated synaptic activity and can replicate HIV-1–associated dendritic pathology. In hippocampal slices exposed to a stable platelet-activating factor analogue, tetanic stimulation that normally induces long-term synaptic potentiation instead promoted development of calcium- and caspase-dependent dendritic beading. Chemical preconditioning with diazoxide, a mitochondrial ATP-sensitive potassium channel agonist, prevented dendritic beading and restored long-term potentiation. In contrast to models invoking excessive glutamate release, these results suggest that physiologic synaptic activity may trigger excitotoxic dendritic injury during chronic neuroinflammation. Furthermore, preconditioning may represent a novel therapeutic strategy for preventing excitotoxic injury while preserving physiologic plasticity.

Authors

Matthew J. Bellizzi, Shao-Ming Lu, Eliezer Masliah, Harris A. Gelbard

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Dendritic injury and neuronal PAF-R expression in HAD. In cortical tissu...
Dendritic injury and neuronal PAF-R expression in HAD. In cortical tissue from patients with HAD (A), dendritic beading and spine loss in Golgi-stained neurons is associated with (B) strong PAF-R immunohistochemical staining on dendrites and neuronal cell bodies identified by coimmunostaining for MAP2. HAD tissue shows fewer MAP2-positive dendritic branches compared with tissue from HIV-1 seropositive controls while PAF-R expression on the remaining dendrites and cell bodies is increased. (C) Higher-power field shows intense PAF-R expression on beaded dendrites in HAD compared with control dendrites. Scale bars: 20 μm.