Abstract
Fetal Alcohol Spectrum Disorder (FASD) is an umbrella term that encompasses a wide range of anatomical and behavioral problems in children who are exposed to alcohol during the prenatal period. There is no effective treatment for FASD, because of lack of complete characterization of the cellular and molecular mechanisms underlying this condition. Alcohol has been previously characterized to affect integrins and growth factor signaling receptors. Integrin Linked Kinase (ILK) is an effector of integrin and growth-factor signaling which regulates various signaling processes. In FASD, a downstream effector of ILK, Glycogen Synthase Kinase 3β (GSK3β) remains highly active (reduced Ser9 phosphorylation). GSK3β has been known to modulate glutamate receptor trafficking and channel properties. Therefore, we hypothesize that the cognitive deficits accompanying FASD are associated with impairments in the ILK signaling pathway. Pregnant Sprague Dawley rats consumed a “moderate” amount of alcohol throughout gestation, or a calorie-equivalent sucrose solution. Contextual fear conditioning was used to evaluate memory performance in 32–33-day-old pups. Synaptic plasticity was assessed in the Schaffer Collateral pathway, and hippocampal protein lysates were used to evaluate ILK signaling. Alcohol exposed pups showed impaired contextual fear conditioning, as compared to control pups. This reduced memory performance was consistent with decrease in LTP as compared to controls. Hippocampal ILK activity and GSK3β Ser21/9 phosphorylation were significantly lower in alcohol-exposed pups than controls. Increased synaptic expression of GluR2 AMPA receptors was observed with immunoprecipitation of post-synaptic density protein 95 (PSD95). Furthermore, immunoprecipitation of ILK revealed a decreased interaction with GluR2. The ILK pathway appears to play a significant role in memory and synaptic plasticity impairments in FASD rats. These impairments appear to be mediated by reduced GSK3β regulation and increased synaptic stabilization of the calcium-impermeable GluR2 AMPA receptors.
Highlights
Alcohol is probably the most commonly used and socially accepted psychoactive substance
The present study constitutes the first report highlighting the involvement of Integrin Linked Kinase (ILK) in FASDrelated memory impairments and synaptic plasticity
We conclude a close association of impaired ILK pathway and synaptic plasticity deficits in prenatal alcohol exposed rat model
Summary
Alcohol is probably the most commonly used and socially accepted psychoactive substance. Alcohol consumption is not recommended during any stage of pregnancy; alcohol use during pregnancy can lead to a range of cognitive and physical consequences in the developing fetus [1]. FASD are the leading cause of mental retardation in the United States. The lifetime cost of each individual with FASD is estimated at $2 million [3]. Despite this great cost and the fact that the neuroanatomical and neurochemical effects of chronic alcoholism have been well elucidated, to date there are no therapeutic interventions available to treat FASD-induced cognitive deficits. Of great concern are “moderate” drinkers (women consuming a maximum of 7 drinks per week) since there is some debate as to whether moderate alcohol consumption is safe during pregnancy [5].
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