KCNQ channels regulate age-related memory impairment

In humans KCNQ2/3 heteromeric channels form an M-current that acts as a brake on neuronal excitability, with mutations causing a form of epilepsy. The M-current has been shown to be a key regulator of neuronal plasticity underlying associative memory and ethanol response in mammals. Previous work ha...

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Bibliographic Details
Published in:PloS one 2013-04, Vol.8 (4), p.e62445
Main Authors: Cavaliere, Sonia, Malik, Bilal R, Hodge, James J L
Format: Article
Language:English
Subjects:
Addictions
Age
Age factors
Aging
Alcohols
Animals
Associative memory
Biology
Brake presses
Channels
Defects
Drosophila
Drosophila - drug effects
Drosophila - genetics
Drosophila - physiology
Drug addiction
Epilepsy
Ethanol
Ethanol - adverse effects
Excitability
Gene expression
Gene Expression Regulation
Humidity
Impairment
Insects
KCNQ Potassium Channels - genetics
KCNQ Potassium Channels - metabolism
KCNQ2 protein
Kinases
Long term memory
Machinery and equipment
Memory
Memory - drug effects
Memory, Short-Term
Mimicry
Mushroom Bodies - cytology
Mushroom Bodies - metabolism
Mutants
Mutation
Nervous system
Neural plasticity
Neurons
Neurons - cytology
Neurons - metabolism
Neuroplasticity
Pharmacology
Physiology
Plasticity
Potassium channels (voltage-gated)
Rodents
Short term memory
Signal Transduction
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Summary:In humans KCNQ2/3 heteromeric channels form an M-current that acts as a brake on neuronal excitability, with mutations causing a form of epilepsy. The M-current has been shown to be a key regulator of neuronal plasticity underlying associative memory and ethanol response in mammals. Previous work has shown that many of the molecules and plasticity mechanisms underlying changes in alcohol behaviour and addiction are shared with those of memory. We show that the single KCNQ channel in Drosophila (dKCNQ) when mutated show decrements in associative short- and long-term memory, with KCNQ function in the mushroom body α/βneurons being required for short-term memory. Ethanol disrupts memory in wildtype flies, but not in a KCNQ null mutant background suggesting KCNQ maybe a direct target of ethanol, the blockade of which interferes with the plasticity machinery required for memory formation. We show that as in humans, Drosophila display age-related memory impairment with the KCNQ mutant memory defect mimicking the effect of age on memory. Expression of KCNQ normally decreases in aging brains and KCNQ overexpression in the mushroom body neurons of KCNQ mutants restores age-related memory impairment. Therefore KCNQ is a central plasticity molecule that regulates age dependent memory impairment.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0062445