MAP1B-dependent Rac activation is required for AMPA receptor endocytosis during long-term depression
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Benoist, Marion
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MAP1B-dependent Rac activation is required for AMPA receptor endocytosis during long-term depression
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Abstract
The microtubule-associated protein 1B (MAP1B) plays
critical roles in neurite growth and synapse maturation
during brain development. This protein is well expressed
in the adult brain. However, its function in mature neurons
remains unknown. We have used a genetically
modified mouse model and shRNA techniques to assess
the role of MAP1B at established synapses, bypassing
MAP1B functions during neuronal development. Under
these conditions, we found that MAP1B deficiency alters
synaptic plasticity by specifically impairing long-term
depression (LTD) expression. Interestingly, this is due to
a failure to trigger AMPA receptor endocytosis and spine
shrinkage during LTD. These defects are accompanied by
an impaired targeting of the Rac1 activator Tiam1 at
synaptic compartments. Accordingly, LTD and AMPA
receptor endocytosis are restored in MAP1B-deficient neurons
by providing additional Rac1. Therefore, these results
indicate that the MAP1B-Tiam1-Rac1 relay is essential for
spine structural plasticity and removal of AMPA receptors
from synapses during LTD. This work highlights the importance
of MAPs as signalling hubs controlling the actin
cytoskeleton and receptor trafficking during plasticity in
mature neurons.
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The EMBO Journal (2013) 32, 2287–2299
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