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Coincidence detection in a neural correlate of classical conditioning is initiated by bidirectional 3‐phosphoinositide‐dependent kinase‐1 signalling and modulated by adenosine receptors
Author(s) -
Keifer Joyce,
Zheng Zhaoqing
Publication year - 2015
Publication title -
the journal of physiology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.802
H-Index - 240
eISSN - 1469-7793
pISSN - 0022-3751
DOI - 10.1113/jphysiol.2014.282947
Subject(s) - neuroscience , tropomyosin receptor kinase b , associative learning , receptor , neurotrophin , microbiology and biotechnology , biology , chemistry , neurotrophic factors , biochemistry
Key points Signalling mechanisms for coincidence detection of paired stimuli during classical conditioning are fundamental for understanding the mechanisms of associative learning. Bidirectional 3‐phosphoinositide‐dependent kinase‐1 (PDK1) activity is signalled by TrkB neurotrophin receptors for paired stimuli and p75 NTR for unpaired stimuli. Adenosine 2A receptors modulate PDK1 responses directly as G proteins and by transactivation of TrkB. Convergence of protein kinase A and PDK1 activity initiates signalling of paired stimuli during classical conditioning.Abstract How the neural substrates for detection of paired stimuli are distinct from unpaired stimuli is poorly understood and a fundamental question for understanding the signalling mechanisms for coincidence detection during associative learning. To address this question, we used a neural correlate of eyeblink classical conditioning in an isolated brainstem from the turtle, in which the cranial nerves are directly stimulated in place of using a tone or airpuff. A bidirectional response is activated in <5 min of training, in which phosphorylated 3‐phosphoinositide‐dependent kinase‐1 (p‐PDK1) is increased in response to paired and decreased in response to unpaired nerve stimulation and is mediated by the opposing actions of neurotrophin receptors TrkB and p75 NTR . Surprisingly, blockade of adenosine 2A (A 2A ) receptors inhibits both of these responses. Pairing also induces substantially increased surface expression of TrkB that is inhibited by Src family tyrosine kinase and A 2A receptor antagonists. Finally, the acquisition of conditioning is blocked by a PDK1 inhibitor. The unique action of A 2A receptors to function directly as G proteins and in receptor transactivation to control distinct TrkB and p75 NTR signalling pathways allows for convergent activation of PDK1 and protein kinase A during paired stimulation to initiate classical conditioning.