Opposed Actions of PKA Isozymes (RI and RII) and PKC Isoforms (cPKCβI and nPKCε) in Neuromuscular Developmental Synapse Elimination

During neuromuscular junction (NMJ) development, synapses are produced in excess. By sensing the activity-dependent release of ACh, adenosine, and neurotrophins, presynaptic receptors prompt axonal competition and loss of the unnecessary axons. The receptor action is mediated by synergistic and anta...

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Bibliographic Details
Published in:Cells (Basel, Switzerland) Switzerland), 2019-10, Vol.8 (11), p.1304
Main Authors: Garcia, Neus, Balañà, Cori, Lanuza, Maria A, Tomàs, Marta, Cilleros-Mañé, Víctor, Just-Borràs, Laia, Tomàs, Josep
Format: Article
Language:English
Subjects:
Acetylcholine receptors (nicotinic)
acetylcholine release
Adenosine receptors
Antibodies
Axon guidance
Biotechnology
Competition
Experiments
Isoenzymes
Isoforms
Kinases
Laboratory animals
Microscopy
Morphology
motor end-plate
muscarinic acetylcholine receptors
Nervous system
Neuromodulation
Neuromuscular junctions
Neurons
Neurotrophic factors
pka
pkc
postnatal synapse elimination
Protein kinase A
Protein kinase C
Proteins
Receptor density
Synapse elimination
Synaptogenesis
trkb receptors
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Summary:During neuromuscular junction (NMJ) development, synapses are produced in excess. By sensing the activity-dependent release of ACh, adenosine, and neurotrophins, presynaptic receptors prompt axonal competition and loss of the unnecessary axons. The receptor action is mediated by synergistic and antagonistic relations when they couple to downstream kinases (mainly protein kinases A and C (PKA and PKC)), which phosphorylate targets involved in axonal disconnection. Here, we directly investigated the involvement of PKA subunits and PKC isoforms in synapse elimination. Selective PKA and PKC peptide modulators were applied daily to the Levator auris longus (LAL) muscle surface of P5-P8 transgenic B6.Cg-Tg (Thy1-YFP) 16 Jrs/J (and also C57BL/6J) mice, and the number of axons and the postsynaptic receptor cluster morphology were evaluated in P9 NMJ. PKA (PKA-I and PKA-II isozymes) acts at the pre- and postsynaptic sites to delay both axonal elimination and nAChR cluster differentiation, PKC activity promotes both axonal loss (a cPKCβI and nPKCε isoform action), and postsynaptic nAChR cluster maturation (a possible role for PKCθ). Moreover, PKC-induced changes in axon number indirectly influence postsynaptic maturation. PKC and PKA have opposed actions, which suggests that changes in the balance of these kinases may play a major role in the mechanism of developmental synapse elimination.
ISSN:2073-4409
2073-4409
DOI:10.3390/cells8111304