Neuroligin 2 governs synaptic morphology and function through RACK1-cofilin signaling in Drosophila

Neuroligins are transmembrane cell adhesion proteins well-known for their genetic links to autism spectrum disorders. Neuroligins can function by regulating the actin cytoskeleton, however the factors and mechanisms involved are still largely unknown. Here, using the Drosophila neuromuscular junction as a model, we reveal that F-Actin assembly at the Drosophila NMJ is controlled through Cofilin signaling mediated by an interaction between DNlg2 and RACK1, factors not previously known to work together. The deletion of DNlg2 displays disrupted RACK1-Cofilin signaling pathway with diminished actin cytoskeleton proteo-stasis at the terminal of the NMJ, aberrant NMJ structure, reduced synaptic transmission, and abnormal locomotion at the third-instar larval stage. Overexpression of wildtype and activated Cofilin in muscles are sufficient to rescue the morphological and physiological defects in dnlg2 mutants, while inactivated Cofilin is not. Since the DNlg2 paralog DNlg1 is known to regulate F-actin assembly mainly via a specific interaction with WAVE complex, our present work suggests that the orchestration of F-actin by Neuroligins is a diverse and complex process critical for neural connectivity. Drosophila Neuroligin2 promotes F-actin assembly through the RACK1-Cofilin signaling pathway to regulate synaptic morphology and function at neuromuscular junctions.

Automated summary

Neuroligins are cell adhesion proteins with genetic links to autism spectrum disorders. They regulate F-Actin assembly through the RACK1-Cofilin signaling pathway to control synaptic morphology and function at neuromuscular junctions.