Balancing act of small GTPases downstream of plexin-A4 signaling motifs promotes dendrite elaboration in mammalian cortical neurons

Oday Abushalbaq, Jiyeon Baek, Avraham Yaron, Tracy S. Tran*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

Abstract

The precise development of neuronal morphologies is crucial to the establishment of synaptic circuits and, ultimately, proper brain function. Signaling by the axon guidance cue semaphorin 3A (Sema3A) and its receptor complex of neuropilin-1 and plexin-A4 has multifunctional outcomes in neuronal morphogenesis. Downstream activation of the RhoGEF FARP2 through interaction with the lysine-arginine-lysine motif of plexin-A4 and consequent activation of the small GTPase Rac1 promotes dendrite arborization, but this pathway is dispensable for axon repulsion. Here, we investigated the interplay of small GTPase signaling mechanisms underlying Sema3Amediated dendritic elaboration in mouse layer V cortical neurons in vitro and in vivo. Sema3A promoted the binding of the small GTPase Rnd1 to the amino acid motif lysine-valine-serine (LVS) in the cytoplasmic domain of plexin-A4. Rnd1 inhibited the activity of the small GTPase RhoA and the kinase ROCK, thus supporting the activity of the GTPase Rac1, which permitted the growth and branching of dendrites. Overexpression of a dominant-negative RhoA, a constitutively active Rac1, or the pharmacological inhibition of ROCK activity rescued defects in dendritic elaboration in neurons expressing a plexin-A4 mutant lacking the LVS motif. Our findings provide insights into the previously unappreciated balancing act between Rho and Rac signaling downstream of specific motifs in plexin-A4 to mediate Sema3A-dependent dendritic elaboration in mammalian cortical neuron development.

Original languageEnglish
Article numbereadh7673
Number of pages14
JournalScience Signaling
Volume17
Issue number819
DOIs
Publication statusPublished - Jan 2024

Bibliographical note

We thank J. P. Zanin and W. Friedman (Rutgers University) for providing the plasmids. We thank J. P. Zanin, V. Danelon, and E. Martinez (Rutgers University) for expert technical assistance.This work is supported by the NJ Governor’s Council for Medical Research and Treatment of Autism (CAUT17BSP022) to T.S.T. and NSF/IOS (1556968 and 2034864) to T.S.T. and A.Y., who is also supported as an incumbent of the Jack & Simon Djanogly Professorial Chair in Biochemistry.

All Science Journal Classification (ASJC) codes

  • Biochemistry
  • Molecular Biology
  • Cell Biology

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