mutagenesis in vivo reveals extensive noncanonical functions of Dscam1 isoforms in neuronal wiring.

PNAS Nexus

MOE Laboratory of Biosystems Homeostasis & Protection and Innovation Center for Cell Signaling Network, College of Life Sciences, Zhejiang University, Hangzhou ZJ310058, People's Republic of China.

Published: May 2023

AI Article Synopsis

  • The study investigates the role of Dscam1, a gene that encodes various cell recognition molecules, in neuronal wiring and function through alternative splicing.
  • Researchers created mutations that changed the composition of Dscam1 isoforms but maintained the normal quantity, observing distinct effects on different neuron types despite normal self-avoidance in dendritic arborization.
  • Findings revealed that the altered isoform composition led to increased dendrite growth while inhibiting axon growth, suggesting that Dscam1 isoformes play a critical and specific role in regulating neuronal development.

Article Abstract

() encodes tens of thousands of cell recognition molecules via alternative splicing, which are required for neural function. A canonical self-avoidance model seems to provide a central mechanistic basis for Dscam1 functions in neuronal wiring. Here, we reveal extensive noncanonical functions of Dscam1 isoforms in neuronal wiring. We generated a series of allelic mutations in , encoding a normal number of isoforms, but with an altered isoform composition. Despite normal dendritic self-avoidance and self-/nonself-discrimination in dendritic arborization (da) neurons, which is consistent with the canonical self-avoidance model, these mutants exhibited strikingly distinct spectra of phenotypic defects in the three types of neurons: up to ∼60% defects in mushroom bodies, a significant increase in branching and growth in da neurons, and mild axonal branching defects in mechanosensory neurons. Remarkably, the altered isoform composition resulted in increased dendrite growth yet inhibited axon growth. Moreover, reducing Dscam1 dosage exacerbated axonal defects in mushroom bodies and mechanosensory neurons but reverted dendritic branching and growth defects in da neurons. This splicing-tuned regulation strategy suggests that axon and dendrite growth in diverse neurons cell-autonomously require Dscam1 isoform composition. These findings provide important insights into the functions of Dscam1 isoforms in neuronal wiring.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10156172PMC
http://dx.doi.org/10.1093/pnasnexus/pgad135DOI Listing

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