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NEURODEVELOPMENT Branch-restricted localization of phosphatase Prl-1 specifies axonal synaptogenesis domains

Journal Contribution - Journal Article

Central nervous system (CNS) circuit development requires subcellular control of synapse formation and patterning of synapse abundance. We identified the Drosophila membrane-anchored phosphatase of regenerating liver (Prl-1) as an axon-intrinsic factor that promotes synapse formation in a spatially restricted fashion. The loss of Prl-1 in mechanosensory neurons reduced the number of CNS presynapses localized on a single axon collateral and organized as a terminal arbor. Flies lacking all Prl-1 protein had locomotor defects. The overexpression of Prl-1 induced ectopic synapses. In mechanosensory neurons, Prl-1 modulates the insulin receptor (InR) signaling pathway within a single contralateral axon compartment, thereby affecting the number of synapses. The axon branch-specific localization and function of Prl-1 depend on untranslated regions of the prl-1 messenger RNA (mRNA). Therefore, compartmentalized restriction of Prl-1 serves as a specificity factor for the subcellular control of axonal synaptogenesis.

Journal: Science

ISSN: 0036-8075

Issue: 6439

Volume: 364

Pages: 454 - +

Publication year:2019

PubMed Id: 31048465
WoS Id: 000466809600026
Institutional Repository URL: https://lirias.kuleuven.be/2798683
DOI: https://doi.org/10.1126/science.aau9952

BOF-keylabel:yes

IOF-keylabel:yes

BOF-publication weight:10

CSS-citation score:1

Authors:International

Authors from:Higher Education

See also: Branch-restricted localization of phosphatase Prl-1 specifies axonal synaptogenesis domains.

Publication

NEURODEVELOPMENT Branch-restricted localization of phosphatase Prl-1 specifies axonal synaptogenesis domains

Journal Contribution - Journal Article

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