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Literature DB >> 30467079

Interactions between the Ig-Superfamily Proteins DIP-α and Dpr6/10 Regulate Assembly of Neural Circuits.

Shuwa Xu¹, Qi Xiao¹, Filip Cosmanescu², Alina P Sergeeva³, Juyoun Yoo¹, Ying Lin¹, Phinikoula S Katsamba³, Goran Ahlsen³, Jonathan Kaufman¹, Nikhil T Linaval¹, Pei-Tseng Lee⁴, Hugo J Bellen⁴, Lawrence Shapiro², Barry Honig⁵, Liming Tan⁶, S Lawrence Zipursky⁷.

Abstract

Drosophila Dpr (21 paralogs) and DIP proteins (11 paralogs) are cell recognition molecules of the immunoglobulin superfamily (IgSF) that form a complex protein interaction network. DIP and Dpr proteins are expressed in a synaptic layer-specific fashion in the visual system. How interactions between these proteins regulate layer-specific synaptic circuitry is not known. Here we establish that DIP-α and its interacting partners Dpr6 and Dpr10 regulate multiple processes, including arborization within layers, synapse number, layer specificity, and cell survival. We demonstrate that heterophilic binding between Dpr6/10 and DIP-α and homophilic binding between DIP-α proteins promote interactions between processes in vivo. Knockin mutants disrupting the DIP/Dpr binding interface reveal a role for these proteins during normal development, while ectopic expression studies support an instructive role for interactions between DIPs and Dprs in circuit development. These studies support an important role for the DIP/Dpr protein interaction network in regulating cell-type-specific connectivity patterns.

Entities: Chemical

Keywords: DIP/Dpr proteins; cell survival; connectome; development; layer-specific circuit; specificity; synapse

Mesh：

Substances：

Year: 2018 PMID： 30467079 PMCID： PMC7501880 DOI： 10.1016/j.neuron.2018.11.001

Source DB: PubMed Journal: Neuron ISSN： 0896-6273 Impact factor: 17.173

48 in total

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