Literature DB >> 30467080

Neuron-Subtype-Specific Expression, Interaction Affinities, and Specificity Determinants of DIP/Dpr Cell Recognition Proteins.

Filip Cosmanescu1, Phinikoula S Katsamba2, Alina P Sergeeva3, Goran Ahlsen2, Saurabh D Patel4, Joshua J Brewer1, Liming Tan5, Shuwa Xu5, Qi Xiao5, Sonal Nagarkar-Jaiswal6, Aljoscha Nern7, Hugo J Bellen6, S Lawrence Zipursky8, Barry Honig9, Lawrence Shapiro10.   

Abstract

Binding between DIP and Dpr neuronal recognition proteins has been proposed to regulate synaptic connections between lamina and medulla neurons in the Drosophila visual system. Each lamina neuron was previously shown to express many Dprs. Here, we demonstrate, by contrast, that their synaptic partners typically express one or two DIPs, with binding specificities matched to the lamina neuron-expressed Dprs. A deeper understanding of the molecular logic of DIP/Dpr interaction requires quantitative studies on the properties of these proteins. We thus generated a quantitative affinity-based DIP/Dpr interactome for all DIP/Dpr protein family members. This revealed a broad range of affinities and identified homophilic binding for some DIPs and some Dprs. These data, along with full-length ectodomain DIP/Dpr and DIP/DIP crystal structures, led to the identification of molecular determinants of DIP/Dpr specificity. This structural knowledge, along with a comprehensive set of quantitative binding affinities, provides new tools for functional studies in vivo.
Copyright © 2018 Elsevier Inc. All rights reserved.

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Year:  2018        PMID: 30467080      PMCID: PMC6309224          DOI: 10.1016/j.neuron.2018.10.046

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


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