Replacing the PDZ-interacting C-termini of DSCAM and DSCAML1 with epitope tags causes different phenotypic severity in different cell populations

Author:

Garrett Andrew M1,Tadenev Abigail LD1,Hammond Yuna T1,Fuerst Peter G23,Burgess Robert W1ORCID

Affiliation:

1. The Jackson Laboratory, Bar Harbor, United States

2. Department of Biological Sciences, University of Idaho, Moscow, United States

3. WWAMI Medical Education Program, University of Idaho, Moscow, United States

Abstract

Different types of neurons in the retina are organized vertically into layers and horizontally in a mosaic pattern that helps ensure proper neural network formation and information processing throughout the visual field. The vertebrate Dscams (DSCAM and DSCAML1) are cell adhesion molecules that support the development of this organization by promoting self-avoidance at the level of cell types, promoting normal developmental cell death, and directing vertical neurite stratification. To understand the molecular interactions required for these activities, we tested the functional significance of the interaction between the C-terminus of the Dscams and multi-PDZ domain-containing scaffolding proteins in mouse. We hypothesized that this PDZ-interacting domain would mediate a subset of the Dscams’ functions. Instead, we found that in the absence of these interactions, some cell types developed almost normally, while others resembled complete loss of function. Thus, we show differential dependence on this domain for Dscams’ functions in different cell types.

Funder

National Eye Institute

National Institute of Neurological Disorders and Stroke

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

Reference44 articles.

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3. Developmentally dynamic colocalization patterns of DSCAM with adhesion and synaptic proteins in the mouse retina;de Andrade;Molecular Vision,2014

4. Crystal structures of a complexed and peptide-free membrane protein-binding domain: molecular basis of peptide recognition by PDZ;Doyle;Cell,1996

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