Selective function of the PDZ domain of Dishevelled in noncanonical Wnt signalling

Author:

Mieszczanek Juliusz1,Strutt Helen23,Rutherford Trevor J.1,Strutt David23,Bienz Mariann1,Gammons Melissa V.1ORCID

Affiliation:

1. MRC Laboratory of Molecular Biology 1 , Cambridge Biomedical Campus, Francis Crick Avenue, Cambridge, CB2 0QH , UK

2. University of Sheffield, School of Biosciences, 2 Firth Court Western Bank, Sheffield, S10 2TN , UK

3. , 2 Firth Court Western Bank, Sheffield, S10 2TN , UK

Abstract

ABSTRACT Dishevelled is a cytoplasmic hub that transduces Wnt signals to cytoplasmic effectors, which can be broadly characterised as canonical (β-catenin dependent) and noncanonical, to specify cell fates and behaviours during development. To transduce canonical Wnt signals, Dishevelled binds to the intracellular face of Frizzled through its DEP domain and polymerises through its DIX domain to assemble dynamic signalosomes. Dishevelled also contains a PDZ domain, whose function remains controversial. Here, we use genome editing to delete the PDZ domain-encoding region from Drosophila dishevelled. Canonical Wingless signalling is entirely normal in these deletion mutants; however, they show defects in multiple contexts controlled by noncanonical Wnt signalling, such as planar polarity. We use nuclear magnetic resonance spectroscopy to identify bona fide PDZ-binding motifs at the C termini of different polarity proteins. Although deletions of these motifs proved aphenotypic in adults, we detected changes in the proximodistal distribution of the polarity protein Flamingo (also known as Starry night) in pupal wings that suggest a modulatory role of these motifs in polarity signalling. We also provide new genetic evidence that planar polarity relies on the DEP-dependent recruitment of Dishevelled to the plasma membrane by Frizzled.

Funder

Cancer Research UK

Medical Research Council

Wellcome Trust

Publisher

The Company of Biologists

Subject

Cell Biology

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