Aurin Vos Sabrina Berkamp Supervisor: Madelon Maurice

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Electrochemical cues regulate assembly of the Frizzled/Dishevelled complex at the plasma membrane during planar epithelial polarization Aurin Vos Sabrina Berkamp Supervisor: Madelon Maurice

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Electrochemical cues regulate assembly of the Frizzled/Dishevelled complex at the plasma membrane during planar epithelial polarization. Aurin Vos Sabrina Berkamp Supervisor: Madelon Maurice. Introduction. Frizzled (Fz) G-protein coupled receptor (membrane protein) - PowerPoint PPT Presentation

Transcript of Aurin Vos Sabrina Berkamp Supervisor: Madelon Maurice

Page 1: Aurin Vos Sabrina Berkamp Supervisor: Madelon Maurice

Electrochemical cues regulate assembly of the

Frizzled/Dishevelled complex at the plasma membrane during planar epithelial polarization

Aurin VosSabrina Berkamp

Supervisor: Madelon Maurice

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Introduction

• Frizzled (Fz)– G-protein coupled receptor (membrane

protein)– Key role in development and cell polarity

• Dishevelled (Dsh) contains 3 domains:– DIX multimerization– PDZ weak binding to frizzled– DEP membrane targeting

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Research goal

To identify and characterize new components involved in forming the Dsh-

Fz complex at the plasma membrane.

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The Screening

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Introducing Nhe2

• Identification of Nhe2– Homology with (human) NHE3– NHE3 = plasma membrane exchanger (Na/H)– NHEs are involved in:

• Formation of alkaline PH and charge microenvironments

• Activation of Rho family GTPases, actin polymerization

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Introducing Nhe2

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Preliminary conclusions

• Knockdown of Nhe2 causes a defect in recruitment of Dsh

• Nhe2 has a homologue in human: Nhe3– A Na/H exchanger causes local higher pH

• Changing cellular pH changes localization

Proton translocation by Nhe2 is required for correct localization Dsh

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Nhe2 – Fz interaction

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Preliminary conclusions

• Nhe2 is essential protein• Overexpression/knockdown of Nhe2

causes PCP phenotypes in Drosophila eyes

• Overexpression of Fz causes PCP phenotype– This phenotype is rescued by Nhe2

knockdown

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Dsh lipid binding

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Dsh lipid binding II

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Preliminary conclusions

• (positively charged) DEP domain of Dsh binds negatively charged lipids

• R,K-to-E mutations abolish this affinity

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Localization of Dsh mutants

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Preliminary conclusions

• R,K-to-E mutation mislocalizes Dsh• Positively charged lipid (sphingosine)

mislocalizes Dsh, but rescues DshKR/E

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Macroscopic effect of mutant

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Preliminary conclusions

• Membrane association of positively charged stretch on DEP domain in Dsh is essential in vivo

• Mutation does not affect canonical pathway, only non-canonical pathway

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Overview

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Questions?

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