Effects of Eph/ephrin signalling and human Alzheimer’s Disease-associated EphA1 on Drosophila behaviour and neurophysiology

Edgar Buhl; Yoon A Kim; Tom A Parsons; Bangfu Zhu; Ismael Santa-Maria; Roger Lefort; James J L Hodge

doi:10.1016/j.nbd.2022.105752

Effects of Eph/ephrin signalling and human Alzheimer’s Disease-associated EphA1 on Drosophila behaviour and neurophysiology

Edgar Buhl^*, Yoon A Kim, Tom A Parsons, Bangfu Zhu, Ismael Santa-Maria, Roger Lefort, James J L Hodge

^*Corresponding author for this work

Research output: Contribution to journal › Article (Academic Journal) › peer-review

14 Citations (Scopus)

102 Downloads (Pure)

Abstract

Alzheimer's disease (AD) is the most prevalent neurodegenerative disease placing a great burden on people living with it, carers and society. Yet, the underlying patho-mechanisms remain unknown and treatments limited. To better understand the molecular changes associated with AD, genome-wide association studies (GWAS) have identified hundreds of candidate genes linked to the disease, like the receptor tyrosine kinase EphA1. However, demonstration of whether and how these genes cause pathology is largely lacking. Here, utilising fly genetics, we generated the first Drosophila model of human wild-type and P460L mutant EphA1 and tested the effects of Eph/ephrin signalling on AD-relevant behaviour and neurophysiology. We show that EphA1 mis-expression did not cause neurodegeneration, shorten lifespan or affect memory but flies mis-expressing the wild-type or mutant receptor were hyper-aroused, had reduced sleep, a stronger circadian rhythm and increased clock neuron activity and excitability. Over-expression of endogenous fly Eph and RNAi-mediated knock-down of Eph and its ligand ephrin affected sleep architecture and neurophysiology. Eph over-expression led to stronger circadian morning anticipation while ephrin knock-down impaired memory. A dominant negative form of the GTPase Rho1, a potential intracellular effector of Eph, led to hyper-aroused flies, memory impairment, less anticipatory behaviour and neurophysiological changes. Our results demonstrate a role of Eph/ephrin signalling in a range of behaviours affected in AD. This presents a starting point for studies into the underlying mechanisms of AD including interactions with other AD-associated genes, like Rho1, Ankyrin, Tau and APP with the potential to identify new targets for treatment.

Original language	English
Article number	105752
Number of pages	13
Journal	Neurobiology of Disease
Volume	170
Early online date	13 May 2022
DOIs	https://doi.org/10.1016/j.nbd.2022.105752
Publication status	Published - 1 Aug 2022

Bibliographical note

Funding Information:
We thank Drs Brian McCabe, Ralf Stanewsky and Scott Waddell for sharing flies and reagents, and 5 anonymous reviewers for helpful comments and suggestions. This work was supported by a Leverhulme Trust grant ( RPG-2016-318 ) and an Alzheimer ' s Research UK grant ( ARUK-IRG2019B-003 ) awarded to J.J.L.H., and NIH grants ( R01NS095922 and P50AG0008702 ) awarded to I . S-M. and NIH grant ( R21AG061722 ) to R.L.

Publisher Copyright:
© 2022 The Authors

Keywords

Alzheimer's disease
Ca2+ imaging
Drosophila melanogaster
Electrophysiology
Eph/ephrin signalling
Locomotor activity
Longevity
Memory
Sleep

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

Access to Document

10.1016/j.nbd.2022.105752

Full-text PDF (final published version)
This is the final published version of the article (version of record). It first appeared online via Wiley at https://doi.org/10.1016/j.nbd.2022.105752 . Please refer to any applicable terms of use of the publisher
Final published version, 3.46 MBLicence: CC BY

Handle.net

Persistent link

Cite this

@article{aa359d856ff74b228e19a6142ff83e87,

title = "Effects of Eph/ephrin signalling and human Alzheimer{\textquoteright}s Disease-associated EphA1 on Drosophila behaviour and neurophysiology",

abstract = "Alzheimer's disease (AD) is the most prevalent neurodegenerative disease placing a great burden on people living with it, carers and society. Yet, the underlying patho-mechanisms remain unknown and treatments limited. To better understand the molecular changes associated with AD, genome-wide association studies (GWAS) have identified hundreds of candidate genes linked to the disease, like the receptor tyrosine kinase EphA1. However, demonstration of whether and how these genes cause pathology is largely lacking. Here, utilising fly genetics, we generated the first Drosophila model of human wild-type and P460L mutant EphA1 and tested the effects of Eph/ephrin signalling on AD-relevant behaviour and neurophysiology. We show that EphA1 mis-expression did not cause neurodegeneration, shorten lifespan or affect memory but flies mis-expressing the wild-type or mutant receptor were hyper-aroused, had reduced sleep, a stronger circadian rhythm and increased clock neuron activity and excitability. Over-expression of endogenous fly Eph and RNAi-mediated knock-down of Eph and its ligand ephrin affected sleep architecture and neurophysiology. Eph over-expression led to stronger circadian morning anticipation while ephrin knock-down impaired memory. A dominant negative form of the GTPase Rho1, a potential intracellular effector of Eph, led to hyper-aroused flies, memory impairment, less anticipatory behaviour and neurophysiological changes. Our results demonstrate a role of Eph/ephrin signalling in a range of behaviours affected in AD. This presents a starting point for studies into the underlying mechanisms of AD including interactions with other AD-associated genes, like Rho1, Ankyrin, Tau and APP with the potential to identify new targets for treatment.",

keywords = "Alzheimer's disease, Ca2+ imaging, Drosophila melanogaster, Electrophysiology, Eph/ephrin signalling, Locomotor activity, Longevity, Memory, Sleep",

author = "Edgar Buhl and Kim, {Yoon A} and Parsons, {Tom A} and Bangfu Zhu and Ismael Santa-Maria and Roger Lefort and Hodge, {James J L}",

note = "Funding Information: We thank Drs Brian McCabe, Ralf Stanewsky and Scott Waddell for sharing flies and reagents, and 5 anonymous reviewers for helpful comments and suggestions. This work was supported by a Leverhulme Trust grant ( RPG-2016-318 ) and an Alzheimer ' s Research UK grant ( ARUK-IRG2019B-003 ) awarded to J.J.L.H., and NIH grants ( R01NS095922 and P50AG0008702 ) awarded to I . S-M. and NIH grant ( R21AG061722 ) to R.L. Publisher Copyright: {\textcopyright} 2022 The Authors",

year = "2022",

month = aug,

day = "1",

doi = "10.1016/j.nbd.2022.105752",

language = "English",

volume = "170",

journal = "Neurobiology of Disease",

issn = "0969-9961",

publisher = "Academic Press",

}

TY - JOUR

T1 - Effects of Eph/ephrin signalling and human Alzheimer’s Disease-associated EphA1 on Drosophila behaviour and neurophysiology

AU - Buhl, Edgar

AU - Kim, Yoon A

AU - Parsons, Tom A

AU - Zhu, Bangfu

AU - Santa-Maria, Ismael

AU - Lefort, Roger

AU - Hodge, James J L

N1 - Funding Information: We thank Drs Brian McCabe, Ralf Stanewsky and Scott Waddell for sharing flies and reagents, and 5 anonymous reviewers for helpful comments and suggestions. This work was supported by a Leverhulme Trust grant ( RPG-2016-318 ) and an Alzheimer ' s Research UK grant ( ARUK-IRG2019B-003 ) awarded to J.J.L.H., and NIH grants ( R01NS095922 and P50AG0008702 ) awarded to I . S-M. and NIH grant ( R21AG061722 ) to R.L. Publisher Copyright: © 2022 The Authors

PY - 2022/8/1

Y1 - 2022/8/1

N2 - Alzheimer's disease (AD) is the most prevalent neurodegenerative disease placing a great burden on people living with it, carers and society. Yet, the underlying patho-mechanisms remain unknown and treatments limited. To better understand the molecular changes associated with AD, genome-wide association studies (GWAS) have identified hundreds of candidate genes linked to the disease, like the receptor tyrosine kinase EphA1. However, demonstration of whether and how these genes cause pathology is largely lacking. Here, utilising fly genetics, we generated the first Drosophila model of human wild-type and P460L mutant EphA1 and tested the effects of Eph/ephrin signalling on AD-relevant behaviour and neurophysiology. We show that EphA1 mis-expression did not cause neurodegeneration, shorten lifespan or affect memory but flies mis-expressing the wild-type or mutant receptor were hyper-aroused, had reduced sleep, a stronger circadian rhythm and increased clock neuron activity and excitability. Over-expression of endogenous fly Eph and RNAi-mediated knock-down of Eph and its ligand ephrin affected sleep architecture and neurophysiology. Eph over-expression led to stronger circadian morning anticipation while ephrin knock-down impaired memory. A dominant negative form of the GTPase Rho1, a potential intracellular effector of Eph, led to hyper-aroused flies, memory impairment, less anticipatory behaviour and neurophysiological changes. Our results demonstrate a role of Eph/ephrin signalling in a range of behaviours affected in AD. This presents a starting point for studies into the underlying mechanisms of AD including interactions with other AD-associated genes, like Rho1, Ankyrin, Tau and APP with the potential to identify new targets for treatment.

AB - Alzheimer's disease (AD) is the most prevalent neurodegenerative disease placing a great burden on people living with it, carers and society. Yet, the underlying patho-mechanisms remain unknown and treatments limited. To better understand the molecular changes associated with AD, genome-wide association studies (GWAS) have identified hundreds of candidate genes linked to the disease, like the receptor tyrosine kinase EphA1. However, demonstration of whether and how these genes cause pathology is largely lacking. Here, utilising fly genetics, we generated the first Drosophila model of human wild-type and P460L mutant EphA1 and tested the effects of Eph/ephrin signalling on AD-relevant behaviour and neurophysiology. We show that EphA1 mis-expression did not cause neurodegeneration, shorten lifespan or affect memory but flies mis-expressing the wild-type or mutant receptor were hyper-aroused, had reduced sleep, a stronger circadian rhythm and increased clock neuron activity and excitability. Over-expression of endogenous fly Eph and RNAi-mediated knock-down of Eph and its ligand ephrin affected sleep architecture and neurophysiology. Eph over-expression led to stronger circadian morning anticipation while ephrin knock-down impaired memory. A dominant negative form of the GTPase Rho1, a potential intracellular effector of Eph, led to hyper-aroused flies, memory impairment, less anticipatory behaviour and neurophysiological changes. Our results demonstrate a role of Eph/ephrin signalling in a range of behaviours affected in AD. This presents a starting point for studies into the underlying mechanisms of AD including interactions with other AD-associated genes, like Rho1, Ankyrin, Tau and APP with the potential to identify new targets for treatment.

KW - Alzheimer's disease

KW - Ca2+ imaging

KW - Drosophila melanogaster

KW - Electrophysiology

KW - Eph/ephrin signalling

KW - Locomotor activity

KW - Longevity

KW - Memory

KW - Sleep

U2 - 10.1016/j.nbd.2022.105752

DO - 10.1016/j.nbd.2022.105752

M3 - Article (Academic Journal)

C2 - 35569721

SN - 0969-9961

VL - 170

JO - Neurobiology of Disease

JF - Neurobiology of Disease

M1 - 105752

ER -

Effects of Eph/ephrin signalling and human Alzheimer’s Disease-associated EphA1 on Drosophila behaviour and neurophysiology

Abstract

Bibliographical note

Keywords

UN SDGs

Access to Document

Handle.net

Fingerprint

Cite this