Increased Aβ42-α7-like nicotinic acetylcholine receptor complex level in lymphocytes is associated with apolipoprotein E4-driven Alzheimer’s disease pathogenesis

Increased Aβ42-α7-like nicotinic acetylcholine receptor complex level in lymphocytes is associated with apolipoprotein E4-driven Alzheimer’s disease pathogenesis

Abstract Background The apolipoprotein E ε4 (APOE4) genotype is a prominent late-onset Alzheimer’s disease (AD) risk factor. ApoE4 disrupts memory function in rodents and may contribute to both plaque and tangle formation. Methods Coimmunoprecipitation and Western blot detection were used to determi...

Full description

Bibliographic Details
Main Authors: Hoau-Yan Wang, Caryn Trocmé-Thibierge, Andres Stucky, Sanket M. Shah, Jessica Kvasic, Amber Khan, Philippe Morain, Isabelle Guignot, Eva Bouguen, Karine Deschet, Maria Pueyo, Elisabeth Mocaer, Pierre-Jean Ousset, Bruno Vellas, Vera Kiyasova
Format: Article
Language:English
Published: BMC 2017-07-01
Series:Alzheimer’s Research & Therapy
Subjects:
Alzheimer’s disease
Mild cognitive impairment
β-Amyloid
Apolipoprotein E
α7 Nicotinic acetylcholine receptor
tau phosphorylation
Online Access:http://link.springer.com/article/10.1186/s13195-017-0280-8
id doaj-e97cddc4fc2a41a0ad02d2ad6caa4d2a
record_format Article
spelling doaj-e97cddc4fc2a41a0ad02d2ad6caa4d2a2020-11-24T23:19:45ZengBMCAlzheimer’s Research & Therapy1758-91932017-07-019111710.1186/s13195-017-0280-8Increased Aβ42-α7-like nicotinic acetylcholine receptor complex level in lymphocytes is associated with apolipoprotein E4-driven Alzheimer’s disease pathogenesisHoau-Yan Wang0Caryn Trocmé-Thibierge1Andres Stucky2Sanket M. Shah3Jessica Kvasic4Amber Khan5Philippe Morain6Isabelle Guignot7Eva Bouguen8Karine Deschet9Maria Pueyo10Elisabeth Mocaer11Pierre-Jean Ousset12Bruno Vellas13Vera Kiyasova14Department of Physiology, Pharmacology and Neuroscience, CUNY School of MedicineInstitut de Recherches Internationales ServierDepartment of Physiology, Pharmacology and Neuroscience, CUNY School of MedicineDepartment of Physiology, Pharmacology and Neuroscience, CUNY School of MedicineDepartment of Physiology, Pharmacology and Neuroscience, CUNY School of MedicineDepartment of Physiology, Pharmacology and Neuroscience, CUNY School of MedicineInstitut de Recherches Internationales ServierInstitut de Recherches Internationales ServierInstitut de Recherches Internationales ServierInstitut de Recherches Internationales ServierInstitut de Recherches Internationales ServierInstitut de Recherches Internationales ServierAlzheimer’s Disease Research and Clinical Center, Inserm U1027, Toulouse University HospitalAlzheimer’s Disease Research and Clinical Center, Inserm U1027, Toulouse University HospitalInstitut de Recherches Internationales ServierAbstract Background The apolipoprotein E ε4 (APOE4) genotype is a prominent late-onset Alzheimer’s disease (AD) risk factor. ApoE4 disrupts memory function in rodents and may contribute to both plaque and tangle formation. Methods Coimmunoprecipitation and Western blot detection were used to determine: 1) the effects of select fragments from the apoE low-density lipoprotein (LDL) binding domain and recombinant apoE subtypes on amyloid beta (Aβ)42-α7 nicotinic acetylcholine receptor (α7nAChR) interaction and tau phosphorylation in rodent brain synaptosomes; and 2) the level of Aβ42-α7nAChR complexes in matched controls and patients with mild cognitive impairment (MCI) and dementia due to AD with known APOE genotypes. Results In an ex vivo study using rodent synaptosomes, apoE141–148 of the apoE promotes Aβ42-α7nAChR association and Aβ42-induced α7nAChR-dependent tau phosphorylation. In a single-blind study, we examined lymphocytes isolated from control subjects, patients with MCI and dementia due to AD with known APOE genotypes, sampled at two time points (1 year apart). APOE ε4 genotype was closely correlated with heightened Aβ42-α7nAChR complex levels and with blunted exogenous Aβ42 effects in lymphocytes derived from AD and MCI due to AD cases. Similarly, plasma from APOE ε4 carriers enhanced the Aβ42-induced Aβ42-α7nAChR association in rat cortical synaptosomes. The progression of cognitive decline in APOE ε4 carriers correlated with higher levels of Aβ42-α7nAChR complexes in lymphocytes and greater enhancement by their plasma of Aβ42-induced Aβ42-α7nAChR association in rat cortical synaptosomes. Conclusions Our data suggest that increased lymphocyte Aβ42-α7nAChR-like complexes may indicate the presence of AD pathology especially in APOE ε4 carriers. We show that apoE, especially apoE4, promotes Aβ42-α7nAChR interaction and Aβ42-induced α7nAChR-dependent tau phosphorylation via its apoE141–148 domain. These apoE-mediated effects may contribute to the APOE ε4-driven neurodysfunction and AD pathologies.http://link.springer.com/article/10.1186/s13195-017-0280-8Alzheimer’s diseaseMild cognitive impairmentβ-AmyloidApolipoprotein Eα7 Nicotinic acetylcholine receptortau phosphorylation
collection DOAJ
language English
format Article
sources DOAJ
author Hoau-Yan Wang
Caryn Trocmé-Thibierge
Andres Stucky
Sanket M. Shah
Jessica Kvasic
Amber Khan
Philippe Morain
Isabelle Guignot
Eva Bouguen
Karine Deschet
Maria Pueyo
Elisabeth Mocaer
Pierre-Jean Ousset
Bruno Vellas
Vera Kiyasova
spellingShingle Hoau-Yan Wang
Caryn Trocmé-Thibierge
Andres Stucky
Sanket M. Shah
Jessica Kvasic
Amber Khan
Philippe Morain
Isabelle Guignot
Eva Bouguen
Karine Deschet
Maria Pueyo
Elisabeth Mocaer
Pierre-Jean Ousset
Bruno Vellas
Vera Kiyasova
Increased Aβ42-α7-like nicotinic acetylcholine receptor complex level in lymphocytes is associated with apolipoprotein E4-driven Alzheimer’s disease pathogenesis
Alzheimer’s Research & Therapy
Alzheimer’s disease
Mild cognitive impairment
β-Amyloid
Apolipoprotein E
α7 Nicotinic acetylcholine receptor
tau phosphorylation
author_facet Hoau-Yan Wang
Caryn Trocmé-Thibierge
Andres Stucky
Sanket M. Shah
Jessica Kvasic
Amber Khan
Philippe Morain
Isabelle Guignot
Eva Bouguen
Karine Deschet
Maria Pueyo
Elisabeth Mocaer
Pierre-Jean Ousset
Bruno Vellas
Vera Kiyasova
author_sort Hoau-Yan Wang
title Increased Aβ42-α7-like nicotinic acetylcholine receptor complex level in lymphocytes is associated with apolipoprotein E4-driven Alzheimer’s disease pathogenesis
title_short Increased Aβ42-α7-like nicotinic acetylcholine receptor complex level in lymphocytes is associated with apolipoprotein E4-driven Alzheimer’s disease pathogenesis
title_full Increased Aβ42-α7-like nicotinic acetylcholine receptor complex level in lymphocytes is associated with apolipoprotein E4-driven Alzheimer’s disease pathogenesis
title_fullStr Increased Aβ42-α7-like nicotinic acetylcholine receptor complex level in lymphocytes is associated with apolipoprotein E4-driven Alzheimer’s disease pathogenesis
title_full_unstemmed Increased Aβ42-α7-like nicotinic acetylcholine receptor complex level in lymphocytes is associated with apolipoprotein E4-driven Alzheimer’s disease pathogenesis
title_sort increased aβ42-α7-like nicotinic acetylcholine receptor complex level in lymphocytes is associated with apolipoprotein e4-driven alzheimer’s disease pathogenesis
publisher BMC
series Alzheimer’s Research & Therapy
issn 1758-9193
publishDate 2017-07-01
description Abstract Background The apolipoprotein E ε4 (APOE4) genotype is a prominent late-onset Alzheimer’s disease (AD) risk factor. ApoE4 disrupts memory function in rodents and may contribute to both plaque and tangle formation. Methods Coimmunoprecipitation and Western blot detection were used to determine: 1) the effects of select fragments from the apoE low-density lipoprotein (LDL) binding domain and recombinant apoE subtypes on amyloid beta (Aβ)42-α7 nicotinic acetylcholine receptor (α7nAChR) interaction and tau phosphorylation in rodent brain synaptosomes; and 2) the level of Aβ42-α7nAChR complexes in matched controls and patients with mild cognitive impairment (MCI) and dementia due to AD with known APOE genotypes. Results In an ex vivo study using rodent synaptosomes, apoE141–148 of the apoE promotes Aβ42-α7nAChR association and Aβ42-induced α7nAChR-dependent tau phosphorylation. In a single-blind study, we examined lymphocytes isolated from control subjects, patients with MCI and dementia due to AD with known APOE genotypes, sampled at two time points (1 year apart). APOE ε4 genotype was closely correlated with heightened Aβ42-α7nAChR complex levels and with blunted exogenous Aβ42 effects in lymphocytes derived from AD and MCI due to AD cases. Similarly, plasma from APOE ε4 carriers enhanced the Aβ42-induced Aβ42-α7nAChR association in rat cortical synaptosomes. The progression of cognitive decline in APOE ε4 carriers correlated with higher levels of Aβ42-α7nAChR complexes in lymphocytes and greater enhancement by their plasma of Aβ42-induced Aβ42-α7nAChR association in rat cortical synaptosomes. Conclusions Our data suggest that increased lymphocyte Aβ42-α7nAChR-like complexes may indicate the presence of AD pathology especially in APOE ε4 carriers. We show that apoE, especially apoE4, promotes Aβ42-α7nAChR interaction and Aβ42-induced α7nAChR-dependent tau phosphorylation via its apoE141–148 domain. These apoE-mediated effects may contribute to the APOE ε4-driven neurodysfunction and AD pathologies.
topic Alzheimer’s disease
Mild cognitive impairment
β-Amyloid
Apolipoprotein E
α7 Nicotinic acetylcholine receptor
tau phosphorylation
url http://link.springer.com/article/10.1186/s13195-017-0280-8
work_keys_str_mv AT hoauyanwang increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT caryntrocmethibierge increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT andresstucky increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT sanketmshah increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT jessicakvasic increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT amberkhan increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT philippemorain increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT isabelleguignot increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT evabouguen increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT karinedeschet increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT mariapueyo increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT elisabethmocaer increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT pierrejeanousset increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT brunovellas increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
AT verakiyasova increasedab42a7likenicotinicacetylcholinereceptorcomplexlevelinlymphocytesisassociatedwithapolipoproteine4drivenalzheimersdiseasepathogenesis
_version_ 1725577156901208064

Similar Items