Zn-dependent β-amyloid Aggregation and its Reversal by the Tetrapeptide HAEE

The pathogenesis of Alzheimer's disease (AD) is associated with the formation of cerebral amyloid plaques, the main components of which are the modified Aβ molecules as well as the metal ions. Aβ isomerized at Asp7 residue (isoD7-Aβ) is the most abundant isoform in amyloid plaques. We hypothesi...

Descripción completa

Detalles Bibliográficos
Autores principales: Mitkevich, Vladimir A, Barykin, Evgeny P, Eremina, Svetlana, Pani, Bibhusita, Katkova-Zhukotskaya, Olga, Polshakov, Vladimir I, Adzhubei, Alexei A, Kozin, Sergey A, Mironov, Alexander S, Makarov, Alexander A, Nudler, Evgeny
Formato: Online Artículo Texto
Lenguaje:English
Publicado: JKL International LLC 2023
Materias:
Short Comminication
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10017155/
https://www.ncbi.nlm.nih.gov/pubmed/37008059
http://dx.doi.org/10.14336/AD.2022.0827
_version_ 1784907519145017344
author Mitkevich, Vladimir A
Barykin, Evgeny P
Eremina, Svetlana
Pani, Bibhusita
Katkova-Zhukotskaya, Olga
Polshakov, Vladimir I
Adzhubei, Alexei A
Kozin, Sergey A
Mironov, Alexander S
Makarov, Alexander A
Nudler, Evgeny
author_facet Mitkevich, Vladimir A
Barykin, Evgeny P
Eremina, Svetlana
Pani, Bibhusita
Katkova-Zhukotskaya, Olga
Polshakov, Vladimir I
Adzhubei, Alexei A
Kozin, Sergey A
Mironov, Alexander S
Makarov, Alexander A
Nudler, Evgeny
author_sort Mitkevich, Vladimir A
collection PubMed
description The pathogenesis of Alzheimer's disease (AD) is associated with the formation of cerebral amyloid plaques, the main components of which are the modified Aβ molecules as well as the metal ions. Aβ isomerized at Asp7 residue (isoD7-Aβ) is the most abundant isoform in amyloid plaques. We hypothesized that the pathogenic effect of isoD7-Aβ is due to the formation of zinc-dependent oligomers, and that this interaction can be disrupted by the rationally designed tetrapeptide (HAEE). Here, we utilized surface plasmon resonance, nuclear magnetic resonance, and molecular dynamics simulation to demonstrate Zn(2+)-dependent oligomerization of isoD7-Aβ and the formation of a stable isoD7-Aβ:Zn(2+):HAEE complex incapable of forming oligomers. To demonstrate the physiological importance of zinc-dependent isoD7-Aβ oligomerization and the ability of HAEE to interfere with this process at the organismal level, we employed transgenic nematodes overexpressing human Aβ. We show that the presence of isoD7-Aβ in the medium triggers extensive amyloidosis that occurs in a Zn(2+)-dependent manner, enhances paralysis, and shortens the animals’ lifespan. Exogenous HAEE completely reverses these pathological effects of isoD7-Aβ. We conclude that the synergistic action of isoD7-Aβ and Zn(2+) promotes Aβ aggregation and that the selected small molecules capable of interrupting this process, such as HAEE, can potentially serve as anti-amyloid therapeutics.
format Online
Article
Text
id pubmed-10017155
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher JKL International LLC
record_format MEDLINE/PubMed
spelling pubmed-100171552023-04-01 Zn-dependent β-amyloid Aggregation and its Reversal by the Tetrapeptide HAEE Mitkevich, Vladimir A Barykin, Evgeny P Eremina, Svetlana Pani, Bibhusita Katkova-Zhukotskaya, Olga Polshakov, Vladimir I Adzhubei, Alexei A Kozin, Sergey A Mironov, Alexander S Makarov, Alexander A Nudler, Evgeny Aging Dis Short Comminication The pathogenesis of Alzheimer's disease (AD) is associated with the formation of cerebral amyloid plaques, the main components of which are the modified Aβ molecules as well as the metal ions. Aβ isomerized at Asp7 residue (isoD7-Aβ) is the most abundant isoform in amyloid plaques. We hypothesized that the pathogenic effect of isoD7-Aβ is due to the formation of zinc-dependent oligomers, and that this interaction can be disrupted by the rationally designed tetrapeptide (HAEE). Here, we utilized surface plasmon resonance, nuclear magnetic resonance, and molecular dynamics simulation to demonstrate Zn(2+)-dependent oligomerization of isoD7-Aβ and the formation of a stable isoD7-Aβ:Zn(2+):HAEE complex incapable of forming oligomers. To demonstrate the physiological importance of zinc-dependent isoD7-Aβ oligomerization and the ability of HAEE to interfere with this process at the organismal level, we employed transgenic nematodes overexpressing human Aβ. We show that the presence of isoD7-Aβ in the medium triggers extensive amyloidosis that occurs in a Zn(2+)-dependent manner, enhances paralysis, and shortens the animals’ lifespan. Exogenous HAEE completely reverses these pathological effects of isoD7-Aβ. We conclude that the synergistic action of isoD7-Aβ and Zn(2+) promotes Aβ aggregation and that the selected small molecules capable of interrupting this process, such as HAEE, can potentially serve as anti-amyloid therapeutics. JKL International LLC 2023-04-01 /pmc/articles/PMC10017155/ /pubmed/37008059 http://dx.doi.org/10.14336/AD.2022.0827 Text en copyright: © 2022 Mitkevich et al. https://creativecommons.org/licenses/by/2.0/this is an open access article distributed under the terms of the creative commons attribution license, which permits unrestricted use, distribution and reproduction in any medium provided that the original work is properly attributed.
spellingShingle Short Comminication
Mitkevich, Vladimir A
Barykin, Evgeny P
Eremina, Svetlana
Pani, Bibhusita
Katkova-Zhukotskaya, Olga
Polshakov, Vladimir I
Adzhubei, Alexei A
Kozin, Sergey A
Mironov, Alexander S
Makarov, Alexander A
Nudler, Evgeny
Zn-dependent β-amyloid Aggregation and its Reversal by the Tetrapeptide HAEE
title Zn-dependent β-amyloid Aggregation and its Reversal by the Tetrapeptide HAEE
title_full Zn-dependent β-amyloid Aggregation and its Reversal by the Tetrapeptide HAEE
title_fullStr Zn-dependent β-amyloid Aggregation and its Reversal by the Tetrapeptide HAEE
title_full_unstemmed Zn-dependent β-amyloid Aggregation and its Reversal by the Tetrapeptide HAEE
title_short Zn-dependent β-amyloid Aggregation and its Reversal by the Tetrapeptide HAEE
title_sort zn-dependent β-amyloid aggregation and its reversal by the tetrapeptide haee
topic Short Comminication
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10017155/
https://www.ncbi.nlm.nih.gov/pubmed/37008059
http://dx.doi.org/10.14336/AD.2022.0827
work_keys_str_mv AT mitkevichvladimira zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee
AT barykinevgenyp zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee
AT ereminasvetlana zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee
AT panibibhusita zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee
AT katkovazhukotskayaolga zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee
AT polshakovvladimiri zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee
AT adzhubeialexeia zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee
AT kozinsergeya zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee
AT mironovalexanders zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee
AT makarovalexandera zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee
AT nudlerevgeny zndependentbamyloidaggregationanditsreversalbythetetrapeptidehaee

Ejemplares similares