Slower Dynamics and Aged Mitochondria in Sporadic Alzheimer’s Disease

Slower Dynamics and Aged Mitochondria in Sporadic Alzheimer’s Disease

Sporadic Alzheimer’s disease corresponds to 95% of cases whose origin is multifactorial and elusive. Mitochondrial dysfunction is a major feature of Alzheimer’s pathology, which might be one of the early events that trigger downstream principal events. Here, we show that multiple genes that control...

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Main Authors: Patricia Martín-Maestro, Ricardo Gargini, Esther García, George Perry, Jesús Avila, Vega García-Escudero
Format: Article
Language:English
Published: Hindawi Limited 2017-01-01
Series:Oxidative Medicine and Cellular Longevity
Online Access:http://dx.doi.org/10.1155/2017/9302761
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spelling doaj-503addd5e0bd4c41a0e6e5bdaba40f082020-11-24T22:58:21ZengHindawi LimitedOxidative Medicine and Cellular Longevity1942-09001942-09942017-01-01201710.1155/2017/93027619302761Slower Dynamics and Aged Mitochondria in Sporadic Alzheimer’s DiseasePatricia Martín-Maestro0Ricardo Gargini1Esther García2George Perry3Jesús Avila4Vega García-Escudero5Centro de Biología Molecular “Severo Ochoa” (UAM-CSIC), Nicolás Cabrera, 1. Cantoblanco 28049 Madrid, SpainCentro de Biología Molecular “Severo Ochoa” (UAM-CSIC), Nicolás Cabrera, 1. Cantoblanco 28049 Madrid, SpainCentro de Biología Molecular “Severo Ochoa” (UAM-CSIC), Nicolás Cabrera, 1. Cantoblanco 28049 Madrid, SpainUniversity of Texas at San Antonio, One UTSA Circle, San Antonio, TX 78249-0667, USACentro de Biología Molecular “Severo Ochoa” (UAM-CSIC), Nicolás Cabrera, 1. Cantoblanco 28049 Madrid, SpainCentro de Biología Molecular “Severo Ochoa” (UAM-CSIC), Nicolás Cabrera, 1. Cantoblanco 28049 Madrid, SpainSporadic Alzheimer’s disease corresponds to 95% of cases whose origin is multifactorial and elusive. Mitochondrial dysfunction is a major feature of Alzheimer’s pathology, which might be one of the early events that trigger downstream principal events. Here, we show that multiple genes that control mitochondrial homeostasis, including fission and fusion, are downregulated in Alzheimer’s patients. Additionally, we demonstrate that some of these dysregulations, such as diminished DLP1 levels and its mitochondrial localization, as well as reduced STOML2 and MFN2 fusion protein levels, take place in fibroblasts from sporadic Alzheimer’s disease patients. The analysis of mitochondrial network disruption using CCCP indicates that the patients’ fibroblasts exhibit slower dynamics and mitochondrial membrane potential recovery. These defects lead to strong accumulation of aged mitochondria in Alzheimer’s fibroblasts. Accordingly, the analysis of autophagy and mitophagy involved genes in the patients demonstrates a downregulation indicating that the recycling mechanism of these aged mitochondria might be impaired. Our data reinforce the idea that mitochondrial dysfunction is one of the key early events of the disease intimately related with aging.http://dx.doi.org/10.1155/2017/9302761
collection DOAJ
language English
format Article
sources DOAJ
author Patricia Martín-Maestro
Ricardo Gargini
Esther García
George Perry
Jesús Avila
Vega García-Escudero
spellingShingle Patricia Martín-Maestro
Ricardo Gargini
Esther García
George Perry
Jesús Avila
Vega García-Escudero
Slower Dynamics and Aged Mitochondria in Sporadic Alzheimer’s Disease
Oxidative Medicine and Cellular Longevity
author_facet Patricia Martín-Maestro
Ricardo Gargini
Esther García
George Perry
Jesús Avila
Vega García-Escudero
author_sort Patricia Martín-Maestro
title Slower Dynamics and Aged Mitochondria in Sporadic Alzheimer’s Disease
title_short Slower Dynamics and Aged Mitochondria in Sporadic Alzheimer’s Disease
title_full Slower Dynamics and Aged Mitochondria in Sporadic Alzheimer’s Disease
title_fullStr Slower Dynamics and Aged Mitochondria in Sporadic Alzheimer’s Disease
title_full_unstemmed Slower Dynamics and Aged Mitochondria in Sporadic Alzheimer’s Disease
title_sort slower dynamics and aged mitochondria in sporadic alzheimer’s disease
publisher Hindawi Limited
series Oxidative Medicine and Cellular Longevity
issn 1942-0900
1942-0994
publishDate 2017-01-01
description Sporadic Alzheimer’s disease corresponds to 95% of cases whose origin is multifactorial and elusive. Mitochondrial dysfunction is a major feature of Alzheimer’s pathology, which might be one of the early events that trigger downstream principal events. Here, we show that multiple genes that control mitochondrial homeostasis, including fission and fusion, are downregulated in Alzheimer’s patients. Additionally, we demonstrate that some of these dysregulations, such as diminished DLP1 levels and its mitochondrial localization, as well as reduced STOML2 and MFN2 fusion protein levels, take place in fibroblasts from sporadic Alzheimer’s disease patients. The analysis of mitochondrial network disruption using CCCP indicates that the patients’ fibroblasts exhibit slower dynamics and mitochondrial membrane potential recovery. These defects lead to strong accumulation of aged mitochondria in Alzheimer’s fibroblasts. Accordingly, the analysis of autophagy and mitophagy involved genes in the patients demonstrates a downregulation indicating that the recycling mechanism of these aged mitochondria might be impaired. Our data reinforce the idea that mitochondrial dysfunction is one of the key early events of the disease intimately related with aging.
url http://dx.doi.org/10.1155/2017/9302761
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