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Reappraisal of the Concept of Accelerated Aging in Neurodegeneration and Beyond

Background: Genetic and epigenetic changes, oxidative stress and inflammation influence the rate of aging, which diseases, lifestyle and environmental factors can further accelerate. In accelerated aging (AA), the biological age exceeds the chronological age. Objective: The objective of this study i...

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Autores principales: Statsenko, Yauhen, Kuznetsov, Nik V., Morozova, Daria, Liaonchyk, Katsiaryna, Simiyu, Gillian Lylian, Smetanina, Darya, Kashapov, Aidar, Meribout, Sarah, Gorkom, Klaus Neidl-Van, Hamoudi, Rifat, Ismail, Fatima, Ansari, Suraiya Anjum, Emerald, Bright Starling, Ljubisavljevic, Milos
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10605227/
https://www.ncbi.nlm.nih.gov/pubmed/37887295
http://dx.doi.org/10.3390/cells12202451
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author Statsenko, Yauhen
Kuznetsov, Nik V.
Morozova, Daria
Liaonchyk, Katsiaryna
Simiyu, Gillian Lylian
Smetanina, Darya
Kashapov, Aidar
Meribout, Sarah
Gorkom, Klaus Neidl-Van
Hamoudi, Rifat
Ismail, Fatima
Ansari, Suraiya Anjum
Emerald, Bright Starling
Ljubisavljevic, Milos
author_facet Statsenko, Yauhen
Kuznetsov, Nik V.
Morozova, Daria
Liaonchyk, Katsiaryna
Simiyu, Gillian Lylian
Smetanina, Darya
Kashapov, Aidar
Meribout, Sarah
Gorkom, Klaus Neidl-Van
Hamoudi, Rifat
Ismail, Fatima
Ansari, Suraiya Anjum
Emerald, Bright Starling
Ljubisavljevic, Milos
author_sort Statsenko, Yauhen
collection PubMed
description Background: Genetic and epigenetic changes, oxidative stress and inflammation influence the rate of aging, which diseases, lifestyle and environmental factors can further accelerate. In accelerated aging (AA), the biological age exceeds the chronological age. Objective: The objective of this study is to reappraise the AA concept critically, considering its weaknesses and limitations. Methods: We reviewed more than 300 recent articles dealing with the physiology of brain aging and neurodegeneration pathophysiology. Results: (1) Application of the AA concept to individual organs outside the brain is challenging as organs of different systems age at different rates. (2) There is a need to consider the deceleration of aging due to the potential use of the individual structure–functional reserves. The latter can be restored by pharmacological and/or cognitive therapy, environment, etc. (3) The AA concept lacks both standardised terminology and methodology. (4) Changes in specific molecular biomarkers (MBM) reflect aging-related processes; however, numerous MBM candidates should be validated to consolidate the AA theory. (5) The exact nature of many potential causal factors, biological outcomes and interactions between the former and the latter remain largely unclear. Conclusions: Although AA is commonly recognised as a perspective theory, it still suffers from a number of gaps and limitations that assume the necessity for an updated AA concept.
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spelling pubmed-106052272023-10-28 Reappraisal of the Concept of Accelerated Aging in Neurodegeneration and Beyond Statsenko, Yauhen Kuznetsov, Nik V. Morozova, Daria Liaonchyk, Katsiaryna Simiyu, Gillian Lylian Smetanina, Darya Kashapov, Aidar Meribout, Sarah Gorkom, Klaus Neidl-Van Hamoudi, Rifat Ismail, Fatima Ansari, Suraiya Anjum Emerald, Bright Starling Ljubisavljevic, Milos Cells Review Background: Genetic and epigenetic changes, oxidative stress and inflammation influence the rate of aging, which diseases, lifestyle and environmental factors can further accelerate. In accelerated aging (AA), the biological age exceeds the chronological age. Objective: The objective of this study is to reappraise the AA concept critically, considering its weaknesses and limitations. Methods: We reviewed more than 300 recent articles dealing with the physiology of brain aging and neurodegeneration pathophysiology. Results: (1) Application of the AA concept to individual organs outside the brain is challenging as organs of different systems age at different rates. (2) There is a need to consider the deceleration of aging due to the potential use of the individual structure–functional reserves. The latter can be restored by pharmacological and/or cognitive therapy, environment, etc. (3) The AA concept lacks both standardised terminology and methodology. (4) Changes in specific molecular biomarkers (MBM) reflect aging-related processes; however, numerous MBM candidates should be validated to consolidate the AA theory. (5) The exact nature of many potential causal factors, biological outcomes and interactions between the former and the latter remain largely unclear. Conclusions: Although AA is commonly recognised as a perspective theory, it still suffers from a number of gaps and limitations that assume the necessity for an updated AA concept. MDPI 2023-10-14 /pmc/articles/PMC10605227/ /pubmed/37887295 http://dx.doi.org/10.3390/cells12202451 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Review
Statsenko, Yauhen
Kuznetsov, Nik V.
Morozova, Daria
Liaonchyk, Katsiaryna
Simiyu, Gillian Lylian
Smetanina, Darya
Kashapov, Aidar
Meribout, Sarah
Gorkom, Klaus Neidl-Van
Hamoudi, Rifat
Ismail, Fatima
Ansari, Suraiya Anjum
Emerald, Bright Starling
Ljubisavljevic, Milos
Reappraisal of the Concept of Accelerated Aging in Neurodegeneration and Beyond
title Reappraisal of the Concept of Accelerated Aging in Neurodegeneration and Beyond
title_full Reappraisal of the Concept of Accelerated Aging in Neurodegeneration and Beyond
title_fullStr Reappraisal of the Concept of Accelerated Aging in Neurodegeneration and Beyond
title_full_unstemmed Reappraisal of the Concept of Accelerated Aging in Neurodegeneration and Beyond
title_short Reappraisal of the Concept of Accelerated Aging in Neurodegeneration and Beyond
title_sort reappraisal of the concept of accelerated aging in neurodegeneration and beyond
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10605227/
https://www.ncbi.nlm.nih.gov/pubmed/37887295
http://dx.doi.org/10.3390/cells12202451
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