Elevated Protein Carbonylation, and Misfolding in Sciatic Nerve from db/db and Sod1(−/−) Mice: Plausible Link between Oxidative Stress and Demyelination

Diabetic peripheral polyneuropathy is associated with decrements in motor/sensory neuron myelination, nerve conduction and muscle function; however, the mechanisms of reduced myelination in diabetes are poorly understood. Chronic elevation of oxidative stress may be one of the potential determinants...

Descripción completa

Detalles Bibliográficos
Autores principales: Hamilton, Ryan T., Bhattacharya, Arunabh, Walsh, Michael E., Shi, Yun, Wei, Rochelle, Zhang, Yiqiang, Rodriguez, Karl A., Buffenstein, Rochelle, Chaudhuri, Asish R., Van Remmen, Holly
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3672154/
https://www.ncbi.nlm.nih.gov/pubmed/23750273
http://dx.doi.org/10.1371/journal.pone.0065725
_version_ 1782272083807436800
author Hamilton, Ryan T.
Bhattacharya, Arunabh
Walsh, Michael E.
Shi, Yun
Wei, Rochelle
Zhang, Yiqiang
Rodriguez, Karl A.
Buffenstein, Rochelle
Chaudhuri, Asish R.
Van Remmen, Holly
author_facet Hamilton, Ryan T.
Bhattacharya, Arunabh
Walsh, Michael E.
Shi, Yun
Wei, Rochelle
Zhang, Yiqiang
Rodriguez, Karl A.
Buffenstein, Rochelle
Chaudhuri, Asish R.
Van Remmen, Holly
author_sort Hamilton, Ryan T.
collection PubMed
description Diabetic peripheral polyneuropathy is associated with decrements in motor/sensory neuron myelination, nerve conduction and muscle function; however, the mechanisms of reduced myelination in diabetes are poorly understood. Chronic elevation of oxidative stress may be one of the potential determinants for demyelination as lipids and proteins are important structural constituents of myelin and highly susceptible to oxidation. The goal of the current study was to determine whether there is a link between protein oxidation/misfolding and demyelination. We chose two distinct models to test our hypothesis: 1) the leptin receptor deficient mouse (dbdb) model of diabetic polyneuropathy and 2) superoxide dismutase 1 knockout (Sod1(−/−)) mouse model of in vivo oxidative stress. Both experimental models displayed a significant decrement in nerve conduction, increase in tail distal motor latency as well as reduced myelin thickness and fiber/axon diameter. Further biochemical studies demonstrated that oxidative stress is likely to be a potential key player in the demyelination process as both models exhibited significant elevation in protein carbonylation and alterations in protein conformation. Since peripheral myelin protein 22 (PMP22) is a key component of myelin sheath and has been found mutated and aggregated in several peripheral neuropathies, we predicted that an increase in carbonylation and aggregation of PMP22 may be associated with demyelination in dbdb mice. Indeed, PMP22 was found to be carbonylated and aggregated in sciatic nerves of dbdb mice. Sequence-driven hydropathy plot analysis and in vitro oxidation-induced aggregation of purified PMP22 protein supported the premise for oxidation-dependent aggregation of PMP22 in dbdb mice. Collectively, these data strongly suggest for the first time that oxidation-mediated protein misfolding and aggregation of key myelin proteins may be linked to demyelination and reduced nerve conduction in peripheral neuropathies.
format Online
Article
Text
id pubmed-3672154
institution National Center for Biotechnology Information
language English
publishDate 2013
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-36721542013-06-07 Elevated Protein Carbonylation, and Misfolding in Sciatic Nerve from db/db and Sod1(−/−) Mice: Plausible Link between Oxidative Stress and Demyelination Hamilton, Ryan T. Bhattacharya, Arunabh Walsh, Michael E. Shi, Yun Wei, Rochelle Zhang, Yiqiang Rodriguez, Karl A. Buffenstein, Rochelle Chaudhuri, Asish R. Van Remmen, Holly PLoS One Research Article Diabetic peripheral polyneuropathy is associated with decrements in motor/sensory neuron myelination, nerve conduction and muscle function; however, the mechanisms of reduced myelination in diabetes are poorly understood. Chronic elevation of oxidative stress may be one of the potential determinants for demyelination as lipids and proteins are important structural constituents of myelin and highly susceptible to oxidation. The goal of the current study was to determine whether there is a link between protein oxidation/misfolding and demyelination. We chose two distinct models to test our hypothesis: 1) the leptin receptor deficient mouse (dbdb) model of diabetic polyneuropathy and 2) superoxide dismutase 1 knockout (Sod1(−/−)) mouse model of in vivo oxidative stress. Both experimental models displayed a significant decrement in nerve conduction, increase in tail distal motor latency as well as reduced myelin thickness and fiber/axon diameter. Further biochemical studies demonstrated that oxidative stress is likely to be a potential key player in the demyelination process as both models exhibited significant elevation in protein carbonylation and alterations in protein conformation. Since peripheral myelin protein 22 (PMP22) is a key component of myelin sheath and has been found mutated and aggregated in several peripheral neuropathies, we predicted that an increase in carbonylation and aggregation of PMP22 may be associated with demyelination in dbdb mice. Indeed, PMP22 was found to be carbonylated and aggregated in sciatic nerves of dbdb mice. Sequence-driven hydropathy plot analysis and in vitro oxidation-induced aggregation of purified PMP22 protein supported the premise for oxidation-dependent aggregation of PMP22 in dbdb mice. Collectively, these data strongly suggest for the first time that oxidation-mediated protein misfolding and aggregation of key myelin proteins may be linked to demyelination and reduced nerve conduction in peripheral neuropathies. Public Library of Science 2013-06-04 /pmc/articles/PMC3672154/ /pubmed/23750273 http://dx.doi.org/10.1371/journal.pone.0065725 Text en © 2013 Hamilton et al http://creativecommons.org/licenses/by/4.0/ 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 the original author and source are properly credited.
spellingShingle Research Article
Hamilton, Ryan T.
Bhattacharya, Arunabh
Walsh, Michael E.
Shi, Yun
Wei, Rochelle
Zhang, Yiqiang
Rodriguez, Karl A.
Buffenstein, Rochelle
Chaudhuri, Asish R.
Van Remmen, Holly
Elevated Protein Carbonylation, and Misfolding in Sciatic Nerve from db/db and Sod1(−/−) Mice: Plausible Link between Oxidative Stress and Demyelination
title Elevated Protein Carbonylation, and Misfolding in Sciatic Nerve from db/db and Sod1(−/−) Mice: Plausible Link between Oxidative Stress and Demyelination
title_full Elevated Protein Carbonylation, and Misfolding in Sciatic Nerve from db/db and Sod1(−/−) Mice: Plausible Link between Oxidative Stress and Demyelination
title_fullStr Elevated Protein Carbonylation, and Misfolding in Sciatic Nerve from db/db and Sod1(−/−) Mice: Plausible Link between Oxidative Stress and Demyelination
title_full_unstemmed Elevated Protein Carbonylation, and Misfolding in Sciatic Nerve from db/db and Sod1(−/−) Mice: Plausible Link between Oxidative Stress and Demyelination
title_short Elevated Protein Carbonylation, and Misfolding in Sciatic Nerve from db/db and Sod1(−/−) Mice: Plausible Link between Oxidative Stress and Demyelination
title_sort elevated protein carbonylation, and misfolding in sciatic nerve from db/db and sod1(−/−) mice: plausible link between oxidative stress and demyelination
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3672154/
https://www.ncbi.nlm.nih.gov/pubmed/23750273
http://dx.doi.org/10.1371/journal.pone.0065725
work_keys_str_mv AT hamiltonryant elevatedproteincarbonylationandmisfoldinginsciaticnervefromdbdbandsod1miceplausiblelinkbetweenoxidativestressanddemyelination
AT bhattacharyaarunabh elevatedproteincarbonylationandmisfoldinginsciaticnervefromdbdbandsod1miceplausiblelinkbetweenoxidativestressanddemyelination
AT walshmichaele elevatedproteincarbonylationandmisfoldinginsciaticnervefromdbdbandsod1miceplausiblelinkbetweenoxidativestressanddemyelination
AT shiyun elevatedproteincarbonylationandmisfoldinginsciaticnervefromdbdbandsod1miceplausiblelinkbetweenoxidativestressanddemyelination
AT weirochelle elevatedproteincarbonylationandmisfoldinginsciaticnervefromdbdbandsod1miceplausiblelinkbetweenoxidativestressanddemyelination
AT zhangyiqiang elevatedproteincarbonylationandmisfoldinginsciaticnervefromdbdbandsod1miceplausiblelinkbetweenoxidativestressanddemyelination
AT rodriguezkarla elevatedproteincarbonylationandmisfoldinginsciaticnervefromdbdbandsod1miceplausiblelinkbetweenoxidativestressanddemyelination
AT buffensteinrochelle elevatedproteincarbonylationandmisfoldinginsciaticnervefromdbdbandsod1miceplausiblelinkbetweenoxidativestressanddemyelination
AT chaudhuriasishr elevatedproteincarbonylationandmisfoldinginsciaticnervefromdbdbandsod1miceplausiblelinkbetweenoxidativestressanddemyelination
AT vanremmenholly elevatedproteincarbonylationandmisfoldinginsciaticnervefromdbdbandsod1miceplausiblelinkbetweenoxidativestressanddemyelination

Ejemplares similares