RNA modifications by oxidation: a novel disease mechanism?

Research output: Contribution to journalJournal articleResearchpeer-review

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RNA modifications by oxidation : a novel disease mechanism? / Poulsen, Henrik E; Specht, Elisabeth; Broedbaek, Kasper; Henriksen, Trine; Ellervik, Christina; Mandrup-Poulsen, Thomas; Tonnesen, Morten; Nielsen, Peter E; Andersen, Henrik U; Weimann, Allan.

In: Free Radical Biology & Medicine, Vol. 52, No. 8, 04.2012, p. 1353-61.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Poulsen, HE, Specht, E, Broedbaek, K, Henriksen, T, Ellervik, C, Mandrup-Poulsen, T, Tonnesen, M, Nielsen, PE, Andersen, HU & Weimann, A 2012, 'RNA modifications by oxidation: a novel disease mechanism?', Free Radical Biology & Medicine, vol. 52, no. 8, pp. 1353-61. https://doi.org/10.1016/j.freeradbiomed.2012.01.009

APA

Poulsen, H. E., Specht, E., Broedbaek, K., Henriksen, T., Ellervik, C., Mandrup-Poulsen, T., Tonnesen, M., Nielsen, P. E., Andersen, H. U., & Weimann, A. (2012). RNA modifications by oxidation: a novel disease mechanism? Free Radical Biology & Medicine, 52(8), 1353-61. https://doi.org/10.1016/j.freeradbiomed.2012.01.009

Vancouver

Poulsen HE, Specht E, Broedbaek K, Henriksen T, Ellervik C, Mandrup-Poulsen T et al. RNA modifications by oxidation: a novel disease mechanism? Free Radical Biology & Medicine. 2012 Apr;52(8):1353-61. https://doi.org/10.1016/j.freeradbiomed.2012.01.009

Author

Poulsen, Henrik E ; Specht, Elisabeth ; Broedbaek, Kasper ; Henriksen, Trine ; Ellervik, Christina ; Mandrup-Poulsen, Thomas ; Tonnesen, Morten ; Nielsen, Peter E ; Andersen, Henrik U ; Weimann, Allan. / RNA modifications by oxidation : a novel disease mechanism?. In: Free Radical Biology & Medicine. 2012 ; Vol. 52, No. 8. pp. 1353-61.

Bibtex

@article{aef04d547e7040999461bc380b985542,
title = "RNA modifications by oxidation: a novel disease mechanism?",
abstract = "The past decade has provided exciting insights into a novel class of central (small) RNA molecules intimately involved in gene regulation. Only a small percentage of our DNA is translated into proteins by mRNA, yet 80% or more of the DNA is transcribed into RNA, and this RNA has been found to encompass various classes of novel regulatory RNAs, including, e.g., microRNAs. It is well known that DNA is constantly oxidized and repaired by complex genome maintenance mechanisms. Analogously, RNA also undergoes significant oxidation, and there are now convincing data suggesting that oxidation, and the consequent loss of integrity of RNA, is a mechanism for disease development. Oxidized RNA is found in a large variety of diseases, and interest has been especially devoted to degenerative brain diseases such as Alzheimer disease, in which up to 50-70% of specific mRNA molecules are reported oxidized, whereas other RNA molecules show virtually no oxidation. The iron-storage disease hemochromatosis exhibits the most prominent general increase in RNA oxidation ever observed. Oxidation of RNA primarily leads to strand breaks and to oxidative base modifications. Oxidized mRNA is recognized by the ribosomes, but the oxidation results in ribosomal stalling and dysfunction, followed by decreased levels of functional protein as well as the production of truncated proteins that do not undergo proper folding and may result in protein aggregation within the cell. Ribosomal dysfunction may also signal apoptosis by p53-independent pathways. There are very few reports on interventions that reduce RNA oxidation, one interesting observation being a reduction in RNA oxidation by ingestion of raw olive oil. High urinary excretion of 8-oxo-guanosine, a biomarker for RNA oxidation, is highly predictive of death in newly diagnosed type 2 diabetics; this demonstrates the clinical relevance of RNA oxidation. Taken collectively the available data suggest that RNA oxidation is a contributing factor in several diseases such as diabetes, hemochromatosis, heart failure, and {\ss}-cell destruction. The mechanism involves free iron and hydrogen peroxide from mitochondrial dysfunction that together lead to RNA oxidation that in turn gives rise to truncated proteins that may cause aggregation. Thus RNA oxidation may well be an important novel contributing mechanism for several diseases.",
author = "Poulsen, {Henrik E} and Elisabeth Specht and Kasper Broedbaek and Trine Henriksen and Christina Ellervik and Thomas Mandrup-Poulsen and Morten Tonnesen and Nielsen, {Peter E} and Andersen, {Henrik U} and Allan Weimann",
note = "Copyright {\textcopyright} 2012 Elsevier Inc. All rights reserved.",
year = "2012",
month = apr,
doi = "10.1016/j.freeradbiomed.2012.01.009",
language = "English",
volume = "52",
pages = "1353--61",
journal = "Free Radical Biology & Medicine",
issn = "0891-5849",
publisher = "Elsevier",
number = "8",

}

RIS

TY - JOUR

T1 - RNA modifications by oxidation

T2 - a novel disease mechanism?

AU - Poulsen, Henrik E

AU - Specht, Elisabeth

AU - Broedbaek, Kasper

AU - Henriksen, Trine

AU - Ellervik, Christina

AU - Mandrup-Poulsen, Thomas

AU - Tonnesen, Morten

AU - Nielsen, Peter E

AU - Andersen, Henrik U

AU - Weimann, Allan

N1 - Copyright © 2012 Elsevier Inc. All rights reserved.

PY - 2012/4

Y1 - 2012/4

N2 - The past decade has provided exciting insights into a novel class of central (small) RNA molecules intimately involved in gene regulation. Only a small percentage of our DNA is translated into proteins by mRNA, yet 80% or more of the DNA is transcribed into RNA, and this RNA has been found to encompass various classes of novel regulatory RNAs, including, e.g., microRNAs. It is well known that DNA is constantly oxidized and repaired by complex genome maintenance mechanisms. Analogously, RNA also undergoes significant oxidation, and there are now convincing data suggesting that oxidation, and the consequent loss of integrity of RNA, is a mechanism for disease development. Oxidized RNA is found in a large variety of diseases, and interest has been especially devoted to degenerative brain diseases such as Alzheimer disease, in which up to 50-70% of specific mRNA molecules are reported oxidized, whereas other RNA molecules show virtually no oxidation. The iron-storage disease hemochromatosis exhibits the most prominent general increase in RNA oxidation ever observed. Oxidation of RNA primarily leads to strand breaks and to oxidative base modifications. Oxidized mRNA is recognized by the ribosomes, but the oxidation results in ribosomal stalling and dysfunction, followed by decreased levels of functional protein as well as the production of truncated proteins that do not undergo proper folding and may result in protein aggregation within the cell. Ribosomal dysfunction may also signal apoptosis by p53-independent pathways. There are very few reports on interventions that reduce RNA oxidation, one interesting observation being a reduction in RNA oxidation by ingestion of raw olive oil. High urinary excretion of 8-oxo-guanosine, a biomarker for RNA oxidation, is highly predictive of death in newly diagnosed type 2 diabetics; this demonstrates the clinical relevance of RNA oxidation. Taken collectively the available data suggest that RNA oxidation is a contributing factor in several diseases such as diabetes, hemochromatosis, heart failure, and ß-cell destruction. The mechanism involves free iron and hydrogen peroxide from mitochondrial dysfunction that together lead to RNA oxidation that in turn gives rise to truncated proteins that may cause aggregation. Thus RNA oxidation may well be an important novel contributing mechanism for several diseases.

AB - The past decade has provided exciting insights into a novel class of central (small) RNA molecules intimately involved in gene regulation. Only a small percentage of our DNA is translated into proteins by mRNA, yet 80% or more of the DNA is transcribed into RNA, and this RNA has been found to encompass various classes of novel regulatory RNAs, including, e.g., microRNAs. It is well known that DNA is constantly oxidized and repaired by complex genome maintenance mechanisms. Analogously, RNA also undergoes significant oxidation, and there are now convincing data suggesting that oxidation, and the consequent loss of integrity of RNA, is a mechanism for disease development. Oxidized RNA is found in a large variety of diseases, and interest has been especially devoted to degenerative brain diseases such as Alzheimer disease, in which up to 50-70% of specific mRNA molecules are reported oxidized, whereas other RNA molecules show virtually no oxidation. The iron-storage disease hemochromatosis exhibits the most prominent general increase in RNA oxidation ever observed. Oxidation of RNA primarily leads to strand breaks and to oxidative base modifications. Oxidized mRNA is recognized by the ribosomes, but the oxidation results in ribosomal stalling and dysfunction, followed by decreased levels of functional protein as well as the production of truncated proteins that do not undergo proper folding and may result in protein aggregation within the cell. Ribosomal dysfunction may also signal apoptosis by p53-independent pathways. There are very few reports on interventions that reduce RNA oxidation, one interesting observation being a reduction in RNA oxidation by ingestion of raw olive oil. High urinary excretion of 8-oxo-guanosine, a biomarker for RNA oxidation, is highly predictive of death in newly diagnosed type 2 diabetics; this demonstrates the clinical relevance of RNA oxidation. Taken collectively the available data suggest that RNA oxidation is a contributing factor in several diseases such as diabetes, hemochromatosis, heart failure, and ß-cell destruction. The mechanism involves free iron and hydrogen peroxide from mitochondrial dysfunction that together lead to RNA oxidation that in turn gives rise to truncated proteins that may cause aggregation. Thus RNA oxidation may well be an important novel contributing mechanism for several diseases.

U2 - 10.1016/j.freeradbiomed.2012.01.009

DO - 10.1016/j.freeradbiomed.2012.01.009

M3 - Journal article

C2 - 22306201

VL - 52

SP - 1353

EP - 1361

JO - Free Radical Biology & Medicine

JF - Free Radical Biology & Medicine

SN - 0891-5849

IS - 8

ER -

ID: 38326051