Open access · CC-BY
via OpenAlex
Associations between Specific Redox Biomarkers and Age in a Large European Cohort: The MARK‐AGE Project
Daniela Weber, Wolfgang Stuetz, Olivier Toussaint, Florence Debacq‐Chainiaux, Martijn E.T. Dollé, Eugène Jansen, Efstathios S. Gonos, Claudio Franceschi, Ewa Sikora, Antti Hervonen, Nicolle Breusing, Thilo Sindlinger, María Moreno‐Villanueva, Alexander Bürkle, Tilman Grune
Oxidative Medicine and Cellular Longevity · 2017 · ▲ 45 citations
Abstract
Oxidative stress and antioxidants play a role in age‐related diseases and in the aging process. We here present data on protein carbonyls, 3‐nitrotyrosine, malondialdehyde, and cellular and plasma antioxidants (glutathione, cysteine, ascorbic acid, uric acid, α ‐tocopherol, and lycopene) and their relation with age in the European multicenter study MARK‐AGE. To avoid confounding, only data from countries which recruited subjects from all three study groups (five of eight centers) and only participants aged ≥55 years were selected resulting in data from 1559 participants. These included subjects from (1) the general population, (2) members from long‐living families, and (3) their spouses. In addition, 683 middle‐aged reference participants (35–54 years) served as a control. After adjustment for age, BMI, smoking status, gender, and country, there were differences in protein carbonyls, malondialdehyde, 3‐nitrotyrosine, α ‐tocopherol, cysteine, and glutathione between the 3 study groups. Protein carbonyls and 3‐nitrotyrosine as well as cysteine, uric acid, and lycopene were identified as independent biomarkers with the highest correlation with age. Interestingly, from all antioxidants measured, only lycopene was lower in all aged groups and from the oxidative stress biomarkers, only 3‐nitrotyrosine was increased in the descendants from long‐living families compared to the middle‐aged control group. We conclude that both lifestyle and genetics may be important contributors to redox biomarkers in an aging population.
◌ CITATION ONLY
Full text is not openly licensed for redistribution here. Read it at the source:
Provenance
- Source
- OpenAlex
- DOI
- 10.1155/2017/1401452
- Canonical
- link ↗
- Fetched
- 2026-07-06 MST
Cite this
APA
Weber, D., Stuetz, W., Toussaint, O., Debacq‐Chainiaux, F., Dollé, M.E., Jansen, E., Gonos, E.S., Franceschi, C., Sikora, E., Hervonen, A., Breusing, N., Sindlinger, T., Moreno‐Villanueva, M., Bürkle, A., & Grune, T. (2017). Associations between Specific Redox Biomarkers and Age in a Large European Cohort: The MARK‐AGE Project. <em>Oxidative Medicine and Cellular Longevity</em>. https://doi.org/10.1155/2017/1401452
Vancouver
Weber D, Stuetz W, Toussaint O, Debacq‐Chainiaux F, Dollé ME, Jansen E, et al. Associations between Specific Redox Biomarkers and Age in a Large European Cohort: The MARK‐AGE Project. Oxidative Medicine and Cellular Longevity. 2017. doi:10.1155/2017/1401452.
BibTeX
@article{daniela2017Associ,
title = {Associations between Specific Redox Biomarkers and Age in a Large European Cohort: The MARK‐AGE Project},
author = {Daniela Weber and Wolfgang Stuetz and Olivier Toussaint and Florence Debacq‐Chainiaux and Martijn E.T. Dollé and Eugène Jansen and Efstathios S. Gonos and Claudio Franceschi and Ewa Sikora and Antti Hervonen and Nicolle Breusing and Thilo Sindlinger and María Moreno‐Villanueva and Alexander Bürkle and Tilman Grune},
journal = {Oxidative Medicine and Cellular Longevity},
year = {2017},
doi = {10.1155/2017/1401452},
}
Research neighborhood
References, citing works, and semantically nearest findings. Click a node to open it.