Cognitive Function Is Associated with the Genetically Determined Efficiency of DNA Repair Mechanisms

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningfagfællebedømt

Standard

Cognitive Function Is Associated with the Genetically Determined Efficiency of DNA Repair Mechanisms. / Cherbuin, Nicolas; Patel, Hardip; Walsh, Erin I.; Ambikairajah, Ananthan; Burns, Richard; Brüstle, Anne; Rasmussen, Lene Juel.

I: Genes, Bind 15, Nr. 2, 153, 2024.

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningfagfællebedømt

Harvard

Cherbuin, N, Patel, H, Walsh, EI, Ambikairajah, A, Burns, R, Brüstle, A & Rasmussen, LJ 2024, 'Cognitive Function Is Associated with the Genetically Determined Efficiency of DNA Repair Mechanisms', Genes, bind 15, nr. 2, 153. https://doi.org/10.3390/genes15020153

APA

Cherbuin, N., Patel, H., Walsh, E. I., Ambikairajah, A., Burns, R., Brüstle, A., & Rasmussen, L. J. (2024). Cognitive Function Is Associated with the Genetically Determined Efficiency of DNA Repair Mechanisms. Genes, 15(2), [153]. https://doi.org/10.3390/genes15020153

Vancouver

Cherbuin N, Patel H, Walsh EI, Ambikairajah A, Burns R, Brüstle A o.a. Cognitive Function Is Associated with the Genetically Determined Efficiency of DNA Repair Mechanisms. Genes. 2024;15(2). 153. https://doi.org/10.3390/genes15020153

Author

Cherbuin, Nicolas ; Patel, Hardip ; Walsh, Erin I. ; Ambikairajah, Ananthan ; Burns, Richard ; Brüstle, Anne ; Rasmussen, Lene Juel. / Cognitive Function Is Associated with the Genetically Determined Efficiency of DNA Repair Mechanisms. I: Genes. 2024 ; Bind 15, Nr. 2.

Bibtex

@article{2360430361b94c7eb028eb2a10cdb1f2,
title = "Cognitive Function Is Associated with the Genetically Determined Efficiency of DNA Repair Mechanisms",
abstract = "Several modifiable risk factors for neurodegeneration and dementia have been identified, although individuals vary in their vulnerability despite a similar risk of exposure. This difference in vulnerability could be explained at least in part by the variability in DNA repair mechanisms' efficiency between individuals. Therefore, the aim of this study was to test associations between documented, prevalent genetic variation (single nucleotide polymorphism, SNP) in DNA repair genes, cognitive function, and brain structure. Community-living participants (n = 488,159; 56.54 years (8.09); 54.2% female) taking part in the UK Biobank study and for whom cognitive and genetic measures were available were included. SNPs in base excision repair (BER) genes of the bifunctional DNA glycosylases OGG1 (rs1052133, rs104893751), NEIL1 (rs7402844, rs5745906), NEIL2 (rs6601606), NEIL3 (rs10013040, rs13112390, rs13112358, rs1395479), MUTYH (rs34612342, rs200165598), NTHL1 (rs150766139, rs2516739) were considered. Cognitive measures included fluid intelligence, the symbol-digit matching task, visual matching, and trail-making. Hierarchical regression and latent class analyses were used to test the associations between SNPs and cognitive measures. Associations between SNPs and brain measures were also tested in a subset of 39,060 participants. Statistically significant associations with cognition were detected for 12 out of the 13 SNPs analyzed. The strongest effects amounted to a 1-6% difference in cognitive function detected for NEIL1 (rs7402844), NEIL2 (rs6601606), and NTHL1 (rs2516739). Associations varied by age and sex, with stronger effects detected in middle-aged women. Weaker associations with brain measures were also detected. Variability in some BER genes is associated with cognitive function and brain structure and may explain variability in the risk for neurodegeneration and dementia.",
keywords = "brain ageing, cognitive decline, DNA repair, inflammation, oxidative stress, single nucleotide polymorphism",
author = "Nicolas Cherbuin and Hardip Patel and Walsh, {Erin I.} and Ananthan Ambikairajah and Richard Burns and Anne Br{\"u}stle and Rasmussen, {Lene Juel}",
year = "2024",
doi = "10.3390/genes15020153",
language = "English",
volume = "15",
journal = "Genes",
issn = "2073-4425",
publisher = "M D P I AG",
number = "2",

}

RIS

TY - JOUR

T1 - Cognitive Function Is Associated with the Genetically Determined Efficiency of DNA Repair Mechanisms

AU - Cherbuin, Nicolas

AU - Patel, Hardip

AU - Walsh, Erin I.

AU - Ambikairajah, Ananthan

AU - Burns, Richard

AU - Brüstle, Anne

AU - Rasmussen, Lene Juel

PY - 2024

Y1 - 2024

N2 - Several modifiable risk factors for neurodegeneration and dementia have been identified, although individuals vary in their vulnerability despite a similar risk of exposure. This difference in vulnerability could be explained at least in part by the variability in DNA repair mechanisms' efficiency between individuals. Therefore, the aim of this study was to test associations between documented, prevalent genetic variation (single nucleotide polymorphism, SNP) in DNA repair genes, cognitive function, and brain structure. Community-living participants (n = 488,159; 56.54 years (8.09); 54.2% female) taking part in the UK Biobank study and for whom cognitive and genetic measures were available were included. SNPs in base excision repair (BER) genes of the bifunctional DNA glycosylases OGG1 (rs1052133, rs104893751), NEIL1 (rs7402844, rs5745906), NEIL2 (rs6601606), NEIL3 (rs10013040, rs13112390, rs13112358, rs1395479), MUTYH (rs34612342, rs200165598), NTHL1 (rs150766139, rs2516739) were considered. Cognitive measures included fluid intelligence, the symbol-digit matching task, visual matching, and trail-making. Hierarchical regression and latent class analyses were used to test the associations between SNPs and cognitive measures. Associations between SNPs and brain measures were also tested in a subset of 39,060 participants. Statistically significant associations with cognition were detected for 12 out of the 13 SNPs analyzed. The strongest effects amounted to a 1-6% difference in cognitive function detected for NEIL1 (rs7402844), NEIL2 (rs6601606), and NTHL1 (rs2516739). Associations varied by age and sex, with stronger effects detected in middle-aged women. Weaker associations with brain measures were also detected. Variability in some BER genes is associated with cognitive function and brain structure and may explain variability in the risk for neurodegeneration and dementia.

AB - Several modifiable risk factors for neurodegeneration and dementia have been identified, although individuals vary in their vulnerability despite a similar risk of exposure. This difference in vulnerability could be explained at least in part by the variability in DNA repair mechanisms' efficiency between individuals. Therefore, the aim of this study was to test associations between documented, prevalent genetic variation (single nucleotide polymorphism, SNP) in DNA repair genes, cognitive function, and brain structure. Community-living participants (n = 488,159; 56.54 years (8.09); 54.2% female) taking part in the UK Biobank study and for whom cognitive and genetic measures were available were included. SNPs in base excision repair (BER) genes of the bifunctional DNA glycosylases OGG1 (rs1052133, rs104893751), NEIL1 (rs7402844, rs5745906), NEIL2 (rs6601606), NEIL3 (rs10013040, rs13112390, rs13112358, rs1395479), MUTYH (rs34612342, rs200165598), NTHL1 (rs150766139, rs2516739) were considered. Cognitive measures included fluid intelligence, the symbol-digit matching task, visual matching, and trail-making. Hierarchical regression and latent class analyses were used to test the associations between SNPs and cognitive measures. Associations between SNPs and brain measures were also tested in a subset of 39,060 participants. Statistically significant associations with cognition were detected for 12 out of the 13 SNPs analyzed. The strongest effects amounted to a 1-6% difference in cognitive function detected for NEIL1 (rs7402844), NEIL2 (rs6601606), and NTHL1 (rs2516739). Associations varied by age and sex, with stronger effects detected in middle-aged women. Weaker associations with brain measures were also detected. Variability in some BER genes is associated with cognitive function and brain structure and may explain variability in the risk for neurodegeneration and dementia.

KW - brain ageing

KW - cognitive decline

KW - DNA repair

KW - inflammation

KW - oxidative stress

KW - single nucleotide polymorphism

U2 - 10.3390/genes15020153

DO - 10.3390/genes15020153

M3 - Journal article

C2 - 38397143

AN - SCOPUS:85185897791

VL - 15

JO - Genes

JF - Genes

SN - 2073-4425

IS - 2

M1 - 153

ER -

ID: 384489671