Literature DB >> 24518833

Human longevity and variation in DNA damage response and repair: study of the contribution of sub-processes using competitive gene-set analysis.

Birgit Debrabant1, Mette Soerensen2, Friederike Flachsbart3, Serena Dato4, Jonas Mengel-From2, Tinna Stevnsner5, Vilhelm A Bohr6, Torben A Kruse7, Stefan Schreiber3, Almut Nebel3, Kaare Christensen8, Qihua Tan2, Lene Christiansen2.   

Abstract

DNA-damage response and repair are crucial to maintain genetic stability, and are consequently considered central to aging and longevity. Here, we investigate whether this pathway overall associates to longevity, and whether specific sub-processes are more strongly associated with longevity than others. Data were applied on 592 SNPs from 77 genes involved in nine sub-processes: DNA-damage response, base excision repair (BER), nucleotide excision repair, mismatch repair, non-homologous end-joining, homologous recombinational repair (HRR), RecQ helicase activities (RECQ), telomere functioning and mitochondrial DNA processes. The study population was 1089 long-lived and 736 middle-aged Danes. A self-contained set-based test of all SNPs displayed association with longevity (P-value=9.9 × 10(-5)), supporting that the overall pathway could affect longevity. Investigation of the nine sub-processes using the competitive gene-set analysis by Wang et al indicated that BER, HRR and RECQ associated stronger with longevity than the respective remaining genes of the pathway (P-values=0.004-0.048). For HRR and RECQ, only one gene contributed to the significance, whereas for BER several genes contributed. These associations did, however, generally not pass correction for multiple testing. Still, these findings indicate that, of the entire pathway, variation in BER might influence longevity the most. These modest sized P-values were not replicated in a German sample. This might, though, be due to differences in genotyping procedures and investigated SNPs, potentially inducing differences in the coverage of gene regions. Specifically, five genes were not covered at all in the German data. Therefore, investigations in additional study populations are needed before final conclusion can be drawn.

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Year:  2014        PMID: 24518833      PMCID: PMC4135411          DOI: 10.1038/ejhg.2013.299

Source DB:  PubMed          Journal:  Eur J Hum Genet        ISSN: 1018-4813            Impact factor:   4.246


  51 in total

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Authors:  D Gaist; M Vaeth; I Tsiropoulos; K Christensen; E Corder; J Olsen; H T Sørensen
Journal:  BMJ       Date:  2000-01-15

3.  Increased effect of the ApoE gene on survival at advanced age in healthy and long-lived Danes: two nationwide cohort studies.

Authors:  Rune Jacobsen; Torben Martinussen; Lene Christiansen; Bernard Jeune; Karen Andersen-Ranberg; James W Vaupel; Kaare Christensen
Journal:  Aging Cell       Date:  2010-10-21       Impact factor: 9.304

4.  Replication of an association of variation in the FOXO3A gene with human longevity using both case-control and longitudinal data.

Authors:  Mette Soerensen; Serena Dato; Kaare Christensen; Matt McGue; Tinna Stevnsner; Vilhelm A Bohr; Lene Christiansen
Journal:  Aging Cell       Date:  2010-10-21       Impact factor: 9.304

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Review 6.  Finding the missing heritability of complex diseases.

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9.  Association of FOXO3A variation with human longevity confirmed in German centenarians.

Authors:  Friederike Flachsbart; Amke Caliebe; Rabea Kleindorp; Hélène Blanché; Huberta von Eller-Eberstein; Susanna Nikolaus; Stefan Schreiber; Almut Nebel
Journal:  Proc Natl Acad Sci U S A       Date:  2009-02-05       Impact factor: 11.205

Review 10.  The DNA damage response: making it safe to play with knives.

Authors:  Alberto Ciccia; Stephen J Elledge
Journal:  Mol Cell       Date:  2010-10-22       Impact factor: 17.970

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  8 in total

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Journal:  Cell Rep       Date:  2020-04-21       Impact factor: 9.423

Review 2.  Human longevity: Genetics or Lifestyle? It takes two to tango.

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Journal:  Elife       Date:  2016-11-22       Impact factor: 8.140

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Journal:  J Gerontol A Biol Sci Med Sci       Date:  2017-03-01       Impact factor: 6.053

5.  The genetic component of human longevity: New insights from the analysis of pathway-based SNP-SNP interactions.

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Review 6.  Mitochondria in the signaling pathways that control longevity and health span.

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7.  GHK and DNA: resetting the human genome to health.

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8.  Boosting ATM activity alleviates aging and extends lifespan in a mouse model of progeria.

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