Literature DB >> 23438186

Characterization of the role of distinct plasma cell-free DNA species in age-associated inflammation and frailty.

Juulia Jylhävä1, Tapio Nevalainen, Saara Marttila, Marja Jylhä, Antti Hervonen, Mikko Hurme.   

Abstract

Plasma cell-free DNA (cf-DNA) has recently emerged as a potential biomarker of aging, reflecting systemic inflammation, and cell death. In addition, it has been suggested that cf-DNA could promote autoinflammation. Because the total cf-DNA pool comprises different cf-DNA species, we quantified the plasma levels of gene-coding cf-DNA, Alu repeat cf-DNA, mitochondrial DNA (mtDNA) copy number, and the amounts of unmethylated and total cf-DNAs. We identified the relationships between these cf-DNA species and age-associated inflammation, immunosenescence, and frailty. Additionally, we determined the cf-DNA species-specific transcriptomic signatures in blood mononuclear cells to elucidate the age-linked leukocyte responses to cf-DNA. The study population consisted of n = 144 nonagenarian participants of the Vitality 90+ Study and n = 30 young controls. In the nonagenarians, higher levels of total and unmethylated cf-DNAs were associated with systemic inflammation and increased frailty. The mtDNA copy number was also directly correlated with increased frailty but not with inflammation. None of the cf-DNA species were associated with immunosenescence. The transcriptomic pathway analysis revealed that higher levels of total and unmethylated cf-DNAs were associated with immunoinflammatory activation in the nonagenarians but not in the young controls. The plasma mtDNA appeared to be inert in terms of inflammatory activation in both the nonagenarians and young controls. These data demonstrate that the plasma levels of total and unmethylated cf-DNA and the mtDNA copy number could serve as biomarkers of frailty. In addition, we suggest that circulating self-DNA, assessed as total or unmethylated cf-DNA, might aggravate immunoinflammatory reactivity in very old individuals.
© 2013 John Wiley & Sons Ltd and the Anatomical Society.

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Year:  2013        PMID: 23438186     DOI: 10.1111/acel.12058

Source DB:  PubMed          Journal:  Aging Cell        ISSN: 1474-9718            Impact factor:   9.304


  40 in total

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2.  Transcriptomic and epigenetic analyses reveal a gender difference in aging-associated inflammation: the Vitality 90+ study.

Authors:  T Nevalainen; L Kananen; S Marttila; M Jylhä; A Hervonen; M Hurme; J Jylhävä
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7.  Circulating cell-free DNA in health and disease - the relationship to health behaviours, ageing phenotypes and metabolomics.

Authors:  Laura Kananen; Mikko Hurme; Alexander Bürkle; Maria Moreno-Villanueva; Jürgen Bernhardt; Florence Debacq-Chainiaux; Beatrix Grubeck-Loebenstein; Marco Malavolta; Andrea Basso; Francesco Piacenza; Sebastiano Collino; Efstathios S Gonos; Ewa Sikora; Daniela Gradinaru; Eugene H J M Jansen; Martijn E T Dollé; Michel Salmon; Wolfgang Stuetz; Daniela Weber; Tilman Grune; Nicolle Breusing; Andreas Simm; Miriam Capri; Claudio Franceschi; Eline Slagboom; Duncan Talbot; Claude Libert; Jani Raitanen; Seppo Koskinen; Tommi Härkänen; Sari Stenholm; Mika Ala-Korpela; Terho Lehtimäki; Olli T Raitakari; Olavi Ukkola; Mika Kähönen; Marja Jylhä; Juulia Jylhävä
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Review 8.  Aging of the human innate immune system in HIV infection.

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Journal:  Blood       Date:  2021-06-03       Impact factor: 25.476

10.  Identification of a prognostic signature for old-age mortality by integrating genome-wide transcriptomic data with the conventional predictors: the Vitality 90+ Study.

Authors:  Juulia Jylhävä; Jani Raitanen; Saara Marttila; Antti Hervonen; Marja Jylhä; Mikko Hurme
Journal:  BMC Med Genomics       Date:  2014-09-11       Impact factor: 3.063

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