Mitochondrial DNA insertions into nuclear DNA affecting chromosome segregation: Insights for a novel mechanism of immunosenescence in mice

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González-Bermúdez BAutor o CoautorPlaza GrAutor o Coautor

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Mitochondrial DNA insertions into nuclear DNA affecting chromosome segregation: Insights for a novel mechanism of immunosenescence in mice

Publicado en:Mechanisms Of Ageing And Development. 207 111722- - 2022-01-01 207(), DOI: 10.1016/j.mad.2022.111722

Autores: González-Sánchez M; García-Martínez V; Bravo S; Kobayashi H; Martínez de Toda I; González-Bermúdez B; Plaza GR; De la Fuente M

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Univ Complutense Madrid, Fac Ciencias Biol, Dept Genet Physiol & Microbiol, E-28040 Madrid, Spain - Autor o Coautor

Univ Politecn Madrid, Ctr Biomed Technol, E-28223 Pozuelo De Alarcon, Spain - Autor o Coautor

Univ Politecn Madrid, ETSI Caminos Canales & Puertos, Dept Mat Sci, E-28040 Madrid, Spain - Autor o Coautor

Resumen

Mitochondrial DNA sequences were found inserted in the nuclear genome of mouse peritoneal T lymphocytes that increased progressively with aging. These insertions were preferentially located at the pericentromeric heterochromatin. In the same individuals, binucleated T-cells with micronuclei showed a significantly increased frequency associated with age. Most of them were positive for centromere sequences, reflecting the loss of chromatids or whole chromosomes. The proliferative capacity of T lymphocytes decreased with age as well as the glutathione reductase activity, whereas the oxidized glutathione and malondialdehyde concentrations exhibited a significant increase. These results may point to a common process that provides insights for a new approach to understanding immunosenescence. We propose a novel mechanism in which mitochondrial fragments, originated by the increased oxidative stress status during aging, accumulate inside the nuclear genome of T lymphocytes in a time-dependent way. The primary entrance of mitochondrial fragments at the pericentromeric regions may compromise chromosome segregation, causing genetic loss that leads to micronuclei formation, rendering aneuploid cells with reduced proliferation capacity, one of the hallmark of immunosenescence. Future experiments deciphering the mechanistic basis of this phenomenon are needed.

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agecancercellscentromerefragmentsgenomeimmunosenescencelife-stylelymphoproliferationmicronucleimicronucleus frequencymtdnaoxidative stressAnimalsChromosome segregationDna, mitochondrialGlutathione disulfideGlutathione reductaseHeterochromatinHigh-resolution organizationImmunosenescenceLymphoproliferationMalondialdehydeMiceMicronucleiMtdnaNumtsOxidative stress

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El trabajo ha sido publicado en la revista Mechanisms Of Ageing And Development debido a la progresión y el buen impacto que ha alcanzado en los últimos años, según la agencia Scopus (SJR), se ha convertido en una referencia en su campo. En el año de publicación del trabajo, 2022, se encontraba en la posición , consiguiendo con ello situarse como revista Q1 (Primer Cuartil), en la categoría Developmental Biology.

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Mitochondrial DNA insertions into nuclear DNA affecting chromosome segregation: Insights for a novel mechanism of immunosenescence in mice

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