Copy Number Variation of Human Satellite III (1q12) With Aging

Elizaveta S Ershova; Elena M Malinovskaya; Marina S Konkova; Roman V Veiko; Pavel E Umriukhin; Andrey V Martynov; Sergey I Kutsev; Natalia N Veiko; Svetlana V Kostyuk

doi:10.3389/fgene.2019.00704

Copy Number Variation of Human Satellite III (1q12) With Aging

Front Genet. 2019 Aug 7:10:704. doi: 10.3389/fgene.2019.00704. eCollection 2019.

Authors

Affiliations

¹ Research Centre for Medical Genetics (RCMG), Moscow, Russia.
² I.M. Sechenov First Moscow State Medical University (Sechenov University), Moscow, Russia.
³ P.K. Anokhin Institute of Normal Physiology, Moscow, Russia.

Abstract

Introduction: Human satellite DNA is organized in long arrays in peri/centromeric heterochromatin. There is little information about satellite copy number variants (CNVs) in aging and replicative cell senescence (RS). Materials and Methods: Biotinylated pUC1.77 probe was used for the satellite III (f-SatIII) quantitation in leukocyte DNA by the non-radioactive quantitative hybridization for 557 subjects between 2 and 91 years old. The effect of RS and genotoxic stress (GS, 4 or 6 µM of K₂CrO₄) on the f-SatIII CNV was studied on the cultured human skin fibroblast (HSF) lines of five subjects. Results: f-SatIII in leukocyte and HSFs varies between 5.7 and 40 pg/ng of DNA. During RS, the f-SatIII content in HSFs increased. During GS, HSFs may increase or decrease f-SatIII content. Cells with low f-SatIII content have the greatest proliferative potential. F-SatIII CNVs in different individuals belonging to the different generations depend on year of their birth. Children (born in 2005-2015 years) differed significantly from the other age groups by low content and low coefficient of variation of f-SatIII. In the individuals born in 1912-1925 and living in unfavorable social conditions (FWW, the Revolution and the Russian Civil War, SWW), there is a significant disproportion in the content of f-SatIII. The coefficient of variation reaches the maximum values than in individuals born in the period from 1926 to 1975. In the group of people born in 1990-2000 (Chernobyl disaster, the collapse of the Soviet Union, and a sharp decline in the population living standard), again, there is a significant disproportion of individuals in the content of f-SatIII. A similar disproportion was observed in the analysis of a group of individuals born in 1926-1975 who in their youth worked for a long time in high-radioactive environment. Conclusion: In generations that were born and who lived in childhood in a period of severe social perturbations or in conditions of environmental pollution, we found a significant increase in leukocyte DNA f-SatIII variability. It is hypothesized that the change of the f-SatIII content in the blood cells reflects the body response to stress of different nature and intensity.

Keywords: aging; copy number variance; genotoxic stress response; replicative senescence; satellite DNA.