Literature DB >> 25786194

Telomere shortening in Down syndrome patients--when does it start?

Aleksandra Gruszecka1, Przemysław Kopczyński2, Dorota Cudziło3, Natalia Lipińska1, Aleksandra Romaniuk1, Wojciech Barczak4,5, Natalia Rozwadowska6, Ewa Totoń1, Błażej Rubiś1.   

Abstract

Down syndrome (DS) is one of the most common aneuploidy. In general population, its prevalence is 1:600-1:800 live births. It is caused by a trisomy of chromosome 21. DS is phenotypically manifested by premature aging, upward slant to the eyes, epicanthus, flattened face, and poor muscle tone. In addition to physical changes, this syndrome is characterized by early onset of diseases specific to old age, such as Alzheimer's disease, vision and hearing problems, and precocious menopause. Since DS symptoms include premature aging, the shortening of telomeres might be one of the markers of cellular aging. Consequently, the aim of the study was to determine the length of the telomeres in leukocytes from the blood of juvenile patients with DS (n=68) compared to an age-matched control group (n=56) and also to determine the diagnostic or predictive value for this parameter. We show that, for the first time, in juveniles, the average relative telomere length in studied subjects is significantly longer than in the control group (50.46 vs. 40.56, respectively arbitrary units [AU]; p=0.0026). The results provide interesting basis for further research to determine the causes and consequences of telomere maintaining and the dynamics of this process in patients with DS.

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Year:  2015        PMID: 25786194      PMCID: PMC4484712          DOI: 10.1089/dna.2014.2746

Source DB:  PubMed          Journal:  DNA Cell Biol        ISSN: 1044-5498            Impact factor:   3.311


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