Title Senescence-associated molecular and epigenetic alterations in mesenchymal stem cell cultures from amniotic fluid of normal and fetus-affected pregnancy /
Authors Savickienė, Jūratė ; Baronaitė, Sandra ; Zentelytė, Aistė ; Treigytė, Gražina ; Navakauskienė, Rūta
DOI 10.1155/2016/2019498
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Is Part of Stem cells international.. New York : Hindawi Publishing Corporation. 2016, 2016, Art. ID 2019498.. ISSN 1687-966X. eISSN 1687-9678
Keywords [eng] amniotic fluid ; mesenchymal stem cells ; epigenetics
Abstract [eng] and wide range of therapeutic applications due to the ease of culture expansion. However, MSCs undergo replicative senescence. So far, the molecular mechanisms that underlie fetal diseases and cell senescence are still poorly understood. Here, we analyzed senescence-associated morphologic, molecular, and epigenetic characteristics during propagation of MSCs derived from AF of normal and fetus-affected pregnancy. AF-MSCs cultures fromboth cell sources displayed quite similarmorphology and expression of specific cell surface (CD44, CD90, and CD105) and stemness (Oct4, Nanog, Sox2, and Rex1) markers but had interindividual variability in proliferation capability and time to reach senescence. Within passages 4 and 8, senescent cultures exhibited typical morphological features, senescence-associated 𝛽-galactosidase activity, increased levels of p16, and decreased levels of miR-17 and miR-21 but showed differential expression of p21, p53, and ATM dependently on the onset of cell senescence. These differences correlated with changes in the level of chromatin modifiers (DNMT1 and HDAC1) and polycomb group proteins (EZH2, SUZ12, and BMI1) parallelingwith changes in the expression of repressive histone marks (H3K9me3 and H3K27me3) and stemness markers (Oct4, Nanog, Sox2, and Rex1). Therefore epigenetic factors are important for AF-MSCs senescence process that may be related with individuality of donor or a fetus malignancy status.
Published New York : Hindawi Publishing Corporation
Type Journal article
Language English
Publication date 2016