DNA damage and repair in differentiation of stem cells and cells of connective cell lineages: A trigger or a complication?

The review summarizes literature data on the role of DNA breaks and DNA repair in differentiation of pluripotent stem cells (PSC) and connective cell lineages. PSC, including embryonic stem cells (ESC) and induced pluripotent stem cells (iPSC), are rapidly dividing cells with highly active DNA dama...

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Main Authors: Nikolajs Sjakste, Una Riekstiņa
Format: Article
Language:English
Published: PAGEPress Publications 2021-05-01
Series:European Journal of Histochemistry
Subjects:
Online Access:https://www.ejh.it/index.php/ejh/article/view/3236
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spelling doaj-97d7a562432248af8acb29e00c9e46c92021-05-04T04:31:09ZengPAGEPress PublicationsEuropean Journal of Histochemistry 1121-760X2038-83062021-05-0165210.4081/ejh.2021.3236DNA damage and repair in differentiation of stem cells and cells of connective cell lineages: A trigger or a complication?Nikolajs Sjakste0Una RiekstiņaUniversity of Latvia The review summarizes literature data on the role of DNA breaks and DNA repair in differentiation of pluripotent stem cells (PSC) and connective cell lineages. PSC, including embryonic stem cells (ESC) and induced pluripotent stem cells (iPSC), are rapidly dividing cells with highly active DNA damage response (DDR) mechanisms to ensure the stability and integrity of the DNA. In PSCs, the most common DDR mechanism is error-free homologous recombination (HR) that is primarily active during S phase of the cell cycle, whereas in quiescent, slow-dividing or non-dividing tissue progenitors and terminally differentiated cells, error-prone non-homologous end joining (NHEJ) mechanism of the double-strand break (DSB) repair is dominating.  Thus, it seems that reprogramming and differentiation induce DNA strand breaks in stem cells which itself may trigger the differentiation process. Somatic cell reprogramming to iPSCs is preceded by a transient increase of the DSBs induced presumably by the caspase-dependent DNase or reactive oxygen species (ROS). In general, pluripotent stem cells possess stronger DNA repair systems compared to the differentiated cells. Nonetheless, during a prolonged cell culture propagation, DNA breaks can accumulate due to the DNA polymerase stalling. Consequently, the DNA damage might trigger the differentiation of stem cells or a replicative senescence of somatic cells. Differentiation process per se is often accompanied by a decrease of the DNA repair capacity. Thus, the differentiation might be triggered by DNA breaks, alternatively the breaks can be a consequence of the decay in the DNA repair capacity of differentiated cells. https://www.ejh.it/index.php/ejh/article/view/3236DNA breaksDNA repairdifferentiationstem cellsconnective tissue
collection DOAJ
language English
format Article
sources DOAJ
author Nikolajs Sjakste
Una Riekstiņa
spellingShingle Nikolajs Sjakste
Una Riekstiņa
DNA damage and repair in differentiation of stem cells and cells of connective cell lineages: A trigger or a complication?
European Journal of Histochemistry
DNA breaks
DNA repair
differentiation
stem cells
connective tissue
author_facet Nikolajs Sjakste
Una Riekstiņa
author_sort Nikolajs Sjakste
title DNA damage and repair in differentiation of stem cells and cells of connective cell lineages: A trigger or a complication?
title_short DNA damage and repair in differentiation of stem cells and cells of connective cell lineages: A trigger or a complication?
title_full DNA damage and repair in differentiation of stem cells and cells of connective cell lineages: A trigger or a complication?
title_fullStr DNA damage and repair in differentiation of stem cells and cells of connective cell lineages: A trigger or a complication?
title_full_unstemmed DNA damage and repair in differentiation of stem cells and cells of connective cell lineages: A trigger or a complication?
title_sort dna damage and repair in differentiation of stem cells and cells of connective cell lineages: a trigger or a complication?
publisher PAGEPress Publications
series European Journal of Histochemistry
issn 1121-760X
2038-8306
publishDate 2021-05-01
description The review summarizes literature data on the role of DNA breaks and DNA repair in differentiation of pluripotent stem cells (PSC) and connective cell lineages. PSC, including embryonic stem cells (ESC) and induced pluripotent stem cells (iPSC), are rapidly dividing cells with highly active DNA damage response (DDR) mechanisms to ensure the stability and integrity of the DNA. In PSCs, the most common DDR mechanism is error-free homologous recombination (HR) that is primarily active during S phase of the cell cycle, whereas in quiescent, slow-dividing or non-dividing tissue progenitors and terminally differentiated cells, error-prone non-homologous end joining (NHEJ) mechanism of the double-strand break (DSB) repair is dominating.  Thus, it seems that reprogramming and differentiation induce DNA strand breaks in stem cells which itself may trigger the differentiation process. Somatic cell reprogramming to iPSCs is preceded by a transient increase of the DSBs induced presumably by the caspase-dependent DNase or reactive oxygen species (ROS). In general, pluripotent stem cells possess stronger DNA repair systems compared to the differentiated cells. Nonetheless, during a prolonged cell culture propagation, DNA breaks can accumulate due to the DNA polymerase stalling. Consequently, the DNA damage might trigger the differentiation of stem cells or a replicative senescence of somatic cells. Differentiation process per se is often accompanied by a decrease of the DNA repair capacity. Thus, the differentiation might be triggered by DNA breaks, alternatively the breaks can be a consequence of the decay in the DNA repair capacity of differentiated cells.
topic DNA breaks
DNA repair
differentiation
stem cells
connective tissue
url https://www.ejh.it/index.php/ejh/article/view/3236
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AT unariekstina dnadamageandrepairindifferentiationofstemcellsandcellsofconnectivecelllineagesatriggeroracomplication
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