Anti-leukemic activity of DNA methyltransferase inhibitor procaine targeted on human leukaemia cells

Chromatin remodeling in DNA is fundamental to gene expression, DNA replication and repair processes. Methylation of promoter regions of tumor-suppressor genes and histone deacetylation leads to gene silencing and transcriptionally repressive chromatin. For the past few decades DNA methylation agents...

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Main Authors: Borutinskaite Veronika, Bauraite-Akatova Justina, Navakauskiene Ruta
Format: Article
Language:English
Published: De Gruyter 2016-11-01
Series:Open Life Sciences
Subjects:
Online Access:https://doi.org/10.1515/biol-2016-0044
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spelling doaj-8e8871789d784af19c225cc5d1d163ae2021-09-05T20:42:21ZengDe GruyterOpen Life Sciences2391-54122016-11-0111132233010.1515/biol-2016-0044biol-2016-0044Anti-leukemic activity of DNA methyltransferase inhibitor procaine targeted on human leukaemia cellsBorutinskaite Veronika0Bauraite-Akatova Justina1Navakauskiene Ruta2Department of Molecular Cell Biology, Institute of Biochemistry, Vilnius University, Sauletekio 7, LT-10257, Vilnius, LithuaniaDepartment of Molecular Cell Biology, Institute of Biochemistry, Vilnius University, Sauletekio 7, LT-10257, Vilnius, LithuaniaDepartment of Molecular Cell Biology, Institute of Biochemistry, Vilnius University, Sauletekio 7, LT-10257, Vilnius, LithuaniaChromatin remodeling in DNA is fundamental to gene expression, DNA replication and repair processes. Methylation of promoter regions of tumor-suppressor genes and histone deacetylation leads to gene silencing and transcriptionally repressive chromatin. For the past few decades DNA methylation agents became very attractive as the targets for cancer therapy. The purpose of this work was to examine the effects of DNMT inhibitor procaine on growth inhibition, apoptosis and differentiation of human leukaemia cells. The changes in expression of genes, proteins and histone modifications caused by procaine were evaluated under different treatments. We demonstrated that procaine arrests growth of human leukaemia cells and in combination with all-trans retinoic acid (ATRA) induces cancer cell differentiation. Procaine causes reduction of expression of DNA methyltransferases as well. The treatment of human leukaemia cells with procaine increase the expression of molecules associated with differentiation (CD11b, E-cadherin, G-CSF) and apoptosis (PPARγ). Moreover, the examined DNMT inhibitor enhances certain gene transcription activation via chromatin remodelling – the changes in histone H3K4(Me)3 and H3K9Ac/S10P modifications were detected. Our results suggest, that DNMT inhibitor – procaine, can be used for further investigations on epigenetic differentiation therapy of leukaemia cells especially when used in combination with retinoic acid.https://doi.org/10.1515/biol-2016-0044dnmtiprocainechromatinremodeling
collection DOAJ
language English
format Article
sources DOAJ
author Borutinskaite Veronika
Bauraite-Akatova Justina
Navakauskiene Ruta
spellingShingle Borutinskaite Veronika
Bauraite-Akatova Justina
Navakauskiene Ruta
Anti-leukemic activity of DNA methyltransferase inhibitor procaine targeted on human leukaemia cells
Open Life Sciences
dnmti
procaine
chromatin
remodeling
author_facet Borutinskaite Veronika
Bauraite-Akatova Justina
Navakauskiene Ruta
author_sort Borutinskaite Veronika
title Anti-leukemic activity of DNA methyltransferase inhibitor procaine targeted on human leukaemia cells
title_short Anti-leukemic activity of DNA methyltransferase inhibitor procaine targeted on human leukaemia cells
title_full Anti-leukemic activity of DNA methyltransferase inhibitor procaine targeted on human leukaemia cells
title_fullStr Anti-leukemic activity of DNA methyltransferase inhibitor procaine targeted on human leukaemia cells
title_full_unstemmed Anti-leukemic activity of DNA methyltransferase inhibitor procaine targeted on human leukaemia cells
title_sort anti-leukemic activity of dna methyltransferase inhibitor procaine targeted on human leukaemia cells
publisher De Gruyter
series Open Life Sciences
issn 2391-5412
publishDate 2016-11-01
description Chromatin remodeling in DNA is fundamental to gene expression, DNA replication and repair processes. Methylation of promoter regions of tumor-suppressor genes and histone deacetylation leads to gene silencing and transcriptionally repressive chromatin. For the past few decades DNA methylation agents became very attractive as the targets for cancer therapy. The purpose of this work was to examine the effects of DNMT inhibitor procaine on growth inhibition, apoptosis and differentiation of human leukaemia cells. The changes in expression of genes, proteins and histone modifications caused by procaine were evaluated under different treatments. We demonstrated that procaine arrests growth of human leukaemia cells and in combination with all-trans retinoic acid (ATRA) induces cancer cell differentiation. Procaine causes reduction of expression of DNA methyltransferases as well. The treatment of human leukaemia cells with procaine increase the expression of molecules associated with differentiation (CD11b, E-cadherin, G-CSF) and apoptosis (PPARγ). Moreover, the examined DNMT inhibitor enhances certain gene transcription activation via chromatin remodelling – the changes in histone H3K4(Me)3 and H3K9Ac/S10P modifications were detected. Our results suggest, that DNMT inhibitor – procaine, can be used for further investigations on epigenetic differentiation therapy of leukaemia cells especially when used in combination with retinoic acid.
topic dnmti
procaine
chromatin
remodeling
url https://doi.org/10.1515/biol-2016-0044
work_keys_str_mv AT borutinskaiteveronika antileukemicactivityofdnamethyltransferaseinhibitorprocainetargetedonhumanleukaemiacells
AT bauraiteakatovajustina antileukemicactivityofdnamethyltransferaseinhibitorprocainetargetedonhumanleukaemiacells
AT navakauskieneruta antileukemicactivityofdnamethyltransferaseinhibitorprocainetargetedonhumanleukaemiacells
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